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B OARD REVIEW
TENTH EDITION
ERRNVPHGLFRVRUJ
MAYO CLINIC SCIENTIFIC PRESS
ERRNVPHGLFRVRUJ EDITOR-IN-CHIEF
Robert D. Ficalora , MD
C O N S U LTA N T,
M AY O C L I N I C , R O C H E S T E R , M I N N E S O TA
A S S O C I AT E P R O F E S S O R O F M E D I C I N E
C O L L E G E O F M E D I C I N E , M AY O C L I N I C
EDITOR
Paul S. Mueller, MD
A S S O C I AT E E D I T O R S
3
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Mayo Foundation does not endorse any particular products or services, and the reference to any products or
services in this book is for informational purposes only and should not be taken as an endorsement by the
authors or Mayo Foundation. Care has been taken to confirm the accuracy of the information presented and
to describe generally accepted practices. However, the authors, editors, and publisher are not responsible for
errors or omissions or for any consequences from application of the information in this book and make
no warranty, express or implied, with respect to the contents of the publication. Th is book should not be
relied on apart from the advice of a qualified health care provider.
The authors, editors, and publisher have exerted efforts to ensure that drug selection and dosage set forth
in this text are in accordance with current recommendations and practice at the time of publication.
However, in view of ongoing research, changes in government regulations, and the constant flow of information
relating to drug therapy and drug reactions, readers are urged to check the package insert for each drug
for any change in indications and dosage and for added wordings and precautions. Th is is particularly important
when the recommended agent is a new or infrequently employed drug.
Some drugs and medical devices presented in this publication have US Food and Drug Administration (FDA)
clearance for limited use in restricted research settings. It is the responsibility of the health care providers
to ascertain the FDA status of each drug or device planned for use in their clinical practice.
9 8 7 6 5 4 3 2 1
Printed in China on acid-free paper
Dedicated to all the patients who help us, as internists, learn, practice, and master internal medicine.
Robert D. Ficalora, MD
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FOREWORD
One of the Department of Medicines strategic goals is to and answers simulate the types of questions included on the
provide premier education in the science and art of medicine. American Board of Internal Medicine examination. The edi-
Established goals include leading the nation in the develop- tors and associate editors added their depth of experience to
ment of lifelong learning programs and educating physician ensure that this edition is the finest in the long history of this
and nonphysician learners at all levels and along all points book. The text is not only informational but also of great assis-
of the education continuum. These goals are attained by tance in preparing for board certification and recertification,
providing state-of-the-art graduate medical education. The and it allows for the practical application of knowledge to
rapid pace at which medical knowledge is being discovered serve our patients.
necessitates frequent updates. Mayo Clinic Internal Medicine
Board Review, Tenth Edition, reflects changes in the science
of medicine and contains features that facilitate retention of
the knowledge imparted. The chapters have been completely Morie A. Gertz, MD
revised to correspond to American Board of Internal Medicine Chair, Department of Internal Medicine
objectives and include evidence-based recommendations. Mayo Clinic, Rochester, Minnesota
Bulleted points allow easy access to key points. The questions Professor of Medicine
and their answers have been placed in a companion volume to College of Medicine
make this text more portable and user-friendly. New questions Mayo Clinic
vii
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PREFACE
Mayo Clinic Internal Medicine Board Review, Tenth Edition, I am grateful to the current and past authors for their
is the result of the combined efforts of Mayo Clinic physi- careful attention and hard work. This book would not exist
cians who practice in all the various subspecialties of Internal without the dedication of the associate editors who labored
Medicine. Many have achieved certificates in medical educa- in isolation over the chapter drafts. We are all indebted to
tion and thus understand how to communicate information staffs of the Department of Medicine; Section of Scientific
to our readersphysicians who are in training and practic- Publications, Joseph G. Murphy, MD, Chair; LeAnn M.
ing clinicians who are preparing for the American Board of Stee and Randall J. Fritz, DVM (editors), Kenna Atherton
Internal Medicine (ABIM) certification and maintenance-of- (manager), Jane M. Craig (editorial assistant), and Alissa K.
certification examinations in internal medicine. Baumgartner (proofreader); and Section of Illustration and
Our annual Mayo Clinic Board Review Course, now in its Design, Deb Veerkamp and Ryan Ledebuhr, at Mayo Clinic
27th year, gives the authors and editors the unique opportunity for their contributions to this edition. I gratefully acknowl-
to interact with our readers and tailor our approach to the way edge the support and cooperation of the publisher, Oxford
the current generation of learners prepares for a high stakes University Press. In particular, I am indebted to my admin-
examination. With the ABIM Certification Examination istrative partner, Michael OBrien, whose unfailing support
Blueprint in mind, we prepared each chapter to be not only helped me through some very difficult times.
readable but also scannable by the reader. Key review points are In the spirit of the previous editions, I trust that Mayo
bulleted in context. We thoroughly updated the information Clinic Internal Medicine Board Review, Tenth Edition, will
and used state-of-the-art guidelines and algorithms whenever serve our readers well in preparation for the primary certifica-
possible. Bullets, tables, and figures throughout each chapter tion or maintenance-of-certification examination.
highlight and summarize important clinical information. The About the cover: The images for the cover were selected to
book is comprehensive and yet easy to study. convey both the content and the purpose of this text. Three
The book chapters reflect the ABIM medical subject content areas (dermatology, pulmonary medicine, and hema-
and cross-content categories and percentages. Authors with tology) and the collaborative learning environment of medi-
wide clinical expertise composed the chapters or subsections cine are represented. Panel descriptions: upper left, erythema
of chapters that reflect the key information. Interesting but multiforme (Figure 47.4); upper right, bronchial carcinoid
extraneous information that was not likely to be included on (Figure 17.20B); lower left, original artwork depicting Mayo
the examination was removed. To facilitate study, questions Clinics group practice and educational excellence; lower
are now in a separate volume for easy reference and porta- right, ring sideroblasts (Figure 34.3).
bility. More than 300 ABIM-format multiple-choice ques-
tions with a single answer and explanation are keyed to each Robert D. Ficalora, MD
chapter. Editor-in-Chief
ix
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CONTENTS
xi
PA RT VI PA RT X I
ENDOCRINOLOGY P S YC H I AT RY
xii CONTENTS
CONTRIBUTOR S
xiii
Fernando C. Fervenza, MD, PhD Mark C. Lee, MD
Consultant, Division of Nephrology & Hypertension Consultant, Division of General Internal Medicine
Mayo Clinic, Rochester, Minnesota; and Mayo Clinic, Rochester, Minnesota; and
Professor of Medicine Assistant Professor of Medicine
College of Medicine, Mayo Clinic College of Medicine, Mayo Clinic
xiv C O N T R I B U TO R S
Paul S. Mueller, MD John J. Poterucha, MD
Chair, Division of General Internal Medicine Consultant, Division of Gastroenterology and Hepatology
Mayo Clinic, Rochester, Minnesota; and Mayo Clinic, Rochester, Minnesota; and
Professor of Biomedical Ethics and of Medicine Professor of Medicine
College of Medicine, Mayo Clinic College of Medicine, Mayo Clinic
C O N T R I B U TO R S xv
M. Rizwan Sohail, MD Pritish K. Tosh, MD
Consultant, Division of Infectious Diseases Mayo Clinic Scholar in Infectious Diseases
Mayo Clinic, Rochester, Minnesota; and Mayo Clinic, Rochester, Minnesota; and
Assistant Professor of Medicine Assistant Professor of Medicine
College of Medicine, Mayo Clinic College of Medicine, Mayo Clinic
Carrie A. Thompson, MD
Consultant, Division of Hematology
Mayo Clinic, Rochester, Minnesota; and
Assistant Professor of Medicine
College of Medicine, Mayo Clinic
xvi C O N T R I B U TO R S
1.
PREPARING FOR THE ABIM EXAMINATION
Robert D. Ficalora, MD
Since 2006, more than 7,000 individuals per year have taken E X A M I N AT I O N F O R M AT
the ABIM initial certification examination, and between 3,000
and 5,000 individuals per year have taken the Maintenance of Almost all of the questions are clinical and based on cor-
Certification (MOC) examination. Pass rates have ranged rect diagnosis and management. Because there is no penalty
from 79% to 94%. Pass rates for first-time takers on both for guessing, candidates should answer every question. Most
examinations exceed those of repeat takers. There is no doubt questions are based on clinical cases. Among these, 75% are
that careful and serious preparation for the examination is related to the outpatient and emergency department settings,
valuable and necessary. Although some individuals can take and the remainder are related to the inpatient setting, includ-
and pass the examination with minimal preparation, most tak- ing the critical care unit and nursing home. Increasing empha-
ers need rigorous preparation. In recent years, board certifica- sis is placed on patient safety and evidence-based quality of
tion has assumed greater importance in the minds of patients. care. Selecting the correct answer to these questions requires
In a 2003 Gallup poll of 1,001 US adults aged 18 years or integration of information provided from several sources (eg,
older, 98% wanted their physicians to be board-certified, 79% history, physical examination, laboratory test results, and
thought that the recertification process was very important, consultations), prioritization of alternatives, or use of clinical
and 54% would choose a new internist if their physicians judgment. Up to one-third of questions are experimental and
board certification had expired. included to test question quality. They are not scored and can-
not be identified during the examination. Patient management
with a cost-effective, evidence-based approach is stressed. Very
E X A M I N AT I O N : B A S I C I N F O R M AT I O N few questions require simple recall of medical facts. There are
no intentional trick questions.
The ABIM website (www.abim.org) has a wealth of informa-
tion for test takers. No one should approach the examina- The ABIM examination has a uniform question approach
tion without reading the ABIM Information and Statistics that stresses clinical reasoning over simple recall.
(http://www.abim.org/exam/prepare.aspx) and the ABIM
Certification and Recertification Exam Guide (http://www.
abim.org/exam/default.aspx). The Exam Day: What to
Expect section, http://www.abim.org/exam/exam-day.aspx, E X A M I N AT I O N C O N T E N T
has up-to-date information about changes to and navigation
of the ABIM approach to computer-based testing, such as the The questions in the examination cover a broad area of internal
following: medicine. They are divided into primary and cross-content groups
1
(http://www.abim.org/pdf/blueprint/im_cert.pdf ). Each ses- improvement module (20 points) with the American College
sion (4 for initial certification and 3 for maintenance of certifi- of Physicians Medical Knowledge Self-assessment Program
cation) contains 60 multiple-choice questions. The question may (MKSAP) (3 modules, 60 points), or one could combine
include a case history, a brief statement, a radiograph, a graph, or an ABIM practice improvement module (20 points) with 6
a photograph (such as a blood smear or Gram stain). Each ques- annual-update ABIM knowledge modules (60 points) and
tion has 5 possible answers, and the candidates should identify the ABIM peer and patient feedback module (20 points). All
the single-best answer. More than 1 answer may appear correct or points are valid for 10 years. Further refinements to this pro-
partially correct for a question. Sample questions are included in cess are likely. Thus, candidates should check for updates on
the ABIM tutorial, http://www.abim.org/exam/prepare.aspx. the ABIM website.
Candidates currently take a computer-based certification Always check the ABIM website for information and
examination that has been designed to provide a flexible, updates.
quiet, and professional environment for examination. The
computer-based test is administered by about 200 centers in The self-evaluation modules evaluate performance in clini-
the United States. Candidates schedule their examination date cal skills, preventive services, practice performance, fund of
according to the updated instructions on the ABIM website, medical knowledge, and feedback from patients and colleagues.
http://www.abim.org/exam/. Candidates are well advised to Successfully completed self-evaluation modules are valid for
access the online tutorial at http://www.abim.org/exam/pre- 10 years. Candidates may apply to begin the MOC process
pare.aspx. This tutorial allows the candidate to become famil- any time after initial certification. The ABIM recommends
iar with answering questions, changing answers, making notes that completion of the self-evaluation modules be spread out
electronically, accessing the table of normal laboratory values, over the certification period. A candidate should complete 1
and marking questions for review. self-assessment module every 1 to 2 years. The ABIM encour-
ages candidates to enroll within 4 years of certification in order
Candidates are advised to familiarize themselves with the to have adequate time to complete the program.
computer-based testing format by accessing the online tutorial.
Candidates who passed the ABIM certification
examination in internal medicine in 1990 and thereafter
have a certificate that is valid for 10 years.
M A I N T E N A N C E O F C E RT I F I C AT I O N The MOC process is called continuous professional
development and consists of a 3-step process.
The diplomate certificates issued to candidates who have
passed the ABIM examination in internal medicine since
1990 are valid for 10 years. The total number of candidates 10 T I P S F O R E F F E C T I VE E X A M I N AT I O N
who took the ABIM MOC examination for the first time in P R E PA R AT I O N
2007 was 3,837. Of these, 83% passed.
1. H AVE A S T U DY P L A N
E N H A N C E M E N T S TO M O C P R O G R A M
We all have busy lives. Successful candidates stress that the
most valuable preparation strategies must include scheduling
In January 2006, the ABIM enhanced the MOC program to
a time to study. Preparing in small, discrete pieces improves
increase flexibility and assess performance in clinical practice. The
recall, facilitates review, and makes the overall task less oner-
3 retained general components (credentialing, self-evaluation,
ous. Spending 3 or 4 hours a week, using various approaches
and secure examination) and the added self-evaluation module
such as directed reading, practice questions, and group review,
each have a point value.
is enough to stay focused. Simply reading by itself is usually a
Every candidate must complete a total of 100 points in
bad strategy. You may not be able to retain much of the ABIM
self-evaluation modules. Unlike the previous system, renewal
material by reading without focus. Start with a question, a
of more than 1 certificate does not necessitate taking addi-
problem to solve, or a patient scenario in mind. This approach
tional self-evaluation modules (ie, the same number of points,
to a study session will help you and your group understand
100, satisfies the requirement to sit for these examinations).
what you are studying, the clinical context, pathophysiology,
Candidates must complete at least 20 points in medical
and management and the reasons for it. Keep asking yourself
knowledge and at least 20 points in practice performance.
why? and why not?
The remaining 60 points may be obtained from comple-
tion of modules developed by ABIM or other organizations
How can I study such a large mass of material?
that meet the ABIM standards. Thus, one could combine an
ABIM knowledge module (20 points) and an ABIM practice Plan a pace of no more than 3 major topics per hour.
2 M AYO C L I N I C I N T E R N A L M E D I C I N E B OA R D R E VI EW
Survey the material. Discuss study material.
Consider the major subsections as potential questions. Do multiple-choice questions in groups.
Review the material in each subsection carefully to answer Indiscriminate reading of articles from many journals
the question. should be avoided.
Recite in your own words. Information in recent journals is unlikely to be included in
the examination.
Revise in your notes.
Take notes! Even if you never look at them again, the act 3. D ET E R M I N E WH AT YO U N E E D TO S T U DY
of synthesizing the information in writing will help you
retain it. For recent graduates attempting primary certification, let
your in-training examination subsection score results guide
To study, use active learning approaches to maximize your study choices. In general, if your score in a given area
efficiency. was below the fifth decile, or fiftieth percentile, you should
consider that an area for intensive review and preparation.
Simply reading, no matter how much, is generally an Use the section called educational objectives, which gives
ineffective preparation strategy. your performance by content area, to guide your choice of
preparation topics.
2. F O R M A S T U DY G RO U P MOC candidates should use practice questions to guide
your study choices. Do as many questions as you can, and
If possible, form a study group. You will be more likely to
monitor your performance by the ABIM blueprint section,
make and stay on a schedule if individuals feel a responsi-
http://www.abim.org/pdf/blueprint/im_cert.pdf.
bility to the groups progress. A group will boost everyones
Serious preparation for the examination actually starts
morale and give a common sense of purpose. A group size of
at the beginning of residency training. In addition to daily
only 2 to 5 candidates permits study of different textbooks,
reading and achieving subspecialty-based proficiency, most
board review materials, and review articles in journals. Make
candidates require a minimum of 6 to 8 months of intense
sure that you have a committed, available group of study
preparation for the examination. Cramming before the exami-
partners. Individuals who push ahead on their own and those
nation, whether by yourself or at a review course, is unlikely to
who dont keep their commitments can sabotage an other-
be successful.
wise productive group. Schedule regular meetings and assign
Use a standard textbook of internal medicine. Ideally,
individuals specific topics. This approach saves time, covers
you should use one good textbook and not jump from one
more topics per session, and allows everyone to retain more
to another. Although online, just-in-time resources may
from the discussion. Take turns acting as group moderator,
be useful for fact checking, they rarely give an inclusive,
to keep to the topic and schedule. The moderator should be
case-based review. The most effective way to use the text-
responsible, congratulating productive members and offer-
book is with patient-centered reading. Read the descrip-
ing a friendly word to someone who might be slacking off. If
tions of the symptoms and signs carefully because often
everyone has a turn, no one person has to be the bad guy.
they are part of the questions in the examination. Table 1.1
Selected review articles on common and important top-
provides several examples of the common descriptions of
ics, such as represented by the ABIM objectives, should be
symptoms and signs that could be part of the examination.
included in every session. Avoid indiscriminate reading of
Rather than reading chapters at random, read the literature
articles from many journals.
in a structured manner to assist in future recall of facts. This
Remember that questions are tested for several examina-
book and similar books are excellent tools for brushing up
tion cycles before they are included in the examination. It is
on important board-relevant information several weeks to
unlikely that new information or current controversies will be
months before the examination. They, however, cannot take
represented on your examination. Notes and other materials
the place of comprehensive textbooks of internal medicine.
the candidates have gathered during residency training can
This book is designed as a study guide rather than a com-
be good sources of information. Finding the justification for
prehensive textbook of medicine. Therefore, it should not
these pearls can cement ones command of a particular topic.
be used as the sole source of medical information for the
These clinical pearls gathered from mentors will be of help
examination.
in remembering certain important points. Always save some
time each session to review questions and discuss the answers
Study first with a standard textbook of internal medicine.
and their rationales. Dont forget to discuss each of the options
in detail. This will develop your thought process and sharpen This book is designed as a study guide and should not be
your test-taking skills. used as the sole source of information for preparation for
the examination.
Keep your study group small and stay focused.
Pay attention to the descriptions of signs and
Make a schedule and read ahead of the discussion. symptoms.
1. P R E PA R I N G F O R T H E A B I M E X A M I N AT I O N 3
Table 1.1 COMMON DESCRIPTIONS OF SIGNS AND SYMPTOMS IN EXAMINATION QUESTIONS
Cardiology
Shortness of breath or asymptomatic Late peaking systolic murmur, intensity decreases with Hypertrophic obstructive
handgrip & increases with squatting cardiomyopathy
Coarctation of aorta
Asymptomatic, headache Hypertension, diminished or absent lower extremity
pulses, systolic murmur, bruit over chest wall
Neurology
Gait impairment, falls, dysphagia, dysarthria Inability to look up & side to side Progressive supranuclear palsy
Diplopia, oscillating images, reading fatigue, Impaired adduction on lateral gaze, with nystagmus in Internuclear ophthalmoplegia
loss of depth perception the contralateral abducting eye (consider multiple sclerosis,
cerebrovascular disease)
Fluctuating memory, confusion, visual hall Mild parkinsonism, dementia Lewy body dementia
ucinations
Inappropriate behavior, dementia, poor social skills Dementia Frontotemporal dementia
Paroxysmal pain affecting the side of the face Usually normal Trigeminal neuralgia affecting
1 of the branches of cranial
nerve V
Muscle stiffness, clumsiness, occasional emotional Brisk reflexes, spasticity (upper motor neuron signs), Amyotrophic lateral sclerosis
lability atrophy, fasciculation (lower motor neuron signs)
Altered mental status, fever, headache Flaccid paralysis, neck rigidity r, altered mental status West Nile virus encephalitis
Infectious disease
Recurrent sinusitis, skin, or pulmonary infections Sinus tenderness, abnormal lung sounds Chronic granulomatous
due to Staphylococcus aureus disorder
Recurrent Neisseria infections Neck rigidity r, altered mental status Inherited deficiencies of
complement (C5, 6, 7, 8, 9),
factor D, or properdin
Recurrent episodes of bacterial pneumonia, sinus- Malnourished, abnormal lung sounds Common variable
itis, diarrhea due to Streptococcus pneumoniae immunodeficiency
Gastroenterology
Cirrhosis of liver, ingestion of raw oysters Fever, hypotension, hemorrhagic bullae, signs of cir- Vibrio vulnificus
rhosis of liver
Diarrhea Pruritus, grouped vesicles over the elbow, knee, scalp, Dermatitis herpetiformis due
or back of neck to celiac sprue
Hepatitis C, photosensitivity Skin fragility, erosions, blisters on dorsum of hand, Porphyria cutanea tarda
hyperpigmentation
Dermatology
Facial rash, photosensitivity Papules & pustules on bridge of nose & face, Rosacea
telangiectasia
Rash Sharply demarcated erythematous papules, silvery Psoriasis
white scales over scalp, extensor surfaces of extremi-
ties, & nails
Cough with sore throat Tender, erythematous pretibial nodules Erythema nodosum
Ulcerative colitis Irregular, undermined ulcer with violaceous border or Pyoderma gangrenosum
scarring in lower extremities
Flushing, diarrhea, rapid heart rate Brown-red macules, urticaria on stroking skin Systemic mastocytosis
4 . C R E AT E A N D D EVOT E T I M E
in a quiet room, and this time may be best reserved for early
Board preparation should be part of your daily routine, like in the morning or on a weekend. Keep in mind that the more
exercising, showering, or brushing your teeth. If you dont time and energy you spend actively learning a topic, the bet-
regularly do some preparation, it will fall off your routine, and ter your command, and the less dependent you will be on rote
your preparation just wont happen. You can spend as little or memorization.
as much time as you want on a particular activity. Often you Some people can study effectively while on a treadmill,
can review familiar topics in small discrete time periods (eg, on a train, or in a car. If you can do this, you can incorpo-
before or after lunch). Less familiar topics may require an hour rate this into your studying routine. How much time it takes
4 M AYO C L I N I C I N T E R N A L M E D I C I N E B OA R D R E VI EW
to perform these tasks varies from person to person and will range from 5 to 10 with some estimated to have 0 to 2. Pace
improve as you solidify your study habits. Regardless, every your preparation by subject:
learning task takes time, and you must budget for that time.
Only you can decide how much time you want to spend in Subjects with a large estimated number of questions are
solitary study, in groups, or in summary objective review. You very likely to be there. Master them.
can make great plans, but life and work arent predictable,
so you should build in some catch-up time for unexpected Subjects with a medium to low estimated number of
distractions. questions will be there in some form. Review them.
You also have to consider how much time it takes to Subjects with a very low estimated number of questions
organize your studying. Review of cardiology may go may be tangential or favorite board zebras. Depending on
quickly, whereas glomerulopathies may take a pad and pen- your available study time, it may be worthwhile for you to
cil to figure out. You may have to travel to study sessions consider them only for last-minute review.
or spend time looking for information to ensure your com-
mand of a given objective. Many candidates try to set aside Plot out your objectives review on a calendar, mixing more and
large blocks of time. With our busy lives, that may be laud- less complex objectives. Leave time for discussion, literature and
able but impractical. Many shorter sessions not only allow online searches, and follow-up for problem items from previous
for study and catch-up but also can be worked in around study sessions. Always plan to cover new material and to periodi-
standing commitments more effectively than large blocks, cally cycle back to previously reviewed difficult or detailed infor-
and thus a missed session wont be a major setback for that mation. Imagine cases that might go with the material at hand.
week. The time you spend will come back to you when you The most effective way to manage your study time is
pass, and a failure only means you have to devote the time to periodically assess your progress through practice tests
all over again. and test questions. It is impossible to overemphasize the
Certifying or recertifying board examinations can be stress- importance of this point. Boardsmanship is a real skill,
ful. The sheer mass of information can be overwhelming to and there is no substitute for familiarity with the form and
some. The press of occupational and personal responsibilities content of the ABIM-type questions. Therefore, you are
makes finding the time to study very difficult, so many opt to strongly encouraged to take at least a few mock examina-
take a review course. A review course should be the final inte- tions and simulate the actual testing environment (ie, no
grating activity once you have completed your own primary breaks, snacks, music, phones, pagers). Taking mock ques-
preparation. To be successful you should go to the review tions is an effective use of a board review or board questions
course prepared and ready to fill in objectives you may have book. Practice material at intervals during your long-term
missed or to learn from experts objectives that you couldnt test preparation schedule. Your schedule should be the most
understand on your own. Dont expect a course to substitute intense in the 3 months before the test. After that, focus on
for primary preparation. Attending a highly focused, no-fluff review, consolidating key points, and resolving previously
course that delivers the information in a concentrated, difficult problems.
high-yield manner right before the examination may seem like Once you or your group has a schedule, stick to it. Add ses-
an easy way out, but it is unlikely to be the difference between sions, but never delete any. Stick to your start and stop times.
success and failure.
Schedule your progress and build in assessment sessions.
Residents: Prepare for the boards during residency.
You will not find that kind of quality time after your Make changes, but no deletions.
residency. Plan to review material that you have chosen several times
Once residency is over and you start fellowship or a job, (minimum twice).
you will not find time to study.
Stay focused throughout the months before the
MOC: Schedule the time. examination.
Schedule multiple short preparation sessions rather than Board review preparation must be at its peak by 3 months
fewer long ones. before the examination. If you have not yet formed a study
Do not rely solely on a review course; they are not a group, now is your last chance.
substitute for primary preparation.
6. A NSWE R Q U E S T I O N S S I M I L A R TO
5. P R E PA R E A P L A N A N D S C H E D U L E IT E X A M I NAT I O N C O N T E N T
All ABIM objectives are not equal. Review the relative per- The purpose of standardized testing is to measure a candi-
centage of the contents of the examination and the number dates command of the material so that scores from different
of questions per objective (http://www.abim.org/pdf/blue- test dates can be reliably compared with one another. The
print/im_cert.pdf ). Note that some areas may have an esti- results must correlate statistically with the results of all the
mated number of questions of 11 to 15, whereas many will test-takers who have answered the same questions. Persons
1. P R E PA R I N G F O R T H E A B I M E X A M I N AT I O N 5
who construct board review materials and questions go to Familiarize yourself with the teaching principle and the
great pains to build them for the same content and content testing objective, which may give you insight into the
level as on the actual board examination. The good ones are questions and the possible responses.
validated and have been tested to make sure that they perform
in a reliable, predictable manner and that they adequately test
7. D O N T F O RG ET A B O U T I M AG E S
the content they purport to test. Any questions prepared for
other courses, local residency, fellowship rotations, or other Every image-based question will also include text or a clini-
venues that cover similar material likely wont test the mate- cal case or both. Dont simply focus on the image without
rial in a way that predicts your performance on the board reading the text. Familiarize yourself with the image and its
examination. Read a board review book, go to a board review details after you have read the case, and then read it again.
course, and always practice answering questions. When you Photographs of skin disorders, radiographs, electrocardio-
practice answering questions, do it as you would during the grams, and other images given in board questions are generally
examination; just reading the book and reading the answers easy ways to score points. Reading the ABIM question stem
likely will not prepare you for the actual test. For every ques- last helps put the pieces of the puzzle in place. Methodically
tion, identify in your own mind the concept being tested. review a radiograph as you would in a patient encounter.
Make sure you read all the wrong answers and make sure you Immediately focusing on an obvious abnormality can distract
understand why they werent the best answer for the question you from a more subtle finding that may alert you to the cor-
asked. rect answer. You may miss the pneumothorax as the cause of
Sometimes candidates try to prepare by studying mate- the dyspnea if you focus only on the heart size and the small
rials that are harder than the real test, such as subspecialty pleural effusion. Likewise for skin findings; use your clinical
boardlevel review courses and practice tests. The idea is that skills to interpret the finding. Is it flat or raised, erythematous
becoming familiar with something harder will make the real or pigmented?
thing easier by comparison. Preparing with something more
challenging can be a good idea in some types of athletic or Approach an image question as you would a patient.
endurance preparation, but it is a bad idea for the ABIM
examination. Because the objectives are specific and pub- Methodically examine the image.
lic, preparing by using objectives for another examination Use the text and the stem to focus your inquiry.
may cause you to misinterpret or overinterpret what is being
asked. Reliably finding the easiest approach to a test question
8. S P E N D S O M E T I M E B E C O M I N G E X P E RT I N
requires being aware that the test cant require you to use a cer-
B OA R D S M A N S H I P
tain higher-level data set or decision tree. Because the harder
material is testing a different skill set, reviewing this may lead Some candidates fail the examination despite intense prepara-
to incorrect answers. tion and the clinical competence necessary to pass the exami-
As silly as this piece of advice may seem, read the ques- nation. Failing usually happens because they dont understand
tions carefully! Doing so can make a big difference in your or interpret the questions properly. The ability to understand
score. If you read questions hastily, there is a high likelihood the nuances of the question format is sometimes referred to as
that you will misinterpret them. Some questions offer incor- boardsmanship. Intelligent interpretation of the questions
rect choices that are designed to answer a common misinter- is very important for candidates who are not well versed in
pretation of the actual question. Be particularly careful with the format of multiple-choice questions. Answer the questions
answers that have more than one part. Only one part may be whose answers you know first, making sure you understand
correct. Other distraction techniques include 2 responses that what is being asked to ensure that they are answered correctly.
are similar except for a word or phrase. Watch for responses It is easy to become overconfident with such questions, and
that contradict others; usually, both of these can be ruled out. thus you may fail to read the questions or the answer options
What if you read a question and the traditional correct answer carefully. Make sure you never make mistakes on easy ques-
isnt an option? What if more than one answer could be cor- tions. Read the final sentence (that appears just before the
rect? Then select the best option available. Be very careful multiple answers) several times to understand how an answer
of responses that are the longest or the unique answer. They should be selected. Recheck the question format before select-
are no more likely or unlikely to be correct despite prevailing ing the correct answer. Read each answer option completely.
wisdom. Occasionally, a response may be only partially correct.
At times, the traditionally correct answer is not listed. In
Dont try to read the board review material from cover to these situations, select the best alternative listed. Watch
cover. for qualifiers such as next, immediately, or initially. Avoid
The best way to prepare is to review and always practice answers that contain absolute or very restrictive words
answering questions. such as always, never, or must. Answer options that contain
absolutes are likely incorrect. Try to think of the correct
To improve your understanding, read the explanation, answer to the question before looking at the list of poten-
and look up additional information related to each of the tial answers. Assume you have been given all the neces-
choicesboth correct and incorrect. sary information to answer the question. If the answer you
6 M AYO C L I N I C I N T E R N A L M E D I C I N E B OA R D R E VI EW
had formulated is not among the list of answers provided, For elderly patients, aim for less aggressive alternatives,
you may have interpreted the question incorrectly. When especially in those with multisystem disease.
a patients case is presented, think of the diagnosis before
Beware of adverse medication effects and
looking at the list of answers. If you do not know the answer
polypharmacy.
to a question, very often you are able to rule out one or sev-
eral answer options. Determine whether your diagnosis is For asymptomatic healthy patients, do nothing and
supported by any of the answers. If you can eliminate any observe.
answers as clearly wrong, you will improve your odds at
guessing. Occasionally, you can use information presented Use your existing fund of knowledge of internal medicine
in one question to help you answer other, difficult ques- and your previous clinical experience.
tions. Many questions are on the test for trial or validation Approach each question as a real-life patient encounter.
purposes and are not scored. If a question seems to you to
be a bad or confusing question, it may be in this category. There are no trick questions.
It is best not to spend an inordinate amount of time trying
to second guess this type of question. Come back to it after 10. P L A N F O R T H E DAY O F T H E E X A M I NAT I O N
you have finished, if you still have time.
You should have adequate time to read and answer all the ques-
When reading long multiple-choice cases: tions; therefore, there is no need to rush or become anxious.
Watch the time to ensure that you are at least halfway through
First read the actual lead line of the question the examination when half of the time has elapsed. Start by
Once you understand what the question is asking: answering the first question and continue sequentially. Almost
all of the questions follow a case-presentation format. At times,
Stay focused and look for clues in the long stem of the subsequent questions will give you information that may help
question. you answer a previous question. Do not be alarmed by lengthy
As you read through the questions: questions; look for the questions salient points. When faced
with a confusing question, do not become distracted by that
Note the key facts and abnormal findings question. Mark it so you can find it later, then go to the next
Skip questions about which you have no idea, and come question and come back to the unanswered ones at the end.
back after a complete first pass Extremely lengthy stem statements or case presentations are
intended to test the candidates ability to separate the essen-
tial from the unnecessary or unimportant information. You
may want to highlight important information presented in
9. US E YO U R R E FL E X E S
the question in order to review this information after reading
Associations, causes, complications, and other relationships the entire question and the answer options. There is no pen-
between a phenomenon or disease and clinical features are alty for guessing, so you should never leave an answer blank.
important to remember and recognize. Each subspecialty has Every time you can eliminate just one choice you increase your
many common connections, and candidates for the ABIM chance of choosing a correct answer by 20%, so its best to
and other examinations may want to prepare lists like this guess among the remaining choices. If you truly have no idea
for different areas. For example, a case that presents a patient about any of the choices, the B answer has been statistically
with health careassociated pneumonia should immediately more likely to be correct. It is better to choose B if you truly
bring to mind antipseudomonal antibiotics, not antibiot- dont know the answer.
ics traditionally used for community-acquired pneumonia.
Combined knee and hip pain should have you consider- Look for the salient points in each question.
ing a gait abnormality rather than abnormality in 2 joints
If a question is confusing, mark it to find it and come back
simultaneously.
to the unanswered questions at the end.
Use the basic fund of knowledge accumulated from clini-
cal experience and reading to solve the questions. Approaching If you must guess, choose B; statistically, it is more likely
the questions as real-life encounters with patients is far better to be correct.
than trying to second-guess the examiners or trying to analyze
whether the question is tricky. As indicated above, the ques- Its really not productive to discuss the questions or answers
tions are never tricky, and there is no reason for the ABIM to after the examination with other candidates. Such discussions
trick the candidates into choosing wrong answers. usually cause more consternation, although some candidates
Use examination techniques to your advantage. Look for may derive a false sense of having performed well on the exam-
target populations in questions. Start with a basic premise in ination. In any case, the candidates are bound by their oath to
mind, then modify it as the information warrants. Examples the ABIM not to discuss or disseminate the questions. Do not
are as follows: study between examination sessions. To minimize stress, stick
to your daily routine; dont start or stop exercising or using
For young patients, aim for aggressive management. caffeine, and dont skip meals or load up on carbohydrates. Be
1. P R E PA R I N G F O R T H E A B I M E X A M I N AT I O N 7
as rested and refreshed as you can be. Forget about your elec- S U M M A RY
tronic devices such as pagers and cell phones.
Preparation for the ABIM examination requires a serious
Dont study the day before the examination or between the and organized approach. Devote adequate time. Familiarize
examination sessions. yourself with the examination format and objectives. Use
commonsense test-taking strategies, including practice tests
Discussing the examination questions with others raises and question analysis. Treat the examination day as you would
anxiety and can adversely affect your performance in the for any competitive event by preparing physically.
next session.
Maintain your normal routine.
8 M AYO C L I N I C I N T E R N A L M E D I C I N E B OA R D R E VI EW
PA RT I
C A R D I O L O GY
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2.
ARRHY THMIAS AND SYNCOPE
Nicole P. Sandhu, MD, PhD, Peter A. Brady, MB, ChB, MD,
G OA L S E VA LUAT I O N O F S U S P E C T E D R H Y T H M
DISORDER S
Discuss the evaluation and management of cardiac
arrhythmias.
E L EC T RO C A R D I O G R A P H Y
Explain the different types of syncope.
Electrocardiography (ECG) is the most simple and
Describe the evaluation and management of cost-effective tool for evaluating rhythm disorders. It can
syncope. provide important clues to the diagnosis (eg, ventricular pre-
excitation in Wolff-Parkinson-White syndrome). Whenever
MECHANISM OF ARRHY THMIAS possible, a current ECG should be compared with previous
recordings.
Abnormal cardiac arrhythmias may be due to reentry, abnor-
mal automaticity, or triggered activity. Reentry is the most
common mechanism for cardiac arrhythmias. Reentrant A M BU L ATO RY E C G M O N I TO R I N G
rhythms may be microreentrant (eg, a small circuit around an Ambulatory ECG (Holter) monitoring allows evaluation of
area of myocardial fibrosis, as in sinus node reentry or atrio- rhythm disturbances and their relationship to daily activi-
ventricular [AV] node reentry) or macroreentrant (eg, around ties. It is useful to have a patient who is undergoing ambula-
an area of myocardial infarction or scar and reentry within tory ECG monitoring keep a diary and correlate symptoms
the atrium, as in atrial flutter or an accessory pathway, such with the recorded heart rhythm during symptoms. Normal
as in Wolff-Parkinson-White syndrome). Three conditions results on Holter monitoring do not rule out a heart rhythm
are needed for reentry to occur: 1) more than 2 anatomically abnormality as a cause of symptoms unless symptoms occur
or functionally distinct pathways (eg, AV nodal reentry), 2) a during the monitoring period. Ambulatory ECG monitor-
unidirectional block in 1 pathway, and 3) slowed conduction ing is also useful for assessing impact of medical and pace-
in the second pathway. maker therapy.
Automatic rhythms are more common in enhanced sym-
pathetic tone, hypoxia, acid-base and electrolyte disturbances, Ambulatory ECG monitoring allows evaluation of rhythm
or atrial or ventricular stretch (eg, exacerbations of congestive disturbances and their relationship with daily activities.
heart failure). Digoxin toxicity is the most common cause of
arrhythmias due to triggered activity. Normal results on Holter monitoring do not rule out a
heart rhythm abnormality unless symptoms occur during
Reentry is the most common mechanism of cardiac monitoring and the rhythm is normal.
arrhythmias.
Automatic rhythms are more common in settings of
enhanced sympathetic tone, hypoxia, acid-base EV E N T R E C O R D I N G
and electrolyte disturbances, or atrial or ventricular
Transtelephonic event recording is similar to ambulatory ECG
stretch.
monitoring but is more useful for documenting heart rate
Arrhythmias due to triggered activity are most often due to and rhythm when symptoms are less frequent (<1 episode
digoxin toxicity (Figures 2.1 and 2.2). per 2448 hours). The device is activated during symptoms
11
Implantable loop event recording is used when symptoms
are infrequent or are of sudden onset. These devices can be
programmed to provide information regarding rhythm dis-
turbances over several months.
T H E R A P Y F O R H E A RT R H Y T H M
DISORDER S
A
Several therapeutic options are available for heart rhythm dis-
AV orders. These include drug therapy, radiofrequency ablation,
and device therapy (pacing for bradyarrhythmias and implant-
V
able cardioverter-defibrillators [ICDs] for tachyarrhythmias).
12 C A R D I O L O GY
Table 2.1 PROPERTIES OF ANTIARRHYTHMIC DRUGS Table 2.2 RELATIVE EFFECTIVENESS OF
ANTIARRHYTHMIC DRUGS
ROUTE OF
THERAPEUTIC
METABOLISM EFFECTIVENESS a
RANGE, HALF-
DRUG mcg/ml LIFE, h Hepatic, % Renal, %
DRUG PVCs VT PSVT AF
Class IA
Quinidine 2+ 2+ 2+ 2+
Quinidine 25 68 80 20
Procainamide 410 36 50 50 Procainamide 2+ 2+ 2+ 2+
Disopyramide 25 48 50 50
Disopyramide 2+ 2+ 2+ 2+
Class IB
Lidocaine 2+ 2+ 0 0
Lidocaine 1.55 14 100 0
Mexiletine 12 816 100 0 Mexiletine 2+ 2+ 0 0
Phenytoin 1020 24 ~100 0
Ibutilideb NI NI NI 2+
Class IC
Flecainide 4+ 2+ 3+ 2+
Flecainide 0.21 1227 75 25
Propafenone Not helpfula 210 100 0 Propafenone 4+ 2+ 3+ 2+
2 . A R R H Y T H M I A S A N D SY N C O P E 13
Table 2.3 TOXICITY AND ADVERSE EFFECTS OF ANTIARRHYTHMIC DRUGS
RISK OF CONGESTIVE
FREQUENCY % PROARRHYTHMIA
HEART FAILURE a
OF ADVERSE ORGAN DURING TREATMENT
DRUG EFFECTS, % TOXICITY FOR VT EF >30% EF 30% ADVERSE EFFECTS
Abbreviations: EF, ejection fraction; L-H, light-headedness; VT, sustained ventricular tachycardia.
a
Congestive heart failure risk: 0, no risk; 4+, high risk.
b
Intravenous therapy for acute cardioversion in patients with atrial fibrillation.
Adapted from MKSAP IX: Part C, Book 1, 1992. American College of Physicians. Used with permission.
Adenosine slows AV conduction and has a half-life of 10 in patients with decreased ventricular function and a history
seconds. of sustained ventricular tachycardia or ventricular fibrillation.
It is indicated for termination of rapid SVT using the AV Proarrhythmia can occur in structurally normal hearts.
node.
All antiarrhythmic drugs can cause arrhythmias.
Adenosine is contraindicated in patients with atrial
fibrillation associated with Wolff-Parkinson-White
syndrome because of the risk of hemodynamic collapse as T R A N S C AT H ET E R R FA
atrial fibrillation transitions to ventricular fibrillation.
Transcatheter RFA using a radiofrequency energy source to
Adverse Effects of Antiarrhythmic Drugs heat tissue has revolutionized the treatment of almost all heart
rhythm disorders. Narrow complex tachycardias such as AV
Proarrhythmic effect (Table 2.3), a common and important nodal reentrant tachycardia or tachycardia due to an accessory
problem of all antiarrhythmic drugs, occurs when the drug pathway (eg, Wolff-Parkinson-White syndrome) are curable
creates an adverse rhythm disturbance, including sinus node with RFA in more than 95% of cases. Atrial tachycardias are
suppression and sinus bradycardia, AV block, or increased fre- curable in more than 90% of cases. Table 2.4 lists arrhythmias
quency of or new-onset atrial or ventricular arrhythmias. An amenable to catheter ablation therapy. Atrial fibrillation (espe-
example, quinidine syncope due to polymorphic ventricular cially paroxysmal atrial fibrillation) and ventricular tachycardia
tachycardia, is shown in Figure 2.4. All antiarrhythmic agents due to reentry around a scar after myocardial infarction can
can be proarrhythmic. The frequency of proarrhythmia is higher also be treated with RFA. RFA prevents further conduction
14 C A R D I O L O GY
AVN, AP, HP, and
ventricular
Propafenone
Atrial, ventricular,
Amiodarone AP, and HP
Sotalol Quinidine
Procainamide
Disopyramide
Lidocainea
Flecainide
Ibutilideb
Bretyliuma
AVN
Dofetilide
Adenosine
Ca++ channel
blockers
-blockers
Digoxinc
a
Ventricular only
b
Atrial only
c
Vagotonic effect
Figure 2.3 The Predominant Targets of Frequently Used Antiarrhythmic Agents. AP indicates accessory pathway; AVN, atrioventricular node; HP,
His-Purkinje system.
of electrical impulses and prevents the abnormal rhythm from atrial fibrillation or atrial flutterassociated heart rates
occurring. Complications include vascular injury, cardiac per- that are refractory to medications. After ablation, perma-
foration, and infection and occur in 1% to 2% of patients. nent pacing is required. This approach results in substantial
There is a 5% risk of creating complete heart block requiring improvement in symptoms and exercise capacity with use of
permanent pacing if the ablated area is close to the normal con- rate-responsive pacing. The major disadvantage is that patients
duction system or if AV nodal reentrant tachycardia is ablated. are pacemaker-dependent and it is irreversible. This approach
Catheter ablation also may be used to achieve complete is reserved for very elderly patients or when other approaches
heart block in 95% of patients with difficult-to-control fail. Catheter ablation techniques aimed at removing the
Figure 2.4 Proarrhythmic Response to Quinidine. Quinidine resulted in prolongation of QT interval, and late-coupled premature ventricular complex
initiated polymorphic ventricular tachycardia, termed torsades de pointes.
2 . A R R H Y T H M I A S A N D SY N C O P E 15
Table 2.4 HEART RHYTHMS AMENABLE TO Box 2.1 INDICATIONS FOR PACEMAKER
CATHETER ABLATION IMPLANTATION
RHYTHM CURABLE TREATABLE
Sinus node dysfunction
SVT AVNRT AF Class I
AVRT (bypass tract) Documented symptomatic bradycardia
EAT Class II
AFL (without fibrillation) HR <40 bpm, symptoms present but not clearly correlated
Ventricular RV outflow tract tachycardia VT due to coronary dis- with bradycardia
Idiopathic LV tachycardia ease & scar after MI Class III
Asymptomatic bradycardia (<40 bpm)
Abbreviations: AF, atrial fibrillation; AFL, atrial flutter; AVNRT, atrioventricular AV block
node reentry tachycardia; AVRT, atrioventricular reentry tachycardia; EAT, ectopic Class I
atrial tachycardia; LV, left ventricular; MI, myocardial infarction; RV, right ventric- Symptomatic 2 or 3 AV block, permanent or intermittent
ular; SVT, supraventricular tachycardia; VT, ventricular tachycardia.
Congenital 3 AV block with wide QRS
Advanced AV block 14 days after cardiac surgery
triggers that cause atrial fibrillation and flutter are used with Class II
increasing success. Asymptomatic type II 2 or 3 AV block with ventricular rate
>40 bpm
Narrow complex tachycardia due to AV nodal reentrant Class III
tachycardia, accessory pathway in Wolff-Parkinson-White Asymptomatic 1 & type I 2 AV block
syndrome, focal atrial tachycardia, atrial flutter, and, often, Myocardial infarction
atrial fibrillation and ventricular tachycardia can be cured Class I
with RFA. Recurrent type II 2 AV block & 3 AV block with wide
In patients with atrial fibrillation or flutter whose heart QRS
rates are refractory to medications, catheter ablation may Transient advanced AV block in presence of BBB
be used to achieve complete heart block. After ablation, Class II
permanent pacing is required. Persistent advanced AV block with narrow QRS
Acquired BBB in absence of AV block
Current therapeutic interventions available to patients with Class III
symptoms due to tachycardia are summarized in Table 2.5. Transient AV block in absence of BBB
Abbreviations: AV, atrioventricular, BBB, bundle branch block; bpm, beats per
D EVI C E T H E R A P Y minute; HR, heart rate.
16 C A R D I O L O GY
Table 2.6 CODE OF PERMANENT PACING
PROGRAMMABLE
CHAMBER(S) PACED CHAMBER(S) SENSED MODE(S) OF RESPONSE CAPABILITIES
D = Dual (atrium & ventricle) D = Dual (atrium & ventricle) D = Dual (triggered & inhibited)
O = None O = None
Early complications (within 30 days of implantation) are 3. Ischemic and nonischemic cardiomyopathy (left
usually related to vascular injury, hematoma, pneumothorax, ventricular ejection fraction [LVEF] <35%) plus
dislodgment of the lead, and extracardiac stimulation. Late com- congestive heart failure (New York Heart Association
plications include lead fracture or insulation defect, infection, [NYHA] class II or III)
pacemaker syndrome, and pacemaker-mediated tachycardia.
4. Ischemic cardiomyopathy due to prior myocardial
Pacemaker-mediated tachycardia is a well-recognized
infarction and LVEF <30%
complication of dual-chamber pacemakers (DDD pacing).
Pacemaker-mediated tachycardia occurs during DDD pacing 5. ICDs provide greater overall mortality reduction in
when there is intact retrograde conduction between the ventricle patients with a history of out-of-hospital arrest or
and atrium. A spontaneous premature ventricular contraction symptomatic sustained ventricular tachycardia than
occurs that conducts retrogradely to the atrium. The tachycardia amiodarone.
rate is typically close to the upper rate limit of the device. Most pace-
makers can recognize and attempt to abort pacemaker-mediated
S U M M A RY O F T H E R A P Y F O R H E A RT R H Y T H M
tachycardia. Pacemaker-mediated tachycardia is corrected by pro-
DISORDERS
gramming changes of the pacemaker generator.
Table 2.5 summarizes the roles of drug therapy, ablation
Early complications occur within 30 days of implantation therapy, and ICD therapy for different supraventricular
and are related to vascular injury, lead displacement, tachyarrhythmias.
pneumothorax, and extracardiac stimulation.
Late complications are related to lead fracture or
insulation defects, infection, pacemaker syndrome, or SPECIFIC ARRHYTHMIAS
pacemaker-mediated tachycardia.
T H E B R A DYC A R D I A S
Implantable Cardioverter-Defibrillators Bradycardia is defined as a heart rate less than 60 beats per
An ICD continuously monitors heart rhythm and can detect minute at rest or a decreased heart rate response to exercise.
and treat abnormal ventricular arrhythmia with overdrive pac- Causes of bradycardia include high vagal tone (most cases
ing (antitachycardia pacing), low-energy cardioversion, or up occur in asymptomatic and often fit and healthy persons),
to 30- to 40-J shocks. ICDs have been shown to improve mor- sinus node dysfunction, drug therapy, heart block, and myo-
tality outcomes among patients who survive sudden cardiac cardial infarction.
death. An ICD is superior for reducing overall mortality in
comparison with empiric amiodarone therapy in patients with Sinus Node Dysfunction
a history of out-of-hospital cardiac arrest or symptomatic sus-
tained ventricular tachycardia. Sinus node dysfunction includes sinus bradycardia, sinus
Indications for ICD implantation include the following: pauses, tachycardia-bradycardia syndrome (Figure 2.5), sinus
arrest, and chronotropic incompetence. In most cases, sinus
1. Documented episode of cardiac arrest caused by node dysfunction is diagnosed on the basis of the history and
ventricular fibrillation not due to a transient or reversible results of ECG and Holter monitoring. EP testing is usually not
cause, documented sustained ventricular tachyarrhythmia necessary. Prolonged monitoring with an event recorder may
(spontaneous or induced by an electrophysiology study) be required to correlate symptoms with bradycardia. Treadmill
not associated with an acute myocardial infarction and testing can distinguish true sinus node dysfunction, in which
not due to a transient or reversible cause a blunted heart rate occurs in response to exercise, from high
vagal tone, in which the heart rate increases appropriately dur-
2. Documented familial or inherited conditions with a high ing exercise to meet metabolic need. EP testing is reserved
risk of life-threatening ventricular tachycardia (eg, long for a minority of patients in whom the arrhythmia mecha-
QT syndrome or hypertrophic cardiomyopathy) nism cannot be determined by ECG or Holter monitoring.
2 . A R R H Y T H M I A S A N D SY N C O P E 17
Figure 2.5 Tachycardia-Bradycardia Syndrome. In this case, episode of atrial fibrillation terminated spontaneously, followed by a 4.5-second pause until
the sinus node recovered. (Adapted from MKSAP IX: Part C, Book 1, c1992. American College of Physicians. Used with permission.)
I aVR V1 V4
II aVL V2 V5
III aVF V3 V6
Figure 2.6 3:2 Mobitz I (or Wenckebach) Second-Degree Atrioventricular Block. Patient had acute inferior myocardial infarction.
18 C A R D I O L O GY
Figure 2.7 Mobitz I Second-Degree Atrioventricular Block. Note gradual PR prolongation. The PR interval after a nonconducted P wave is shorter
than the PR interval preceding the nonconducted P wave.
Figure 2.8 Mobitz II Second-Degree Atrioventricular Block. There was no change in the PR interval before or after a nonconducted P wave.
interval either before or after the nonconducted P wave (Figure Third-Degree (Complete) Heart Block
2.8). The ventricular escape rhythm is either a junctional escape Complete heart block is diagnosed when there is no rela-
focus, with a conduction pattern similar to that seen during nor- tion between atrial rhythm and ventricular rhythm, and atrial
mal rhythm, or a ventricular escape focus, with a wide QRS con- rhythm is faster than ventricular escape rhythm (Figure 2.9).
duction pattern. Mobitz II block is usually due to conduction Treatment is with permanent pacing.
disease in the His-Purkinje system. It often heralds complete
heart block, and permanent pacing should be considered. Complete heart block is treated with permanent pacing.
Mobitz I block is identified by gradual prolongation of the Bifascicular block refers to left bundle branch block
PR interval before a nonconducted P wave, and the PR (both fascicles blocked), right bundle branch block with
interval after the nonconducted P wave is shorter than the left anterior fascicular block (marked left axis deviation),
PR interval before the nonconducted P wave. or right bundle branch block with left posterior fascicular
block (right axis deviation). Patients presenting with syn-
Mobitz II block is diagnosed from the sudden
cope and bifascicular block may have intermittent complete
nonconduction of a P wave without alteration in any PR
heart block due to conduction system disease or ventricu-
interval.
lar tachycardia caused by underlying myocardial disease.
Mobitz II block often heralds complete heart block, and Permanent pacing can be used to treat syncope due to com-
permanent pacing should be considered. plete heart block.
Figure 2.9 Complete Heart Block. Atrial rate was 70 beats per minute and ventricular escape rhythm was 30 beats per minute.
2 . A R R H Y T H M I A S A N D SY N C O P E 19
I aVR V1 V4
II aVL V2 V5
III aVF V3 V6
II
V1
V5
Bifascicular block usually is associated with structural heart neck abnormalities, such as lymph node enlargement, prior
disease and progresses to complete heart block in about 1% neck surgery, or a regional tumor, can cause carotid sinus
of asymptomatic persons. hypersensitivity syndrome. Most patients do not have spon-
taneous syncope. Carotid sinus massage may be performed
High-degree (high-grade) AV block is diagnosed when over the carotid bifurcation at the angle of the jaw for 5 sec-
there is a 2:1 or higher AV conduction block (Figure 2.10). onds while monitoring heart rate and blood pressure to test
It can be due to a Wenckebach or Mobitz II mechanism. A for this cause, but only in patients without a carotid bruit or
Wenckebach mechanism is more likely if QRS conduction a history of cerebrovascular disease. One-third of patients
(duration) is normal, whereas a Mobitz II mechanism is more with a hyperactive carotid sinus reflex have a pure cardioin-
likely if the QRS complex demonstrates additional conduc- hibitory component manifested only by a pause in ventricular
tion disease, such as bundle branch block. activity exceeding 3 seconds. Fifteen percent of patients have
a pure vasodepressor component, with a normal heart rate
High-grade AV block is diagnosed when the ECG shows a maintained but a decrease in systolic blood pressure of more
2:1 or higher AV conduction block. than 50 mm Hg. Sixty percent of patients have a combined
response of both cardioinhibitory and vasodepressor compo-
nents. Permanent pacing may prevent the cardioinhibitory
Carotid Sinus Hypersensitivity Syndrome
response, but the vasodepressor response continues to pro-
Approximately 40% of patients older than 65 years have a duce symptoms.
hyperactive carotid sinus reflex (a 3-second pause or a decrease AV sequential pacing is the primary form of therapy for the
in systolic blood pressure of 50 mm Hg) (Figure 2.11). Rarely, cardioinhibitory component, and elastic stockings are used to
Figure 2.11 Sinus Pause With Junctional Escape Beats Before Sinus Rhythm Returns. Test was done during carotid sinus massage.
20 C A R D I O L O GY
treat the vasodepressor component. Occasionally, the condi- Catheter ablation of atrial flutter has a success rate of
tion responds to anticholinergic medications. Surgical tech- >90%.
niques to treat this condition are often unsuccessful.
Atrial flutter is associated with the same risk of
thromboembolism as atrial fibrillation and should be
Patients with a hyperactive carotid sinus reflex experience
treated similarly to atrial fibrillation with regard to
a 3-second pause or a decrease of 50 mm Hg in systolic
anticoagulation.
blood pressure.
In atrial flutter, the ECG shows a characteristic sawtooth
The cardioinhibitory component is treated with AV
pattern with an atrial rate of 240320 beats per minute.
sequential pacing, and elastic stockings are used to treat the
vasodepressor component. AV node conduction rate and ventricular rate control are
achieved with the pharmacologic therapy used in atrial
Anticholinergics are occasionally helpful, and surgical
fibrillation; success rates for control of atrial flutter are
procedures are usually unsuccessful.
30%50%.
T H E TAC H YC A R D I A S
Atrial Fibrillation
Atrial Flutter
Atrial fibrillation is characterized by continuous and irregular
Atrial flutter is identified on the ECG by the characteristic activity of the ECG baseline caused by swarming electric cur-
sawtooth pattern of atrial activity at a rate of 240 to 320 beats rents in the atria and is the most common arrhythmia encoun-
per minute. Patients with normal conduction systems main- tered in clinical practice. Its prevalence increases with age;
tain 2:1 AV conduction; the ventricular rate is often close 5% of patients 65 or older are affected. Common associated
to 150 beats per minute. Higher degrees of AV block (3:1 or conditions include hypertension, cardiomyopathy, valvular
higher) in the absence of drugs that slow AV nodal conduc- heart disease (particularly mitral stenosis), sleep-disordered
tion (digoxin, -adrenergic blockers, calcium channel antago- breathing, sick sinus syndrome, Wolff-Parkinson-White
nists) suggest the presence of intrinsic AV conduction disease syndrome (especially in young patients), alcohol use (holi-
(Figure 2.12). In patients with 2:1 AV conduction and a heart day heart), and thyrotoxicosis. Atrial fibrillation should be
rate of 150 beats per minute, 1 of the flutter waves is often bur- distinguished from atrial flutter (uniform flutter waves) and
ied in the QRS complex. Carotid sinus massage (or transient multifocal atrial tachycardia (isoelectric interval between
AV node blockade with adenosine) may help reveal the flutter premature atrial contractions that have 3 or more different
waves to establish the diagnosis. morphologic forms).
Pharmacologic therapy for atrial flutter is used to slow AV
node conduction and control the ventricular rate or to con- Atrial fibrillation is the most common arrhythmia in
trol the flutter itself. The same medications used to treat atrial clinical practice; its prevalence increases with age.
fibrillation are used to treat atrial flutter. Success rates for the
control of atrial flutter are 30% to 50%. Catheter ablation has Hypertension, cardiomyopathy, valvular heart disease,
a success rate of more than 90%. A permanent pacemaker is sleep apnea, sick sinus syndrome, Wolff-Parkinson-White
needed after AV node ablation. The atria continue to flutter or syndrome, excess alcohol intake, and thyrotoxicosis are
fibrillate but symptoms are improved. commonly associated with atrial fibrillation.
I aVR V1 V4
V2
II aVL V5
III aVF V3 V6
Figure 2.12 Atrial Flutter With 3:1 Conduction. Patient had atrioventricular conduction disease.
2 . A R R H Y T H M I A S A N D SY N C O P E 21
Atrial fibrillation should be distinguished from atrial The 3 main categories of drugs used to blunt the AV node
flutter and multifocal atrial tachycardia. response in atrial fibrillation are digitalis glycosides, -blocking
agents, and calcium channel blockers. These are summarized
in Table 2.7. None of these agents prevent recurrent atrial
Therapy for Atrial Fibrillation fibrillation.
The therapeutic approach to patients with atrial fibrillation Digoxin acts indirectly by increasing vagal tone and at
is determined by the severity of symptoms and comorbid con- therapeutic concentration has no direct effect in slowing AV
ditions. Therapeutic options include rate control (pharmaco- node conduction. Because of its mechanism of action, digoxin
logic agents or ablation to slow AV node conduction), stroke is less effective than -blockers or calcium channel blockers,
prophylaxis in patients at risk of stroke, and rhythm con- particularly with exercise, when an increase in sympathetic
trol (treatment aims to restore and maintain sinus rhythm). tone results in more rapid AV node conduction. The optimal
Rhythm control is essential in patients with symptoms despite role for digoxin in atrial fibrillation is therapy for patients
adequate rate control. Symptoms associated with atrial fibril- with left ventricular dysfunction (because of the drugs posi-
lation include palpitations, shortness of breath, fatigue, chest tive inotropy) or as adjunctive therapy for patients receiving
pain, and, rarely, presyncope or syncope. Separate from rhythm -blockers or calcium channel blockers. Digoxin alone is no
evaluation, assessment of stroke risk is necessary. Several better than placebo for terminating atrial fibrillation.
risk scores are available, but the most clinically useful is the
CHADS2 scoring system (congestive heart failure, hyperten- Digoxin is less effective than -blockers or calcium channel
sion, age >75 years, diabetes, and previous stroke). Rhythm blockers for controlling ventricular rate and is best used
control is most appropriate in patients with symptoms due to as an adjunctive agent because of its inotropic effect in
atrial fibrillation. In asymptomatic patients, rate control has patients with impaired ventricular function.
mortality outcomes similar to those with rhythm control. In
all patients, initial management should be rate control using -Blockers (eg, propranolol, metoprolol, atenolol) slow
AV nodal blocking agents and an assessment of stroke risk AV node conduction and may be particularly useful when
and need for anticoagulation before deciding on a long-term atrial fibrillation complicates hyperthyroidism or myocardial
strategy. Pharmacologic agents useful for rate control and infarction. -Blockers also decrease the risk of postoperative
rhythm control are shown in Table 2.7. In patients at risk of myocardial infarction and are useful for postoperative atrial
stroke based on the CHADS2 score, the use of drug therapy fibrillation. Carvedilol decreases mortality of patients with
or ablative therapy to maintain and restore sinus rhythm may chronic heart failure. Esmolol, because of its intravenous for-
not reduce stroke risk. mulation and short half-life, is particularly useful for acute
management of atrial fibrillation.
Therapy for atrial fibrillation is based on the presence or
absence of symptoms and comorbid conditions. -Blockers slow the ventricular rate in atrial fibrillation, but
they do not terminate atrial fibrillation (although they may
Adequate rate control (with anticoagulation therapy if prevent it postoperatively).
risk of stroke is increased) has outcomes similar to those of
rhythm control.
Calcium channel blockers are divided into 2 groups: dihy-
Restoration of sinus rhythm may not reduce stroke risk. dropyridines (eg, nifedipine, amlodipine, and felodipine)
AGENTS COMMENTS
Abbreviations: AV, atrioventricular; CHF, congestive heart failure; MI, myocardial infarction.
22 C A R D I O L O GY
and nondihydropyridines (eg, diltiazem and verapamil). should be continued for a minimum of 4 weeks after car-
Dihydropyridine agents have little or no effect on AV node dioversion because of the increased risk of thromboembo-
conduction and no role in the management of atrial fibrilla- lism in the weeks after cardioversion or indefinitely in select
tion. Verapamil and diltiazem are both available as intrave- patients with other risk factors for stroke. Current guide-
nous and oral preparations and are well suited for acute and lines do not mandate anticoagulation in the setting of car-
chronic rate control. Both agents have negative inotropic dioversion for atrial fibrillation of recent onset (<48 hours).
effects and must be used cautiously in CHF. Anticoagulation guidelines for atrial flutter are identical
to those for atrial fibrillation. An alternative approach for
Diltiazem and verapamil are the only effective calcium patients with atrial fibrillation for more than 2 days is hepa-
channel blockers for rate control in atrial fibrillation. rin therapy with transesophageal echocardiography and
cardioversion if no thrombus is found followed by antico-
Adenosine has no role in the treatment of atrial fibrilla- agulation for 3 to 4 weeks.
tion but can be useful diagnostically by transiently slowing
the ventricular rate and thus permitting visualization of atrial To reduce stroke risk, patients with atrial fibrillation
activity. of >2 days should receive anticoagulation with
When pharmacologic rate control fails (due to persistent warfarin for 3 weeks before cardioversion and for 4
symptoms or intolerance of medications), catheter ablation of weeks after.
the AV junction may be considered. This approach is more
than 95% effective for controlling symptoms and carries min- An alternative approach is heparin therapy and
imal risk. The major disadvantage is creation of pacemaker transesophageal echocardiography to exclude left atrial
dependence. In patients with paroxysmal atrial fibrillation a appendage thrombus followed by anticoagulation for 34
dual-chamber pacemaker is implanted, whereas in patients weeks after cardioversion.
with persistent atrial fibrillation a single-chamber ventricu-
lar pacemaker (programmed to VVIR mode) is implanted. For chronic stroke prevention, warfarin therapy should be
Dual-chamber pacemakers have a mode-switching function used in patients with atrial fibrillation due to rheumatic val-
that permits tracking of P waves during sinus rhythm and vular disease because they have a markedly increased risk of
reverts to VVIR (or DDIR) mode pacing when atrial fibril- stroke. Most patients have nonrheumatic atrial fibrillation.
lation recurs. Warfarin decreases the incidence of thromboembolism by
close to 80% in this population. Risk of thromboembolism
Catheter ablation of the AV node should be considered can be determined using the CHADS2 score (Table 2.8). For
when pharmacologic rate control fails. patients in whom warfarin therapy is indicated, an interna-
tional normalized ratio should be maintained in the range of
Rhythm control (maintenance of sinus rhythm) controls symp- 2.0 to 3.0.
toms effectively. Common types of pharmacologic rhythm con-
trol include class IC antiarrhythmic agents (eg, propafenone Clinical risk factors for stroke in nonrheumatic atrial
and flecainide), which are good first choices and often can be fibrillation include CHF, hypertension, age >75 years,
given safely in the outpatient setting (with ECG and treadmill diabetes mellitus, and previous transient ischemic attack or
testing at 3 days to exclude proarrhythmic effect). These drugs stroke.
should be avoided in patients with structural heart disease.
Amiodarone and dofetilide (class III agents) are generally safe
in patients with prior myocardial infarction and those with
Table 2.8 RISK FACTORS FOR THROMBOEMBOLISM IN
systolic dysfunction. Other class I drugs (IA and IB) are rarely
NONRHEUMATIC ATRIAL FIBRILLATION
used.
STROKE RISK RECOMMENDED
Avoid class IC drugs in patients with structural heart CHADS2 CRITERIA POINTS SCORE THERAPY
disease.
Congestive heart 1 Low=0 Aspirin 100300
Amiodarone is generally safe in patients with a history of failure mg daily
myocardial infarction or systolic dysfunction. Hypertension 1 Moderate Warfarin or
aspirin
For acute stroke risk, electrical cardioversion from atrial Age 75 years 1
fibrillation is commonly used to control atrial fibrillation. Diabetes mellitus 1
Previous stroke or TIA 2 High=26 Warfarin (INR 23)
Patients with atrial fibrillation lasting more than 2 days
should receive anticoagulation before cardioversion. Three
Abbreviations: INR, international normalized ratio; TIA, transient ischemic
weeks of warfarin therapy before cardioversion substan- attack.
tially decreases the incidence of cardioversion-associated
Data from Gage BF, Waterman AD, Shannon W, Boechler M, Rich MW, Radford
thromboembolism to 0% to 1.6% (compared with up to MJ. Validation of clinical classification schemes for predicting stroke: results from the
7% in the absence of anticoagulation). Anticoagulation National Registry of Atrial Fibrillation. JAMA. 2001 Jun 13;285(22):286470.
2 . A R R H Y T H M I A S A N D SY N C O P E 23
Echocardiographic risk factors for stroke are depressed -Blockers or calcium channel blockers may be useful in
ventricular function and left atrial enlargement. patients with PSVT and comorbid conditions such as
hypertension.
Patients <60 years of age with structurally normal
hearts and no history of hypertension are at low risk for
Multifocal atrial tachycardia is an automatic atrial rhythm
thromboembolism and require no specific therapy other
diagnosed when 3 or more distinct atrial foci (P waves of differ-
than aspirin.
ent morphology) are present and the rate exceeds 100 beats per
There is no difference in stroke risk between paroxysmal minute (Figure 2.14). This rhythm occurs primarily in patients
and chronic atrial fibrillation. with decompensated lung disease and associated hypoxia,
increased catecholamines (exogenous and endogenous), atrial
Warfarin substantially decreases the risk of
stretch, and local tissue acid-base and electrolyte disturbances.
thromboembolism in patients with atrial fibrillation.
Digoxin worsens multifocal atrial tachycardia (shortens atrial
refractoriness). Multifocal atrial tachycardia is best treated
with calcium channel blockers and correction of the underly-
Other Supraventricular Tachycardias ing medical illnesses, including increasing oxygenation.
Tachycardia (rate >100 beats per minute) should be character- Multifocal atrial tachycardia is diagnosed when 3 or more
ized as a narrow complex or a wide complex tachycardia. distinct atrial foci are present and the heart rate exceeds
100 beats per minute. The P waves all have a different
Paroxysmal Supraventricular Tachycardia
morphology.
Paroxysmal supraventricular tachycardia (PSVT) is due
to a reentrant mechanism with an abrupt onset and termina- Multifocal atrial tachycardia is best treated with
tion, a regular rate, and a narrow QRS complex (Figure 2.13), nondihydropyridine calcium channel blockers and
unless there is a rate-related or preexisting bundle branch treatment of underlying medical conditions.
block. Acutely, PSVT responds to vagal maneuvers; adenosine
(or verapamil if PSVT is recurrent) terminates the arrhythmia
in 90% of patients. PSVT generally is not a life-threatening Differentiating Supraventricular Tachycardia With
arrhythmia; it often occurs in an otherwise normal heart. It Aberrancy From Ventricular Tachycardia
is more serious and can lead to cardiac decompensation when Wide QRS tachycardia may be due to supraventricu-
it is associated with underlying heart disease. The preferred lar tachycardia with aberrancy or to ventricular tachycar-
method for management of symptomatic PSVT is cath- dia (Figure 2.15). Findings useful for identifying ventricular
eter ablation, which has success rates of more than 90%. For tachycardia are listed in Box 2.2.
patients with PSVT and other comorbidities (eg, hyperten- Wide QRS tachycardias are ventricular in origin in more
sion), in whom catheter ablation is not feasible or preferred, than 85% of cases and are often well tolerated. The absence of
-blockers or calcium channel blockers may be useful for treat- hemodynamic compromise during tachycardia does not prove
ing both conditions. the tachycardia is supraventricular in origin.
A simple approach to a wide complex tachycardia is to
Catheter ablation is preferred for management of review the morphologic features of the complex in lead V1
symptomatic PSVT; it has a high success rate. and decide whether the pattern is that of right or left bundle
24 C A R D I O L O GY
Figure 2.14 Multifocal Atrial Tachycardia. Simultaneous recordings show 3 or more P waves of different morphology. (Lower tracing, adapted from
MKSAP IX: Part C, Book 1, c1992. American College of Physicians. Used with permission.)
I aVR V1 V4
II aVL V2 V5
III aVF V3 V6
Figure 2.15 Ventricular Tachycardia With a Wide QRS Complex, Northwest Axis, and Fusion Complexes. Patient had normal blood pressure.
2 . A R R H Y T H M I A S A N D SY N C O P E 25
Box 2.2 FINDINGS THAT IDENTIFY VENTRICULAR
TACHYCARDIA
Evidence of AV dissociation with P waves marching through the
QRS complexes
A QRS width >0.14 s if the tachycardia has a right bundle branch
block pattern & >0.16 s if the tachycardia has a left bundle branch
block pattern
Northwest axis (axis between 90 & 180)
A different QRS morphology in patients with a preexisting bundle
branch block
A history of structural heart disease
26 C A R D I O L O GY
Ventricular Ectopy and Nonsustained Ventricular
Tachycardia
Management of frequent ventricular ectopy and nonsustained
ventricular tachycardia is based on the underlying cardiac
lesion. In symptomatic patients, management includes reas-
surance, -blockers or calcium channel blockers for disturb-
ing symptoms, and, in rare cases of frequent monomorphic
symptomatic ventricular ectopy, catheter ablation. Patients
with a structurally normal heart and complex ectopy or non-
sustained ventricular tachycardia have an excellent prognosis.
Management includes reassurance or, if bothersome symp-
toms persist, calcium channel blockers or -blockers.
2 . A R R H Y T H M I A S A N D SY N C O P E 27
Drug therapy has no demonstrated benefit. Progressive ventricular dysfunction may result from
persistent atrial fibrillation with a rapid ventricular rate.
Survival outcomes are improved with ICD therapy.
This condition is often reversible because control of the
ventricular rate leads to improved ventricular function.
Torsades de Pointes
Torsades de pointes is a form of ventricular tachycardia with a
Ventricular Arrhythmias During Acute Myocardial
characteristic polymorphic morphologic pattern described as
Infarction
a twisting of the points (torsades de pointes) (Figure 2.20).
It is related to ventricular fibrillation and occurs in the Prevention of myocardial ischemia and the use of -blockers
setting of QT interval prolongation and acute myocardial are essential during and after acute myocardial infarction
ischemia or infarction. Common causes include medications to decrease the frequency of life-threatening ventricular
that prolong the QT interval (eg, quinidine, procainamide, arrhythmias. Asymptomatic complex ventricular ectopy,
disopyramide, sotalol, and tricyclic antidepressants), electro- including nonsustained ventricular tachycardia, should
lyte disturbance (hypokalemia), or bradycardia (especially not be treated empirically with lidocaine or amiodarone
after myocardial infarction). Acute treatment options include in the acute phase because the risk of proarrhythmia out-
temporary overdrive pacing (if due to bradycardia) and cor- weighs the potential benefit of therapy for reducing the
rection of electrolyte abnormality. QT interval prolongation incidence of sudden cardiac death after hospital dismissal.
may be due to an inherited disorder of cardiac ion channels. Ventricular tachycardia and fibrillation occurring within
Patients with this abnormality require evaluation and, in some 24 hours after myocardial infarction are independent risk
cases, implantation of a cardioverter-defibrillator. factors for in-hospital mortality but not for subsequent
total mortality or mortality due to an arrhythmic event
Torsades de pointes occurs in the setting of QT after hospital dismissal and do not require antiarrhythmic
prolongation and acute myocardial infarction or ischemia. therapy. Ventricular tachycardia and fibrillation occurring
more than 24 hours after an acute myocardial infarction
Patients with cardiac ion channel abnormalities require (without ongoing ischemia or reinfarction) are independent
evaluation and consideration of ICD implantation. risk factors for increased total mortality and death due to an
arrhythmic event after hospital dismissal. Patients may be
assessed with EP testing; treatment is usually with an ICD.
Tachycardia-Mediated Cardiomyopathy Use of a prophylactic ICD after myocardial infarction is not
supported by available data. Refractory ventricular tachy-
Persistent atrial fibrillation with a rapid ventricular rate cardia and fibrillation during acute myocardial infarction
may lead to progressive ventricular dysfunction (termed should be treated with intravenously administered lidocaine
tachycardia-mediated cardiomyopathy). It is reversible in most or amiodarone.
cases because control of the ventricular rate improves ven-
tricular function. In patients presenting with tachycardia and Life-threatening arrhythmias are reduced with use of
congestive heart failure, or found to have left ventricular dys- -blockers during and after an acute myocardial infarction.
function during evaluation, it can be difficult to determine
whether heart failure is causing tachycardia or tachycardia has Ventricular tachycardia and fibrillation occurring >24
caused the heart failure. In a patient with heart failure and a hours after an acute myocardial infarction are independent
rhythm with an abnormal P-wave axis, tachycardia-mediated risk factors for increased total mortality and death due to
cardiomyopathy should be suspected. arrhythmia after dismissal.
Figure 2.20 Torsades de Pointes in a Patient With Long QT Syndrome. (Adapted from Hammill SC. Electrocardiographic diagnoses: criteria and
definitions of abnormalities. In: Murphy JG, Lloyd MA, editors. Mayo Clinic cardiology: concise textbook. 4th ed. Rochester [MN]: Mayo Clinic
Scientific Press and New York [NY]: Oxford University Press; c2013. p. 20538. Used with permission of Mayo Foundation for Medical Education
and Research.)
28 C A R D I O L O GY
There is no evidence for the prophylactic use of an ICD Box 2.3 MAJOR CAUSES OF SYNCOPE
after myocardial infarction. CARDIOGENIC NONCARDIOGENIC
Treat refractory ventricular tachycardia and fibrillation
during acute myocardial infarction with intravenously Cardiogenic syncope Neurologic
Structural heart disease Metabolic
administered lidocaine or amiodarone. Coronary artery disease Psychiatric
Rhythm disturbances
Reflex syncope
Vasovagal
Role of Pacing in Acute Myocardial Infarction Carotid sinus hypersensitivity
Situational
Among patients with an acute inferior myocardial infarction, Micturition
5% to 10% have Mobitz I second-degree or third-degree block Deglutition
in the absence of bundle branch block. This finding usually is Defecation
transient, tends not to recur, and requires pacing only if there Glossopharyngeal neuralgia
are symptoms due to bradycardia. Bundle branch block occurs Postprandial
Tussive
in 10% to 20% of patients with an acute myocardial infarc- Valsalva maneuver
tion. The appearance of a new bundle branch block is an indi- Oculovagal
cation for prophylactic temporary pacing. Patients in whom Sneeze
transient complete heart block develops in association with a Instrumentation
bundle branch block are at risk for recurrent complete heart Diving
After exercise
block and should undergo permanent pacing. A new bundle Orthostatic hypotension
branch block that never progresses to complete heart block
is not an indication for permanent pacing. Death of patients Adapted from Shen W-K, Gersh BJ. Fainting: approach to management. In:
with myocardial infarction and bundle branch block usually Low PA, editor. Clinical autonomic disorders: evaluation and management.
is due to advanced heart failure, not complete heart block. 2nd ed. Philadelphia (PA): Lippincott-Raven; c1997. p. 64979. Used with
permission of Mayo Foundation for Medical Education and Research.
Second-degree (Mobitz II) block with bilateral bundle branch
block and third-degree (complete) AV block warrant pacing.
heart disease or patients with structural heart disease after
Bundle branch blocks develop in up to 20% of patients other causes of syncope have been excluded. Tilt-table test-
after acute myocardial infarction. ing is not indicated after a single episode of syncope without
Pacing is only required in the setting of symptomatic injury or in a high-risk setting with obvious vasovagal clinical
bradycardia. features.
Syncope is defined as a transient loss of consciousness with Coronary artery disease, previous Isolated syncope without
spontaneous recovery. It can be categorized as cardiogenic myocardial infarction underlying cardiovascu-
(about 30% of cases are due to bradycardia or tachycardia), Structural heart disease lar disease
noncardiogenic (about 35% vasovagal and 10%25% ortho- Left ventricular dysfunction Younger age
Congestive heart failure Symptoms consistent with a
static, situational, seizures, drug-related, for example), or Older age vasovagal cause
unknown (10%25%) (Box 2.3). Abrupt onset Normal ECG
Serious injuries
Abnormal ECG (presence of Q
EVA LUAT I O N O F S Y N C O P E wave, bundle branch block, or
atrial fibrillation)
The history and physical examination are highly valuable for
the evaluation of syncope. Risk factors for a cardiogenic cause
Abbreviation: ECG, electrocardiogram.
of syncope are listed in Box 2.4. Recommendations for evalu- a
In patients who present with a prodrome (eg, nausea, diaphoresis), a neurocar-
ation of patients with syncope are outlined in Figure 2.21. diogenic mechanism is likely. Patients who experience rapid recovery (less than
Consider EP testing in patients at increased risk for cardio- 510 minutes) rarely have a neurologic cause for syncope and are most likely to
genic syncope. EP testing is usually not indicated if an arrhyth- have syncope due to seizure or brain hypoperfusion because recovery in such
circumstances takes hours. Thus, for cases in which recovery from syncope is
mogenic cause (bradycardia or tachycardia) of syncope has rapid and no residual neurologic signs or symptoms are present, detailed (and
been established unless other arrhythmias are suspected. A expensive) neurologic evaluation should be avoided.
noninvasive approach should be considered in patients at low Adapted from Shen W-K, Gersh BJ. Fainting: approach to management. In:
risk for cardiogenic syncope. Tilt-table testing is effective in Low PA, editor. Clinical autonomic disorders: evaluation and management.
suspected vasovagal syncope. Tilt-table testing is also indi- 2nd ed. Philadelphia (PA): Lippincott-Raven; c1997. p. 64979. Used with
permission of Mayo Foundation for Medical Education and Research.
cated for patients with recurrent syncope without structural
2 . A R R H Y T H M I A S A N D SY N C O P E 29
History, physical,
ECG echo
No
Conduction or structural
heart disease
Yes No
Suspected neuro-
EP tilt
cardiogenic syncope
Yes No
Work-up
Negative Tilt, CSM
and treat
Figure 2.21 Diagnostic Pathway for Evaluation of Syncope. AS indicates aortic stenosis; CHB, complete heart block; CSM, carotid sinus massage;
ECG, electrocardiography; echo, echocardiography; EP, electrophysiologic study; tilt, tilt-table testing; VT, ventricular tachycardia.
History and physical examination provide key information -Blockers and pacemakers have limited or no benefit in
needed to diagnose the cause of syncope. patients with vasovagal syncope.
Tilt-table testing is effective in patients with suspected
vasovagal syncope, recurrent syncope without structural
heart disease, or structural heart disease in whom other S U M M A RY
causes of syncope have been excluded.
Reentry is the most common mechanism of cardiac
arrhythmias.
M A NAG E M E N T O F S Y N C O P E
Ambulatory ECG monitoring allows evaluation of
Pacemaker therapy is appropriate for sinus node dysfunction rhythm disturbances and their relationship with daily
and AV conduction disease. Management of recurrent neu- activities.
rocardiogenic syncope (vasovagal syncope) includes educa-
tion about the mechanism and triggering factors, instruction Syncope suggestive of a cardiogenic mechanism and
regarding appropriate action (eg, sitting or lying down to avert palpitations likely due to a rhythm disorder are common
episodes), instruction regarding maintenance of increased indications for EP testing.
intravascular volume, and instruction on maneuvers to pre- Sinus node dysfunction includes sinus bradycardia, sinus
vent venous pooling. Midodrine, which promotes increased pause, tachycardia-bradycardia syndrome, sinus arrest, and
venous return, may be considered. Serotonin reuptake block- chronotropic incompetence.
ers may be effective in a subgroup of patients. -Blockers have
limited or no benefit. Pacemaker therapy has a limited role in Syncope is categorized as cardiogenic, noncardiogenic, or
preventing vasovagal syncope. unknown.
30 C A R D I O L O GY
3.
CARDIAC EXAMINATION, VALVULAR HEART DISEASE,
AND CONGENITAL HEART DISEASE
Kyle W. Klarich, MD
Accurate bedside assessment is essential and allows appro- Jugular venous pressure varies with respiration, is
priate, cost-effective, and efficient ordering of tests. This nonpalpable, and can be obstructed with gentle
chapter presents the salient features of the clinical cardiac pressure.
examination, cardiac imaging techniques, and the diagnosis Biventricular failure, constrictive pericarditis,
and management of valvular and congenital heart diseases. pericardial tamponade, cor pulmonale, and
superior vena cava syndrome increase jugular venous
pressure.
C A R D I AC P H YS I C A L E X A M I N AT I O N
Abnormalities of the venous waves suggest various car-
JU GU L A R VEN O US P R E S SU R E diac conditions. Increased jugular venous pressure indicates
possible fluid overload (common in congestive heart fail-
Jugular venous pressure reflects right atrial pressure and the ure). The likelihood of congestive heart failure is increased
relationship between right atrial filling and emptying into 4 times if jugular venous pressure is increased. Large a waves
the right ventricle (Figure 3.1). Changes in wave amplitude may indicate tricuspid stenosis, right ventricular hypertro-
may indicate structural disease and rhythm changes. Normal phy, pulmonary hypertension (ie, increased right ventricular
jugular venous pressure is 6 to 8 cm H2O. It is best evaluated end-diastolic pressure). Cannon a waves are due to atria con-
with the patient supine at an angle of at least 45. The right tracting intermittently against a closed atrioventricular valve
atrium lies 5 cm below the sternal angle, and thus the esti- (atrioventricular dissociation). Rapid x + y descent indicates
mated jugular venous pressure equals the height of the jugu- constrictive pericarditis. Kussmaul sign (paradoxical increase
lar venous pressure above the sternal angle + 5 cm (Figure in jugular venous pressure with inspiration) occurs in peri-
3.1). The normal venous profile contains 3 positive waves cardial tamponade, constriction, and right ventricular fail-
and 2 negative waves. Positive waves are a, atrial contraction; ure. Large, fused cv waves are due to tricuspid regurgitation.
c, closure of tricuspid valve; and v, atrial filling. Negative Increased jugular venous pressure can be associated with pul-
waves are the x descent (the downward motion of the right monary embolus, superior vena cava syndrome, tamponade,
ventricle) and the y descent (the early right ventricular filling and constrictive pericarditis.
phase). The a wave comes just before the first heart sound,
and the v wave comes during the ejection phase of the left
Venous wave abnormalities can help identify the
ventricle.
underlying cardiac condition.
The examiner must distinguish jugular venous pressure
from carotid pulsations: jugular venous pressure varies with Increased jugular venous pressure can be associated
respiration, is nonpalpable, and can be eliminated by apply- with pulmonary embolus, superior vena cava syndrome,
ing gentle pressure at descent (diastole). When the pressure tamponade, and constrictive pericarditis.
31
3 cm (from sternal notch) QRS
+ 5 cm (from right ventricle to sternal notch)
8 cm H2O jugular venous pressure T
P
ECG
a
x a
c
Normal v
x
JVP waveform y
Heart tones S1 S2
Top level of
venous pulsation
3 cm Severe TR
5 cm Moderate TR
JVP Mild TR
with TR
Normal (no TR)
ECG
Heart tones S1 S2
Figure 3.1 Evaluation of Jugular Venous Pressure ( JVP). ECG indicates electrocardiogram; S1, first heart sound; S2, second heart sound; TR, tricuspid
regurgitation.
32 C A R D I O L O GY
4. Hyperdynamic, descended, and enlarged with rapid filling
wave: mitral regurgitation, aortic regurgitation
AV closes
5. Tapping quality, localized, nondisplaced: normal but may 120
indicate mitral stenosis AV opens
Aorta pressure
75
Pressure, mm Hg
A D D I T I O NA L C A R D I AC PA L PAT I O N
A palpable aortic valve component (A2) at the right upper MV opens
MV closes
sternum suggests a dilated aorta (eg, aneurysm, dissection, v
severe aortic regurgitation, poststenotic dilatation in aor- Left atrial a c x y
tic stenosis, hypertension). Severe tricuspid regurgitation pressure
10
may cause a pulsatile liver palpable in the right epigastrium. 0
Left ventricular
pressure
Hepatojugular reflux (distention of the external jugular vein S1 S2(A2P2)
3 or 4 beats after compression of the liver) may also occur.
The apical impulse rotates medially and may be appreciated Time
in the epigastrium (which can be confused with a pulsatile
liver) in patients with severe emphysema. Right ventricular Figure 3.2 The Normal Cardiac Cycle. A2 indicates the aortic valve
hypertrophy results in sustained lift, best appreciated in the component of S2; AV, aortic valve; MV, mitral valve; P2, pulmonary valve
fourth intercostal space along the left parasternal border. component of S2; S1, first heart sound; S2, second heart sound.
Diastolic overload (eg, atrial septal defect, anomalous pul-
monary venous return) results in a vigorous outward and semilunar valves, creating the second heart sound (S2).
upward motion but may not be sustained. The pulmonary Another period follows when both sets of valves are closed.
valve component (P2) may be palpable in the second right Pressure decreases below the left atrial pressure, leading to
intercostal space in marked pulmonary hypertension. This the usually silent opening of the atrioventricular valves.
may be physiologic in slender people with a small anteropos- Early rapid filling followed by slow filling of the ventri-
terior diameter. cles is followed by atrial contraction. The mnemonic for
valve sequenceS1-S2 (right ventricular-left ventricular
Pressure overload of the right ventricle usually results in sequenceis Many Things Are Possible [MTAP]: S1 =
sustained lift of the sternum and a palpable pulmonary mitral opens before tricuspid; S2 = aortic closes before pul-
closure. monary) under normal conditions.
Volume overload (eg, regurgitant lesions, atrial septal
defect) usually is appreciated as dynamic and forceful but S1: closure of the atrioventricular valves due to
not sustained impulses. increased left ventricular pressure after atrial
contraction.
THRILLS
Thrills indicate marked turbulent flow (eg, aortic stenosis, First Heart Sound
severe mitral regurgitation, and ventricular septal defect) and
S1 consists of audible mitral valve closure followed by tri-
distinction of a grade 4 murmur.
cuspid valve closure. A loud S1 occurs with mitral stenosis
and short PR intervals (the mitral valve is open when the
left ventricle begins to contract and then slaps shut). S1 also
H E A RT S O U N D S is augmented in hypercontractile states (eg, fever, exercise,
thyrotoxicosis, pheochromocytomas, anxiety, and anemia).
Knowledge of how the heart sounds are related to the car- Conversely, S1 is decreased if the mitral valve is heavily calci-
diac cycle allows an understanding of cardiac auscultation fied and immobile (severe mitral stenosis) and with a long
(Figure 3.2). The cardiac cycle starts with atrial contrac- PR interval, poor left ventricular function, and rapid dia-
tion; this increases ventricular pressure just before closure stolic filling (due to premature mitral valve closure) as in
of the atrioventricular valves, which generates the first aortic regurgitation.
heart sound (S1). There is a period of time while the left
ventricle generates pressure, known as the isovolumic con-
S1 is loud with a short PR interval, mitral stenosis, and
traction time, when the atrioventricular and semilunar
hypercontractile states.
valves are closed. Normally silent semilunar valve open-
ings then occur, followed by blood ejection from the left S1 is quiet with a heavily calcified mitral valve, long
ventricle to the aorta (creating the pulse). As the ventricle PR interval, left ventricular dysfunction, and aortic
relaxes, aortic pressure decreases; this decrease closes the regurgitation.
3. C A R D I AC E X A M I N AT I O N, VA LV U L A R H E A RT D I S E A S E , A N D C O N G E N I TA L H E A RT D I S E A S E 33
AP A P A P P A regurgitation, mitral regurgitation, and cardiomyopathy). It is
Expiration
a normal variant in very fit young adults.
34 C A R D I O L O GY
Cardiac murmur
No further work-up
Figure 3.4 Recommendations for Evaluating Heart Murmurs. *If electrocardiography or chest radiography has been performed and the results are
abnormal, echocardiography is recommended. (Adapted from Bonow RO, Carabello BA, Chatterjee K, de Leon AC Jr, Faxon DP, Freed MD, et al;
American College of Cardiology/American Heart Association Task Force on Practice Guidelines. 2008 Focused update incorporated into the ACC/
AHA 2006 guidelines for the management of patients with valvular heart disease: a report of the American College of Cardiology/American Heart
Association Task Force on Practice Guidelines [Writing Committee to revise the 1998 guidelines for the management of patients with valvular heart
disease]. Endorsed by the Society of Cardiovascular Anesthesiologists, Society for Cardiovascular Angiography and Interventions, and Society of
Thoracic Surgeons. J Am Coll Cardiol. 2008 Sep 23;52[13]:e1142 and Bonow RO, Carabello BA, Chatterjee K, de Leon AC Jr, Faxon DP, Freed
MD, et al; 2006 Writing Committee Members; American College of Cardiology/American Heart Association Task Force. 2008 Focused update
incorporated into the ACC/AHA 2006 guidelines for the management of patients with valvular heart disease: a report of the American College of
Cardiology/American Heart Association Task Force on Practice Guidelines [Writing Committee to Revise the 1998 Guidelines for the Management
of Patients With Valvular Heart Disease]: endorsed by the Society of Cardiovascular Anesthesiologists, Society for Cardiovascular Angiography and
Interventions, and Society of Thoracic Surgeons. Circulation. 2008 Oct 7;118[15]:e523661. Epub 2008 Sep 26. Used with permission.)
and tricuspid and pulmonary regurgitation). The Valsalva to hypertrophic cardiomyopathy. The effects of maneuvers are
maneuver increases intrathoracic pressure, inhibiting venous shown in Table 3.1.
return and thus decreasing preload. Most cardiac murmurs
and sounds diminish in intensity during the Valsalva maneu- Bedside maneuvers that alter cardiac murmurs are as
ver because of decreased ventricular filling and cardiac output. follows:
The exception is hypertrophic obstructive cardiomyopathy, in
which the murmur increases because of dynamic left ventricu- Inspiration
lar outflow obstruction accentuated by decreased preload. The Valsalva maneuver
Valsalva maneuver is the classic way to distinguish between
the murmurs of aortic stenosis and hypertrophic cardiomyo- Handgrip
pathy. Handgrip increases cardiac output and systemic arterial Change in posture
pressure, decreasing the gradient across a stenotic aortic valve.
A change in posture from supine to upright causes decreased Squatting
venous return, reducing stroke volume and thus a reflex Inhalation of amyl nitrite
increase in heart rate and peripheral resistance. Squatting and
the Valsalva maneuver have opposite hemodynamic effects. The Valsalva maneuver distinguishes between aortic
Squatting increases peripheral resistance and venous return. stenosis and hypertrophic cardiomyopathy.
Amyl nitrite pharmacologically decreases afterload. The
amyl nitrite is inhaled and transiently lowers blood pressure, I M AG I N G I N C A R D I O L O GY
increasing the murmurs of hypertrophic cardiomyopathy and
aortic stenosis. Its main use is to determine the gradient in Appropriate choice of an imaging method aids in the diag-
patients with dynamic left ventricular outflow obstruction due nosis, quantification, and prognosis of various diseases.
3. C A R D I AC E X A M I N AT I O N, VA LV U L A R H E A RT D I S E A S E , A N D C O N G E N I TA L H E A RT D I S E A S E 35
Table 3.1 EFFECTS OF PHYSICAL MANEUVERS AND OTHER FACTORS ON VALVULAR DISEASES
MITRAL
MANEUVER OR FACTOR RESULT REGURGITATION MVP AORTIC STENOSIS HOCM
Valsalva p preload p n p n
Post-PVC n contractility = p n na
p afterload
Abbreviations: HOCM, hypertrophic obstructive cardiomyopathy; MVP, mitral valve prolapse; PVC, premature ventricular complex.
a
Although the murmur increases, the peripheral pulse decreases because of the increase in outflow obstruction.
Left ventricular function is the most commonly ordered end-systole and thus stroke volume, ejection fraction, cardiac
assessment. Various techniques are available, as outlined in output, and muscle mass can be determined. Echocardiography
Table 3.2. Focused clinical questioning allows selection of the is noninvasive, lending itself to serial image acquisition. It is
most appropriate technique. easily available and the most widely used imaging technology
in cardiology.
Regional wall motion abnormalities are identified by
Coronary Angiography
assessing endocardial motion and wall thickening. Valve mor-
This was the first imaging method to permit visualization of phology (eg, pliability, degree of calcification, morphologic
the cardiac chambers and direct assessment of left ventricular abnormalities, and flail segments) and intracardial and peri-
size and function. It is an invasive technique. Risks include the cardial structures can be analyzed. With exercise or pharma-
use of ionizing radiation, iodine allergy, and impaired renal cologic (usually dobutamine) stress, regional wall motion can
function. Coronary angiography is considered the standard be assessed at rest and with stress.
technique to assess the location and extent or quantity of cor- The use of Doppler with echocardiography allows direct
onary artery stenosis. Left ventricular function assessment by measurements of blood velocities across valves and conduits
contrast ventriculography can be performed during coronary (eg, left ventricular outflow tract and vessels), permitting cal-
angiography. culation of stroke volume, cardiac output, valve gradients, and
severity of regurgitant lesions and semiquantitation of intra-
cardiac and extracardiac shunts. Obesity, severe cachexia, and
Echocardiography
extensive lung disease (eg, smoking-related disorders, chronic
Echocardiography generates images and gives temporal-spatial obstructive pulmonary disease, and restrictive lung disease)
resolution for timing the motion of heart structures during reduce the ability to obtain adequate images in transthoracic
the cardiac cycle. Left ventricular volumes in end-diastole and echocardiography in a small percentage of cases.
VARIABLE ASSESSED
COST-
METHOD LVEF RV Function LV Mass RWMA EFFECTIVENESS a
Electron beam computed tomography Yes Yes, quantitativec Yes Yes +++
Abbreviations: LV, left ventricular; LVEF, left ventricular ejection fraction; RNA, radionuclide angiography; RV, right ventricular;
RWMA, regional wall motion abnormalities.
a
+, Least expensive; ++++, most expensive.
b
If performed without coronary angiography.
c
Quantitative, absolute measurements of global ventricular volumes possible to facilitate measure of RV ejection fraction.
36 C A R D I O L O GY
Transesophageal echocardiography minimizes the interfer-
ence of bones, muscle, and obesity, but it requires sedation and
the most operator experience and is more operator-dependent.
Echocardiography cannot visualize the coronary arteries like
angiography.
Contrast echocardiography enhances the echocardio-
graphic signal using an enhancing agent. Some of these agents
are smaller than red blood cells and cross the pulmonary vas-
cular bed. Clinical applications include better endocardium
visualization.
Radionuclide Imaging
Radionuclide imaging uses 2 techniques: labeling erythrocytes
with an isotope to assess endocardial motion or using perfu-
sion tracers (thallium, sestamibi) to assess differences between
resting and stress blood flow.
Radionuclide Angiography Figure 3.5 Myocardial Perfusion Image for a Patient With Exertional
Erythrocytes are labeled with technetium, and images are Angina (Class III) of Recent Onset. Low-level exercise with 1-mm
acquired over multiple cardiac cycles. This imaging technique ST-segment depression at 2 minutes into exercise. The left column
depicts the stress images with a representative short-axis tomogram
is not suitable for patients with atrial fibrillation and mark- (upper left panel) and the horizontal long axis (lower left panel). In
edly variable RR intervals. Left ventricular function can be the right column are the rest images, with corresponding short-axis
quantified very accurately. Excellent discrimination between tomogram in the right upper panel and the corresponding horizontal
low ejection fractions, particularly during serial assessment, long-axis tomogram in the right lower panel. Note the severely reduced
is possible. In contrast, echocardiography is less accurate for uptake in the apical, septal, anterior, and inferior segments (arrows). At
rest, there is nearly complete normalization in all segments. Subsequent
quantification of left ventricular function in severely dysfunc- angiography indicated complete occlusion of the right coronary artery
tional ventricles. and 80% stenosis in the proximal left anterior descending coronary artery.
The circumflex coronary artery did not show a critical lesion.
Myocardial Perfusion Imaging
Thallium and sestamibi are the most commonly used
isotopes. They distribute to the myocardium according to size, function, and muscle mass and of cardiac chamber size.
blood flow and are avidly taken up by myocytes. Imaging can It can assess anatomical structure, distinguish viable myocar-
be performed at rest and after exercise (Figure 3.5). During dium from scarred myocardium, and characterize tissue. It can
stress (exercise or pharmacologic), uptake is usually reduced differentiate plaque composition and may be able to identify
(hypoperfusion) in damaged myocardium. At rest, thallium vulnerable plaques.
redistributes and there is preferential washout of the normal
myocardium and preferential uptake of the hypoperfused myo- Electron Beam Computed Tomography
cardium. Sestamibi is irreversibly taken up by the myocardium
and a repeat resting injection is needed to show resting flow con- Electron beam computed tomography allows high-fidelity,
ditions. The extent and severity of the perfusion defect provide high-resolution, 3-dimensional images of the entire heart. It
information about the disease prognosis. It is also used to assess requires only 1 heartbeat to complete a scan cycle. It is ideally
residual ischemia after a myocardial infarction and to assess suited for serial studies in left ventricular remodeling because
therapeutic efficacy in patients treated medically or by inter- of its high precision and accuracy. Drawbacks are the require-
vention. Imaging study results should be viewed along with the ments for a contrast agent and use of ionizing radiation. It is
data available from the exercise or stress electrocardiogram. currently the most widely used technique in the field of early
detection of coronary atherosclerosis because of its ease of
Gated Sestamibi Imaging application (rapid acquisition time, no contrast agent) and
With this technique, myocardium motion is imaged standardization. It detects coronary calcium, a component of
throughout the cardiac cycle, allowing regional wall motion coronary plaque.
analysis similar to that of echocardiography. Post-stress images
are acquired with a considerable time delay and mainly reflect
resting contractility. Positron Emission Tomography
Positron emission tomography allows high-spatial and tempo-
ral resolution imaging and currently is the reference standard
Magnetic Resonance Imaging for the assessment of myocardial viability. However, the com-
Magnetic resonance imaging is a noninvasive, 3-dimensional plexity of the technology and the cost currently limit its use to
imaging technique that allows assessment of left ventricular tertiary academic centers.
3. C A R D I AC E X A M I N AT I O N, VA LV U L A R H E A RT D I S E A S E , A N D C O N G E N I TA L H E A RT D I S E A S E 37
VA LV U L A R H E A RT D I S E A S E When calcification is extensive, A2 becomes inaudible.
60
extensive, A2 becomes inaudible. Progression Angina
015 mm Hg/y
40
Congenital bicuspid valvular aortic stenosis occurs in 2% 0.12 cm2/y
of the population, affects males more than females, and is Symptoms CHF
20 Syncope
the most common cause of aortic stenosis in adults younger Sudden death (<5%)
than 55 years.
0
Bicuspid aortic valve is associated with ascending aortic 0 1 2 3 4 5 6 7 8
aortopathy that can lead to aneurysm formation. Screening Years
of relatives is important.
Figure 3.6 Natural History of Aortic Stenosis (AS). CHF indicates
Degenerative aortic valve disease is the most common congestive heart failure. (Adapted from Ross J Jr, Braunwald E. Aortic
cause of aortic stenosis in adults older than 55 years. stenosis. Circulation. 1968 Jul 1;38 Suppl 1:617. Used with permission.)
38 C A R D I O L O GY
of the aortic cusps. The ejection systolic murmur becomes effective treatment for patients with severe obstruction (Figure
louder and peaks later with increasing severity, radiating to the 3.7).
carotid arteries and the apex.
Aortic stenosis can be diagnosed with bedside physical
The pulse is parvus (minimal) and tardus (delayed) in examination.
hemodynamically significant aortic stenosis.
The most important physical finding is observation of
The ejection systolic murmur becomes louder with parvus and tardus pulse contour.
increasing severity.
Dyspnea, chest pain, angina, syncope, or newly diagnosed
A2 is diminished, delayed, or absent with progressive aortic congestive heart failure may herald progression to severe
stenosis. aortic stenosis.
Aortic valve replacement is the only effective treatment of
Diagnosis symptomatic aortic stenosis.
Electrocardiography in aortic stenosis may show left ven-
tricular hypertrophy; echocardiography is more sensitive and AO RT I C R E GU RG I TAT I O N
specific. Left bundle branch block is common; in later stages The pathophysiology of aortic regurgitation is that of volume
of the condition, conduction abnormalities may develop (eg, and pressure overload on the left ventricle, leading to hypertro-
complete heart block) if calcium impinges on the conducting phy and dilatation. It can be related to either the aortic valve
system. On chest radiography, the heart size is usually normal or the aortic root, and the condition can be acute or chronic
even when the stenosis is severe and the left ventricle fails; (Table 3.4). Acute aortic regurgitation may be associated with
enlargement of the heart may not be evident until left ventric- an aortic dissection.
ular remodeling occurs in the late stages. The aortic root may
show poststenotic dilatation, now recognized as an aortopa- Valvular
thy. In degenerative aortic valve disease, calcium may be seen
in the valve leaflets and in the intervalvular fibrosa, especially Causes of valvular aortic regurgitation include 1) congenital
on a lateral view. bicuspid valve, 2) rheumatic fever, 3) endocarditis, 4) degen-
erative aortic valve disease, 5) seronegative arthritis, 6) ankylo-
Echocardiography is the best way to diagnose aortic sing spondylitis, and 7) rheumatoid arthritis.
stenosis and assess its severity.
Aortic Root Dilatation
The differential diagnosis of aortic stenosis includes 1)
hypertrophic cardiomyopathy (note different carotid upstroke Various conditions have been associated with aortic root
and change in murmur with Valsalva maneuver) and 2) mitral dilatation. Advancing age is one factor; hypertension acceler-
regurgitation (murmur may radiate anteriorly and upward along ates this process. Aortic regurgitation associated with age or
the aorta, particularly if there is rupture of chordae of the poste- hypertension is common and usually mild. Marfan syndrome
rior mitral valve leaflet; no radiation to the carotid arteries). may cause progressive dilatation of the aortic root and sinuses
Aortic stenosis can be diagnosed with bedside physical exam- (cystic medial necrosis). Prophylactic -adrenergic blocker
ination. The most important physical finding is the parvus and therapy slows the rate of aortic dilatation and reduces the
tardus pulse contour. The degree of aortic stenosis can be dif- development of aortic complications in some patients with
ficult to determine, particularly in older patients. Noninvasive Marfan syndrome. When the aortic root reaches 5 to 5.5 cm or
Doppler echocardiography is useful for assessing aortic valve area more in diameter, it should be replaced. Syphilis is an uncom-
and gradients and correlates well with invasive catheter-based mon cause of aortic regurgitation and usually causes aortic
assessment of the same. Severe aortic stenosis is present when root dilatation above the sinuses, sparing the sinuses. Syphilis
the mean Doppler gradient is more than 40 mm Hg, the valve is associated with aortic root calcium on chest radiography.
area is less than 1.0 cm2, and the valve index is 0.6 cm2/m2 or less.
Progression of aortic stenosis is highly variable; on average, it is Marfan syndrome can be associated with aortic root
about 0.12 cm2 per year. Progression to symptoms can be insidi- dilatation.
ous; the onset of clinical symptoms is an ominous prognostic Hypertension and advancing age are common causes of
sign. Survival after symptom onset is 1 to 3 years (Figure 3.6). aortic regurgitation (usually mild).
Treatment Symptoms
All patients should be educated about worrisome symptoms The symptoms of acute aortic regurgitation are extreme: pul-
that may develop. Dyspnea, chest pain, angina, syncope, or monary edema, shock, and, often, chest pain (in the setting of
newly diagnosed congestive heart failure are important clini- aortic dissection). The symptoms of chronic aortic regurgita-
cal evidence for surgical intervention and should be promptly tion can develop insidiously because of compensatory mecha-
evaluated (Table 3.3). Aortic valve replacement is the only nisms of the heart. The most common symptoms of severe
3. C A R D I AC E X A M I N AT I O N, VA LV U L A R H E A RT D I S E A S E , A N D C O N G E N I TA L H E A RT D I S E A S E 39
Table 3.3 QUANTITATION OF THE SEVERITY OF AORTIC STENOSIS AND TREATMENT
GUIDELINES
aortic regurgitation include fatigue, dyspnea, palpitations, and Echocardiography is best suited to gather the important func-
exertional angina. tional and hemodynamic data needed to make management
decisions in patients with aortic regurgitation.
Physical Examination Because chronic aortic regurgitation has a long, silent,
well-compensated natural history, left ventricular size, aortic
Severe aortic regurgitation is associated with physical findings root size and morphology, valve morphology, and left ven-
that include a bounding, rapidly collapsing Corrigan pulse tricular function (ejection fraction) should be followed with
resulting from wide pulse pressure; bisferiens pulse (may be echocardiography.
present); de Musset head nodding; Duroziez sign (systolic Chest radiography shows an enlarged cardiac shadow and
and diastolic [to-and-fro] murmur on gentle compression prominence of the left ventricle in a leftward and inferior pat-
with stethoscope) over the femoral artery; and Quincke sign tern. The aorta also may be enlarged, especially in Marfan syn-
(pulsatile capillary nail bed). Mller sign (systolic pulsations drome. Table 3.5 outlines the natural history of severe aortic
of the uvula) is often noted. The left ventricular impulse is dif- regurgitation.
fuse and hyperdynamic. The apical impulse is often displaced
downward. A diastolic decrescendo murmur is heard at either Findings indicative of aortic regurgitation are a bounding,
the left or the right sternal border, and the S2 may be paradoxi- rapidly collapsing Corrigan pulse, diastolic decrescendo
cally split because of increased left ventricular volume. murmur, and an S2 that may be paradoxically split.
Murmur duration is related to the rate of pressure equili-
bration between the aorta and the left ventricle. Aortic In aortic regurgitation, electrocardiography may show left
regurgitation with physiologic diastolic pressures results in ventricular hypertrophy.
a holodiastolic murmur. The shorter the aortic regurgita- Echocardiography is useful to confirm the diagnosis and
tion murmur, the faster the pressure equilibration, thus the guide therapy.
more severe the aortic regurgitation (higher left ventricular
end-diastolic pressure). The loudness of the murmur does
not correlate with the severity of aortic regurgitation, par- Treatment
ticularly in acute aortic regurgitation (such as with dissec-
tion). A systolic flow murmur is common, because of the Acute severe aortic regurgitation is a surgical emergency. If
increased ejection volume. It does not necessarily indicate untreated, severe pulmonary congestion, arrhythmias, and
aortic stenosis. circulatory collapse will develop. As a bridge to operation,
nitroprusside to reduce peripheral resistance and encourage
forward flow or inotropic agents to augment cardiac output
Diagnosis
may be considered. An intra-aortic balloon pump is contrain-
Acute aortic regurgitation may not be identified on bedside dicated because it will worsen regurgitation.
examination if a patient presents with little or no murmur.
Electrocardiography often shows left ventricular hypertrophy. Acute aortic regurgitation is a surgical emergency.
40 C A R D I O L O GY
Severe Aortic Stenosis
Vmax >4 m/s
AVA <1.0 cm2
Mean gradient >40 mm Hg
Symptoms?
Yes Equivocal No
Normal
Exercise test LV ejection fraction
Symptoms
BP
Less than 50% Normal
Figure 3.7 Management Strategy for Patients With Severe Aortic Stenosis. Preoperative coronary angiography should be performed routinely as
determined by age, symptoms, and coronary risk factors. Cardiac catheterization and angiography may also be helpful when there is discordance
between clinical findings and those on electrocardiography. AVA indicates aortic valve area; BP, blood pressure; CABG, coronary artery bypass graft
surgery; echo, echocardiography; LV, left ventricular; Vmax, maximal velocity across aortic valve by Doppler echocardiography. (Adapted from Bonow
RO, Carabello BA, Chatterjee K, de Leon AC Jr, Faxon DP, Freed MD, et al; American College of Cardiology/American Heart Association Task
Force on Practice Guidelines. 2008 focused update incorporated into the ACC/AHA 2006 guidelines for the management of patients with valvular
heart disease: a report of the American College of Cardiology/American Heart Association Task Force on Practice Guidelines [Writing Committee
to revise the 1998 guidelines for the management of patients with valvular heart disease]. Endorsed by the Society of Cardiovascular Anesthesiologists,
Society for Cardiovascular Angiography and Interventions, and Society of Thoracic Surgeons. J Am Coll Cardiol. 2008 Sep 23;52[13]:e1142 and
Bonow RO, Carabello BA, Chatterjee K, de Leon AC Jr, Faxon DP, Freed MD, et al; 2006 Writing Committee Members; American College of
Cardiology/American Heart Association Task Force. 2008 Focused update incorporated into the ACC/AHA 2006 guidelines for the management of
patients with valvular heart disease: a report of the American College of Cardiology/American Heart Association Task Force on Practice Guidelines
[Writing Committee to Revise the 1998 Guidelines for the Management of Patients With Valvular Heart Disease]: endorsed by the Society of
Cardiovascular Anesthesiologists, Society for Cardiovascular Angiography and Interventions, and Society of Thoracic Surgeons. Circulation. 2008
Oct 7;118[15]:e523661. Epub 2008 Sep 26. Used with permission.)
Chronic aortic regurgitation is a combined volume and Asymptomatic left ventricular dysfunction may develop
pressure overload on the left ventricle. The left ventricle com- in a subset of patients. Several factors have been suggested to
pensates by dilating and increasing compliance. Patients with prompt surgical intervention before left ventricular dysfunc-
aortic regurgitation may remain asymptomatic for decades. tion develops: an end-systolic dimension more than 55 mm, an
The development of symptoms usually reflects left ventricular end-diastolic dimension more than 75 mm, or an ejection frac-
dysfunction, and survival is limited (10% annual mortality) tion of 50% or less (Figure 3.8). Asymptomatic patients with
unless surgical intervention is prompt. Medical management a dilated left ventricle must be followed carefully. Evidence of
(eg, angiotensin-converting enzyme inhibitor or nifedipine) left ventricular systolic dysfunction at rest, progressive diastolic
slows ventricular dilatation in patients with severe aortic regur- dysfunction, or rapidly progressive left ventricular dilatation
gitation and may help delay operation. Compensation is not should prompt surgical treatment. The ability to repair (rather
maintained indefinitely, and eventually left ventricular filling than replace) the valve may favor earlier operation (before left
pressure increases, coronary flow reserve diminishes, and left ventricular dilatation has occurred).
ventricular dysfunction develops insidiously. Angina, even in
the absence of epicardial coronary stenosis, may be present as Asymptomatic patients with a dilated left ventricle should
a result of supply-and-demand mismatch. be carefully followed for progression.
3. C A R D I AC E X A M I N AT I O N, VA LV U L A R H E A RT D I S E A S E , A N D C O N G E N I TA L H E A RT D I S E A S E 41
Table 3.4 AORTIC REGURGITATION: SYMPTOMS AND If ejection fraction decreases below normal, operation is
FINDINGS ON EXAMINATION indicated.
ACUTE CHRONIC
42 C A R D I O L O GY
Chronic Severe Aortic Regurgitation
Reevaluation
Clinical evaluation + Echo
Symptoms?
No Yes
Equivocal
Class I
Exercise test
Symptoms Class I AVR
No symptoms
LV function?
Class I
RVG or MRI
Class IIa
LV SD >55 mm or
dimensions? DD >75 mm
Class IIb
SD <45 mm or SD 4550 mm or SD 5055 mm or
DD <60 mm DD 6070 mm DD 7075 mm Abnormal
Consider
Stable? Stable? Stable? hemodynamic
response to exercise
Yes No, or initial study Yes No, or initial study Yes Normal
Figure 3.8 Management Strategy for Patients With Chronic Severe Aortic Regurgitation. Preoperative coronary angiography should be performed
routinely as determined by age, symptoms, and coronary risk factors. Cardiac catheterization and angiography may also be helpful when there is
discordance between clinical findings and those on echocardiography. Stable refers to stable echocardiographic measurements. In some centers,
serial follow-up may be performed with radionuclide ventriculography (RVG) or magnetic resonance imaging (MRI) rather than echocardiography
(Echo) to assess left ventricular (LV) volume and systolic function. AVR indicates aortic valve replacement; DD, end-diastolic dimension; EF, ejection
fraction; eval, evaluation; SD, end-systolic dimension. (Adapted from Bonow RO, Carabello BA, Chatterjee K, de Leon AC Jr, Faxon DP, Freed MD,
et al; American College of Cardiology/American Heart Association Task Force on Practice Guidelines. 2008 focused update incorporated into the
ACC/AHA 2006 guidelines for the management of patients with valvular heart disease: a report of the American College of Cardiology/American
Heart Association Task Force on Practice Guidelines [Writing Committee to revise the 1998 guidelines for the management of patients with valvular
heart disease]. Endorsed by the Society of Cardiovascular Anesthesiologists, Society for Cardiovascular Angiography and Interventions, and Society
of Thoracic Surgeons. J Am Coll Cardiol. 2008 Sep 23;52[13]:e1142 and Bonow RO, Carabello BA, Chatterjee K, de Leon AC Jr, Faxon DP, Freed
MD, et al; 2006 Writing Committee Members; American College of Cardiology/American Heart Association Task Force. 2008 Focused update
incorporated into the ACC/AHA 2006 guidelines for the management of patients with valvular heart disease: a report of the American College of
Cardiology/American Heart Association Task Force on Practice Guidelines [Writing Committee to Revise the 1998 Guidelines for the Management
of Patients With Valvular Heart Disease]: endorsed by the Society of Cardiovascular Anesthesiologists, Society for Cardiovascular Angiography and
Interventions, and Society of Thoracic Surgeons. Circulation. 2008 Oct 7;118[15]:e523661. Epub 2008 Sep 26. Used with permission.)
3. C A R D I AC E X A M I N AT I O N, VA LV U L A R H E A RT D I S E A S E , A N D C O N G E N I TA L H E A RT D I S E A S E 43
The left ventricle is unaffected in mitral stenosis. It is small,
vigorous, and possibly underfilled (reduced preload) in late
mitral stenosis. Intervention on the mitral valve is not rec-
ommended until there are symptoms of exertional dyspnea,
pulmonary edema, or moderate pulmonary hypertension.
Marked volume overload of the left atrium leads to increased
stroke risk as a result of stagnation of blood flow and throm-
bus formation. Atrial fibrillation is frequent and intermittent
in the early stages. Intermittent screening may be warranted,
and anticoagulation should be considered early.
Once symptoms are present, treatment is with either surgi-
cal valve replacement or percutaneous balloon valvuloplasty.
Percutaneous mitral valve balloon valvuloplasty is first-line
therapy when mitral valve leaflets are pliable and noncalcified
and when regurgitation is minimal; valve replacement may be
delayed for at least 10 years with this approach. Intervention for
Figure 3.9 Chest Radiograph From a Patient With Severe Mitral
mitral stenosis is indicated with exertional dyspnea, pulmonary
Stenosis. The straight left heart border, prominent pulmonary artery, edema, or moderate pulmonary hypertension (>50 mm Hg).
large left atrium, right ventricular contour, and pulmonary venous
hypertension are typical findings.
M IT R A L R EGU RG ITAT I O N
Etiology and Pathophysiology
Table 3.6 SEVERITY OF MITRAL STENOSIS, BY VALVE
AREA, GRADIENT, AND PULMONARY PRESSURE The mitral valve is a complex structure, and regurgitation can
result from abnormalities of 3 anatomical locations: leaflet,
VALVE AREA, MEAN GRADIENT, SYSTOLIC PAP,
SEVERITY cm 2 mm hg mm hg
tensor apparatus (chordal and papillary muscles), and myocar-
dium. Common causes of mitral regurgitation include mitral
Mild 1.52 <6 Normal valve prolapse syndrome and myxomatous degeneration, infec-
tive endocarditis, left ventricular dilatation in congestive heart
Moderate 11.5 611 50 failure, collagen vascular disease, ischemia, rheumatic heart
Severe <1 12 >50 disease, and left ventricular dilatation due to cardiomyopathy
CLINICAL PRESENTATION
44 C A R D I O L O GY
(Table 3.7). In the case of ischemic mitral regurgitation, the substantial ventricular dysfunction. It is important to follow
posterior medial papillary muscle with its single blood supply patients closely to determine the optimal timing of surgical
(compared with anterolateral, which has a dual blood supply) intervention.
is more susceptible.
Treatment
Symptoms
There is no universally accepted medical treatment for mitral
Chronic mitral regurgitation causes left ventricular volume regurgitation. The onset of clinical symptoms warrants inter-
overload with reduced afterload. Given time, the left ventri- vention (mitral valve repair or replacement). Asymptomatic
cle compensates by increasing stroke volume. A long asymp- patients with a normal or hyperdynamic ejection fraction can
tomatic phase is thus possible. The most common symptoms continue to have regular observation. Operation should be
include fatigue, dyspnea (due to increased left atrial pressure), considered for symptomatic patients (preoperative left ven-
and pulmonary edema. Symptoms often worsen with atrial tricular function considerably influences the postoperative
fibrillation. outcome), and, because afterload is increased when the mitral
valve is replaced, left ventricular function may actually deterio-
Common causes of mitral regurgitation are mitral valve rate after mitral valve repair or replacement. In most patients,
prolapse and myxomatous degeneration, ischemia, and ejection fraction decreases approximately 10% after mitral
infective endocarditis. valve repair or replacement.
In mildly symptomatic patients, operation may be con-
Fatigue, dyspnea, and pulmonary edema are the most sidered, particularly if serial examinations show progressive
common symptoms and are worsened by atrial fibrillation. cardiac enlargement. Earlier operation may be indicated in
patients who are suitable for mitral valve repair rather than
Physical Examination replacement, especially when the ejection fraction is less than
Findings of mitral regurgitation include a diffuse and hyperdy- 60% or the left ventricular end-systolic dimension is more
namic left ventricular impulse, which may be visible, and a pal- than 40 mm (Figure 3.10).
pable rapid filling wave. The S2 may be obliterated, and there
is a holosystolic murmur. There may be an S3 (or S3 and a flow In symptomatic patients with severe mitral regurgitation,
rumble) and an S4. An S3 with a low-pitched early diastolic operation should be considered.
rumble indicates severe regurgitation; it represents a volume In asymptomatic patients with an ejection fraction <60%
murmur, but coexisting mitral stenosis needs to be ruled out. or left ventricular end-systolic dimension >40 mm,
In acute mitral regurgitation, the murmur may be short operation may be considered, especially if mitral valve
because of increased left atrial pressure. In severe mitral regur- repair is possible and surgical risk is relatively low.
gitation, the carotid upstroke may appear parvus, because of
the low forward stroke volume, but not tardus. The left atrium
may be palpable with systole, and the left ventricle, with dias-
M IT R A L VA LVE P RO L A P S E
tole. The cause of mitral regurgitation may be suspected by the
radiation of the auscultated murmur. A murmur that is due to Pathophysiology and Natural History
a rupture of the anterior leaflet chordae leads to a posteriorly
directed jet of mitral regurgitation and a murmur that radiates Mitral valve prolapse is the most common cause of both valvu-
to the axilla and back. When posterior leaflet chordae rupture, lar heart disease and mitral regurgitation in the United States.
the murmur radiates to the sternum and possibly the carotid Mitral valve prolapse refers to a systolic billowing of one or
arteries. both mitral leaflets into the left atrium with or without mitral
regurgitation. In patients with mitral valve prolapse, as with
other causes of mitral regurgitation, the degree of left atrial
A diffuse, hyperdynamic left ventricular impulse,
and left ventricular dilatation depends on the severity of mitral
holosystolic murmur, lack of S2, and an S3 are findings on
regurgitation. Mitral valve prolapse is associated with secun-
examination.
dum atrial septal defect and supraventricular arrhythmias.
A murmur radiating to the axilla and back is due to
anterior chord rupture, whereas posterior chord rupture Valvular heart disease and mitral regurgitation are most
leads to a murmur heard at the sternal border and the often due to mitral valve prolapse.
carotid arteries.
In Marfan syndrome, the supporting apparatus is often
involved with dilatation of the mitral annulus in addition
to elongated chordae and redundant leaflets, abnormali-
Diagnosis
ties leading to mitral valve prolapse. Other valves also may
Chest radiography may first show a dilated left atrium and be involved with the same myxomatous degeneration, which
then, as mitral regurgitation increases, dilatation of the left leads to tricuspid valve prolapse (occurring in approximately
ventricle. A low or low-normal ejection fraction suggests 40% of patients with mitral valve prolapse), pulmonic valve
3. C A R D I AC E X A M I N AT I O N, VA LV U L A R H E A RT D I S E A S E , A N D C O N G E N I TA L H E A RT D I S E A S E 45
Chronic Severe Mitral Regurgitation
Reevaluation
Clinical evaluation + Echo
No Symptoms? Yes
LV function? LV function?
Class I Class I
Chordal
New-onset AF?
preservation
Pulmonary HT?
likely?
MV repair
Yes If not possible, Yes
Class IIa MVR Class IIa
No No
MV repair
Medical therapy
likely?*
Yes*
Class IIa MV repair
No
Clinical eval
every 6 mo
Echo every
12 mo
Figure 3.10 Management Strategy for Patients With Chronic Severe Mitral Regurgitation. *Mitral valve (MV) repair may be performed in
asymptomatic patients with normal left ventricular (LV) function if performed by an experienced surgical team and if the likelihood of successful MV
repair is greater than 90%. AF indicates atrial fibrillation; Echo, echocardiography; EF, ejection fraction; ESD, end-systolic dimension; eval, evaluation;
HT, hypertension; MVR, mitral valve replacement. (Adapted from Bonow RO, Carabello BA, Chatterjee K, de Leon AC Jr, Faxon DP, Freed MD,
et al; American College of Cardiology/American Heart Association Task Force on Practice Guidelines. 2008 focused update incorporated into the
ACC/AHA 2006 guidelines for the management of patients with valvular heart disease: a report of the American College of Cardiology/American
Heart Association Task Force on Practice Guidelines [Writing Committee to revise the 1998 guidelines for the management of patients with valvular
heart disease]. Endorsed by the Society of Cardiovascular Anesthesiologists, Society for Cardiovascular Angiography and Interventions, and Society
of Thoracic Surgeons. J Am Coll Cardiol. 2008 Sep 23;52[13]:e1142 and Bonow RO, Carabello BA, Chatterjee K, de Leon AC Jr, Faxon DP, Freed
MD, et al; 2006 Writing Committee Members; American College of Cardiology/American Heart Association Task Force. 2008 Focused update
incorporated into the ACC/AHA 2006 guidelines for the management of patients with valvular heart disease: a report of the American College of
Cardiology/American Heart Association Task Force on Practice Guidelines [Writing Committee to Revise the 1998 Guidelines for the Management
of Patients With Valvular Heart Disease]: endorsed by the Society of Cardiovascular Anesthesiologists, Society for Cardiovascular Angiography and
Interventions, and Society of Thoracic Surgeons. Circulation. 2008 Oct 7;118[15]:e523661. Epub 2008 Sep 26. Used with permission.)
prolapse (about 10%), and aortic valve prolapse (2%). Other complication of mitral valve prolapse, although the overall
connective tissue disorders may be associated with mitral incidence is low. There is a low risk for sudden cardiac death
valve prolapse. (Figure 3.11).
Mitral valve prolapse syndrome has a benign course in most
patients. Patients with diagnostic findings of click-murmur on Mitral valve prolapse and other valvular prolapse can
auscultation, thickened mitral leaflets on echocardiography, occur in Marfan syndrome and other connective tissue
and left ventricular and atrial enlargement are at high risk for disorders.
future complications, including atrial fibrillation, systemic
embolism, and pulmonary hypertension. There is also a life- Risks for mitral valve prolapse include infective
long risk for ruptured mitral valve chordae, which may lead endocarditis (low risk), ruptured chordae leading to acute
to acute decompensation. Infective endocarditis is a serious decompensation, and sudden cardiac death (low risk).
46 C A R D I O L O GY
event monitors may be useful for documenting arrhythmias.
Echocardiography is the most useful noninvasive test for defin-
ing mitral valve prolapse. The definition includes more than 2
Symptoms or complications
Male mm of posterior displacement of 1 or both leaflets into the left
Female Murmur atrium. All patients with mitral valve prolapse should have an
+ initial echocardiogram to establish the diagnosis, stratify risk,
Thick MV
+
and define possible associated lesions (eg, atrial septal defect).
Increased Serial echocardiograms are not necessary in asymptom-
Murmur
LV/LA atic patients with mitral valve prolapse. Echocardiographic
size follow-up should be done if there are clinical indications of
+
Thick MV progression.
Murmur
None Treatment
0
Reassurance is a major part of the management of patients
with mitral valve prolapse because most are asymptomatic and
Age
lack a high-risk profile. A normal lifestyle and regular exercise
are encouraged. Patients should be educated about when to
Figure 3.11 Risk Factors for Complications in Mitral Valve Prolapse. seek medical advice (worsening symptoms). Subacute bacte-
LA indicates left atrial; LV, left ventricular; MV, mitral valve. (Adapted rial endocarditis prophylaxis is no longer indicated for mitral
from Boudoulas H, Kolibash AJ Jr, Wooley CF. Mitral valve prolapse: a
heterogeneous disorder. Primary Cardiol. 1991;17[2]:2943. Used with valve prolapse without a history of endocarditis.
permission.) According to Bonow et al, common symptoms include
palpitations, chest pain that rarely resembles classic angina
pectoris, dyspnea, and fatigue. Patients should be advised to
Physical Examination discontinue caffeine, alcohol, and tobacco use. Patients with
Mitral valve prolapse is usually diagnosed with cardiac auscul- recurrent palpitations often respond to -adrenergic block-
tation in asymptomatic patients or incidentally on echocar- ers or calcium channel blockers. Orthostatic symptoms due
diography. The classic auscultatory finding is the midsystolic to postural hypotension and tachycardia are treated with vol-
click, a high-pitched sound of short duration. There may be ume expansion, preferably by liberalizing fluid and salt intake.
multiple clicks. According to Bonow et al clicks result from Transient cerebral ischemic episodes occur with increased inci-
sudden tensing of the mitral valve apparatus as the leaflets dence in patients with mitral valve prolapse, and some patients
prolapse into the left atrium during systole. The midsystolic need long-term anticoagulation (Table 3.8).
click(s) is frequently followed by a mid-late systolic murmur
that is high-pitched, musical, or honking and often loudest Serial echocardiograms are not necessary in asymptomatic
at the cardiac apex. The character and intensity of the clicks patients with mitral valve prolapse.
and the murmur vary with left ventricle loading conditions. Most patients with mitral valve prolapse can be reassured
Dynamic auscultation helps establish the diagnosis. Changes and encouraged to lead a normal lifestyle.
in left ventricular end-diastolic volume result in changes in
the timing of the click(s) and murmur. When end-diastolic Palpitations, chest pain, dyspnea, and fatigue are common
volume is decreased (eg, with standing), the critical volume symptoms.
is achieved earlier in systole and the click-murmur complex Transient ischemic attacks may occur, and long-term
occurs earlier after S1. By contrast, any maneuver that augments anticoagulation may be indicated.
the volume of blood in the ventricle (eg, squatting), reduces
myocardial contractility, or increases left ventricular afterload According to Bonow et al, asymptomatic patients with
lengthens the time from onset of systole to initiation of mitral mitral valve prolapse and no serious mitral regurgitation can
valve prolapse, and the systolic click or murmur moves toward be evaluated clinically every 3 to 5 years. Serial echocardiog-
S2 (Figure 3.12). raphy is necessary only in patients who have high-risk features
on the initial echocardiogram.
Classically, in mitral valve prolapse, a midsystolic click(s) Surgery may be required in a small subset of patients.
caused by sudden tensing of the mitral valve apparatus The thickened, redundant mitral valve often can be repaired
during prolapse, often followed by a mid-late systolic rather than replaced; repair has a low operative mortal-
high-pitched murmur, is heard. ity rate and excellent short- and long-term results. Repair is
often sufficient in patients who have a flail mitral leaflet due
to rupture or marked elongation of the chordae tendineae.
Diagnosis
Recommendations for surgery in patients with mitral valve
Results of electrocardiography most often are normal, although prolapse and mitral regurgitation are the same as those for
24-hour ambulatory electrocardiographic recordings or patients with other forms of severe mitral regurgitation.
3. C A R D I AC E X A M I N AT I O N, VA LV U L A R H E A RT D I S E A S E , A N D C O N G E N I TA L H E A RT D I S E A S E 47
S1 C S2 S1 C S2 S1 C S2 S1 C S2
SM SM SM SM
S1 C S2 S1 C S2 S1 C S2 S1 C S2
Figure 3.12 Auscultation Findings in Mitral Valve Prolapse. C indicates click; S1, S2, heart sound (first, second); SM, systolic murmur; , murmur.
48 C A R D I O L O GY
Table 3.8 RECOMMENDATIONS FOR USE OF ASPIRIN About 50% of patients need valve replacement 1015 years
AND ORAL ANTICOAGULANTS IN MITRAL VALVE after original valve placement due to degeneration and
PROLAPSE calcification.
INDICATIONS CLASS
Mechanical Valves
1. Aspirin therapy for cerebral transient ischemic I
attacks Newer-generation mechanical valves (eg, the bileaflet St. Jude
valve) are less thrombogenic than prior models, but all mechani-
2. Warfarin therapy for patients aged 65 years, in I cal valves have risk for thromboembolism and necessitate
atrial fibrillation with hypertension, mitral regurgi- long-term anticoagulation (Table 3.9). Hemolysis may occur
tation murmur, or history of heart failure
with mechanical prostheses, especially if there is a perivalvular
3. Aspirin therapy for patients aged <65 years, in atrial I leak. Anticoagulation complications include hemorrhage and
fibrillation with no history of mitral regurgitation, thrombosis (when anticoagulation is subtherapeutic). The rate of
hypertension, or heart failure minor hemorrhages is 2% to 4% per year, and that of major hem-
4. Warfarin therapy after stroke I orrhages is 1% to 2% per year. Risk for complications, including
endocarditis, is approximately 1% per year. All patients with a val-
5. Warfarin therapy for transient ischemic attacks IIa vular prosthesis require antibiotic prophylaxis for endocarditis.
despite aspirin therapy
6. Aspirin therapy after stroke in patients with con- IIa Mechanical valves have risk for thromboembolism, and
traindications to anticoagulants systemic anticoagulation is required.
7. Aspirin therapy for patients in sinus rhythm with IIb Anticoagulation can be associated with hemorrhage and
echocardiographic evidence of high-risk mitral
valve prolapse
thrombosis; therapeutic range must be strictly managed.
All patients with a valvular prosthesis require antibiotic
Data from Bonow RO, Carabello BA, Chatterjee K, de Leon AC Jr, Faxon DP, Freed prophylaxis for endocarditis.
MD, et al; American College of Cardiology/American Heart Association Task
Force on Practice Guidelines. 2008 focused update incorporated into the ACC/
AHA 2006 guidelines for the management of patients with valvular heart disease:
a report of the American College of Cardiology/American Heart Association Task C O N G E N I TA L H E A RT D I S E A S E
Force on Practice Guidelines (Writing Committee to revise the 1998 guidelines for
the management of patients with valvular heart disease). Endorsed by the Society
of Cardiovascular Anesthesiologists, Society for Cardiovascular Angiography and
Interventions, and Society of Thoracic Surgeons. J Am Coll Cardiol. 2008 Sep AT R I A L S E P TA L D E FEC T
23;52(13):e1142 and Bonow RO, Carabello BA, Chatterjee K, de Leon AC Jr,
Faxon DP, Freed MD, et al; 2006 Writing Committee Members; American College There are multiple types of atrial septal defects (Table 3.10).
of Cardiology/American Heart Association Task Force. 2008 Focused update incor-
porated into the ACC/AHA 2006 guidelines for the management of patients with
valvular heart disease: a report of the American College of Cardiology/American Secundum Atrial Septal Defect
Heart Association Task Force on Practice Guidelines (Writing Committee to
Revise the 1998 Guidelines for the Management of Patients With Valvular Heart Patients with secundum atrial septal defect often survive to
Disease): endorsed by the Society of Cardiovascular Anesthesiologists, Society for
Cardiovascular Angiography and Interventions, and Society of Thoracic Surgeons.
adulthood and may be asymptomatic. If the defect has gone
Circulation. 2008 Oct 7;118(15):e523661. Epub 2008 Sep 26. undetected, atrial fibrillation frequently develops in the sixth
decade of life along with onset of symptoms, usually dyspnea
with subsequent tricuspid regurgitation and right-sided heart
pericardial (bovine valve, eg, Ionescu-Shiley). Because tis- failure. Stroke may occur as a result of paradoxic embolism.
sue valves are not as thrombogenic as mechanical valves,
most patients in sinus rhythm do not require anticoagula- Secundum atrial septal defect is found on routine
tion after the first 3 to 6 months. Patients with atrial fibrilla- examination with fixed split S2.
tion have increased risk for systemic embolism, particularly
Stroke may occur as a result of paradoxic embolism.
with a mitral prosthesis. Tissue valves degenerate and calcify,
and approximately 50% of patients need valve replacement
Electrocardiography characteristically shows right bundle
at 10 to 15 years. Tissue valves may calcify very rapidly in
branch block and right axis deviation. Chest radiography shows
patients aged 20 years or younger. Tissue valves last longer
pulmonary plethora, a prominent pulmonary artery, and right
in the tricuspid position than in left heart positions. Aortic
ventricular enlargement (Figure 3.13). Echocardiography is
valves are more durable than mitral valves. Prosthesis failure
warranted for definitive diagnosis.
can be detected by clinical evaluation and 2-dimensional and
Doppler echocardiography.
Sinus Venosus Atrial Septal Defect
Tissue valves are not as thrombogenic as mechanical valves.
An uncommon condition, this occurs in the superior portion of
Most patients with tissue valves in sinus rhythm do not the atrial septum. It is often associated with anomalous pulmo-
require anticoagulation. nary veins, usually the right upper. If echocardiography shows
3. C A R D I AC E X A M I N AT I O N, VA LV U L A R H E A RT D I S E A S E , A N D C O N G E N I TA L H E A RT D I S E A S E 49
Table 3.9 RECOMMENDATIONS FOR ANTITHROMBOTIC THERAPY IN PATIENTS WITH PROSTHETIC HEART
VALVES a
THERAPY
VALVE TYPE Aspirin, 75100 mg/day Warfarin, INR 2.03.0 Warfarin, INR 2.53.5 No Warfarin
Mechanical valve
Abbreviations: AVR, aortic valve replacement; INR, international normalized ratio; MVR, mitral valve replacement.
a
Depending on a patients clinical status, antithrombotic therapy must be individualized. Aspirin is recommended in virtually all patients receiving warfarin. Risk factors
are atrial fibrillation, left ventricular dysfunction, previous thromboembolism, and hypercoagulable condition. The international normalized ratio should be maintained
between 2.5 and 3.5 for aortic disk valves and Starr-Edwards valves.
Adapted from Bonow RO, Carabello BA, Chatterjee K, de Leon AC Jr, Faxon DP, Freed MD, et al; American College of Cardiology/American Heart Association Task
Force on Practice Guidelines. 2008 focused update incorporated into the ACC/AHA 2006 guidelines for the management of patients with valvular heart disease: a report
of the American College of Cardiology/American Heart Association Task Force on Practice Guidelines (Writing Committee to revise the 1998 guidelines for the manage-
ment of patients with valvular heart disease). Endorsed by the Society of Cardiovascular Anesthesiologists, Society for Cardiovascular Angiography and Interventions,
and Society of Thoracic Surgeons. J Am Coll Cardiol. 2008 Sep 23;52(13):e1142 and Bonow RO, Carabello BA, Chatterjee K, de Leon AC Jr, Faxon DP, Freed MD, et
al; 2006 Writing Committee Members; American College of Cardiology/American Heart Association Task Force. 2008 Focused update incorporated into the ACC/
AHA 2006 guidelines for the management of patients with valvular heart disease: a report of the American College of Cardiology/American Heart Association Task
Force on Practice Guidelines (Writing Committee to Revise the 1998 Guidelines for the Management of Patients With Valvular Heart Disease): endorsed by the Society
of Cardiovascular Anesthesiologists, Society for Cardiovascular Angiography and Interventions, and Society of Thoracic Surgeons. Circulation. 2008 Oct 7;118(15):e523
661. Epub 2008 Sep 26. Used with permission.
Sinus venosus 10 Vena cava Anomalous PV Incomp RBBB, ectopic P wave, R axis
Ostium primum 1015 Lower septum Cleft MV, Down syndrome Incomp RBBB, L axis (LAHB)
Abbreviations: ECG, electrocardiography; Incomp, incomplete; L axis, left axis deviation; LAHB, left anterior hemiblock; MV, mitral valve; P wave, atrial depolarization
wave on ECG; PV, pulmonary veins; R axis, right axis deviation; RBBB, right bundle branch block.
right ventricular volume overload and no secundum defect (sur- congenitally cleft and produces various degrees of mitral
face echocardiography can miss the sinus venosus area), consider regurgitation.
sinus venosus atrial septal defect or anomalous pulmonary veins.
Diagnosis
On electrocardiography, findings are different from those
Primum Atrial Septal Defect (Partial Atrioventricular
of secundum type; left axis deviation and right bundle branch
Canal)
block are evident. More than 75% of patients have first-degree
This is a defect in the lower portion of the septum due to atrioventricular block. The chest radiographic findings are
partial atrioventricular canal defect. The mitral valve is often the same as those for secundum atrial septal defect, but there
50 C A R D I O L O GY
membranous septum or in the muscular septum. A small ven-
tricular septal defect generally presents with a loud holosystolic
murmur in an asymptomatic patient, and often a thrill at the
left sternal edge, usually around the fourth interspace, is heard.
Large defects may produce a mitral diastolic flow rumble (due
to increased volume) at the apex, especially when the shunt
is more than 2.5:1, and may cause considerable symptoms
early in life. Ventricular septal defects are usually detected in
early childhood, and in developed countries they are usually
closed when discovered. If undiscovered until late childhood
or adulthood, a large ventricular septal defect often has pro-
gressed to Eisenmenger syndrome (severe pulmonary hyper-
tension) and cannot be closed (see Eisenmenger Syndrome
below). Patients may present with symptoms of subacute bac-
terial endocarditis; thus, endocarditis prophylaxis is essential
if Eisenmenger syndrome develops. Affected women of child-
bearing age should be advised against pregnancy.
3. C A R D I AC E X A M I N AT I O N, VA LV U L A R H E A RT D I S E A S E , A N D C O N G E N I TA L H E A RT D I S E A S E 51
are more rigid, the risk for stroke is increased. The decision
about phlebotomy ideally should be guided by a specialist in
adult congenital heart disease. Fluid should be replaced con-
comitantly in patients with Eisenmenger syndrome because
hypotension and syncope may be fatal as a result of exacerba-
tion of right-to-left shunting and hypoxia. Volume depletion,
considerable exercise, and vasodilation should be avoided.
P U L MO NA RY S T E N O S I S
Pulmonary stenosis may occur as an isolated lesion or in associa-
tion with a ventricular septal defect. Valvular pulmonary stenosis
often causes few or no symptoms. The valve is frequently pli-
able, and it may be bicuspid. Thickened dysplastic valves, often
stenotic, occur in association with the Noonan syndrome.
Figure 3.14 Typical Chest Radiograph From a Patient With Valvular
Thickened dysplastic valves, often stenotic, occur with the Pulmonary Stenosis. Normal cardiac size and marked prominence of
main and left pulmonary arteries represent poststenotic dilatation. This
Noonan syndrome. does not occur with infundibular pulmonary stenosis. Lung fields appear
mildly oligemic.
Physical Examination
common in males and frequently is associated with a bicus-
A late P2 may be heard; with severe stenosis, the P2 becomes
pid aortic valve. Only about 20% of cases are diagnosed in
inaudible. The pulmonary opening click is the only right-sided
adulthood. This is the most common cardiac anomaly asso-
sound that gets softer with inspiration as the pulmonary valve
ciated with Turner syndrome. Other associations include
partially opens with the inspiratory increase in venous return.
aneurysms of the circle of Willis and aortic dissection or
Later in life, the valve may become so thick, calcified, and
rupture. There is an increased incidence of aortic dissec-
immobile that the ejection click disappears. Findings of pul-
tion or rupture in Turner syndrome, even in the absence of
monary stenosis include a prominent a wave in the jugular
coarctation. As a result of the coarctation, systemic collat-
venous pulse and an ejection systolic click.
eral vessels develop from the subclavian and axillary arter-
ies through the internal mammary, scapular, and intercostal
Diagnosis arteries and may be identified by rib notching on the chest
radiograph.
Electrocardiography shows right ventricular hypertrophy.
Poststenotic pulmonary dilatation, especially of the left pulmo-
Coarctation of the aorta is more common in males.
nary artery (Figure 3.14), is the chest radiographic hallmark.
The diagnosis is reliably made with 2-dimensional echocar- The condition is frequently associated with a bicuspid
diography, and Doppler echocardiography reliably predicts aortic valve.
the gradient and estimates right ventricular pressure. In
Only 20% of cases are diagnosed in adulthood.
asymptomatic patients, treatment is indicated when the right
ventricular systolic pressure approaches more than two-thirds It is the most common cardiac anomaly associated with
the systemic blood pressure. The treatment of choice for a pli- Turner syndrome.
able noncalcified valve is percutaneous balloon valvuloplasty.
There are 5 major complications of coarctation of the
Two-dimensional and Doppler echocardiography establish aorta: 1) cardiac failure, 2) aortic valve disease, 3) aortic rup-
the diagnosis of pulmonary stenosis. ture or dissection, 4) endarteritis, and 5) rupture of an aneu-
rysm of the circle of Willis. The risk for aneurysmal rupture
C OA RC TAT I O N O F T H E AO RTA
is increased by hypertension. Systemic hypertension may be
the presenting clinical finding in adults younger than 50 years.
This condition is usually either a discrete or a long segment Some patients complain of pain and fatigue in the legs on
of narrowing adjacent to the left subclavian artery. It is more exercise, reminiscent of claudication.
52 C A R D I O L O GY
Symptoms coronary artery disease, heart failure, stroke, or ruptured or
dissected aorta. Age at operation is important. The 20-year
Coarctation should be considered in patients with hyperten- survival rate is 91% in patients who have operation when they
sion who are younger than 50 years. There may be coexistent are younger than 14 years and 79% in patients who have opera-
lower extremity claudication. Patients may present with symp- tion when they are older than 14 years.
toms of aortic rupture, dissection, congestive heart failure,
or associated conditions of Turner syndrome, circle of Willis
Surgical repair is the accepted treatment of coarctation of
aneurysm, or bicuspid valve.
the aorta.
Coarctation may cause hypertension in adults younger
than 50 years. E B S T E I N A N O M A LY
3. C A R D I AC E X A M I N AT I O N, VA LV U L A R H E A RT D I S E A S E , A N D C O N G E N I TA L H E A RT D I S E A S E 53
tall P waves (so-called Himalayan P waves) and right bundle Association Task Force on Practice Guidelines. 2008 focused
branch block. Two-dimensional and Doppler echocardiogra- update incorporated into the ACC/AHA 2006 guidelines for the
management of patients with valvular heart disease: a report of
phy precisely delineate the anatomy. Cardiac catheterization the American College of Cardiology/American Heart Association
is unnecessary. Electrophysiologic study may be necessary to Task Force on Practice Guidelines (Writing Committee to revise
delineate a bypass tract. the 1998 guidelines for the management of patients with val-
vular heart disease). Endorsed by the Society of Cardiovascular
Anesthesiologists, Society for Cardiovascular Angiography and
Treatment Interventions, and Society of Thoracic Surgeons. J Am Coll Cardiol.
2008 Sep 23;52(13):e1142.
The long asymptomatic phase supports postponing surgi- Bonow RO, Carabello BA, Chatterjee K, de Leon AC Jr, Faxon DP,
cal intervention until the patient has significant symptoms. Freed MD, et al; 2006 Writing Committee Members; American
Patients may require anticoagulation if an atrial septal defect College of Cardiology/American Heart Association Task Force.
is present and paradoxical emboli have occurred. 2008 Focused update incorporated into the ACC/AHA 2006 guide-
lines for the management of patients with valvular heart disease: a
report of the American College of Cardiology/American Heart
Conditions associated with Ebstein anomaly are secundum Association Task Force on Practice Guidelines (Writing Committee
atrial septal defect, preexcitation syndrome, and bundle of to Revise the 1998 Guidelines for the Management of Patients With
Kent. Valvular Heart Disease): endorsed by the Society of Cardiovascular
Anesthesiologists, Society for Cardiovascular Angiography and
Tachycardia may be an indication for an electrophysiologic Interventions, and Society of Thoracic Surgeons. Circulation. 2008
study to identify an accessory atrioventricular pathway. Oct 7;118(15):e523661. Epub 2008 Sep 26.
Lucas RV Jr, Edwards JE. The floppy mitral valve. Curr Probl Cardiol.
Anticoagulation should be considered in the setting of an 1982 Jul;7(4):148.
atrial septal defect if paradoxical emboli have occurred. Orourke RA, Crawford MH. The systolic click-murmur syndrome:
clinical recognition and management. Curr Probl Cardiol. 1976
Mar-Apr;1(1):160.
Task Force on Practice Guidelines (Committee on Management of
SUGGESTED RE ADING Patients with Valvular Heart Disease). ACC/AHA guidelines for the
management of patients with valvular heart disease: a report of the
Bonow RO, Carabello BA, Chatterjee K, de Leon AC Jr, Faxon DP, American College of Cardiology/American Heart Association. J Am
Freed MD, et al; American College of Cardiology/American Heart Coll Cardiol. 1998 Nov;32(5):1486588.
54 C A R D I O L O GY
4.
THE HEART AND SYSTEMIC DISEASE, PREGNANCY
AND HEART DISEASE, AND MISCELLANEOUS
CARDIAC DISORDER S
Kyle W. Klarich, MD
55
Physical Examination date, glycemic control has not been shown to lower the inci-
dence of cardiovascular events.
Cardiac enlargement can be caused by myocardial disease
or a pericardial effusion. The pulse volume is decreased as a
Patients with diabetes may present with nonclassic
result of reduced contractility. Sinus bradycardia usually is
symptoms or silent ischemia; congestive heart failure may
present. Other findings may include macroglossia, thinning
be the first clinical manifestation of diabetic coronary
or loss of the lateral third of the eyebrows, coarse hair and
disease.
dry skin, and myxedema. Chest radiography shows increased
cardiac size. Electrocardiography shows low voltage of QRS Aggressive risk factor modification reduces cardiovascular
with prolonged intervals of QRS, PR, and QT. events and mortality in patients with diabetes.
Hypothyroidism-related cardiomyopathy can be reversed
Blood pressure and lipid management and monitoring
with early treatment.
for urinary protein excretion are cornerstones of care.
Physical findings in hypothyroidism include cardiac
Coronary artery bypass grafting was previously shown to
enlargement, reduced myocardial contractility, and
reduce the death rate more than percutaneous transluminal
pericardial effusion (in one-third of patients).
coronary angioplasty in patients with diabetes or those with
Atherosclerosis is accelerated. multivessel coronary artery disease. However, stents and gly-
coprotein IIb/IIIa inhibitors were not routinely used in prior
Hypothyroidism may lead to a reversible dilated
studies. Therefore, diabetes is not an absolute indication for
cardiomyopathy.
the use of coronary artery bypass grafting.
Treatment
A MY L O I D O S I S
Reversal of cardiac involvement occurs with early treatment of
hypothyroidism. Effects
Amyloidosis leads to extracellular deposition of insoluble
proteins in organs and is classified by the precursor plasma
D I A B ET E S M E L L I T US proteins forming the extracellular fibril deposits. The primary
Effects systemic type, AL, is due to monoclonal immunoglobulin free
light chains. The hereditary (familial) type is due to mutant
Diabetes mellitus is associated with premature atherosclero- transthyretin deposition, and its inheritance is autosomal
sis, which is twice as prevalent in diabetic men and 3 times dominant. The wild-type transthyretin type (wild-type TTR,
more prevalent in diabetic women than in a nondiabetic senile type) is due to normal wild-type transthyretin deposi-
population. Patients with diabetes have a higher prevalence tion. The secondary type (AA type) is related to amyloid A
of hypertension and hyperlipidemia. Angina and myocardial protein, usually the result of multiple myeloma. The heart is
infarction manifest with nonclassic symptoms, or patients frequently involved, especially by the AL type. Nearly 90% of
may have silent ischemia. Congestive heart failure may be the patients with primary amyloidosis have clinical manifestations
first manifestation of coronary artery disease among diabetics. of cardiac dysfunction.
Cardiomyopathy not associated with coronary atherosclero- Cardiomyopathy may result from protein infiltration,
sis may also exist; this may be caused by small-vessel disease. which causes thickened ventricular myocardium. Amyloid
Fatal myocardial infarction is more common in patients with deposition in the atrioventricular cardiac valves may
diabetes than in those who do not have diabetes. occur. Amyloid can also deposit in small vessels and lead to
ischemia.
Cardiac involvement may occur in secondary amyloid-
Treatment
osis, but it is usually not a prominent feature. Secondary
Aggressive management of traditional risk factors for cor- amyloidosis occurs in association with chronic diseases
onary artery disease lowers mortality. Diabetic-specific risk such as rheumatoid arthritis, tuberculosis, chronic infec-
factors for coronary artery disease include glycemic con- tion, neoplasm (especially multiple myeloma), and chronic
trol and urinary protein excretion. The use of antihyperten- renal failure. In senile amyloidosis, the heart is the most
sive agents for aggressive blood pressure lowering (systolic commonly involved organ, and prevalence increases after
pressure 120 mm Hg, diastolic pressure 80 mm Hg) age 60 years.
reduces mortality. Statins and fibrates are effective for pri-
mary and secondary prevention of coronary artery disease
in patients with both diabetes and hyperlipidemia. Aspirin
Clinical Features
also is effective for primary and secondary prevention. Cardiac amyloidosis may cause congestive heart failure,
Angiotensin-converting enzyme inhibitors reduce cardio- arrhythmias, sudden death, angina, chest pain, pericardial
vascular events and mortality in patients with diabetes who effusion (usually not hemodynamically significant), and
are older than 55 years and have additional risk factors. To regurgitant murmurs. The natural history is usually intractable
56 C A R D I O L O GY
because of ventricular failure. Diastolic abnormalities are this is a nonspecific finding, and 20% to 25% of patients
common early in the disease process and are classic for restric- with cardiac amyloid may have normal electrocardiographic
tive cardiomyopathy, which indicates a poor prognosis. findings. Echocardiography is particularly useful, showing
increased left ventricular wall thickness, in contradistinc-
Cardiac involvement in primary amyloidosis is common, tion to the small (or normal) voltage on electrocardiography
particularly in the AL (primary systemic) type. (Figure 4.1). Echocardiographic tissue characteristics are
often described as having a granular or speckled appearance.
Cardiac involvement in secondary amyloidosis is not a The atria generally are dilated. The cardiac valves may show
prominent feature but may occur. some thickening and regurgitation. A small pericardial effu-
Senile amyloidosis frequently involves the heart. sion may be present. Diastolic function generally is abnormal;
in the early stages of the disease, findings consistent with pro-
Amyloid heart disease can cause multiple cardiac longed relaxation are found, whereas restrictive filling (con-
abnormalities, ranging from regurgitant murmurs and sistent with high left ventricular filling pressures) is found in
arrhythmias to sudden death. later stages.
I aVR V1 V4
II aVL V2 V5
III aVF V3 V6
II
V1
V5
C A RC I N O I D H E A RT D I S E A S E
Treatment
Effects
Treatment of the underlying tumor is important for symp-
Liver or lung metastases from carcinoid tumors can pro- tom relief. In the setting of right heart failure (eg, intracta-
duce a classic syndrome (in only about 4% of patients) ble edema, ascites, and dyspnea), surgery may be warranted.
due to production of serotonin-like substances. These Surgical therapies include tricuspid valve replacement and
substances cause cutaneous flushing, wheezing, and diar- pulmonary valve resection.
rhea (the carcinoid syndrome) and are toxic to cardiac
valves. Cardiac involvement occurs in approximately 50%
of patients with hepatic or pulmonary metastasis; toxic
H Y P E R E O S I N O P H I L I C S Y N D RO M E
effects generally affect right-sided cardiac valves. Left-sided
valves can be affected if a cardiac shunt is present; such a Effects
shunt allows right-to-left movement of serotonin-like sub-
stances via the bloodstream. Carcinoid lesions are fibrous This syndrome, with persistent eosinophil concentrations of
plaques that form on valvular endocardium. The valve leaf- more than 1.5 109/L, typically affects young, usually male,
lets become thickened, relatively immobile, and retracted. patients. Causes include idiopathic hypereosinophilia, Lffler
Regurgitation results, with some stenosis of the tricuspid endocarditis, reactive or allergic eosinophilia, leukemic or
and the pulmonary valves. neoplastic eosinophilia, and Churg-Strauss syndrome. All of
these may have cardiac manifestations.
Serotonin-like substances produced by metastatic
carcinoid tumors are toxic to heart valves and may lead to Clinical Features
regurgitation and stenosis.
Patients typically present with weight loss, fatigue, dyspnea, syn-
Right-sided valves are most commonly affected. cope, and systemic embolization. Pulmonary involvement should
58 C A R D I O L O GY
prompt consideration of Churg-Strauss syndrome. Cardiac R H EU M ATO I D A RT H R I T I S
manifestations include arrhythmias, myocarditis, conduction
Nearly all cardiac components, including pericardium, myo-
abnormalities, and thrombosis. Cardiac eosinophilic deposi-
cardium, valves, coronary arteries, and aorta, may be affected
tion may occur, with clot formation in the ventricular apices and
in patients with rheumatoid arthritis. Granulomatous inflam-
the inflow surfaces of the mitral and tricuspid valves. Matting
mation and nongranulomatous inflammation of valve leaf-
down of the atrioventricular valves occurs, causing considerable
lets occur but rarely lead to severe valvular incompetence.
regurgitation. Scarring occurs where the clot formed, leading to
Associated pericarditis is typically associated with a low glu-
endomyocardial fibrosis and restrictive cardiomyopathy.
cose level and complement depletion in the pericardial fluid.
Rheumatoid nodules in the conduction system can lead to
Arrhythmias, myocarditis, conduction abnormalities, and heart block. Aortitis and pulmonary hypertension due to pul-
thrombosis may occur in hypereosinophilic syndrome. monary vasculitis are very rare complications.
Valve involvement may lead to regurgitation, fibrosis, and
restrictive cardiomyopathy. Pericardial fluid is low in glucose and complement.
Churg-Strauss syndrome should be considered if Rheumatoid nodule involvement in the conduction system
pulmonary involvement is present. may lead to heart block.
Nongranulomatous and granulomatous involvement of
S Y S T E M I C LU P US E RY T H E M ATO S US valvular tissue may lead to valve incompetence.
Systemic lupus erythematosus may involve any of the car-
diac structures. Special features of involvement include the A N K Y L O S I N G S P O N DY L I T I S
antiphospholipid syndrome and Libman-Sacks endocarditis.
Cardiac involvement may include pericarditis, characterized Approximately 10% of patients with ankylosing spondylitis
by a positive antinuclear antibody in the pericardial fluid, have aortic dilatation and aortic regurgitation. Aortic valve
myocarditis (more common in patients with anti-Ro anti- cusp distortion and retraction also may cause considerable
body), valvulopathy, and coronary arteritis. Libman-Sacks aortic regurgitation. Fibrosis and inflammation of the conduc-
endocarditis, which results in noninfective vegetations, occurs tion system may occur.
in up to 50% of patients with systemic lupus erythematosus.
The vegetations do not generally embolize or interfere with Cardiac abnormalities of ankylosing spondylitis include
valvular function. Congenital heart block may occur in new- aortic dilatation, aortic valve regurgitation, and conduction
borns of mothers with lupus with anti-La and anti-Ro anti- system abnormalities.
bodies due to myocarditis and to inflammation and fibrosis of
the conduction system (neonatal lupus).
M A R FA N S Y N D RO M E
The vegetations of Libman-Sacks endocarditis generally do Degeneration of elastic tissues occurs in this autosomal domi-
not cause clinical problems. nant condition. Features include arachnodactyly, tall stature,
pectus excavatum, kyphoscoliosis, and lenticular disloca-
Offspring of mothers with SS-a and SS-b antibodies are at
tion. Cardiac involvement is common, including mitral valve
risk for congenital heart block.
prolapse, aortic regurgitation due to aortic dilatation, and
increased risk of aortic dissection. Long-term -adrenergic
S C L E RO D E R M A blockade decreases the rate of aortic dilatation and the risk of
aortic dissection. Dissection occurs rarely in an aorta less than
Cardiac involvement is manifested by intramural coronary
55 mm in diameter. When dissection occurs, it tends to start
involvement and immune-mediated endothelial injury, which
in the ascending aorta and extend along the entire aorta.
is often associated with the Raynaud phenomenon clinically
(due to peripheral small vessel involvement). Other systemic
features include sclerotic skin changes and esophageal abnor- Degeneration of elastic tissues results in considerable risk
malities. Cardiac involvement is the third most common cause of aortic regurgitation and aortic dissection. Mitral valve
of mortality in patients with scleroderma. Conduction defects prolapse may occur.
occur in up to 20% of patients, and a usually asymptomatic
pericardial effusion is found in a third of patients. Indirect
cardiac involvement due to pulmonary hypertension and cor FR I E D R E I C H ATAX I A
pulmonale is frequent.
This autosomal recessive neurologic disorder involves the
heart in up to 90% of cases. It usually manifests as a symmet-
Cardiac involvement is the third most common cause of
ric hypertrophy of the myocardium and less commonly as a
mortality in patients with scleroderma.
dilated cardiomyopathy.
Conduction defects may occur in up to 20% of patients,
and pericardial effusions are also common. Cardiac involvement is very common in Friedreich ataxia.
60 C A R D I O L O GY
Although not absolute contraindications, the follow- delivery in the left lateral position, and a short second stage
ing conditions are of concern in pregnancy: 1) atrial sep- of labor. Facilitated delivery may be needed if labor pro-
tal defect (deep venous thrombosis may lead to paradoxic gresses slowly.
embolus) and 2) coarctation (increased risk of dissection and
rupture). Patients at risk during pregnancy should minimize Pregnant women with cardiac disease require careful
physical activity to prevent increased cardiac output, reduce monitoring during delivery.
dietary sodium, and minimize anemia with iron and vitamin
supplements. Vaginal delivery is safer for most women with cardiac dis-
ease; with vaginal delivery, average blood loss is 500 mL, as
Absolute contraindications to pregnancy include Marfan opposed to cesarean section, with an average blood loss of 800
syndrome, Eisenmenger syndrome, primary pulmonary mL. Cesarean section is typically performed only for obstetric
hypertension, symptomatic severe aortic or mitral valve indications. American Heart Association guidelines state that
stenosis, and symptomatic dilated cardiomyopathy. there is no need for antibiotic prophylaxis in an uncompli-
cated vaginal delivery.
Bed rest is indicated if congestive heart failure develops.
Arrhythmias such as atrial fibrillation must be treated promptly. Vaginal delivery is safer for the majority of patients with
Cardioversion can be performed with apparently low risk to cardiac disease; cesarian section is typically used for
the fetus. Fetal cardiac monitoring should also be performed. obstetric indications only.
Occasionally patients require surgery. Operation during the
first trimester is associated with a markedly increased rate of
fetal loss. Percutaneous aortic, mitral, and pulmonary balloon
M A NAG E M E N T O F P RO S T H ET I C VA LV E S
valvuloplasty have been performed during pregnancy and may
D U R I N G P R E G NA N C Y
obviate cardiopulmonary bypass. Careful lead shielding of the
fetus is necessary because of the use of ionizing radiation. Most women of childbearing age who want to bear children
and who also need a valve replacement elect to have a biologic
Arrhythmias must be promptly treated and cardioversion valve. Anticoagulants are usually not required in the setting of
can be safely performed in pregnant patients. sinus rhythm. A biologic valve obligates patients to additional
heart surgery. Women with mechanical valves require warfa-
rin, posing a problem with teratogenicity (first trimester) and
M E D I C A L T H E R A P Y D U R I N G P R EG NA N C Y
increased risk of spontaneous abortion. Pregnancy should be
diagnosed as soon as possible, therapy should be switched to
Many cardiac drugs cross the placenta but can be used safely unfractionated subcutaneous heparin, and the activated par-
when necessary. These include digoxin, quinidine, procain- tial thromboplastin time should be monitored. High-risk
amide, -adrenergic blockers, and verapamil. -Adrenergic pregnancy teams adept at management are essential to early
blockers are associated with fetal growth retardation, neonatal management.
bradycardia, and hypoglycemia and should be used cautiously.
Patients with hypertrophic cardiomyopathy may require high In pregnant patients with mechanical valves, therapy
doses, and fetal growth must be monitored. should be switched from warfarin to unfractionated
Angiotensin-converting enzyme inhibitors (which cause subcutaneous heparin.
fetal renal dysgenesis), phenytoin (which causes hydantoin
syndrome and teratogenicity), and warfarin (which causes
teratogenicity and abortion) should be avoided in pregnancy.
H Y P E RT E N S I O N A N D P R E G NA N C Y
Drugs to avoid in pregnancy include angiotensin- High blood pressure during pregnancy is defined as a systolic
converting enzyme inhibitors, phenytoin, and warfarin. blood pressure increase of >30 mm Hg, a diastolic blood
pressure increase of 15 mm Hg or more, or an absolute dia-
stolic blood pressure of 90 mm Hg or more. It may be due
D E L I VE RY I N T H E S ET T I N G O F C A R D I AC
to 1) chronic hypertension (blood pressure 140/80 mm
DISEASE
Hg before pregnant state), 2) transient hypertension (devel-
ops during pregnancy), 3) preeclampsia (starts at 20 weeks
Rapid hemodynamic swings occur during delivery. About of pregnancy), or 4) a combination. Methyldopa is the most
500 mL of blood is released into the circulation with extensively studied drug for hypertension during pregnancy
each uterine contraction. Cardiac output increases with and is safe. -Adrenergic blockers are safe and efficacious
advancing labor, and oxygen consumption increases 3-fold. but may cause growth retardation and fetal bradycardia.
High-risk patients need careful monitoring (possibly with Angiotensin-converting enzyme inhibitors are contraindi-
Swan-Ganz catheterization to maintain preload at an opti- cated. Hydralazine is used if dual therapy is indicated, but
mal level), maternal and fetal electrocardiographic monitor- it may cause fetal thrombocytopenia. Calcium channel
ing, careful analgesia and anesthesia to avoid hypotension, blockers have been used more commonly in recent years.
Chest pain is the presenting symptom of pericarditis, and a Tamponade leads to multiple clinical findings, including
friction rub may be heard on examination. pulsus paradoxus and Kussmaul sign.
Causes
Treatment
Causes include viral or idiopathic pericarditis, autoimmune
and collagen vascular diseases, and postmyocardial infarction. Emergency pericardiocentesis guided by echocardiography is
Postcardiotomy syndrome may occur weeks to months after necessary in hemodynamically compromised patients.
open heart procedures. It presents with pyrexia, increased sedi-
mentation rate, and pleural or pericardial chest pain. Incidence
C O N S T R I C T I VE P E R I C A R D I T I S
decreases with age. Management is with anti-inflammatory
agents. Pericarditis is also associated with radiation and neo- Constrictive pericarditis is characterized by dissociation of
plasm (especially Hodgkin disease, leukemia, and lymphoma). respiratory-induced changes in intrathoracic and intracardiac
Melanoma and breast, thyroid, and lung tumors can metasta- pressures. Ventricular filling is limited by the constraining
size to the pericardium and cause pericarditis or pericardial pericardium, an effect leading to lower ventricular volume,
effusion. Uremia and tuberculosis also can cause pericarditis. higher end-diastolic pressures, and decreased cardiac output.
Idiopathic viral pericarditis is the most likely diagnosis in the The most common causes are recurrent viral pericarditis,
62 C A R D I O L O GY
irradiation, previous open heart operation, tuberculosis, and Treatment
neoplastic disease.
The treatment of choice for constrictive pericarditis is
pericardiectomy.
Constriction causes decreased ventricular filling.
C A R D I AC T U M O R S
Symptoms
Symptoms of constrictive pericarditis are predominantly Metastatic tumors are far more common than primary cardiac
right-sided failure, peripheral edema, ascites, and often dysp- tumors (>20-fold). The most frequent metastases to the heart
nea and fatigue. are melanoma, lymphoma, and breast, lung, and esophageal
tumors. More than half of patients with malignant melanoma
have metastases to the heart.
Physical Examination The most common primary benign tumors of the adult
heart are cardiac myxoma, fibroma, and papillary fibroelas-
In constrictive pericarditis, the jugular venous pressure is toma. Primary tumors are extremely rare. Cardiac tumors may
increased (best observed when the patient is sitting or stand- cause circulatory problems, valve dysfunction, myocardial
ing), and inspiratory distention of neck veins (Kussmaul infiltrationrelated complications, invasion into local struc-
sign) is present. The jugular venous pressure may show tures, or embolization.
rapid descents; a pericardial knock is present in fewer than
50% of cases. Ascites and peripheral edema are usually pres- Primary cardiac tumors are much rarer than metastatic
ent. Chest radiography may show pericardial calcification tumors.
and cardiac enlargement. No specific changes are found on
electrocardiography. The the most common primary cardiac tumor is myxoma,
a benign tumor. Most cardiac myxomas are sporadic, but a
Typical examination findings in constrictive pericarditis are subset of these tumors is familial. The majority (75%85%)
Kussmaul sign and signs consistent with right-sided heart are located in the left atrium, 18% are in the right atrium, and
failure. the rest are ventricular. Most atrial tumors arise from the atrial
septum, usually adjacent to the fossa ovalis. About 95% are
solitary. Most have a short stalk, are gelatinous and friable, and
tend to embolize. They occasionally calcify and may be visible
Diagnosis
on chest radiography.
A high degree of clinical suspicion is necessary because A familial syndrome, Carney complex, involves multiple,
the diagnosis of constrictive pericarditis can be challeng- often recurrent, cardiac and extracardiac myxomas, lentigino-
ing. Echocardiography, particularly with Doppler, shows sis (spotty pigmentation) and other pigmentation abnormali-
the hemodynamic effects of respiratory changes in mitral ties, endocrine tumors, and schwannomas. Myxomas present
and tricuspid inflow velocities and other classic changes. at a young age compared with sporadic myxomas.
Pericardial thickness may be delineated by computed tomog-
raphy and magnetic resonance imaging, but up to 20% of Myxomas are the most common primary cardiac tumor.
constraining pericardium may not be thickened according
to computed tomographic criteria. Magnetic resonance Blood flow obstruction, embolization, and systemic effects
scanning can show pericardial inflammation. Restrictive are the most common complications. Systemic emboli may
cardiomyopathy is the main differential diagnosis and dif- occur in 30% to 60% of patients with left-sided myxoma, fre-
ferentiation can be difficult. Myocardial disease is likely if quently to the brain and lower extremities. Coronary embo-
pulmonary artery systolic pressure is more than 50 mm Hg lization is rare, but it should be considered in a young patient
or if end-diastolic pulmonary artery pressure is more than with no known previous cardiac disease. Systemic effects are
30% of systolic pressure, but both are nonspecific findings. fatigue, fever, weight loss, and arthralgia. Systemic effects
In very difficult cases, cardiac catheterization for hemody- may be associated with an increased sedimentation rate, leu-
namic measurements may be necessary to show the intra- kocytosis, hypergammaglobulinemia, and anemia. Increased
ventricular dependence and dissociation of intracardiac and immunoglobulins are usually of immunoglobulin G class.
intrathoracic pressures. Left atrial tumors prolapse into the mitral valve orifice,
producing symptoms of mitral stenosis (dyspnea, orthopnea,
Constrictive pericarditis is diagnosed from respiratory cough, pulmonary edema, and hemoptysis). Classically, symp-
changes noted on Doppler echocardiography. toms occur with a change in body position. Physical findings
suggest mitral stenosis. Pulmonary hypertension may occur.
The major confounding diagnosis is restrictive
An early diastolic sound, the tumor plop, may be heard, with
cardiomyopathy.
the timing of an S3. The later timing and lower frequency dif-
Diastolic pressure is increased and equal in all 4 chambers. ferentiate it from an opening snap.
64 C A R D I O L O GY
5.
HEART FAILURE AND CARDIOMYOPATHIES
Nicole P. Sandhu, MD, PhD, Naveen L. Pereira, MD,
65
At Risk for Heart Failure Heart Failure
Figure 5.1 Stages in the Development of Heart Failure and Recommended Therapy by Stage. ACEI indicates angiotensin-converting enzyme inhibitor;
ARB, angiotensin receptor blocker; EF, ejection fraction; FHx CM, family history of cardiomyopathy; HF, heart failure; LV, left ventricular; LVH, left
ventricular hypertrophy; MI, myocardial infarction. (Adapted from Hunt SA, Abraham WT, Chin MH, Feldman AM, Francis GS, Ganiats TG, et al;
American College of Cardiology Foundation; American Heart Association. 2009 Focused update incorporated into the ACC/AHA 2005 guidelines
for the diagnosis and management of heart failure in adults: a report of the American College of Cardiology Foundation/American Heart Association
Task Force on Practice Guidelines Developed in Collaboration With the International Society for Heart and Lung Transplantation. J Am Coll
Cardiol 2009 Apr 14;53[15]:e190. Erratum in: J Am Coll Cardiol. 2009 Dec 15;54[25]:2464 and Hunt SA, Abraham WT, Chin MH, Feldman
AM, Francis GS, Ganiats TG, et al. 2009 Focused update incorporated into the ACC/AHA 2005 Guidelines for the Diagnosis and Management of
Heart Failure in Adults: a report of the American College of Cardiology Foundation/American Heart Association Task Force on Practice Guidelines:
developed in collaboration with the International Society for Heart and Lung Transplantation. Circulation. 2009 Apr 14;119[14]:e391479. Epub
2009 Mar 26. Erratum in: Circulation. 2010 Mar 30;121[12]:e258. Used with permission.)
66 C A R D I O L O GY
Box 5.1 CONDITIONS THAT PROMPT Table 5.1 MANAGEMENT OF HIGH-OUTPUT AND
HOSPITALIZATION IN HEART FAILURE LOW-OUTPUT HEART FAILURE
CONGESTION AT REST
Hypotension PERFUSION
AT REST NO YES
Worsening renal function
Altered mentation
Normal Warm & dry Warm & wet
Dyspnea at rest PCWP normal PCWP increased
Significant arrhythmias CI normal (compensated) CI normal
Disturbed electrolytes p
Lack of outpatient care Hospitalize r
Nesiritide or vasodilatorsa
Diuretics
who have exclusively exertional symptoms, are not severely Low Cold & dry Cold & wet
congested on examination, and have adequate vascular perfu- PCWP low or normal PCWP increased
sion (warm extremities, adequate blood pressure) may receive CI decreased CI decreased
treatment as outpatients. The stages of heart failure develop- p p
ment and management are outlined in Figure 5.1. Hospitalize Hospitalize
Cautious hydration Nesiritide or vasodilatorsa
Inotropic drugsb Diuretics
Patients with significant symptoms and signs of acute
decompensated heart failure should be hospitalized. Abbreviations: CI, cardiac index; PCWP, pulmonary capillary wedge pressure; r,
patient may or may not require hospitalization, depending on clinical assessment.
Outpatient management may be reasonable in the setting
a
of exertional symptoms only, minimal congestion, and Vasodilators: nitroglycerin or nitroprusside.
good vascular perfusion. b
Inotropic drugs: milrinone or dobutamine.
5. H E A RT FA I LU R E A N D C A R D I O M YO PAT H I E S 67
Paroxysmal nocturnal dyspnea and orthopnea have greater disease exacerbation must be excluded. Clinical stratification
diagnostic weight than exertional dyspnea, and increased guides initial treatment (usually parenteral) (Figure 5.2).
venous pressure has greater diagnostic weight than edema. Once clinical improvement begins, treatment is adjusted to
optimize hemodynamics, minimize symptoms, and allow tran-
Use of the modified Framingham criteria can assist in
sition to oral medications. The mechanism of heart failure and
diagnosing heart failure but will not be as helpful in
precipitating factors are defined, patient and family education
patients with low-output heart failure without associated
are provided, and dismissal (including follow-up) is planned.
congestion.
Consideration of common alternate diagnoses (pulmonary
Increased intracardiac pressure or chamber dilatation leads
embolism and chronic obstructive pulmonary disease) is
to increased production of natriuretic peptides, substances
important when heart failure is diagnosed.
produced by the heart. Accordingly, measurement of B-type
natriuretic peptide or N-terminal pro-brain natriuretic pep-
tide complements the clinical diagnosis of heart failure. In M E C H A N I S M S O F H E A RT FA I LU R E
general, the degree of increase reflects the degree of myocar- Selection of proper therapy depends on correctly identifying
dial dysfunction. Increased levels of these peptides do not the mechanism of heart failure. A simple categorical framework
distinguish systolic from diastolic, left from right, or acute is given in Table 5.2. Left ventricular myocardial dysfunction
from chronic cardiac dysfunction. Interpreting these levels has is the most common cause of heart failure. Accurate diagnosis
caveats (Box 5.3). In addition, there is substantial variability of is essential because treatment and prognosis are based on the
levels in stable patients, up to 50%. cause of heart failure. Diagnosis is initially based on physical
The utility of the natriuretic peptide values for diagnos- examination and noninvasive testing, such as echocardiogra-
ing heart failure has been best shown in patients without phy or radionuclide angiography.
prior known cardiac disease. Interpretation of intermediately
increased levels can be difficult in patients with a prior history The most common cause of heart failure is left ventricular
of ventricular dysfunction or heart failure who are receiving myocardial dysfunction.
medical treatment. The negative predictive value of normal
natriuretic peptide levels (in the absence of constriction, mor- Therapy depends on the mechanism of heart failure.
bid obesity, or mitral stenosis) is more powerful than their
positive predictive value. Natriuretic peptide values are most P R EC I P ITAT I N G FAC TO R S
useful in patients without a prior diagnosis of heart failure and
New-onset or worsening heart failure symptoms may represent
in patients not receiving treatment for heart failure.
only natural disease progression. However, 1 or more precipi-
tating factors may be responsible for symptomatic deteriora-
Natriuretic peptide levels are increased in the setting of
tion (Box 5.4). If these factors are not identified and corrected,
increased intracardiac pressure or chamber dilatation.
heart failure symptoms often return after initial therapy.
The type of cardiac dysfunction cannot be distinguished The most common precipitants are dietary indiscretion (eg,
using natriuretic peptide values. sodium, excess fluid, and alcohol), medication nonadherence
due to cost, regimen complexity, lack of patient understand-
The negative predictive value of normal natriuretic peptide ing, and suboptimally controlled hypertension.
levels is generally greater than their positive predictive Evaluation should follow these steps: 1) a medical history,
value. which includes sodium and fluid intake, medication use and
compliance, and sleep history from bedroom partners; 2) chest
M A NAG E M E N T O F AC U T E H E A RT FA I LU R E radiography to look for pneumonitis; 3) electrocardiography
and measurement of cardiac biomarkers to document heart
At the time of initial diagnosis, the common alternative diagno- rhythm and identify myocardial ischemia or injury; and 4) cul-
ses of pulmonary embolism or chronic obstructive pulmonary tures of blood, urine, and sputum on the basis of the history.
Other tests should include determination of complete blood
count and thyroid-stimulating hormone and creatinine levels.
Box 5.3 PITFALLS IN THE INTERPRETATION OF
NATRIURETIC PEPTIDE VALUE
Precipitating factors must be sought and treated.
NP HIGHER THAN NP LOWER THAN Dietary indiscretion, medication noncompliance, regimen
EXPECTED EXPECTED complexity, and uncontrolled hypertension are common
precipitants of heart failure decompensation.
Women Obesity
Elderly Acute heart failure
Renal failure Heart failure due to mitral stenosis C A R D I O M YO PAT H I E S
Constriction
Cardiomyopathies are divided into primary and secondary
Abbreviation: NP, natriuretic peptide.
cardiomyopathies, and the primary disorders are further
68 C A R D I O L O GY
Heart Stratify clinically & Identify patients who need
failure? initiate treatment specific adjuvant treatment
(ACS, acute valve regurgitation,
acute bradyarrhythmia or malignant
tachyarrhythmia, airway, ventilation,
or oxygen problem)
Minimize symptoms,
optimize hemodynamics
EF low?
Figure 5.2 Approach to Acute Heart Failure. ACS indicates acute coronary syndrome; EF, ejection fraction.
CAUSE TREATMENT
Myocardial
Dilated cardiomyopathy (including ischemic) Angiotensin-converting enzyme inhibitors, angiotensin receptor blockers, -adrenergic
blockers (eg, carvedilol, metoprolol succinate, bisoprolol), diuretics, aldosterone antag-
onists, nitrates, digoxin, nitrates & hydralazine in combination, transplant, coronary
revascularization, left ventricular aneurysmectomy (surgical ventricular remodeling),
cardiac resynchronization therapy, cardiac defibrillator
Hypertrophic cardiomyopathy E-Adrenergic blockers, verapamil, disopyramide, surgical myectomy, septal alcohol abla-
tion, dual-chamber pacing
Restrictive cardiomyopathy Diuretics, heart transplant, treatment of underlying systemic disease
Pericardial
Tamponade Pericardiocentesis
Constrictive pericarditis Pericardiectomy
Pulmonary hypertension Prostacyclin infusion, calcium channel blockers, heart-lung transplant, endothelin antago-
nists, phosphodiesterase type 5 inhibitor
High output
Hyperthyroidism, Paget disease, Correction of underlying cause
arteriovenous fistula
5. H E A RT FA I LU R E A N D C A R D I O M YO PAT H I E S 69
Box 5.4 PRECIPITATING FACTORS IN HEART FAILURE disease, myocarditis, postpartum cardiomyopathy,
toxins and drugs, and tachycardia-induced
Diet (excessive sodium or fluid intake, alcohol) cardiomyopathy.
Noncompliance with medication or inadequate dosing
Sodium-retaining medications (NSAIDs)
Infection (bacterial or viral) Clinical Presentation
Myocardial ischemia or infarction
The presentation is highly variable. The patient may be
Arrhythmia (atrial fibrillation, bradycardia)
asymptomatic and the diagnosis prompted by examination,
Breathing disorders of sleep
chest radiography, electrocardiography (ECG), or imaging
Worsening renal function
findings. Patients may have symptoms of mild to severe heart
Anemia
failure (New York Heart Association [NYHA] functional
Metabolic (hyperthyroidism, hypothyroidism)
class II-IV). Atrial and ventricular arrhythmias are common
Pulmonary embolus
in dilated cardiomyopathy. Physical examination may indi-
cate increased jugular venous pressure, a right ventricular lift
Abbreviation: NSAIDs, nonsteroidal anti-inflammatory drugs.
(if there is right heart involvement), low-volume upstroke
of the carotid artery, displaced and sustained left ventricular
impulse (possibly with a rapid filling wave), audible third or
cardiomyopathy indicates left ventricular dysfunction without
fourth heart sounds, and an apical systolic murmur of mitral
any known cause. The right ventricle may be normal, hypertro-
regurgitation. Pulsus alternans may occur in patients with
phied, or dilated.
advanced heart failure. Pulmonary examination may have
normal results or indicate crackles or evidence of pleural
A dilated left ventricle is the major abnormality in dilated effusion.
cardiomyopathy.
The right ventricle may be normal, hypertrophied, or The clinical presentation of dilated cardiomyopathy is
dilated. highly variable.
Atrial and ventricular arrhythmias are common.
Many cases of dilated cardiomyopathy are genetic with
at least 1 identifiable affected family member in up to 30%
The ECG is almost always abnormal and frequently indicates
of cases. Other causes of left ventricular dysfunction include
left ventricular hypertrophy, intraventricular conduction delay,
severe coronary artery diseasethe most common cause in
or bundle branch block. Rhythm abnormalities may include
the United States(hibernating myocardium), previous
premature atrial contractions, atrial fibrillation, premature ven-
infarction, uncontrolled hypertension, ethanol abuse, myo-
tricular contractions, or short bursts of ventricular tachycardia.
carditis, hyperthyroidism or hypothyroidism, postpartum
The chest radiograph often shows left ventricular enlargement
cardiomyopathy, toxins and drugs (including doxorubicin
and pulmonary venous congestion. The diagnosis is based on
and trastuzumab), tachycardia-induced cardiomyopathy, infil-
the findings of left ventricular enlargement and reduced ejec-
trative cardiomyopathy (ie, hemochromatosis, sarcoidosis),
tion fraction, which can be measured with echocardiography,
AIDS, and pheochromocytoma.
radionuclide angiography, left ventriculography, cine computed
tomography, or magnetic resonance imaging.
The most common cause of dilated cardiomyopathy in the
United States is coronary artery disease.
The diagnosis of dilated cardiomyopathy requires evidence
Other causes of left ventricular dysfunction include of left ventricular enlargement and reduced ejection
uncontrolled hypertension, ethanol abuse, thyroid fraction by cardiac imaging.
Restrictive N/n N N p
cardiomyopathy
70 C A R D I O L O GY
Evaluation
C
After diagnosis, treatable secondary causes of left ventricular B
dysfunction should be sought. Tests of thyroid function should
be done to exclude hyperthyroidism or hypothyroidism.
Stroke Volume
Transferrin levels should be measured to screen for hemochro- Low A E
matosis. Measurement of the serum angiotensin-converting output D
enzyme level should be considered if sarcoidosis is a possibil-
ity. Metanephrine levels should be measured if there is a his-
tory of severe labile hypertension or unusual spells. Ethanol or Pulmonary
drug abuse history should be obtained. congestion
In severe coronary artery disease, reversible left ventricu-
lar dysfunction can be caused by hibernating myocardium.
Preload
With revascularization, left ventricular function may improve
gradually. Identifying affected patients is difficult. Currently, Figure 5.3 Starling Curve. Blue line is patient with normal contractility,
the reference standard is positron emission tomography to and red line is one with depressed systolic function. Normally, stroke
evaluate metabolic activity. Viability protocols used in stress volume depends on preload of the heart. Increasing preload increases
echocardiography and radionuclide perfusion imaging are stroke volume (A to B). Myocardial dysfunction causes a shift of the
curve downward and to the right (C to D), causing a severe decrease in
more widely available than positron emission tomography stroke volume, which leads to symptoms of fatigue and lethargy. The
and are useful for identifying hibernating myocardium. compensatory response to decrease in stroke volume is an increase in
preload (D to E). Because the diastolic pressure-volume relationship
Treatable secondary causes of left ventricular dysfunction, is curvilinear, increased left ventricular volume produces increased left
such as thyroid disease and hemochromatosis, should be ventricular end-diastolic pressure, causing symptoms of pulmonary
congestion. Note flat portion of the curve at its upper end; here, there is
sought. little increase in stroke volume for increase in preload.
Hibernating myocardium in the setting of severe coronary
artery disease can lead to reversible left ventricular
dysfunction. Starling curve (Figure 5.3). Afterload is the tension, force,
or stress on the ventricular wall muscle fibers after fiber
Tachycardia-induced cardiomyopathy can occur in patients shortening begins. Left ventricular afterload is increased by
with prolonged periods of tachycardia (usually atrial fibrilla- aortic stenosis and systemic hypertension but is decreased
tion or flutter or prolonged atrial tachycardia). Because sys- by mitral regurgitation. Ventricular enlargement increases
tolic dysfunction can be completely reversed with treatment afterload.
of tachycardia, identifying these causes is important. Figure 5.4 illustrates the neurohormonal response to
Acute myocarditis may cause left ventricular dysfunc- decreased myocardial contractility. Decreased cardiac out-
tion; the natural history is unknown. Many patients have put activates baroreceptors and the sympathetic nervous
development of persistent left ventricular dysfunction, system. Sympathetic nervous system stimulation causes
whereas others have improvement with time. Thus, it is nec- increased heart rate and contractility. -Stimulation of the
essary to remeasure left ventricular function 3 to 6 months arterioles causes increases in afterload. The renin-angiotensin
after diagnosis and treatment. Endomyocardial biopsy may system is activated by sympathetic stimulation, decreased
help diagnose myocarditis. Immunosuppressive therapy does renal blood flow, and decreased renal sodium, in turn acti-
not improve outcome and should be reserved for patients vating aldosterone, causing increased renal retention of
with giant cell myocarditis, concomitant skeletal myositis, sodium, which leads to pulmonary congestion. Low renal
or clinical deterioration despite standard pharmacologic blood flow causes renal sodium retention. Increased angio-
therapy. tensin II causes vasoconstriction and increased afterload.
In congestive heart failure, the compensatory mechanisms
Myocarditis often leads to persistent left ventricular that increase preload eventually cause a malcompensatory
dysfunction, but some patients may have improvement increase in afterload, in turn causing further decrease in
over time. Left ventricular function should be reassessed 3 stroke volume.
to 6 months after diagnosis and treatment. In the subacute and chronic stages of heart failure, neu-
rohormonal (adrenergic, angiotensin II) and other signal-
ing pathways lead to myocyte dysfunction and cell death.
Pathophysiology
Increased collagen production results in progressive cardiac
The hemodynamic, pathophysiologic, and biologic aspects fibrosis. Progressive myocardial dysfunction and remodeling
of heart failure must be appreciated to understand treat- are the natural history of untreated myocardial disease.
ment of dilated cardiomyopathy. Preload is the ventricu-
lar volume at the end of diastole (end-diastolic volume). Initial compensatory neurohormonal mechanisms lead to
Typically, when it is increased, stroke volume increases. The long-term mal-compensatory increases in afterload and
relationship of stroke volume to preload is illustrated by the subsequent decreased stroke volume.
5. H E A RT FA I LU R E A N D C A R D I O M YO PAT H I E S 71
CO
Sympathetic NS
Receptor
LVEDP
Renin
SV HR
Pulmonary Angiotensin I
congestion
ACE Further
myocardial
damage
Angiotensin II Receptor
Figure 5.4 Neurohormonal Response to
Decreased Myocardial Contractility. ACE
LV dilatation Na+ Aldosterone Afterload
indicates angiotensin-converting enzyme;
CO, cardiac output; HR, heart rate; LV,
left ventricular; LVEDP, left ventricular
end-diastolic pressure; NS, nervous system;
SV, stroke volume.
+ + +
ACE
Prostaglandins
Nitric oxide Inactive
Angiotensinogen II
peptide
72 C A R D I O L O GY
Nonpharmacologic management is essential and includes diuretics. Occasionally, a combination of thiazides and loop
sodium and fluid restriction, alcohol avoidance, daily diuretics is needed for severe fluid retention. The addition of
weight monitoring, and regular aerobic exercise. spironolactone can help in patients with hypokalemia and may
provide additional benefit by blocking aldosterone-mediated
Medications augment nonpharmacologic therapy.
effects.
ACE inhibitor use decreases mortality in patients with
moderate and severe heart failure, provides symptomatic Diuretics should be used for patients with heart failure and
improvement in patients with NYHA class II-IV heart volume overload.
failure symptoms, and reduces the need for hospitalization.
Diuretic doses should be minimized to avoid unwanted
metabolic adverse effects.
Angiotensin II receptor blockers provide hemodynamic
benefits similar to those of ACE inhibitors in patients with Drugs directly affecting myocardial contractility include
dilated cardiomyopathy. They can be used in patients who have digoxin, phosphodiesterase inhibitors (milrinone), and
cough and angioedema with use of ACE inhibitors because -agonists (dopamine and dobutamine). Digoxin provides
they do not inhibit the breakdown of bradykinin (the cause symptomatic relief when the ejection fraction is less than
of cough and angioedema). They are less beneficial than ACE 40%, but it does not improve survival. It is useful for ven-
inhibitors in the reverse remodeling of the myocardium, and tricular rate control and atrial fibrillation and in patients who
thus they remain second-line treatment. are symptomatic despite treatment with ACE inhibitors and
-blockers. Because digoxin is excreted by the kidneys, dosage
Angiotensin II receptor blockers provide hemodynamic must be decreased in older patients and patients with renal
benefits similar to those of ACE inhibitors. dysfunction. Because of drug-drug interactions, digoxin dos-
age should be decreased with concomitant administration of
They remain second-line agents for patients who cannot
amiodarone, verapamil, and quinidine. Short-term parenteral
tolerate ACE inhibitors.
inotropic agents (milrinone and dobutamine) may improve
symptoms, but long-term use increases mortality, and there-
-Adrenergic blockers (-blockers) improve symptoms fore these drugs should be used transiently in the hospital for
and ejection fraction and decrease hospitalizations and mor- low-output states and occasionally for palliative purposes in
tality in patients with systolic heart failure. They may have refractory end-stage heart failure.
unwanted hemodynamic effects in the acute setting (negative
inotropic effects, attenuation of heart rate response that may Digoxin, phosphodiesterase inhibitors (milrinone), and
be maintaining cardiac output in the setting of reduced stroke -agonists (dopamine and dobutamine) directly affect
volume), but they provide long-term benefit by modifying the myocardial contractility.
unfavorable biologic effects of enhanced adrenergic tone. This
benefit may take up to 6 months to observe. These drugs are Digoxin dosage needs to be decreased in azotemic and
most useful for patients with asymptomatic left ventricular older patients.
dysfunction after myocardial infarction and NYHA class II or
III symptoms. They can be given cautiously to patients with Aldosterone antagonists may provide additional benefit
class IV symptoms but should not be given to patients with by inhibiting fibrosis and combating mechanical and electri-
substantial volume overload and cardiogenic shock. Initial cal remodeling. Significant survival benefit has been shown in
dosing should be low, with close clinical follow-up. Upward patients with NYHA class III-IV heart failure. Eplerenone,
titration of the -blocker dose should be slow and cautious. The a selective aldosterone inhibitor, provides survival benefit
likelihood of patients continuing treatment with -blockers is at 30 days and 1 year in patients after infarction and who
much higher when treatment is initiated during a hospitaliza- have left ventricular dysfunction and either heart failure or
tion for heart failure. Well-studied -blockers with established diabetes. However, eplerenone has a considerable risk of
benefit for patients with heart failure include metoprolol suc- hyperkalemia and thus must be given carefully with cau-
cinate, carvedilol, and bisoprolol. tious follow-up, avoidance of nonsteroidal anti-inflammatory
drugs, and prompt attention to illnesses predisposing patients
-Blockers are effective and essential therapy in patients to dehydration.
with dilated cardiomyopathy.
Aldosterone antagonists can be used in highly symptomatic
Initiation of -blocker therapy should be avoided in heart patients already receiving baseline therapy or in patients
failure when there is substantial volume overload. with either heart failure or diabetes early after infarction.
Diuretics are part of the routine management of symptoms Patients with hyperkalemia or renal dysfunction should
and signs of systemic and pulmonary congestion. Diuretic not receive these drugs.
doses should be minimized when possible because of associ-
ated neurohormonal activation and electrolyte imbalance. High-dose nitrates and hydralazine in combination pro-
Fluid overload can be treated initially with thiazide or loop vide symptomatic improvement and improved mortality in
5. H E A RT FA I LU R E A N D C A R D I O M YO PAT H I E S 73
patients with heart failure, but this approach is inferior to Implanted defibrillators improve survival in patients with
ACE inhibitors when used alone. It is used in patients who both ischemic and nonischemic dilated cardiomyopathy
are unable to tolerate ACE inhibitors or angiotensin recep- who have ejection fractions less than 35% despite optimal
tor blockers because of renal insufficiency or hyperkalemia. medical therapy.
The combination has been shown to increase survival in
African-American patients when given as adjunctive therapy
to ACE inhibitors and -blockers. Cardiac Replacement Therapy
Heart transplant is the procedure of choice for patients
The combination of nitrates and hydralazine with dilated cardiomyopathy and severe, refractory symp-
improves symptoms and mortality, especially in toms. With a successful transplant, the 1-year survival rate
the African-American population with dilated can exceed 90%. Early referral to a heart transplant center
cardiomyopathy. is recommended for patients with refractory heart failure.
Long-term complications include rejection, infection, hyper-
Amlodipine and felodipine are safe in patients with tension, hyperlipidemia, malignancy, and accelerated coro-
dilated cardiomyopathy. They can be used to treat hyperten- nary vasculopathy. Donor availability is the major limiting
sion that persists despite optimal dosages of ACE inhibitors factor. In selected patients, left ventricular assist devices have
and -blockers, but they do not provide a survival benefit. now been approved by the US Food and Drug Administration
First-generation calcium channel blockers (verapamil, dilti- and are used either as a bridge to transplant or as final (destina-
azem, nifedipine) are contraindicated because of their negative tion) therapy.
inotropic effects.
The procedure of choice for patients with severely
First-generation calcium channel blockers (verapamil, symptomatic dilated cardiomyopathy despite optimal
diltiazem, nifedipine) are contraindicated because of their medical management is heart transplant.
negative inotropic effects. With a successful transplant, the 1-year survival rate can
exceed 90%.
Anticoagulation with warfarin is recommended for
patients in atrial fibrillation and those with intracardiac
thrombus or a history of systemic or pulmonary throm-
boembolism. Retrospective studies have suggested that aspi- H E A RT FA I LU R E W I T H P R E S E RVE D
rin may diminish the benefits of ACE inhibitors by blocking E J E C T I O N F R AC T I O N
prostaglandin-induced vasodilatation. An increased incidence
of hospitalizations for heart failure in patients with dilated Approximately half of hospitalized patients with newly diag-
cardiomyopathy receiving aspirin was also observed. The nosed heart failure have a normal ejection fraction. Many
most common recommendation is to use low-dose aspirin in of these patients have contractile abnormalities that could
patients with heart failure and coronary artery disease. be identified by more sophisticated evaluation techniques,
but ejection fraction is the most widely available measure of
Anticoagulation with warfarin is recommended in patients systolic function and remains the standard. This is a hetero-
with atrial fibrillation, intracardiac thrombus, or a history geneous group of disorders and includes hypertrophic and
of thromboembolism. restrictive cardiomyopathies, infiltrative cardiac disorders, and
constrictive pericarditis.
Aspirin therapy (low dose) should be reserved for patients
with heart failure and coronary artery disease. Approximately half of patients with newly diagnosed heart
failure have a normal ejection fraction.
Device Therapy
Implanted defibrillators improve survival when used at least Many patients have a history of hypertension. Some have
40 days after a myocardial infarction in patients with ischemic fairly normal diastolic filling properties at rest, but exertional
and nonischemic dilated cardiomyopathies who have ejection hypertension, ischemia, or both cause deterioration of diastolic
fractions less than 35% despite optimal medical therapy. They filling properties, resulting in increased filling pressure. Others
should be offered to patients who have a reasonable functional have abnormal baseline diastolic compliance with superimposed
status with at least 1 year of survival. Patients in sinus rhythm volume overload, which increases diastolic filling pressures.
with ventricular dyssynchrony may benefit from biventricular Other patients have exuberant heart rate responses to exercise
pacing (cardiac resynchronization therapy). Current implan- with inadequate diastolic filling periods, and others rely on the
tation criteria are sinus rhythm, QRS duration more than 120 atrial contribution to ventricular filling and suffer when atrial
milliseconds, NYHA class III-IV, ejection fraction less than fibrillation develops. Some have low output due to severe regur-
35%, and optimal medical management. Cardiac resynchroni- gitant valve disease (including severe tricuspid regurgitation) or
zation therapy results in improvement in symptoms, exercise bradycardia. Severe occult renal insufficiency is also a common
capacity, and left ventricular ejection fraction and survival in finding in this condition. It is important to try to understand
well-selected patients. the mechanism of diastolic dysfunction in any given patient to
74 C A R D I O L O GY
tailor the most effective treatment, which might include some The classic presentation of hypertrophic cardiomyopathy is
combination of antihypertensive or coronary revascularization the triad of angina, syncope, and dyspnea.
strategies, diuretic treatment, ventricular rate slowing or support
The prognosis for older patients may be better than that for
(pacemaker), restoration of sinus rhythm, valvular intervention,
younger patients.
or renal replacement therapy. Morbidity and mortality in this
group of patients are high, approaching the rates in patients Affected patients have a 1.5% per-year risk of progression
with reduced ejection fraction. to dilated cardiomyopathy.
H Y P E RT R O P H I C C A R D I O M YO PAT H Y PAT H O P H YS I O L O GY
Signs and symptoms of hypertrophic cardiomyopathy are
Hypertrophic cardiomyopathy is a rare (approximately 0.2% caused by 4 major abnormalities: diastolic dysfunction, left
prevalence in the general population) heterogeneous group ventricular outflow tract obstruction, mitral regurgitation,
of disorders characterized by increased thickness of the ven- and ventricular arrhythmias.
tricle and preserved ejection fraction. The hypertrophy may Diastolic dysfunction is caused by many mechanisms,
be regional (involving the septum, mid left ventricle, or apex) including marked abnormalities in calcium metabolism
or concentric. Obstruction in the left ventricular outflow tract (abnormal ventricular relaxation), high afterload due to
or mid-ventricular cavity may occur. Diagnosis is based on left ventricular tract obstruction (also delays ventricular
increased myocardial wall thickness on echocardiogram in the relaxation) and severe hypertrophy and increased muscle
absence of an underlying cause such as hypertension, aortic mass (decreased compliance). Diastolic dysfunction leads
stenosis, chronic renal failure, or infiltrative disease. Because to increased left ventricular diastolic pressure, angina, and
of its hereditary nature, first-degree relatives of patients should dyspnea. Coronary microvascular dysfunction also contrib-
be screened, and genetic counseling is advised for patients con- utes to angina and dyspnea. In many patients, dynamic left
sidering childbearing. ventricular tract obstruction is caused by the hypertrophied
septum encroaching into the left ventricular outflow tract.
Hypertrophic cardiomyopathy is a heterogeneous family Subsequently, the anterior leaflet of the mitral valve is sucked
of genetic disorders characterized by increased ventricular in (systolic anterior motion), and left ventricular outflow
thickness. tract obstruction is created. Because of this pathophysiologic
Diagnosis is based on increased myocardial wall thickness process, dynamic outflow tract obstruction increases dramati-
in the absence of a cause on the echocardiogram. cally with decreased preload, decreased afterload, or increased
contractility. Systolic anterior motion of the mitral valve dis-
torts the mitral valve apparatus during systole and may cause
considerable mitral regurgitation. Thus, the degree of mitral
S Y M P TO M S regurgitation is also dynamically influenced by the degree of
left ventricular outflow tract obstruction. Patients with severe
Hypertrophic cardiomyopathy appears to have a bimodal mitral regurgitation usually have severe symptoms of dyspnea.
distribution of age at presentation. Affected young males Cellular disorganization leads to abnormalities in the conduc-
(typically teens or early 20s) often present with syncope tion system; thus, patients are prone to ventricular arrhyth-
and sudden death. Recently, an X-linked variant known as mias. Frequent ventricular arrhythmias may cause sudden
LAMP2 cardiomyopathy (Danon disease) was described in death or syncope.
younger patients. Affected older patients (sixth and seventh
decades of life) typically present with shortness of breath and Diastolic dysfunction is caused by abnormal ventricular
angina and may have a better prognosis than young patients. relaxation or decreased compliance.
The classic presentation in the younger group is a young ath-
lete undergoing a physical examination found to have a heart Abnormal ventricular relaxation may be due to abnormal
murmur or left ventricular hypertrophy on electrocardiog- calcium metabolism or high afterload (due to outflow tract
raphy. The classic presentation in the older group is an older obstruction).
woman who has development of pulmonary edema after non-
cardiac surgery and worsening with diuresis, afterload reduc- Left ventricular outflow tract obstruction and mitral regur-
tion, and inotropic support (due to worsening dynamic left gitation are caused by distortion of the mitral valve apparatus
ventricular outflow tract obstruction). The classic symptom (systolic anterior motion), and they are dynamically influ-
triad is syncope, angina, and dyspnea. The symptoms are simi- enced by preload, afterload, and contractility.
lar to those of valvular aortic stenosis. The per-year frequency
of evolution from hypertrophic to dilated cardiomyopathy is
E X A M I NAT I O N
1.5%. This may reflect either the natural history or a super-
imposed secondary process such as ischemia. The treatment The carotid artery upstroke and left ventricular impulse are
of a burnt-out hypertroph is then the same as that of other abnormal in patients with hypertrophic cardiomyopathy. The
dilated cardiomyopathies. carotid artery upstroke is more rapid than that in aortic stenosis.
5. H E A RT FA I LU R E A N D C A R D I O M YO PAT H I E S 75
If left ventricular outflow tract obstruction is extensive, the the murmur intensity and the pulse volume increase with the
carotid artery upstroke has a bifid quality. In the setting of beat following a premature ventricular contraction.
considerable left ventricular hypertrophy, the left ventricular
impulse is sustained and there is often a palpable a wave. The The diagnosis of hypertrophic cardiomyopathy is suspected
first heart sound is normal, but the second heart sound is para- by palpating a sustained left ventricular impulse and rapid
doxically split. Patients with excessive left ventricular outflow upstroke of the carotid artery.
tract obstruction may have a triple apical impulse and a loud
systolic ejection murmur. The murmur changes in intensity The outflow murmur intensity and carotid upstroke change
with changes in loading conditions (Box 5.5). A holosystolic with changes in loading conditions of the heart.
murmur of mitral regurgitation may be present; it increases in
intensity with increases in the dynamic left ventricular outflow
tract obstruction. Maneuvers affect the mitral regurgitant D I AG N O S T I C T E S T I N G
murmur of hypertrophic obstructive cardiomyopathy differ-
ently than other mitral regurgitant murmurs. When mitral A marked left ventricular hypertrophy pattern on electro-
regurgitation is not due to hypertrophic obstructive cardio- cardiography (Figure 5.6) is usually seen in patients with
myopathy, the murmur increases with increasing afterload and hypertrophic cardiomyopathy, whereas patients with apical
varies little with changes in contractility and preload. When hypertrophy have deep, symmetric T-wave inversions across
mitral regurgitation is due to hypertrophic cardiomyopathy, the precordium (Figure 5.7). Electrocardiographic abnor-
increased afterload decreases the dynamic left ventricular out- malities may precede echocardiographic abnormalities; thus,
flow obstruction and thus the degree of mitral regurgitation. surveillance echocardiography is appropriate in patients with
In patients with hypertrophic cardiomyopathy with obstruc- suspicious electrocardiographic results.
tion, the intensity of the ejection murmur increases, whereas
the arterial pulse volume decreases on the beat following a pre- In hypertrophic cardiomyopathy, electrocardiography
mature ventricular contraction (the Brockenbrough sign) as shows marked left ventricular hypertrophy.
a result of postectopic increased contractility and decreased
afterload, resulting in more dynamic obstruction. These Echocardiography shows severe hypertrophy of the myo-
changes differ from those in patients with fixed left ventricular cardium (left ventricular wall thickness >16 mm in diastole)
outflow tract obstruction (eg, aortic stenosis) in whom both without any other identified cause. Hypertrophy may be in
any part of the myocardium. Doppler echocardiography can
be used to diagnose left ventricular outflow tract obstruction,
measure its severity, and detect mitral regurgitation. Cardiac
catheterization is no longer necessary to diagnose dynamic left
Box 5.5 DYNAMIC LEFT VENTRICULAR OUTFLOW ventricular outflow tract obstruction.
TRACT OBSTRUCTION
Presence of outflow tract obstruction, its severity, and
Increased obstruction presence of mitral regurgitation may be assessed with
Decreased afterload echocardiography, and cardiac catheterization is no longer
Amyl nitrite needed.
Vasodilators
Increased contractility Patients with hypertrophic cardiomyopathy may have
Postpremature ventricular contraction beat sudden death. Because of the strong association between ven-
Digoxin tricular arrhythmias and sudden death, 48- to 72-hour Holter
Dopamine monitoring is recommended for all patients with hypertrophic
Decreased preload cardiomyopathy. Predictors of sudden death include a per-
Squat-to-stand sonal or family history of sudden death, severe left ventricular
Nitrates hypertrophy, ventricular tachycardia on Holter monitoring
Diuretics or electrophysiologic study, and history of syncope. Genetic
Valsalva maneuver (strain phase) markers may identify patients with a strong propensity for
Decreased obstruction sudden death. In some patients, carefully supervised stress
Increased afterload testing may be indicated to search for induced ventricular
Handgrip tachycardia, to determine exercise tolerance, and to evaluate
Stand-to-squat the variables contributing to symptoms.
Decreased contractility
-Adrenergic blockers Predictors of sudden death in hypertrophic
Verapamil cardiomyopathy are personal or family history of sudden
Disopyramide death, history of syncope, ventricular tachycardia on
Increased preload Holter monitoring or electrophysiologic study, and severe
Fluids left ventricular hypertrophy.
76 C A R D I O L O GY
I aVR V1 V4
II aVL V2 V5
III aVF V3 V6
Figure 5.6 Electrocardiogram in Hypertrophic Cardiomyopathy. Marked left ventricular hypertrophy is noted.
I aVR V1 V4
II aVL V2 V5
III aVF V3 V6
Figure 5.7 Electrocardiogram in Apical Hypertrophic Cardiomyopathy. Deep, symmetric T-wave inversions are shown in precordial leads.
5. H E A RT FA I LU R E A N D C A R D I O M YO PAT H I E S 77
48- to 72-Hour Holter monitoring is recommended for all Avoid certain
patients with hypertrophic cardiomyopathy. medications
T R E AT M E N T Screen
relatives
Symptomatic Patients
For symptomatic patients, initial treatment is with drugs that Risk for EP
decrease contractility in an attempt to decrease left ventricu- sudden death? evaluation
lar outflow tract obstruction (Figure 5.8). The most effective
medication is a high dose of -blockers (equivalent of >240
mg propranolol/day). Although verapamil may be used if
-adrenergic blockade fails, it may cause sudden hemodynamic Holter-TMET VT
deterioration in patients with high resting left ventricular
outflow tract gradients because of its vasodilating properties.
Disopyramide may improve symptoms by decreasing left ven-
tricular outflow tract obstruction, but anticholinergic adverse
effects limit its use. All drugs that reduce afterload or pre- Yearly
load and those that increase contractility must be avoided in reassessment
patients with hypertrophic cardiomyopathy. Diuretics may be
cautiously used for volume-overloaded states.
Figure 5.9 Treatment of Asymptomatic Hypertrophic Cardiomyopathy.
Treat symptomatic patients initially with -blockers. EP indicates electrophysiologic; TMET, treadmill exercise test; VT,
ventricular tachycardia.
Verapamil may be used if -blockade fails, but it may cause
sudden hemodynamic collapse in patients with high resting
outflow tract gradients and must be used cautiously. nonsustained ventricular tachycardia is controversial (Figure
5.9). No antiarrhythmic agent is uniformly effective, and any
Avoid any drug that reduces preload or afterload or agent may make the arrhythmia worse. In select patients with
increases contractility. multiple risk factors for sudden death, empiric amiodarone
or an implantable cardiac defibrillator might be chosen. In
Asymptomatic Patients patients who have had an out-of-hospital arrest, the treatment
of choice is an implantable cardiac defibrillator.
Asymptomatic patients should be assessed for risk of sud-
den cardiac death. Treatment of asymptomatic patients with
An implantable cardiac defibrillator is the treatment of
choice for patients with out-of-hospital arrest and for
certain patients at high risk for sudden cardiac death.
High-dose
Verapamil or -blocker
disopyramide R E S T R I C T I VE C A R D I O M YO PAT H Y
78 C A R D I O L O GY
cardiomyopathy. Familial cases, often with associated periph- D I AG N O S I S
eral myopathy, have been reported. Endomyocardial fibrosis
Restrictive cardiomyopathy is diagnosed with echocardiog-
is probably an end stage of eosinophilic syndromes in which
raphy. Typical findings are normal left ventricular cavity size,
there is intracavitary thrombus filling of the left ventricle. This
preserved ejection fraction, and marked biatrial enlargement.
restricts filling and causes increased diastolic pressures. Fibrosis
In the setting of right heart failure, the inferior vena cava is
also may involve the mitral valve, causing severe mitral regur-
enlarged. In amyloid heart disease, echocardiography demon-
gitation. There may be 2 different forms of endomyocardial
strates thickened myocardium with a scintillating appearance,
fibrosis: active inflammatory eosinophilic myocarditis (tem-
a pericardial effusion, and thickened regurgitant valves. In
perate zones) and chronic endomyocardial fibrosis (tropical
endomyocardial fibrosis, there is an apical thrombus (with-
zones).
out underlying apical akinesis) or thickening of the endocar-
dium under the mitral valve, which often tethers the valve,
The 2 major categories of primary restrictive causing mitral regurgitation. Other causes of restrictive car-
cardiomyopathy are idiopathic and endomyocardial diomyopathy have nonspecific echocardiographic features.
fibrosis. Cardiac catheterization shows increase and end-equalization
Fibrosis may involve the mitral valve, leading to mitral of all end-diastolic pressures. A typical square-root sign or
regurgitation. dip-and-plateau pattern consistent with early rapid filling is
present. Endomyocardial biopsy usually is not helpful, except
Infiltration diseases involving the myocardium (eg, amy- to confirm the diagnosis of amyloidosis.
loidosis) have a presentation and pathophysiology similar to
those of primary restrictive cardiomyopathy. Signs and symp- Restrictive cardiomyopathy is diagnosed with
toms similar to those of restrictive cardiomyopathy also may echocardiography.
develop after radiation therapy and anthracycline chemother-
apy. Although other infiltrative diseases (eg, sarcoidosis, hemo-
chromatosis) initially may mimic restrictive cardiomyopathy,
they usually progress to a dilated cardiomyopathy by the time T R E AT M E N T
they cause cardiac symptoms. Treatment of idiopathic restrictive cardiomyopathy is usually
symptom-based. Diuretics decrease filling pressures and give
Infiltrative diseases (eg, amyloidosis) may cause restrictive symptomatic relief, but these effects may be at the expense
cardiomyopathy. of further decreasing cardiac output. Heart transplant is the
Radiation therapy and anthracycline therapy may cause only proven therapy for patients with severe restrictive car-
cardiac syndromes with signs and symptoms similar to diomyopathy. Corticosteroids are appropriate during the early
those of restrictive cardiomyopathy. stages of eosinophilic endocarditis. Endomyocardial fibrosis
can be surgically resected and the mitral valve can be replaced,
although mortality is significant.
S I G NS A N D SY M P TO M S
Patients with restrictive cardiomyopathy usually present with Treatment of idiopathic restrictive cardiomyopathy is
symptoms of right heart failure such as edema, dyspnea, and symptom-based.
ascites. Atrial arrhythmias due to passive atrial enlargement Diuretics decrease filling pressures.
are frequently present, and the patient may present with atrial
fibrillation. Jugular venous pressure is almost always increased, Heart transplant is the only proven therapy for severe
with rapid x and y descents. The precordium is quiet, and restrictive cardiomyopathy.
heart sounds are soft. There may be an apical systolic murmur
of mitral regurgitation and a left sternal border murmur of It is important to differentiate restrictive cardiomyopathy
tricuspid regurgitation. A third heart sound may be present. from constrictive pericarditis. Both have similar presentations
Dullness at the bases of the lungs is consistent with bilateral and findings on clinical examination and diagnostic studies.
pleural effusions. Electrocardiography is usually low or normal However, in constrictive pericarditis, pericardiectomy pro-
voltage with atrial arrhythmias. Chest radiography may show duces symptomatic improvement and, frequently, survival.
pleural effusions with a normal cardiac silhouette or atrial Therefore, exploratory thoracotomy may be indicated in
enlargement. patients with normal left ventricular systolic function, large
atria, and severe increase of diastolic filling pressures if doubt
Restrictive cardiomyopathy frequently presents as right remains after anatomical (computed tomography or magnetic
heart failure with dyspnea, edema, and ascites. resonance imaging) and other tests (echocardiography, car-
diac catheterization).
Atrial arrhythmias are common.
Jugular venous pressure is increased, with rapid x and y Differentiate restrictive cardiomyopathy from constrictive
descents. pericarditis.
5. H E A RT FA I LU R E A N D C A R D I O M YO PAT H I E S 79
6.
ISCHEMIC HEART DISEASE
Abhiram Prasad, MD
Ischemic heart disease may be asymptomatic or present with Smoking more than doubles the risk of ischemic heart
stable angina, nonST-elevation acute coronary syndrome, disease and increases mortality by 50%. The relative risk of
ST-elevation myocardial infarction (MI), or sudden death. smokers who quit smoking decreases rapidly, approaching the
Ischemic heart disease causes nearly 800,000 deaths annually. levels of nonsmokers within 2 to 3 years. Plasma levels of total
Notably, about a third of deaths annually in the United States and LDL cholesterol are important risk factors for ischemic
are due to MI. Primary prevention and new treatments have heart disease. A 1% decrease in total serum cholesterol reduces
led to a substantial decrease in death from acute MI since 1970 risk by 2% to 3%. Lowering the LDL level slows progression
(Figure 6.1). and may result in regression of coronary atherosclerosis.
Lowering the LDL level also prevents coronary events, possi-
bly due to atherosclerotic plaque stabilization.
P R E VE N T I O N For every 1-mm-Hg decrease in diastolic blood pressure,
the risk for MI is reduced by 2% to 3%. The risk for MI is
The Framingham risk score is the most commonly used model decreased 35% to 55% with maintenance of an active vs a
to calculate the 10-year risk for development of ischemic heart sedentary lifestyle. Adjusted mortality rates for ischemic
disease (http://hp2010.nhlbihin.net/atpiii/calculator.asp). heart disease are 2 to 3 times higher in men and 3 to 7 times
The score is derived from a the patients risk factors: age, sex, higher in women with diabetes mellitus compared with the
low-density lipoprotein (LDL) cholesterol level, high-density rates in men and women without diabetes. Heavy alcohol
lipoprotein (HDL) cholesterol level, systemic blood pressure, use increases the risk of ischemic heart disease, but moderate
diabetes mellitus, and smoking history (Circulation. 1998 consumption decreases risk. Metabolic syndrome is present in
May 12;97[18]:183747). 20% of the US population, and it is associated with a twofold
Ischemic heart disease risk factors for which interventions to threefold increase in mortality from cardiovascular dis-
have been proved to reduce cardiac events include tobacco ease. Aspirin is recommended for persons at intermediate risk
use, serum LDL cholesterol level, serum HDL level, and for ischemic heart disease and at low risk for bleeding. This
80
40 ischemic events after MI more than would be expected from
their effect on atherosclerosis progression alone, possibly due to
stabilization of lipid-rich, rupture-prone plaques. Statins decrease
30
overall mortality by 30% and coronary event-related mortality by
% Discharged Dead
Age 65 Years 42% in patients with a prior MI and high cholesterol (>220 mg/
20 dL). Statins reduce the risk for fatal heart disease or recurrent MI
by 24% in patients with a prior MI and average levels of choles-
terol (total cholesterol <240 mg/dL; LDL, >125 mg/dL).
10 The following are indications for cholesterol-lowering
Age 45-64 Years therapy:
0
1970 1975 1980 1985 1990 1995 2000 2005 1. Known coronary artery disease (or diabetes mellitus,
peripheral vascular disease, multiple risk factors that
Year confer a 10-year risk for coronary artery disease of more
than 20% calculated using a modified Framingham risk
Figure 6.1 Case-Fatality Rate for Acute Myocardial Infarction in the
United States, 19702004. (Adapted from National Heart, Lung,
score) and LDL level more than 100 mg/dL. Goal LDL
and Blood Institute. Morbidity and mortality: 2007 chart book on level is less than 100 mg/dL (optimal <70 mg/dL)
cardiovascular, lung, and blood diseases. Bethesda [MD]: National
Institutes of Health; 2007.) 2. Two or more risk factors for coronary artery disease and
level more than 130 mg/dL
includes patients with an absolute risk of more than 15% over 3. 0 or 1 risk factor for coronary artery disease and LDL level
10 years by Framingham score or patients with diabetes with a more than 160 mg/dL
risk of more than 10% over 10 years. The role of aspirin in the
primary prevention of stroke or overall cardiovascular mortal- Therapeutic targets include treatment of metabolic
ity is uncertain. Estrogen replacement therapy is not indicated syndrome, increased triglyceride levels, and low HDL
in women with cardiovascular disease, and it may be harmful. level. Therapeutic lifestyle changes, including a low-fat,
low-cholesterol diet, weight management, and physical
Smoking is a major risk factor for ischemic heart disease, and activity are essential for cholesterol lowering. Soluble fiber
smoking cessation leads to a rapid reversal in imposed risk. (1025 g/day) and plant stanols or sterols (2 g/day) should be
considered as therapeutic options.
Management of hyperlipidemia and hypertension are Novel risk factors proposed for ischemic heart disease,
essential for reducing the risk of ischemic heart disease. especially in patients who do not have the conventional risk
Aspirin is recommended for patients at high or factors, include increased blood levels of lipoprotein(a),
intermediate risk of ischemic heart disease. Estrogen homocysteine, small dense LDL particle (phenotype B), and
therapy should not be used in women with cardiovascular fibrinogen. Additionally, acute and chronic inflammation
disease because it may be harmful. and possibly lifetime exposure to pathogens (eg, Chlamydia,
cytomegalovirus, and Helicobacter) have been proposed as
Secondary prevention aims to prevent recurrent ischemic potential factors in the pathophysiology of atherosclerosis.
events in patients with known ischemic heart disease. Smoking
cessation and optimum treatment of hyperlipidemia, hyperten- Secondary prevention refers to therapeutic interventions to
sion, and diabetes mellitus are essential. Statin drugs reduce prevent recurrent ischemic events.
Increased LDL cholesterol level Age Inflammatory markers (eg, C-reactive protein)
Low HDL cholesterol level Male sex Small, dense LDL
Cigarette smoking Family history of premature CADa Lipoprotein (a)
Hypertension Homocysteine
Diabetes mellitus Fibrinogen
Sedentary lifestyle
Obesity
Metabolic syndrome
Stress & depression
Socioeconomic factors
Abbreviations: CAD, coronary artery disease; HDL, high-density lipoprotein; LDL, low-density lipoprotein.
a
Age at onset less than 55 years in men and less than 65 years for primary relatives.
6. I S C H E M I C H E A RT D I S E A S E 81
Considerable attempts at risk factor modification (diabetes The most frequent site of atherosclerotic plaque disrup-
mellitus, tobacco use, hyperlipidemia, hypertension, tion is lipid-laden coronary artery lesions with mild to moder-
dietary changes, weight management, physical activity) are ate angiographic stenosisnot severely stenotic lesions. The
warranted. culprit lesion is at a site with less than 50% stenosis in up to
two-thirds of cases of unstable angina or MI.
Statins reduce ischemic heart diseaserelated events.
Modifiable (and possibly some nonmodifiable) risk factors
lead to chronic endothelial injury that may progress
through endogenous changes to more advanced changes in
M E C H A N I S M O F AT H E R O S C L E R O S I S
the coronary vessel wall.
The response-to-injury hypothesis is the most prevalent expla- These changes may lead to unstable angina or MI.
nation of atherosclerosis. The stages of the process are as
follows: The most frequent site of plaque disruption is an artery
Stage I: Chronic injury to the arterial endothelium due to with less than 50% stenosis.
risk factors such as hypercholesterolemia, hypertension, diabetes
mellitus, tobacco abuse, inflammation, and possibly infections C H R O N I C S TA B L E A N G I N A
Stage II: Release of toxic products by macrophages, lead-
ing to platelet adhesion and smooth muscle cell migration and
PAT H O P H YS I O L O GY
proliferation resulting in formation of fibrointimal lesions or
lipid plaques A mismatch between myocardial oxygen demand and supply
Stage III: Disruption of the lipid-rich plaque leads to causes myocardial ischemia. Demand is determined by heart
thrombus formation. Acute coronary syndrome (unstable rate, afterload, contractility, and wall tension. With a dilated,
angina or myocardial infarction) results from thrombus orga- poorly contractile left ventricle, the contribution of wall tension
nization and atherosclerosis or vessel occlusion (Figure 6.2). to myocardial oxygen consumption outweighs the other factors.
A
Stage I Risk factors PLT
LDL
IL-1 Monocytes
Endothelial ET +
injury
+
Big ET () EDRF Adhesion
ET
SMC +
B
Stage II
82 C A R D I O L O GY
Normally, coronary blood flow can increase up to 5 times Silent Ischemia
to meet effort-related increases in myocardial oxygen demands.
The double product [(heart rate) u (systolic blood pressure)] Silent ischemia is common in patients with chronic stable cor-
is a useful index for quantifying myocardial oxygen demand. onary artery disease, with unstable angina, or after myocardial
Ischemia occurs when flow reserve is inadequate, usually the infarction. Patients with diabetes may have silent ischemia,
result of fixed coronary artery disease. possibly due to neuropathy. Silent ischemia is also more com-
Restriction of resting blood flow sufficient to cause rest- mon in the elderly. It is defined as the presence of dynamic
ing ischemia does not occur unless vessel stenosis is more ST-segment depression in the absence of symptoms. Medical
than 95%. However, decreased overall flow reserve begins therapy is similar to that for symptomatic ischemia. Whether
to occur at about 60% vessel stenosis, and symptoms of percutaneous coronary intervention or coronary artery bypass
exercise-induced ischemia may begin. The temporal sequence grafting should be performed for silent ischemia in the absence
of events during ischemia are diastolic dysfunctionoabnormal of other markers of high risk is unknown. The prognosis for
perfusionoregional wall motion abnormalitiesoelectrocar- this condition is the same as that for symptomatic ischemia.
diographic (ECG) changesopain.
N O N I N VA S I V E T E S T I N G F O R I S C H E M I A
Mismatched oxygen demand and supply lead to myocardial Ancillary tests for ischemic heart disease include measure-
ischemia. ment of left ventricular function, stress testing, and coronary
Heart rate, afterload, contractility, and wall tension are the angiography.
factors that determine myocardial oxygen consumption
and demand. Left Ventricular Function
When the left ventricle is dilated and contracts poorly, Left ventricular function is the most important predictor
wall tension plays a larger role in myocardial oxygen of prognosis and should be measured in all patients with
consumption than other factors. 2-dimensional echocardiography, radionuclide angiography,
or left ventricular angiography.
Vessel stenosis >95% leads to resting ischemia, but
decreased flow reserve begins with about 60% stenosis,
leading to exertional ischemia. Stress Testing
Exercise stress testing to identify ischemia is performed using
ECG monitoring, thallium or technetium-sestamibi scan-
C L I N I C A L P R E S E N TAT I O N
ning (to assess myocardial perfusion), or echocardiography
Symptomatic Chronic Stable Coronary Artery Disease (to assess left ventricular function). Heart rate, blood pressure,
and the onset of subjective symptoms are monitored.
Typical angina is characterized by retrosternal pain occurring The stress ECG is positive for ischemia if there is a flat or
with cardiovascular stress and relieved by rest or nitroglycerin. downsloping ST-segment depression of 1 mm or more with
Atypical angina is defined by the presence of 2 of these 3 fea- exertion, whereas it is uninterpretable when there is more than
tures. Noncardiac chest pain is defined by the presence of 1 or 1 mm of resting ST-segment depression, left bundle branch
none of these features. block, left ventricular hypertrophy, paced rhythm, or preexci-
Angina may be precipitated by any activity that increases myo- tation (Wolff-Parkinson-White syndrome). Digoxin therapy
cardial oxygen consumption. The pain has various descriptions results in an uninterpretable stress ECG. A stress imaging test
such as pressure, burning, stabbing, ache, hurt, or heaviness, or it (eg, sestamibi or echocardiography) is indicated in patients
may be described as shortness of breath. It can be substernal or epi- with an uninterpretable ECG.
gastric, and it may radiate to the neck, jaw, shoulder, back, elbow, or
wrist. In stable angina, the pain lasts 2 to 30 minutes and is usually Exercise stress testing identifies ischemia and is
relieved by rest. Uncommon findings that may occur with ische- used with ECG monitoring, perfusion scanning, or
mia include a fourth heart sound and mitral regurgitant murmur echocardiography.
due to papillary muscle dysfunction. ST-segment depression may
be found on the ECG, indicating subendocardial ischemia. Careful attention to patient and ECG characteristics is
important for determining whether the stress ECG is
Angina can have typical or atypical symptoms and may be interpretable.
described in various ways by patients. Stress imaging should be used in patients who have or are
Stable angina pain is usually relieved by rest or anticipated to have an uninterpretable stress ECG.
nitroglycerin.
Treadmill exercise testing can identify high-risk patients.
A fourth heart sound and mitral regurgitant murmur due A patient is at high risk if the following results are obtained:
to papillary muscle dysfunction are uncommon.
Subendocardial ischemia may be manifested by 1. A positive ECG in stage I of the Bruce protocol or at a
ST-segment depression on ECG. heart rate less than 120 beats per minute
6. I S C H E M I C H E A RT D I S E A S E 83
2. ST-segment depression more than 2 mm of ischemia need to be localized (for planning revasculariza-
tion procedures).
3. ST-segment depression more than 6 minutes in duration
after stopping exercise
Only when the resting ECG is uninterpretable, the
4. Decrease in blood pressure ECG result is thought to be false-positive, or mapping of
ischemic regions is necessary should imaging stress testing
5. Multiple perfusion or wall motion defects (>25% of be used instead of ECG exercise stress testing.
segments with exercise) and an increase in left ventricular
end-systolic volume with exercise Pharmacologic stress tests are used for patients who can-
not exercise. These tests include the use of vasodilators such
Patients who achieve a good workload with appropri- as adenosine and dipyridamole (redistribute flow away from
ate blood pressure and heart rate responses without marked ischemic myocardium). The tests are generally performed with
ST-segment depression have an excellent prognosis; therefore, perfusion agents such as thallium or sestamibi. Alternatively,
medical management may be preferred in these patients. dobutamine is used as a chronotropic and inotropic agent
Imaging-based stress testing slightly increases the sen- to increase myocardial oxygen demand, and imaging is per-
sitivity and specificity of ECG exercise testing. In nuclear formed with echocardiography.
perfusion imaging, the tracer is injected at peak exercise
and labels areas of hypoperfusion as a defect or cold spot.
Pharmacologic stress testing is used when patients are
Scanning is repeated a few hours later at rest, and persis-
unable to exercise.
tent cold spots indicate infarction, whereas reperfused areas
indicate areas of inducible ischemia. In patients with left
bundle branch block or severe left ventricular hypertrophy, Stress tests should not be used for the diagnosis of ische-
thallium and sestamibi scanning give false-positive results mic heart disease in patients at high or low risk. Stress test-
during exercise stress. ing is appropriate for patients at intermediate risk to rule in
or rule out ischemia. The pretest probability of ischemic heart
Stress imaging modestly improves sensitivity and specificity disease is estimated using the following criteria: age (men >40
of ECG exercise stress testing. years and women >60 years), male sex, and symptom status (in
decreasing order of risk: typical angina, atypical angina, non-
Left bundle branch block and severe left ventricular cardiac chest pain, asymptomatic) (Table 6.1 and Figure 6.3).
hypertrophy lead to false-positive exercise thallium and
sestamibi stress tests. Stress testing of low-risk and high-risk patients is not
recommended.
In exercise echocardiography, 2-dimensional echocardiog-
raphy is performed at rest and at peak exercise. The test is pos-
Noninvasive Coronary Angiography
itive for ischemia if new regional wall motion abnormalities
develop, global systolic function decreases, or left ventricular Computed tomography and magnetic resonance imaging can
end-systolic volume increases. be used for noninvasive coronary angiography. However, the
diagnostic accuracy and applicability to clinical practice of
In exercise echocardiography, new regional wall motion these novel imaging methods have not been established, and
abnormalities, decline in global systolic dysfunction, or they should not be considered an alternative to invasive coro-
increased left ventricular end-systolic volume indicate nary angiography. Computed tomography requires the use of
ischemia. contrast media and produces suboptimal images in patients
with greater than mild coronary calcification or an irregular
Exercise stress testing should not be performed for patients rhythm. Noninvasive imaging may have a role in symptomatic
with high-risk unstable angina, patients who have had acute patients with a low to moderate pretest probability of ische-
MI in the prior 2 days, or patients with symptomatic severe mic heart disease given its high negative predictive value. A
aortic stenosis, uncontrolled heart failure, or uncontrolled useful role for noninvasive angiography is for imaging coro-
arrhythmia. Consider invasive angiography to define coronary nary anomalies. It is not recommended for screening asymp-
artery anatomy and evaluate the need for revascularization in tomatic patients or patients with established ischemic heart
patients with poor prognostic factors. disease. In addition, the clinical utility of coronary calcium
scores derived by computed tomography is not established.
Patients at high risk for an adverse event during exertion
should not undergo exercise stress testing. Noninvasive coronary imaging is useful for imaging
coronary artery anomalies.
Imaging stress tests are considerably more expensive
The clinical role of noninvasive angiography is otherwise
than the ECG exercise test and should not be routinely used
unclear.
instead of ECG exercise testing for diagnostic purposes,
except when the result of resting ECG is uninterpretable, The clinical use of coronary calcium scores has not been
the ECG result is possibly false-positive, or specific regions established.
84 C A R D I O L O GY
Table 6.1 PRETEST PROBABILITY OF CORONARY ARTERY DISEASE BY AGE, SEX, AND SYMPTOMS a
a
High indicates more than 90%; intermediate, 10% to 90%; low, less than 10%; very low, less than 5%.
Data from Gibbons RJ, Balady GJ, Bricker JT, Chaitman BR, Fletcher GF, Froelicher VF, et al; American College of Cardiology/American Heart Association
Task Force on Practice Guidelines (Committee to Update the 1997 Exercise Testing Guidelines). ACC/AHA 2002 guideline update for exercise testing: summary
article: a report of the American College of Cardiology/American Heart Association Task Force on Practice Guidelines (Committee to Update the 1997 Exercise
Testing Guidelines). Circulation. 2002 Oct 1;106(14):188392 and Gibbons RJ, Balady GJ, Bricker JT, Chaitman BR, Fletcher GF, Froelicher VF, et al; American
College of Cardiology/American Heart Association Task Force on Practice Guidelines. Committee to Update the 1997 Exercise Testing Guidelines. ACC/AHA
2002 guideline update for exercise testing: summary article. A report of the American College of Cardiology/American Heart Association Task Force on Practice
Guidelines (Committee to Update the 1997 Exercise Testing Guidelines). J Am Coll Cardiol. 2002 Oct 16;40(8):153140. Erratum in: J Am Coll Cardiol. 2006
Oct 17;48(8):1731.
6. I S C H E M I C H E A RT D I S E A S E 85
A stepwise approach should be used when introduc- does not occur with the longer-acting calcium channel
ing a pharmacologic strategy to treat myocardial ischemia. blockers or in patients with normal systolic function, but
Medications should be titrated according to symptoms. The they should be avoided in patients with left ventricular sys-
dose of a first-line drug should be optimized before adding tolic dysfunction. If a calcium channel blocker is required
additional agents. for patients with left ventricular systolic dysfunction, amlo-
dipine is preferred.
Medical therapy includes risk factor modification,
antiplatelet therapy, and medications to relieve ischemia. Because short-acting calcium channel blockers may cause
reflex tachycardia, they are relatively contraindicated.
A stepwise approach should be used for pharmacological
treatment of myocardial ischemia. However, if a short-acting calcium channel blocker
is required in a patient with left ventricular systolic
-Adrenergic blockers (-blockers) are the most effec- dysfunction, amlodipine is preferred.
tive and are first-line drugs for ischemic heart disease. They
relieve angina by decreasing heart rate, reducing contractil- Ranolazine (Ranexa) is a second-line drug used as an
ity, and decreasing afterload (blood pressure). They are the adjunct to one of the aforementioned drugs. Experience with
most effective drugs for reducing the double product (heart its use is limited. The mode of action is unknown.
rate blood pressure) with exercise. -Blockers may improve For patients with left ventricular dysfunction or nocturnal
survival for some patients with ischemic heart disease, par- angina, diuretics and angiotensin-converting enzyme inhibi-
ticularly those with prior MI or depressed left ventricu- tors decrease wall tension. They may be beneficial for sec-
lar systolic function. -Blockers should not be used in the ondary prevention in ischemic heart disease regardless of the
setting of marked bronchospastic disease, decompensated degree of systolic function.
heart failure, or bradycardia. However, they should be given Diuretics and angiotensin-converting enzyme inhibitors
to patients with left ventricular systolic dysfunction in the decrease wall tension in patients with left ventricular dysfunc-
absence of overt heart failure. The target resting heart rate tion or nocturnal angina.
is 70 beats per minute or less and dose should be titrated to
effect. Angiotensin-converting enzyme inhibitors may be
beneficial for secondary prevention for all patients with
-Blockers should be considered first-line therapy for ischemic heart disease.
ischemic heart disease.
Contraindications include severe bronchospastic disease,
decompensated heart failure, or bradycardia in which P E RCU TA N EO US C O RO NA RY I N T E RV E N T I O N
additional heart rate reduction cannot be tolerated.
Percutaneous coronary intervention (PCI) for chronic stable
Target heart rate <70 beats per minute; titrate dose to angina relieves symptoms but does not reduce the risk of MI
effect. or death. It is indicated for treatment in symptomatic patients,
particularly those who remain symptomatic despite optimized
Nitrates should be added if symptoms continue despite medical therapy. An initial medical strategy is reasonable for
optimal -blocker therapy. Nitrates cause venodilatation and most patients at low to moderate risk of an event (based on
decreasing wall tension, thus relieving angina. Nitrate toler- symptoms and the findings on stress testing or angiography).
ance can develop with continuous exposure. Thus, a nitrate- There is no clear role for PCI in management of asymptomatic
free interval is important, particularly when using short-acting disease.
preparations. Sublingual nitroglycerin should be given to all
symptomatic patients for use as needed. PCI relieves symptoms, but it does not alter the risk of MI
or death.
Nitrates should be added if symptoms continue despite
PCI is indicated for patients who remain symptomatic
optimal -blocker therapy.
despite optimal medical therapy.
Include a nitrate-free interval to avoid nitrate tolerance.
PCI should not be used to treat asymptomatic disease.
All patients with ischemic heart disease should carry
sublingual nitroglycerin for as-needed use. PCI is performed at the time of coronary angiography.
During percutaneous transluminal coronary angioplasty
Calcium channel blockers decrease afterload, heart rate, (PTCA), the device is placed across a coronary stenosis and
and contractility. Short-acting calcium channel blockers, a balloon is inflated to increase the area of the lumen. This
specifically the dihydropyridines (eg, amlodipine, nife- procedure splits the atheroma and stretches the vessel. The
dipine), may cause reflex tachycardia and increased mortal- major problem is restenosis, occurring in 30% to 40% of
ity; therefore, they are relatively contraindicated in patients patients within 6 months. Antiplatelet agents may decrease
with ischemic heart disease. This detrimental effect probably the rate of acute closure, but they do not prevent restenosis.
86 C A R D I O L O GY
Other catheter-based therapies such as atherectomy and laser Box 6.2 MANAGEMENT OF PATIENTS WITH
have high restenosis rates and are infrequently used. DRUG-ELUTING STENTS WHO NEED NONCARDIAC
SURGERY OR AN INVASIVE PROCEDURE
PCI uses an intracoronary balloon to open a coronary WITHIN 1 YEAR OF PERCUTANEOUS CORONARY
stenosis. INTERVENTION
Restenosis is a common problem.
Defer elective procedures for 1 year after stent placement &
Antiplatelet agents may decrease vessel closure rate, but consider less invasive alternatives that may be performed in
they do not prevent restenosis. patients receiving dual antiplatelet therapy
Intracoronary stent placement at the time of PCI decreases Aspirin therapy must be continued during the perioperative
restenosis. Stents are used in approximately 90% of PCIs. The period, unless absolutely contraindicated
restenosis rate after successful bare-metal stent implantation For urgent procedures, consider performing them without
is 20% to 30%. Stents also are used to treat acute complica- discontinuing dual antiplatelet therapy or with aspirin alone.
tions of PTCA such as acute dissection and have decreased the The relative risks of perioperative bleeding vs stent thrombosis
need for emergency coronary artery bypass grafting (CABG). must be discussed with the surgical team. The risk of postop-
However, for patients who have restenosis within a stent, the erative stent thrombosis is low, but it increases if use of one or
rate of recurrent restenosis is high (>60%) if another proce- both of the antiplatelet agents is discontinued. If stent throm-
dure is performed. bosis occurs, the associated morbidity & mortality are high
Intracoronary stent placement decreases restenosis. If clopidogrel therapy must be withheld for an urgent
operation, withhold therapy for 5 days preoperatively. Ideally,
Acute complications of PTCA (eg, coronary artery clopidogrel therapy should be resumed with a 300-mg loading
dissection) can be treated with stents. dose on the day of operation
The rate of recurrent stenosis is high when another
procedure is performed to treat restenosis.
The success rate for PCI is greater than 95%. Potential
Drug-eluting stents are coated with and release drugs complications include myocardial infarction (<5%), vascular
that considerably decrease restenosis (5%10%). They are the complications (1%), emergency CABG (0.2%), and mortality
most commonly used stents. They are associated with a higher (<0.5%). The risks of the procedure are higher during emer-
risk for very late (>1 year) stent thrombosis than bare-metal gency procedures, in the elderly, and in patients with severely
stents. reduced ejection fraction, acute coronary syndromes, or severe
Dual antiplatelet therapy is initiated at the time of stent diffuse coronary artery disease.
deployment to prevent early restenosis. Duration varies
according to the type of stent (Table 6.2). Recommendations Drug-eluting stents considerably decrease the likelihood of
regarding discontinuation of dual antiplatelet therapy for non- restenosis after angioplasty.
cardiac surgery are outlined in Box 6.2.
Very late stent thrombosis is higher with drug-eluting
stents than with bare-metal stents.
Table 6.2 ANTIPLATELET THERAPY USED WITH Long-duration dual antiplatelet therapy is used in the
CORONARY STENTS setting of drug-eluting stents.
THERAPY DURATION Caution must be exercised when considering
discontinuation of dual anti-platelet therapy for a surgical
Aspirin Indefinitely procedure.
Clopidogrel (Plavix)
or prasugrel
(Effient)
PCI is the preferred revascularization strategy for
Bare-metal stent At least 1 month for patient with stable single-vessel disease, young patients (age <50 years), elderly
disease. At least 12 months for an acute patients with significant comorbid conditions, and patients
coronary syndrome (unstable angina & myo- who are not surgical candidates.
cardial infarction). If the risk of substantial
bleeding outweighs the anticipated benefit,
earlier discontinuation should be considered S U RG I C A L T R E AT M E N T
Drug-eluting stent 12 months (a subset of patients may require
long-term therapy). If the risk of morbidity CABG uses the saphenous vein (occlusion rate of 20% at
because of bleeding outweighs the antici- 1 year and 50% at 5 years) and internal mammary artery
pated benefits afforded by thienopyridine (occlusion rate <10% at 10 years). CABG provides excellent
therapy, earlier discontinuation should be symptom relief (partial relief in >90%, complete relief in
considered
>70%).
6. I S C H E M I C H E A RT D I S E A S E 87
The indications for CABG (over medical therapy or PCI) is with aspirin and other nonsteroidal anti-inflammatory
are symptom relief in patients whose limiting symptoms are drugs. Rarely, constrictive pericarditis may be a late complica-
unresponsive to other management strategies and prolonging tion. The diagnosis should be suspected in patients present-
the life of patients with severe disease. ing months to years after cardiac surgery with congestive heart
failure with predominantly right-sided signs of fluid overload,
Internal mammary artery grafting results in better including increased jugular venous pressure but normal left
long-term patency than saphenous vein grafting. ventricular ejection fraction.
Indications for CABG include symptom relief in patients
Postcardiotomy syndrome may occur 2 weeks to 2 months
not responding to other management approaches and
after surgery.
decreasing mortality due to severe disease.
It is defined by fever, pericarditis, and increased erythrocyte
CABG reduces mortality in patients with severe disease, sedimentation rate.
including left main coronary artery disease, 3-vessel disease
Treatment is with aspirin and other nonsteroidal
with moderately depressed left ventricular function, 3-vessel
anti-inflammatory drugs.
disease with severe ischemic symptoms at a low workload,
and multivessel disease with proximal left anterior descend- Constrictive pericarditis is a rare late complication.
ing artery involvement. CABG does not prevent myocar-
dial infarction, improve left ventricular function, or decrease
ventricular arrhythmias. Recommendations for surgery are M E D I C A L VS C AT H ET E R-BA S E D VS S U RG I C A L
derived from randomized trials of CABG vs medical therapy. THERAPY
In meta-analyses, a survival benefit in favor of CABG com-
pared with medical therapy has been observed for all patients The decision about which therapy to use for a patient with
with 3-vessel disease. chronic stable angina must be individualized. Factors to con-
sider include disease severity, ischemia, and symptoms, and
CABG reduces mortality in patients with defined severe the patients age, lifestyle, and personal preference. The inci-
coronary artery disease and offers a survival benefit dence of MI and emergency CABG with PCI is similar to
compared to medical management in patients with 3-vessel that with medical management. PCI neither decreases risk for
disease. MI nor improves resting left ventricular function or survival.
Procedure-related mortality is lower with PCI than with CABG.
In-hospital mortality after CABG varies widely (about 1%
in most elective cases to 30% in high-risk cases). Mortality PCI and medical management have a comparable
increases with age, female sex, reduced left ventricular func- incidence of MI and emergency CABG.
tion, diffuse multivessel disease, recent acute coronary syn- PCI neither decreases risk for MI nor improves resting left
drome, diabetes mellitus, repeat CABG, and emergency ventricular function or survival.
surgery. Complications of CABG include sternal wound
infection (especially in patients with diabetes mellitus), severe There are more procedure-related infarctions and strokes
left ventricular dysfunction (from perioperative myocardial with CABG than with PCI, and the duration of hospitaliza-
infarction or inadequate cardioprotection), and late constric- tion is longer after CABG. The overall rates of death or myo-
tive pericarditis. cardial infarction at 5-year follow-up are similar for PCI and
CABG (85%90% free of death and 80% free of myocardial
CABG is associated with a widely varying in-hospital infarction), except for patients with severe disease. This sub-
mortality rate depending on underlying patient risk factors. group includes patients with left main coronary artery disease,
Mortality is higher in patient with diabetes, women, and 3-vessel disease with moderately depressed left ventricular
patients who are older, have diffuse multivessel disease, function, 3-vessel disease with severe ischemic symptoms at a
have reduced left ventricular function, have had a recent low workload, and multivessel disease with proximal left ante-
acute coronary syndrome, had prior CABG, or are rior descending artery involvement. CABG offers a survival
undergoing emergency surgery. benefit in these patients. Patients with multivessel or ana-
tomically complex disease who have CABG have less angina,
Complications include wound infection, severe left require less antianginal medication, and are less likely to need
ventricular dysfunction, and constrictive pericarditis. a repeat revascularization procedure. For patients with diabe-
tes mellitus and diffuse multivessel disease, survival is higher
with CABG than with PCI. Increased survival is related to
P O S TC A R D I OTO MY S Y N D RO M E
having a patent internal mammary artery graft to the left ante-
Postcardiotomy syndrome occurs 2 weeks to 2 months post- rior descending artery.
operatively and consists of fever, pericarditis, and increased
erythrocyte sedimentation rate. Rarely, it presents as pericar- CABG is related to more procedure-related infarctions
dial tamponade. It is likely an autoimmune process. Treatment and strokes.
88 C A R D I O L O GY
CABG offers a survival benefit in patients with defined generally have complete coronary artery occlusion leading to
severe coronary artery disease. transmural injury.
CABG offers a survival benefit in patients with diabetes
Acute coronary syndromes include unstable angina and
and in patients with diffuse multivessel disease.
acute MI.
Acute coronary syndromes include unstable angina and acute Recent (d24 h) severe angina
MI (both ST-segment elevation and nonST-segment eleva- n Cardiac markers
tion MI). At the time of initial presentation, the differentia-
tion of these patients from those with noncardiac chest pain is ST deviation t0.5 mm
based on clinical assessment. Abbreviations: CAD, coronary artery disease; TIMI, Thrombolysis in
The resting ECG is essential for the evaluation and tri- Myocardial Infarction trial.
age of a patient presenting with an acute coronary syndrome. Adapted from Antman EM, Cohen M, Bernink PJLM, McCabe CH, Horacek
Those without ST-segment elevation have unstable angina or T, Papuchis G, et al. The TIMI risk score for unstable angina/nonST elevation
nonST-segment elevation MI, usually the result of subtotal MI: a method for prognostication and therapeutic decision making. JAMA.
2000 Aug 16;284(7):83542. Used with permission.
coronary artery occlusion. Patients with ST-segment elevation
6. I S C H E M I C H E A RT D I S E A S E 89
45 the myocardial oxygen demand-supply mismatch. Sedation
40
may decrease anxiety and catecholaminergic stimulation of
the heart. -Adrenergic blockade is the treatment of choice to
35 decrease myocardial oxygen demand.
Rate Composite End Point, %
90 C A R D I O L O GY
Symptoms suggestive of ACS
Treatment as indicated
No ST elevation ST elevation
by alternative diagnosis
Evaluate for
Not high risk High risk
reperfusion therapy
Observe
See ACC/AHA guidelines
12 h from symptom onset
for ST-elevation
myocardial infarction
Negative Positive
Potential diagnoses: Diagnosis of ACS Admit to
nonischemic discomfort; confirmed hospital
low-risk ACS or highly likely
Arrangements for
outpatient follow-up
Figure 6.5 Algorithm for Evaluation and Management of Patients Suspected of Having Acute Coronary Syndrome (ACS). ACC indicates American
College of Cardiology; AHA, American Heart Association; LV, left ventricular. (Adapted from Anderson JL, Adams CD, Antman EM, Bridges
CR, Califf RM, Casey DE Jr, et al. ACC/AHA 2007 guidelines for the management of patients with unstable angina/nonST-elevation myocardial
infarction: a report of the American College of Cardiology/American Heart Association Task Force on Practice Guidelines [Writing Committee
to Revise the 2002 Guidelines for the Management of Patients With Unstable Angina/NonST-Elevation Myocardial Infarction]. J Am Coll
Cardiol. 2007 Aug 14;50[7]:e1157 and Anderson JL, Adams CD, Antman EM, Bridges CR, Califf RM, Casey DE Jr, et al; American College of
Cardiology; American Heart Association Task Force on Practice Guidelines [Writing Committee to Revise the 2002 Guidelines for the Management
of Patients With Unstable Angina/Non ST-Elevation Myocardial Infarction]; American College of Emergency Physicians; Society for Cardiovascular
Angiography and Interventions; Society of Thoracic Surgeons; American Association of Cardiovascular and Pulmonary Rehabilitation; Society for
Academic Emergency Medicine. ACC/AHA 2007 guidelines for the management of patients with unstable angina/non ST-elevation myocardial
infarction: a report of the American College of Cardiology/American Heart Association Task Force on Practice Guidelines [Writing Committee
to Revise the 2002 Guidelines for the Management of Patients With Unstable Angina/Non ST-Elevation Myocardial Infarction]: developed in
collaboration with the American College of Emergency Physicians, the Society for Cardiovascular Angiography and Interventions, and the Society of
Thoracic Surgeons: endorsed by the American Association of Cardiovascular and Pulmonary Rehabilitation and the Society for Academic Emergency
Medicine. Circulation. 2007 Aug 14;116[7]:e148304. Epub 2007 Aug 6. Erratum in: Circulation. 2008 Mar 4;117[9]:e180. Used with permission.)
High-risk patients should undergo invasive strategy, sudden, complete occlusion of the artery. Without collateral
whereas nonhigh-risk patients can receive more circulation, 90% of the myocardium supplied by the occluded
conservative treatment, which can be switched to an coronary artery is infarcted within 3 hours. Transmural
invasive strategy if high-risk factors emerge. MI develops if the condition is untreated. Patients with
ST-segment elevation MI require urgent diagnosis and ther-
apy to preserve the myocardium because prompt reperfusion
therapy improves survival.
S T-S EG M E N T E L EVAT I O N MYO C A R D I A L
I N FA RC T I O N
Plaque rupture may ultimately lead to sudden, complete
Pathophysiology occlusion of a coronary artery, resulting in an ST-segment
elevation MI.
An ST-segment elevation MI is the result of events occurring
after rupture of an intracoronary plaque. Plaque rupture causes Rapid reperfusion leads to improved myocardial
platelet adhesion and aggregation, thrombus formation, and preservation and survival.
6. I S C H E M I C H E A RT D I S E A S E 91
Conservative Strategy Invasive Strategy
Initiate anticoagulant therapy (class I, LOE: A) Initiate anticoagulant therapy (class I, LOE: A)
Acceptable options: enoxaparin or UFH (class I, LOE: A) Acceptable options: enoxaparin or UFH (class I, LOE: A),
or fondaparinux (class I, LOE: B), but enoxaparin or bivalirudin or fondaparinux (class I, LOE: B)
fondaparinux is preferable (class IIa, LOE: B)
Clopidogrelb
Any subsequent events necessitating angiography?a IV GP IIb/IIIa inhibitorb
(class IIa,
LOE: B)
EF 40% EF >40% Stress test
Diagnostic angiography
(class IIa,
LOE: B)
(class I, LOE: A)
Figure 6.6B Therapeutic Pathways for Acute Ischemia. Initial invasive
Diagnostic Not low Low
angiography risk risk
strategy. b Evidence exists that GP IIb/IIIa inhibitors may not be
necessary if a patient received a preloading dose of at least 300 mg
(class I, of clopidogrel at least 6 hours earlier (class I, LOE B for clopidogrel
LOE: A)
administration) and bivalirudin is selected as the anticoagulant (class
Continue ASA indefinitely (class I, LOE: A) IIa, LOE B). ASA indicates acetylsalicylic acid; EF, ejection fraction;
Continue clopidogrel for at least 1 month (class I, LOE: A) GP, glycoprotein; IV, intravenous; LOE, level of evidence; LVEF, left
and ideally up to 1 year (class I, LOE: B) ventricular ejection fraction; UFH, unfractionated heparin. (Both A
Discontinue IV GP IIb/IIIa if started previously (class I, LOE: A) and B adapted from Anderson JL, Adams CD, Antman EM, Bridges
Discontinue anticoagulant therapy (class I, LOE: A) CR, Califf RM, Casey DE Jr, et al. ACC/AHA 2007 guidelines for
the management of patients with unstable angina/nonST-elevation
Figure 6.6A Therapeutic Pathways for Acute Ischemia. Initial conservative myocardial infarction: a report of the American College of Cardiology/
strategy. a Recurrent symptoms/ischemia, heart failure, or serious American Heart Association Task Force on Practice Guidelines [Writing
arrhythmia. Abbreviations are defined in the legend for Figure 6.6B. Committee to Revise the 2002 Guidelines for the Management of
Patients With Unstable Angina/NonST-Elevation Myocardial
Infarction]. J Am Coll Cardiol. 2007 Aug 14;50[7]:e1157 and
Anderson JL, Adams CD, Antman EM, Bridges CR, Califf RM, Casey
MI is a major public health problem in the United DE Jr, et al. ACC/AHA 2007 guidelines for the management of patients
Statesabout 1 million patients annually are admitted for with unstable angina/nonST-elevation myocardial infarction: a report
an acute coronary syndrome, including MI. ST-segment of the American College of Cardiology/American Heart Association
elevation accounts for 20% of these cases. More than 30% Task Force on Practice Guidelines [Writing Committee to Revise the
of patients with MI die before reaching a hospital. With 2002 Guidelines for the Management of Patients With Unstable Angina/
NonST-Elevation Myocardial Infarction]. Circulation. 2007 Aug
improved cardiac care, mortality from MI has declined, 14;116[7]:e148-e304. Epub 2007 Aug 6. Erratum in: Circulation. 2008
primarily due to treatment of ventricular arrhythmias. Mar 4;117[9]:e180. Used with permission.)
-Adrenergic blockade has also decreased in-hospital and
post-hospital mortality by 30% to 40%. Reperfusion therapy
has contributed to improved survival. Currently, the overall
in-hospital mortality for patients with an ST-segment eleva- affected myocardium may be decreased and the myocar-
tion MI is 5% to 10%. dium remains viable. Systolic contraction returns hours to
days later.
Plaque rupture leads to sudden occlusion of the coronary
artery; when untreated, it results in myocardial death. Myocardial stunning may occur due to ischemia, but with
early reperfusion the myocardium remains viable and
Prompt arterial reperfusion improves survival.
systolic contraction returns.
The advent of improved cardiac care has improved
survival. Infarct remodeling occurs mainly after a large anteroapical
MI. An area of infarction may undergo thinning, dilatation,
Stunned myocardium occurs when reversible systolic and dyskinesis. Myocardial remodeling may lead to congestive
dysfunction of the myocardium follows transient, nonle- heart failure and increased mortality. Adverse infarct remod-
thal ischemia. With early reperfusion, contraction of the eling may be reduced with early initiation of therapy with
92 C A R D I O L O GY
angiotensin-converting enzyme inhibitors or angiotensin
receptor blockers (if angiotensin-converting enzyme inhibi- Cardiac troponinno reperfusion
tors are contraindicated). Cardiac troponinreperfusion
100
CK-MBno reperfusion
Myocardial remodeling after an MI increases the risk of CK-MBreperfusion
2
Presentation and Diagnosis Upper reference limit
1
Patients with ST-segment elevation MI commonly present
0
with angina-like pain lasting longer than 20 minutes associated
0 1 2 3 4 5 6 7 8
with typical ECG changes and increased levels of cardiac bio-
Days After Onset of STEMI
markers (Figure 6.7). However, more than 25% to 30% of MIs
are silent, and silent MIs often occur in patients with diabetes Figure 6.7 Cardiac Biomarkers in ST-Segment Elevation Myocardial
mellitus and in the elderly. In addition, women having an MI Infarction (STEMI). Typical cardiac biomarkers that are used to
often present without typical angina-like pain. Symptoms evaluate patients with STEMI include the MB isoenzyme of creatine
such as nausea, jaw pain, upper back pain, and shortness of kinase (CK-MB) and cardiac-specific troponins. The horizontal line
breath should be considered possible indicators of ischemia, depicts the upper reference limit (URL) for the cardiac biomarker in
the clinical chemistry laboratory. The URL is that value representing
in addition to chest pain or pressure. the 99th percentile of a reference control group without STEMI.
The kinetics of release of CK-MB and cardiac troponin in patients
An ST-segment elevation MI may present with typical who do not undergo reperfusion are shown in the solid blue and red
angina-like chest pain but often does not. curves as multiples of the URL. Note that when patients with STEMI
undergo reperfusion, as depicted in the dotted blue and dotted red
Women, persons with diabetes, and the elderly are less curves, the cardiac biomarkers are detected sooner, increase to a
likely to experience typical angina-like pain during an MI; higher peak value, but decline more rapidly, resulting in a smaller
thus, a high degree of clinical suspicion is essential. area under the curve and limitation of infarct size. (Adapted from
Antman EM, Anbe DT, Armstrong PW, Bates ER, Green LA, Hand
Persons with diabetes and the elderly are more likely to M, et al. ACC/AHA guidelines for the management of patients
with ST-elevation myocardial infarction: a report of the American
suffer a silent MI.
College of Cardiology/American Heart Association Task Force on
Practice Guidelines [Committee to Revise the 1999 Guidelines for
An acute MI is usually diagnosed on the basis of ECG the management of patients with acute myocardial infarction]. J Am
changes (ST elevation or depression or pathologic Q-wave Coll Cardiol. 2004 Aug 4;44[3]:E1-E211 and Antman EM, Anbe DT,
development that meets criteria for diagnosis) in the setting Armstrong PW, Bates ER, Green LA, Hand M, et al; American College
of Cardiology; American Heart Association Task Force on Practice
of ischemic symptoms, biochemical markers of myocardial Guidelines; Canadian Cardiovascular Society. ACC/AHA guidelines
damage, or other evidence of myocardial damage not due to for the management of patients with ST-elevation myocardial
another potential cause. infarction: a report of the American College of Cardiology/American
Heart Association Task Force on Practice Guidelines [Committee to
Revise the 1999 Guidelines for the Management of Patients with Acute
Management Myocardial Infarction]. Circulation. 2004 Aug 31;110[9]:e82292.
Errata in: Circulation. 2005 Apr 19;111[15]:20134. Circulation. 2007
Bed rest, pain management, and sedation are essential and Apr 17;115[15]:e411. Circulation. 2010 Jun 15;121[23]:e441. Used with
beneficial in the acute stage of myocardial infarction to permission.)
decrease myocardial oxygen demand. Oxygen has little
benefit after 2 or 3 hours unless hypoxia (oxygen saturation
<90%) is present. Modest hypoxemia is common as a result should be administered upon admission. Clopidogrel (75
of ventilation-perfusion lung mismatch, even with uncompli- mg daily) is an alternative in patients with aspirin allergy
cated MI. Continuous ECG monitoring is required to detect or intolerance. Clopidogrel therapy is also indicated in
tachyarrhythmias and bradyarrhythmias. patients given thrombolytics and should be started on day
1 and continued during the hospitalization and possibly up
Measures to reduce myocardial oxygen demand are essential. to 4 weeks.
Oxygen has some benefit but little beyond 23 hours of
Aspirin in combination with thrombolytic therapy leads to
presentation unless hypoxemia is present.
decreased recurrent MI and improved survival.
Aspirin (325 mg) reduces recurrent MI and mortal- Dual antiplatelet therapy (aspirin and clopidogrel) is
ity when given in addition to thrombolytic therapy and indicated.
6. I S C H E M I C H E A RT D I S E A S E 93
Anticoagulation prevents recurrent infarction (especially -Adrenergic blockade leads to decreased pain, myocardial
after thrombolytic therapy, when it should be administered oxygen demand, ventricular fibrillation, platelet
for at least 24 hours), deep vein thrombosis, and intracar- aggregation, and sympathetic effects on heart muscle.
diac thrombus formation. Long-duration anticoagulation
is indicated for higher-risk patients (large anterior myo- Calcium channel blockers are generally not used in patients
cardial infarction for which reperfusion therapy was not with an acute MI. However, diltiazem may be used to control
given or was unsuccessful, atrial fibrillation, previous embo- ventricular rate in atrial fibrillation, especially if -adrenergic
lus). Thromboembolism is uncommon in patients in whom blockers are contraindicated. Amlodipine may be used to treat
reperfusion therapy is successful. Unfractionated heparin or hypertension after the acute phase.
low-molecular-weight heparin can be used. Angiotensin-converting enzyme inhibitors prevent ven-
tricular remodeling, especially after a large anterior myo-
Anticoagulation reduces recurrent infarction and other cardial infarction. Oral therapy may be initiated within the
complications of an ST-segment elevation MI. first 24 hours if blood pressure and renal function are stable.
If thrombolytic therapy was not used or was unsuccessful, Angiotensin-converting enzyme inhibitors are absolutely
atrial fibrillation is present, or the patient had a prior embolic indicated in patients with anterior infarction, congestive heart
event, anticoagulation should be used for a longer duration. failure, or left ventricular ejection fraction less than 40%. It is
reasonable to treat all patients after ST-segment elevation myo-
Nitroglycerin is useful for certain patients with MI: those cardial infarction in the absence of hypotension or contrain-
with pulmonary edema, severely increased blood pressure, dications. Angiotensin-receptor blockers are recommended as
or persistent myocardial ischemia. Intravenous nitroglycerin an alternative in patients who are intolerant of or allergic to
should be given instead of long-acting oral nitrates. Nitrate angiotensin-converting enzyme inhibitors.
intolerance develops with infusions of more than 24 hours in
duration. Intravenous nitroglycerin should not be given in the Avoid calcium channel blockers during an acute MI.
setting of low blood pressure (systolic <90 mm Hg) or right Consider diltiazem for rate control in atrial fibrillation if
ventricular infarction or in patients who have used a phos- -adrenergic blockers cannot be used.
phodiesterase inhibitor (eg, sildenafil) within the previous 24
hours (48 hours for tadalafil). Angiotensin-converting enzyme inhibitors prevent
ventricular remodeling after an MI and should be
Nitroglycerin should be used in the setting of pulmonary considered for all patients after ST-segment elevation MI
edema, severe hypertension, or persistent ischemia. unless contraindicated.
Nitroglycerin tolerance develops when infusions are used Long-term aldosterone blockade (spironolactone or
for longer than 24 hours. eplerenone) is indicated for patients without renal dysfunc-
Intravenous nitroglycerin should be avoided in the setting tion (creatinine, <2.0 mg/dL for women and <2.5 mg/dL
of hypotension, right ventricular infarct, or recent use of for men) or hyperkalemia (potassium, <5.0 mEq/L) who are
phosphodiesterase inhibitors. receiving therapeutic doses of angiotensin-converting enzyme
inhibitors and have a left ventricular ejection fraction of less
-Adrenergic blockade during and after MI lowers mortal- than 40% with either symptomatic heart failure or diabetes
ity in the hospital and after discharge. Oral -adrenergic block- mellitus.
ers should be administered at presentation to patients who do
not have contraindications. Intravenous administration may Consider aldosterone blockade when the left ventricular
be considered in hypertensive patients. Contraindications to ejection fraction is less than 40% in patients with diabetes
-adrenergic blockers are bradycardia (heart rate <60 beats mellitus or symptomatic heart failure when therapeutic
per minute), second- or third-degree atrioventricular block, doses of angiotensin-converting enzyme inhibitors are
hypotension (systolic blood pressure <100 mm Hg), acute being used.
heart failure, cardiogenic shock, and cocaine-induced myo- Renal dysfunction and hyperkalemia are contraindications
cardial infarction. The need for continued treatment should to use of aldosterone blockade agents.
be reassessed periodically. Beneficial effects include decreased
pain, decreased myocardial oxygen demand, reduced ventricu- Glycoprotein IIb/IIIa inhibitors are given only if primary
lar fibrillation, decreased platelet aggregability, and decreased PCI is performed, and their use is generally initiated in the
sympathetic effects on the myocardium. -Adrenergic block- cardiac catheterization laboratory. They are not indicated in
ers are most beneficial for patients with a large infarction who patients treated with thrombolytics.
are at higher risk for complications.
Glycoprotein IIb/IIIa inhibitors should be used when PCI
-Adrenergic blockers improve survival. is performed.
Exercise caution with the use of -adrenergic blockers in Glycoprotein IIb/IIIa inhibitors are not indicated with
the setting of contraindications. thrombolysis.
94 C A R D I O L O GY
Magnesium does not seem to have a therapeutic role after ischemia. Reperfusion therapy is not indicated for patients
MI and should be given only for the treatment of torsades de with ST-segment depression or those who present late (>12
pointes or if a patient has documented hypomagnesemia of hours after symptom onset) and are asymptomatic without
potential clinical significance. hemodynamic compromise or serious arrhythmia. Fibrinolytic
therapy is less beneficial for patients 75 years or older.
Avoid magnesium unless treating torsades de pointes or
hypomagnesemia. PCI is not indicated after successful fibrinolytic therapy
(no evidence of ongoing ischemia or symptoms).
Reperfusion Therapy ST-segment depression, late presentation (>12 hours
Early reperfusion therapy decreases mortality by approximately after symptoms started), and lack of symptoms with
25%. The extent of myocardial salvage and degree of beneficial normal hemodynamics and normal cardiac rhythm are
effect on mortality are measurably improved the earlier rep- contraindications to reperfusion therapy.
erfusion occurs. Mortality is as low as 1% when fibrinolysis is Fibrinolysis is less beneficial in elderly patients.
given less than 90 minutes after the onset of pain. The major-
ity of delays to reperfusion lie in time to patient presentation, Major complications of intravenous fibrinolysis include
transport, and in-hospital institution of therapy. Reperfusion major bleeding (5%6%), intracranial bleeding (0.5%), major
at 2 to 6 hours results in a lesser effect on myocardial salvage allergic reaction (0.1%1.7%), and hypotension (2%10%).
but still has an important effect on survival. The incidence of myocardial rupture may be higher in patients
who are given thrombolytic therapy late (>12 hours after pain
Early reperfusion decreases mortality considerably. onset). Several agents are available for intravenous fibrinolysis,
When reperfusion occurs 26 hours after onset of including streptokinase (a nonselective thrombolytic agent)
symptoms, less myocardium is salvaged but survival is still and tissue plasminogen activator (selectively binds to and
improved. lyses preformed fibrin). Tissue plasminogen activator has the
fastest onset of action. The dosage is 100 mg over 90 minutes.
Reperfusion therapy with fibrinolytics (thrombolytics) Newer thrombolytic agents such as reteplase and tenecteplase
or primary PCI is indicated for patients presenting within offer better selectivity for active thrombus, but their efficacy
12 hours of onset of symptoms with the following findings: is equivalent to that of tissue plasminogen activator in clini-
1+ mm of ST-segment elevation in 2 adjacent leads, a new (or cal trials. Their greatest advantage is the ability to admin-
presumably new) left bundle branch block, or a true posterior ister them as a bolus, which reduces drug errors and speeds
myocardial infarction. delivery. Streptokinase is rarely used in the United States, and
PCI is more effective than fibrinolysis for restoring nor- tenecteplase and reteplase are now the most commonly used
mal coronary blood flow (TIMI grade 3) (90% vs 65%70%). fibrinolytics.
However, intravenous fibrinolysis allows faster administration
and is more widely available. The preferred strategy depends Major complications of fibrinolysis are bleeding (including
on time since the onset of symptoms, transportation time to intracranial), allergic reaction, and hypotension.
a skilled PCI laboratory, risk profile of the patient, and con- Late fibrinolysis may increase the incidence of myocardial
traindications to fibrinolytics. Primary PCI is indicated for rupture.
patients with immediate access to a high-volume catheteriza-
tion laboratory, a contraindication to intravenous fibrinolysis, After intravenous fibrinolytic administration, a high-grade
high-risk ST-segment elevation MI (eg, cardiogenic shock or residual lesion is usually present. Reocclusion or ischemia
pulmonary edema), or continued ischemia after thrombolytic occurs in 15% to 20% of patients and reinfarction occurs
therapy (rescue PCI). in 2% to 3%. Heparin should be given in conjunction with
intravenous fibrinolysis with tissue-specific plasminogen
PCI is more effective than fibrinolysis for restoring normal activators used to prevent reinfarction. The indications for
coronary blood flow but is less widely available and in most coronary angiography or PCI after intravenous fibrinolysis
settings cannot be initiated as quickly. are spontaneous or inducible ischemia, cardiogenic shock,
Several factors determine the preferred strategy. pulmonary edema, ejection fraction less than 40%, and seri-
ous arrhythmias.
PCI is indicated in the setting of high-risk ST-segment
elevation MI, ongoing or recurrent ischemia after fibrinolytic
Reocclusion or ischemia occur in 15% to 20% of patients
therapy, or contraindications to fibrinolytic therapy.
after fibrinolysis.
Consider PCI rather than fibrinolysis when a skilled,
Heparin should be used with a tissue plasminogen
high-volume PCI laboratory is immediately available.
activator to prevent reinfarction.
Routine immediate PCI after successful fibrinolytic ther- Spontaneous or inducible ischemia, cardiogenic shock,
apy is not indicated in the absence of ongoing symptoms or pulmonary edema, ejection fraction <40%, and serious
6. I S C H E M I C H E A RT D I S E A S E 95
arrhythmias are indications for angiography (and possible Cardiogenic shock may occur in extreme circumstances;
PCI) after fibrinolysis. treat with fluid resuscitation and dobutamine.
Reperfusion therapy is indicated.
Acute Mechanical Complications of ST-Segment
Elevation MI Myocardial free wall rupture causes abrupt decompensa-
tion. Free wall rupture occurs in 85% of all ruptures. It usually
Mechanical complications are relatively uncommon in patients occurs 2 to 14 days after transmural MI, most commonly in
who receive reperfusion therapy and include cardiogenic elderly hypertensive women, and usually presents as electro-
shock, myocardial free wall rupture, papillary muscle rupture, mechanical dissociation or death. Tamponade may occur if the
and ventricular septal defects. Right ventricular infarct may rupture is contained in the pericardium. If the diagnosis can
also occur after an inferior MI. be made with emergency echocardiography, surgery should be
performed. If the rupture is sealed off, a pseudoaneurysm may
Mechanical complications are relatively uncommon after occur. Surgical treatment is required because of the high inci-
reperfusion therapy. dence of further rupture.
Papillary muscle rupture usually occurs 2 to 10 days after
Most cases of cardiogenic shock are due to extensive left MI. It is associated with inferior myocardial infarction because
ventricular dysfunction. Echocardiography is helpful to deter- of the single blood supply to the posteromedial papillary
mine the mechanism of cardiogenic shock. The mortality muscle. Rupture of papillary muscle is heralded by the sudden
from cardiogenic shock is 50% (Table 6.3). onset of dyspnea and hypotension. Although a murmur may
be present, it may not be audible because of equalization of left
Severe left ventricular dysfunction is the most common atrial and left ventricular pressures. The diagnosis is made with
cause of cardiogenic shock after ST-segment echocardiography. The treatment is intra-aortic balloon pump
elevation MI. and emergency surgery.
Ventricular septal defects usually occur 1 to 20 days after
Right ventricular infarction occurs in up to 40% of patients MI and are equally frequent in inferior and anterior MIs.
with inferior myocardial infarction, can present hours to days Ventricular septal defects associated with inferior MIs have a
after the infarction, and is diagnosed from increased jugular poorer prognosis because of the serpiginous nature of the rup-
venous pressure in the presence of clear lung fields. ST-segment ture and associated ventricular infarction. They are indicated
elevation in lead V4R is diagnostic of a large right ventricular by the abrupt onset of dyspnea and hypotension. A loud mur-
infarction and portends increased mortality. In extreme cir- mur and systolic thrill are almost always present. The diagnosis
cumstances, right ventricular infarction can cause cardiogenic is made with echocardiography. Treatment is intra-aortic bal-
shock due to compromised left ventricle filling. Treatment loon pump and an emergency operation.
includes intravenous fluid resuscitation and dobutamine infu-
sion. When right ventricular infarction is recognized early,
reperfusion therapy is indicated.
PreHospital-Discharge Evaluation
Risk stratification for long-term outcomes is required before
Right ventricular infarction is relatively common after an hospital discharge and should include left ventricular func-
inferior ST-segment elevation MI and causes increased tion determination, assessment of risk for arrhythmias, and
jugular venous pressure with clear lung fields. ST elevation identification of inducible ischemia. A submaximal treadmill
in lead V4R is diagnostic. test can be performed before discharge, 4 to 6 days after MI.
Abbreviations: CO, cardiac output; NA, not applicable; PADP, pulmonary artery diastolic pressure; PAWP, pulmonary artery wedge pressure; RA, right atrial pressure.
96 C A R D I O L O GY
Alternatively, a symptom-limited treadmill test can be per- used to suppress ventricular ectopy. Angiotensin-converting
formed safely 10 to 21 days after MI. If a submaximal treadmill enzyme inhibitors decrease mortality after anterior MI and
test is performed before discharge, a late symptom-limited depressed left ventricular function, presumably by inhibiting
treadmill test should be performed at follow-up evaluation 3 infarct remodeling. A rehabilitation program is essential for
to 6 weeks after MI. High-risk patients identified by treadmill the patients well-being and cardiovascular fitness. An auto-
exertion testing have an ST-segment depression greater than matic implantable cardioverter-defibrillator should be consid-
1 mm, a decrease in blood pressure, or an inability to achieve ered if the ejection fraction is less than 35% 1 month after MI
4 metabolic equivalents on the exercise test. Imaging exer- in patients with an expected survival of at least 1 year.
cise tests may identify additional high-risk patients by dem-
onstrating multiple areas of ischemia. Pharmacologic stress Optimize risk factors, including exercise program, weight
tests (dobutamine echocardiography, dipyridamole thallium loss, and dietary modifications.
scanning, or adenosine thallium scanning) may be useful for
patients unable to exercise. Tobacco users must be counseled to quit and assistance
offered.
Risk stratification is required before hospital discharge. Provide aspirin and statins to decrease recurrent MI and
mortality.
Risk stratification includes determination of left ventricular
function, arrhythmia risk assessment, and identification of -Adrenergic blockers improve survival after MI,
inducible ischemia. particularly in high-risk patients.
Angiotensin-converting enzyme inhibitors decrease
Increasingly, rather than a stress test, a delayed invasive
remodeling and are recommended.
(pharmacoinvasive) strategy is being practiced in which
coronary angiography is performed at least 4 hours after Antiarrhythmic agents are not recommended.
fibrinolysis and before hospital discharge. PCI is performed
in the majority of patients, and few undergo CABG or med- Consider an automatic implantable cardioverter-defibrillator
ical therapy alone. The choice between PCI and CABG is in patients with an ejection fraction <35% 1 month after MI
based on factors similar to those used to make the decision if the life expectancy is at least 1 year.
in patients with stable coronary artery disease. This strategy
is associated with lower recurrent ischemia and infarction
compared with the ischemia-guided approach described S U M M A RY
above.
Optimal risk factor modification is essential, including an The Framingham risk score is derived from a patients risk
exercise program, weight loss, and dietary modifications. The factors for ischemic heart disease.
goal of treatment is to decrease the low-density lipoprotein Modifiable (and possibly some nonmodifiable) risk factors
cholesterol level to 100 mg/dL or less (optimal <70). If the lead to chronic endothelial injury that may progress
level is more than 100 mg/dL, statin treatment should be ini- through endogenous changes to more advanced changes in
tiated before discharge. All tobacco users should be counseled the coronary vessel wall.
and nicotine cessation must be stressed.
Aspirin and statins decrease recurrent MI and mortality Mismatched oxygen demand and supply lead to myocardial
and should be given to all patients unless contraindicated. ischemia.
-Adrenergic blockers improve survival after MI and are most
Coronary artery spasm may occur in the setting of arterial
effective in high-risk patients (ie, decreased left ventricular
injury and endothelial dysfunction.
function and ventricular arrhythmias). Chronic therapy may
not be required for low-risk patients. Antiarrhythmic agents Acute coronary syndromes include unstable angina and
are associated with increased mortality and should not be acute MI.
6. I S C H E M I C H E A RT D I S E A S E 97
7.
VASCULAR DISEASES
Henna Kalsi, MD, and Robert D. McBane, MD
98
A A
Figure 7.1 Chest Radiographs Show a Large Mass in Left Posterior Aspect
of Chest. A, Anteroposterior. B, Lateral.
Figure 7.2 Imaging of Thoracic Aortic Aneurysm. A, Magnetic resonance
angiogram (longitudinal view) shows a large ascending aortic aneurysm
between aneurysm size and risk of rupture (diameter <4.0 cm, and moderate aortic regurgitation. B, Computed tomogram shows a
0%; 4.05.9 cm, 16%; 6.0 cm, 31%). saccular aneurysm in the mid descending thoracic aorta (arrow).
The diagnosis is confirmed with magnetic resonance
imaging (MRI) (Figure 7.2A), computed tomography
(CT) (Figure 7.2B), or transesophageal echocardiography Diastolic hypertension, traumatic aneurysm, and associated
(TEE). vascular disease worsen prognosis.
Diastolic hypertension, large aneurysm size (critical hinge
point for rupture: >6 cm at the ascending aorta and >7 cm at Medical management places strong emphasis on control
the descending thoracic aorta), traumatic aneurysm, and asso- of systemic hypertension with a goal blood pressure of less
ciated coronary and carotid artery disease worsen prognosis. than 140/90 mm Hg (130/80 mm Hg if there is coexisting
The cumulative risk of rupture after 5 years is 20%, but rupture diabetes mellitus). Preferred antihypertensive agents include
risk is a function of aneurysm size at recognition. -adrenergic blockers or angiotensin receptor blockers;
blood pressure should be reduced to the lowest point tolera-
Confirm the diagnosis of TAA with CT, MRI, or TEE. ble. -Adrenergic blocking drugs should be administered to
all patient with Marfan syndrome who have aortic aneurysm
Complications of TAA include rupture, dissection, and to reduce the growth rate of aortic dilatation unless contrain-
rarely thrombosis. dicated. Statin therapy to achieve a target low-density lipo-
Aneurysmal size is an important factor in determining risk protein cholesterol value of 70 mg/dL or less is warranted
of rupture. (class IIa).
7. VA S C U L A R D I S E A S E S 99
Smoking cessation is warranted. Unless surgical repair is other diseases must be considered, including connective tissue
already indicated, serial follow-up of patients combines clin- diseases (Marfan syndrome, Ehlers-Danlos syndrome, pseudo-
ical assessment with noninvasive imaging tests. Elective sur- xanthoma elasticum), infection, trauma, or vasculitis (Takayasu
gical repair is indicated for ascending TAA of 5.5 cm or more arteritis and temporal arteritis). Twenty-five percent of patients
and for descending TAA of 6.0 cm or more or if the growth with AAA have an affected relative; thus, a familial predisposi-
rate exceeds 0.5 cm per year in either. Elective repair is indi- tion is suspected. Most AAAs are infrarenal. Suprarenal AAAs
cated in patients with Marfan syndrome, Loeys-Dietz syn- (2%5%) are usually due to distal extension of a thoracic aneu-
drome, or Ehlers-Danlos syndrome when size is more than rysm (thoracoabdominal aneurysm).
4.5 cm. Elective repair is indicated in patients with bicuspid aor-
tic valves if the diameter of the aortic root or ascending aorta is AAA is 5 times more likely to develop in men than women.
5.0 cm or more or if growth rate exceeds 0.5 cm per year.
Atherosclerosis (and its risk factors) is a major risk factor
for AAA.
Medical management of TAA with aggressive risk factor
modification is strongly advised. Patients with certain connective tissue diseases or
vasculitides are at higher-than-average risk to develop AAA.
Unless surgical repair is already indicated, follow patients
with clinical assessment in combination with noninvasive Twenty-five percent of patients with AAA have an affected
imaging to assess for changes in aneurysm diameter. relative.
Elective repair is indicated when the aneurysm size reaches
Most patients with AAA are asymptomatic. Livedo retic-
5.5 cm for ascending TAA, 6 cm for descending TAA, or
ularis, blue toes with palpable pulses, hypertension, renal
5.0 cm in patients with bicuspid aortic valve; when growth
insufficiency, increased erythrocyte sedimentation rate, and
rate of any TAA exceeds 0.5 cm per year; or in patients
transient eosinophilia imply AAA-associated atheroem-
with Marfan, Loeys-Dietz, or Ehlers-Danlos syndrome
bolism (Figure 7.3). Abdominal or low back pain suggests
and an aneurysm size >4.5 cm (Circulation. 2010 Apr
aneurysm instability. The triad of severe abdominal pain, hypo-
6;121[13]:e266369. Epub 2010 Mar 6).
tension, and a tender abdominal mass characterize AAA rupture.
The annual risk of rupture is directly related to aneurysm size:
Abdominal Aortic Aneurysm 4.0 cm, <2%; 5.0 cm, 5%; 6.0 cm, 10%; and 7.0 cm or more, 20%.
The abdominal aorta is the commonest site of aneurysm. Men
Most patients with AAA are asymptomatic.
are 5 times more commonly affected than women, and the inci-
dence increases with age. The prevalence of AAA is 3% among History and physical examination features are important
persons 50 years or older. Most aneurysms are due to athero- for identifying AAA instability, rupture, and associated
sclerosis. Tobacco use is a considerable risk factor. However, atheroembolism.
A B
Figure 7.3 Findings in a Patient With Atheroembolism. A and B, Livedo reticularis (upper aspect of thighs, plantar surface of feet) and multiple blue
toes.
100 C A R D I O L O GY
Severe abdominal pain, hypotension, and a tender One-time screening is advised for men 65 to 75 years old
abdominal mass should increase suspicion of AAA who have any smoking history and men older than 60 years
rupture. who have an affected first-degree relative (http://www.
uspreventiveservicestaskforce.org/uspstf/uspsaneu.htm).
Annual risk of rupture is related to aneurysm size.
Medical management includes modification of ather-
The most common physical examination finding is a osclerotic risk factors, including blood pressure control
pulsatile abdominal mass. The sensitivity of abdominal (preferably with a -adrenergic blocker), tobacco cessation,
palpation for the detection of AAA is relatively low: 43% and statin therapy. Patients should be followed with serial
overall (57% for aneurysms >4.0 cm in diameter and 29% imaging of the aneurysm every 6 to 12 months if the aneu-
for aneurysms <4.0 cm in diameter). A 1-time screening rysm is more than 4.0 cm and every 2 to 3 years if it is less
ultrasonography for men 65 to 75 years old who have ever than 4.0 cm.
smoked is recommended, and AAA screening is indicated Endovascular repair of AAA with stent grafts is an alterna-
for men 60 years or older who have a first-degree family tive to open surgical repair. Endovascular and surgical repair
history of AAA. Ultrasonography, CT and CT angiogra- are associated with similar risks of overall and aneurysm-related
phy, or MRI and MR angiography are reliable for diagnosis mortality. Graft-related complications are higher for endovas-
(Figure 7.4). cular AAA repair. An endoleak (ie, persistent flow into the
aneurysm sac, most often due to patent branch vessels feed-
A pulsatile abdominal mass is the most common physical ing the aneurysm sac) is the most common graft-related com-
finding of AAA, but the sensitivity of abdominal palpation plication. It is usually repaired by catheter-based techniques.
for AAA detection is low. Because of the risk of endovascular leak, serial CT angiog-
raphy surveillance is required indefinitely. For this reason,
endovascular repair is often reserved for older patients with
A
increased surgical risk, whereas open repair is recommended
for younger patients at low to average surgical risk.
T H O R AC I C AO RT I C D I S S E C T I O N
Aortic dissection begins with a tear through the arterial intima
that allows pulsating blood to penetrate along the media lon-
gitudinally, separating the arterial wall. The dissection extends
before either reentering the lumen through a second intimal tear
or exiting the artery through an adventitial tear. Dissection can
be catastrophic, leading to occlusion of the affected artery or
its branch vessels or to arterial rupture with varying degrees of
blood loss. Causes include atherosclerosis (and its risk factors),
hypertension, cystic medial necrosis (ascending aorta, including
connective tissue disease processes such as Marfan syndrome),
bicuspid or unicuspid aortic valve, or trauma (blunt or penetrat-
ing). Dissection may also be iatrogenic, such as cardiac surgery
Figure 7.4 Imaging of Abdominal Aortic Aneurysm. A, Ultrasonogram
or invasive angiography. Aortic dissection may complicate preg-
(transverse view) shows a 4.7-cm aneurysm. B, Computed tomogram nancy in at-risk women; when this occurs, it is usually in the third
(contrast-enhanced) shows aneurysm (arrow). trimester. An intramural hematoma (10% of dissection cases)
7. VA S C U L A R D I S E A S E S 101
may also occur if bleeding develops within the media without 45% (compared with 15% if absent). Focal neurologic deficits
intimal tear or flowing blood within a false lumen. A penetrat- imply carotid transection. Hypotension, tachycardia, jugular
ing aortic ulcer (10% of dissection cases) results from an area venous distension, systemic vascular congestion, and pul-
of aortic ulceration that penetrates through the internal elastic sus paradoxus suggest pericardial tamponade due to rupture
lamina with bleeding into the media, often in a segment of ather- into the pericardium. Congestive heart failure is usually due
omatous plaque. Incomplete rupture of the thoracic aorta (in the to acute, severe aortic regurgitation. Acute myocardial infarc-
region of the aortic isthmus) results from a sudden deceleration tion, pericarditis, and complete heart block may also occur.
injury, frequently a motor vehicle crash (Figure 7.5).
The majority of patients with aortic dissection report
Aortic dissection may be due to atherosclerosis, aortic valve sudden severe chest, back, or abdominal pain. The pain is
anomalies, connective tissue diseases, or trauma or may be often described as ripping, tearing, or stabbing.
iatrogenic.
In-hospital mortality is increased in the setting of a pulse
Catastrophic outcomes may result from aortic dissection. deficit.
Penetrating aortic ulcers and intramural hematomas may Pericardial tamponade due to rupture into the pericardium
occur in 10% of dissections. is a potentially devastating result of dissection.
Sudden deceleration injuries, usually due to motor vehicle Severe aortic regurgitation due to aortic annulus disruption
accidents, may cause incomplete aortic rupture. may lead to congestive heart failure.
Other cardiac consequences include acute myocardial
Symptoms of aortic dissection include sudden-onset, infarction, pericarditis, and complete heart block.
severe, often migratory pain in the anterior aspect of the chest,
back, or abdomen; these occur in 70% to 80% of patients (sen- Focal neurologic deficits imply transection of the carotid
sitivity 90%, specificity 84%). The pain is often described as artery.
ripping, tearing, or stabbing. Hypertension is present in
70% of patients. Additional findings include a diastolic mur- Chest radiography may show widening of the superior
mur due to aortic regurgitation (from disruption of the aor- mediastinum (Figure 7.6) and supracardiac aortic shadow,
tic annulus; 20%), pulse deficits (30%), neurologic changes deviation of the trachea from the midline, a discrepancy in
(20%), and syncope (13%). A pulse deficit portends a worse diameter between the ascending aorta and the descending
outcome; when it is present, in-hospital mortality increases to aorta, and pleural effusion. Electrocardiography most com-
monly shows left ventricular hypertrophy, but ST-segment
depression, ST-segment elevation, T-wave changes, and the
changes of acute pericarditis and complete heart block occur
in up to 55% of patients. Diagnosis is readily and accurately
102 C A R D I O L O GY
A B
Figure 7.7 Imaging of Aortic Dissection. A and B, Multiplane transesophageal echocardiograms. Longitudinal view (A) shows an intimal flap in the
ascending aorta. In diastole (B), the intimal flap prolapses through the aortic valve (arrow). C, Computed tomogram (contrast-enhanced) shows a
spiraling intimal flap in the transverse aortic arch.
confirmed with TEE, CT angiography, and MR angiography, substernal pain, aortic valve incompetence, decreased pulse
all of which are both sensitive and specific (Figure 7.7). Test or blood pressure in the right arm, decreased right carotid
choice is determined by availability and local expertise. pulse, pericardial friction rub, syncope, and ischemic electro-
cardiographic changes. Patients with Marfan syndrome typi-
Chest radiographic findings may include superior cally have type A dissections. Clinical clues to type III aortic
mediastinal widening, a supracardiac aortic shadow, dissection include interscapular pain, hypertension, and left
tracheal deviation, pleural effusion, or discrepant ascending pleural effusion.
and descending aortic diameter.
Type I and II dissections involve the ascending thoracic
Left ventricular hypertrophy is a common electrocardio-
aorta. They are also known as proximal or type A
graphic finding, but ST- and T-wave changes, electrical
dissections.
changes due to pericarditis, and complete heart block may
also occur. Type III dissections are confined to the descending
aorta. They are also called distal or type B
TEE or angiography (by CT or MRI) provides an accurate
dissections.
diagnosis, but test choice is determined by availability, the
patients hemodynamic stability, and radiology expertise. Various clinical findings can provide clues to the dissection
location and classification.
Aortic dissections are classified by location relative to
the ascending aorta (Figure 7.8). Aortic dissection involving Acute dissections of the ascending thoracic aorta require
the ascending aorta is designated as type I or II (proximal, urgent surgical repair because of the high mortality, whereas
type A), and dissection confined to the descending thoracic acute dissections of the descending thoracic aorta should be
aorta is designated as type III (distal, type B). Clinical clues managed medically with aggressive blood pressure and heart
to type I and type II (ascending) aortic dissection include rate control. Intravenous -adrenergic blockers (goal heart
7. VA S C U L A R D I S E A S E S 103
Box 7.1 INITIAL PHARMACOLOGIC THERAPY FOR
ACUTE AORTIC DISSECTION
Hypertensive patients
Sodium nitroprusside intravenously (2.55.0 mcg/kg per min)
with
Propranolol intravenously (1 mg every 46 h)
Goal: Systolic blood pressure in the range of 110 mm Hg (or the
lowest level maintaining a urine output of 2530 mL/h) until
oral medication is started
or
Esmolol, metoprolol, or atenolol intravenously (in place of
propranolol)
or
Labetolol intravenously (in place of sodium nitroprusside & a
-blocker)
Normotensive patients
Propranolol intravenously (1 mg every 46 h) or orally (2040
mg every 6 h) (metoprolol, atenolol, esmolol, or labetalol
may be used in place of propranolol)
Type I Type II Type III
104 C A R D I O L O GY
stable, investigations and patient status should direct Coronary and carotid artery disease are common comorbid
further management. conditions. Hypertension, tobacco use, trauma, infection,
familial tendency, and some connective tissue diseases and
Surgical repair of dissections of the descending thoracic
vasculitides are additional risk factors. Although most periph-
aorta is needed when organ malperfusion is present,
eral artery aneurysms are asymptomatic, rupture, infection,
aneurysm enlargement occurs, blood pressure or symptoms
embolization, and pressure on surrounding structures can also
cannot be controlled, or the dissection progresses despite
occur. Rupture is less common in peripheral artery aneurysms
best medical management.
than embolization.
Surgical repair of dissections of the descending thoracic
aorta should be considered when aortic diameter is greater Men >60 years old are more likely than younger men
than 4.0 cm or there is a persistently patent false lumen. or women to have peripheral artery aneurysms due to
atherosclerosis.
T H O R AC I C AO RT I C AT H E RO S C L E RO S I S Additional risk factors include trauma, infection, familial
tendency, and some connective tissue diseases and
The presence of thoracic aortic atheroma or thrombus (including vasculitides.
at the arch) is a considerable risk factor for ischemic stroke and
systemic embolization. Treatment with a statin and antiplatelet Most peripheral artery aneurysms are asymptomatic.
therapy is recommended for patients with aortic arch atheroma to Rupture is less common than embolization.
reduce the risk of stroke, unless contraindicated. Anticoagulation
with warfarin (goal international normalized ratio, 2.03.0) may Iliac artery aneurysms are usually associated with AAA,
be a reasonable option and can be considered in patients with but they may occur as an isolated finding. Obstructive uro-
prior stroke. TEE accurately assesses aortic atheromatous disease. logic symptoms, iliac vein obstruction, and unexplained groin
Aortic arch atheroma larger than 4.0 mm and mobile thrombus or perineal pain can be caused by iliac artery aneurysm and
of any are substantial risk factors for embolization. should be investigated. Repair is indicated when the aneurysm
Other complications of thoracic aortic atherosclerosis size is 3.5 cm or more. Femoral artery aneurysm repair is indi-
include subclavian stenosis leading to intermittent arm claudi- cated at a size of 3.0 cm or more. Popliteal artery aneurysm may
cation or subclavian steal syndrome. When these occur, rever- lead to thromboembolization, neuropathy, or thrombophlebi-
sal of blood flow (eg, during arm exercise) may lead to transient tis in the popliteal distribution, venous obstruction, infection,
cerebral ischemia. Physical findings may include reduced or rupture. Repair is indicated when the aneurysm is more
upper extremity pulses or blood pressure differential between than 2 cm or when thrombus is present. The greatest concern
arms. Delayed pulsation in an arm may be noted (Circulation. for popliteal aneurysm is thromboembolism to distal arteries.
2010 Apr 6;121[13]:e266369. Epub 2010 Mar 6). Popliteal artery aneurysm is bilateral in 50% of patients, and
40% of patients have 1 or more aneurysms at other sites, most
Atheromatous disease of the thoracic aorta is a considerable commonly the abdominal aorta.
risk factor for stroke and systemic embolization.
Statins and antiplatelet therapy are recommended. Iliac and popliteal artery aneurysms can occur in the
setting of AAA but may occur in isolation.
Anticoagulation should be considered in patients with a
prior history of stroke. Carotid and coronary artery disease are common comorbid
conditions in the setting of iliac artery aneurysms.
Intermittent arm claudication due to subclavian stenosis or
subclavian steal syndrome may occur with thoracic aortic Embolism is the most common complication of femoral
atherosclerosis. and popliteal artery aneurysms.
Subclavian steal syndrome may lead to transient cerebral Repair is indicated at an aneurysm size of >3.5 cm for the
ischemia due to blood flow reversal. iliac artery, >3.0 cm for the femoral artery, and >2 cm for
the popliteal artery, or when an aneurysm is symptomatic.
Reduced arm pulses, blood pressure discrepancy between
arms, or delayed pulsation in an arm should raise suspicion
of subclavian steal syndrome.
P E R I P H E R A L A RT E RY D I S E A S E
Peripheral artery disease of the legs may be symptomatic at
presentation (50%) or may be found incidentally (50%). Of
P E R I P H E R A L A RT E R I A L C O N D I T I O N S symptomatic patients, 40% have intermittent claudication and
10% have critical limb ischemia at diagnosis. Intermittent clau-
dication is the most common symptom and is defined as exer-
P E R I P H E R A L A RT E RY A N EU RYS M S
tional pain involving the calf that impedes walking, resolves
Peripheral artery aneurysms are most common in men older within 10 minutes of rest, and neither begins at rest nor resolves
than 60 years because they are most often due to atherosclerosis. on walking (Monogr Ser World Health Organ. 1968;56:
7. VA S C U L A R D I S E A S E S 105
Table 7.1 DIFFERENTIAL DIAGNOSIS OF Table 7.2 GRADING SYSTEM FOR LOWER-EXTREMITY
INTERMITTENT CLAUDICATION AND ARTERIAL OCCLUSIVE DISEASE
PSEUDOCLAUDICATION
ABI
CLAUDICATION PSEUDOCLAUDICATION GRADE Supine Resting Postexercisea
106 C A R D I O L O GY
All patients with peripheral artery disease should walking distance has been shown to improve 200% to 300%
receive aspirin (81325 mg daily) or clopidogrel if they are when treadmill or track walking is used to the point of symp-
aspirin-allergic to reduce the risk of limb loss, need for vascu- tom reproduction with rest intervals in 30- to 60-minute ses-
lar surgery, and incidence of major coronary and cerebrovas- sions, 3 times weekly for 3 months.
cular events. Clopidogrel (75 mg daily) has been shown to be
more effective than aspirin for preventing major atheroscle- All patients with peripheral artery disease should
rotic vascular events in patients with peripheral artery disease participate in supervised walking to improve walking
(Lancet. 1996 Nov 16;348[9038]:132939). Cilostazol can be distance.
used for relief of claudication symptoms and improves walk-
ing distance to claudication compared with pentoxifylline or Absolute indications for revascularization (surgical bypass
placebo, but it is contraindicated in patients with heart failure. or angioplasty and stenting) include ischemic rest pain and
Although there is no evidence that treatment of hypertension nonhealing ulceration. Ischemic ulcers are typically found at
alters the progression of claudication, blood pressure should pressure points on the foot (eg, between toes kissing ulcers)
be controlled to reduce morbidity and death due to cardiovas- and point of contact with a shoe (eg, medial aspect of great toe,
cular and cerebrovascular disease. The angiotensin-converting lateral aspect of fifth toe, and heels). A relative indication for
enzyme inhibitor ramipril reduces the risk of ischemic cardi- revascularization includes lifestyle-limiting intermittent clau-
ovascular events in patients with peripheral artery disease and dication. Duplex ultrasonography, MR angiography, and CT
may increase walking distance in select patients, in addition angiography define anatomic localization of disease and pro-
to its renal protective effects in diabetes. Statins reduce car- vide a roadmap necessary for endovascular or surgical therapeu-
diovascular events in patients with peripheral artery disease, tic planning.
reduce new or worsening claudication, and improve walk- Indications for amputation are severe rest pain with no
ing distance and pain-free walking time. All patients with revascularization option, limb gangrene, or life-threatening
peripheral artery disease should receive treatment to reduce infection. Below-knee amputation is associated with a mortal-
the low-density lipoprotein cholesterol value to less than 100 ity rate of 10% perioperatively and 25% at 1 year. The primary
mg/dL (<70 mg/dL in patients with atherosclerosis in other healing rate with below-knee amputation is 60%, and 15% of
circulatory beds). Systemic antibiotic therapy should be ini- patients will eventually need above-knee amputation.
tiated promptly in patients with critical limb ischemia, skin
ulcerations, or evidence of limb infection. Patients at risk of Ischemic rest pain and nonhealing ulcers are absolute
critical limb ischemia (ABI <0.4 in a nondiabetic patient or indications for revascularization (surgical or percutaneous),
any diabetic with known lower extremity peripheral artery whereas lifestyle-limiting intermittent claudication is a
disease) should undergo regular foot inspection to detect relative indication for revascularization.
objective signs of critical limb ischemia ( J Vasc Surg. 2007
Jan;45[Suppl S]:S567). Foot care and protection are of par- Pressure points and contact points with footwear are
amount importance in patients with diabetes mellitus who common locations for ischemic ulcers.
have peripheral artery disease. The combination of peripheral Ultrasonography, MR angiography, and CT angiography
neuropathy, small-vessel disease, and peripheral artery disease are used to define location of disease and allow mapping
in patients with diabetes mellitus makes foot trauma more for revascularization.
likely to be associated with a nonhealing wound or ulcer.
Below-knee amputation has a 60% primary healing rate,
Medical management of peripheral artery disease includes but it is associated with a 10% perioperative mortality rate
treatment with aspirin or clopidogrel and statin therapy. and a 25% 1-year mortality rate. Fifteen percent of patients
Lipid levels (low-density lipoprotein) should be lowered, will need above-knee amputation in the future.
and angiotensin-converting enzyme inhibitor therapy with
ramipril should be considered. Blood pressure management
is strongly encouraged. AC U T E A RT E R I A L O C C LUS I O N
Cilostazol relieves claudication symptoms and increases Acute arterial occlusion is suggested by the sudden onset of
walking distance. extreme pain and paresthesia of the involved limb. It is impor-
tant to distinguish thrombus due to local plaque rupture
Regular foot inspection for signs of critical limb ischemia from an embolic source because the natural histories of these
is necessary in diabetics and patients with peripheral artery 2 mechanisms differ. Features suggestive of local thrombus
disease who are at risk (ABI <0.4). include known arterial occlusive disease of the involved limb,
Foot care and foot protection are particularly important in which can be identified by examining the pulse integrity of the
patients with diabetes mellitus because of the increased risk limbs. An embolic cause is suggested by the presence of car-
of nonhealing wounds or ulcers in the setting of peripheral diac disease (valvular or ischemic), atrial fibrillation, proximal
neuropathy and small-vessel disease. aneurysm, or proximal atherosclerotic disease.
The 6 Ps suggestive of acute arterial occlusion include pain,
Supervised walking should be part of the initial treat- pallor, paresthesia, paralysis, poikilothermy (coldness), and
ment for all patients with peripheral artery disease. Maximal pulselessness.
7. VA S C U L A R D I S E A S E S 107
The 6 Pspain, pallor, paresthesia, paralysis, carotid artery stenosis of less than 60% is associated with an
poikilothermy, and pulselessnesshelp distinguish annual stroke risk of less than 1%.
acute arterial occlusion due to plaque rupture from local
thrombus. Carotid artery disease contributes substantially to ischemic
strokes.
An embolic source is suggested by the presence of valvular
or ischemic cardiac disease, atrial fibrillation, proximal An asymptomatic bruit may lead to the diagnosis of carotid
aneurysms, or proximal atherosclerosis; plaque rupture artery disease.
due to local thrombus is suggested by a history of prior
occlusive disease and pulse asymmetry. When carotid artery disease is medically managed, the
annual stroke risk is 3% in asymptomatic significant
stenosis (>70%) and >15% in symptomatic significant
Therapeutic results from thrombectomy are much better in
stenosis.
embolism than in local thrombus. Amputation rates are con-
siderably higher for patients with local thrombus. Infrequent The annual stroke risk of medically managed carotid artery
causes of arterial occlusion include dissection, traumatic stenosis of <60% is <1%.
transection, vasculitis, sepsis or disseminated intravascular
coagulation, compartment syndrome, vasospasm, foreign body Treatment of hypertension, hyperlipidemia, and diabe-
embolization, or tumor. Tissue tolerance to ischemia varies by tes and cessation of tobacco use are strongly recommended.
tissue type. Nerve injury occurs within 4 hours, whereas muscle Antiplatelet therapy should be initiated or continued. Carotid
(6 hours) and skin (10 hours) are relatively more resistant to endarterectomy reduces the annual risk of stroke to 1.8% for
ischemia. Angiography is performed after initiation of intrave- asymptomatic carotid stenosis of 60% or more and to about 4%
nous heparin therapy and foot protection. After confirmation of for symptomatic carotid stenosis of more than 70%. The risk
the diagnosis, initial therapeutic options include intra-arterial of adverse outcomes (stroke, myocardial infarction, or death)
thrombolysis and surgery (thromboembolectomy). If throm- of carotid artery stenting is similar to that of carotid artery sur-
bolysis is the initial treatment, percutaneous treatment or sur- gery in asymptomatic patients with significant carotid artery
gical therapy is usually indicated for the underlying stenosis (if stenosis. Carotid artery endarterectomy has been shown to
present) for improvement of long-term patency rates. be superior to carotid artery stenting in patients with sympto-
matic severe carotid artery disease.
Thrombectomy is more effective for treating acute arterial
occlusion that is due to embolism. Management of hypertension, hyperlipidemia, and
Patients with acute arterial occlusion due to local thrombus diabetes are necessary. Antiplatelet therapy should be
are more likely to require amputation. started or continued.
Rarely, arterial occlusion is due to dissection, trauma, Tobacco cessation should be stressed.
vasculitis, sepsis or disseminated intravascular occlusion, Patients with symptomatic severe carotid artery disease
compartment syndrome, vasospasm, foreign body have better outcomes with carotid endarterectomy than
embolism, or tumor. with stenting.
108 C A R D I O L O GY
Table 7.3 CLINICAL CRITERIA FOR Patients have a considerable history of tobacco use.
THROMBOANGIITIS OBLITERANS
Smoking cessation ameliorates the disease course, reducing
Age <40 y (often <30 y)
the risk of ulcers and amputation.
7. VA S C U L A R D I S E A S E S 109
at the point where the artery crosses the outlet. Subclavian Treatment for neurogenic thoracic outlet syndrome is pri-
artery aneurysms tend to thrombose and embolize, processes marily and initially conservative with physical therapy. Severe
that present with embolic digital artery occlusion. cases in which conservative therapy fails may benefit from
thoracic outlet decompression and first rib resection. Patients
Mechanical compression or irritation of the neurovascular with upper extremity venous thrombosis related to thoracic
bundle as it exits the chest cavity through the thoracic outlet syndrome (effort thrombosis or Paget-Schroetter syn-
outlet results in thoracic outlet syndromes, a group of often drome) receive aggressive thrombolytic therapy, anticoagu-
disabling disorders. lation, and first rib resection. Patients with upper extremity
arterial thrombosis related to thoracic outlet syndrome often
The most common thoracic outlet syndrome is neurogenic present with digital ischemia related to thromboembolism
and presents with ulnar nerve distribution numbness, pain, from an axillary-subclavian artery aneurysm. These patients
and tingling. Symptoms are provoked with arm elevation are aggressively treated with surgical repair of the aneurysm,
or when patients work with their arms above their heads. anticoagulation, and thoracic outlet decompression.
A cervical rib arising from the C7 pedicle (rather than the
T1 pedicle) may be present. Neurogenic thoracic outlet syndrome is treated
with physical therapy. In severe cases, thoracic outlet
Symptoms are relieved by arm lowering. decompression and first rib resection may be needed.
Paget-Schroetter syndrome (subclavian vein thrombosis) Upper extremity venous thrombosis (Paget-Schroetter
may be present in patients presenting with venous thoracic syndrome) should be aggressively treated with
outlet syndrome. thrombolytics, anticoagulation, and first rib resection.
Subclavian artery vein aneurysm results from repetitive Thoracic outlet syndromeassociated upper extremity
trauma at the point where the artery crosses the outlet; this arterial thrombosis often presents with digital ischemia
occurs in about 5% of patients with thoracic outlet syndrome. due to embolism from an axillary-subclavian artery
Subclavian vein aneurysms may thrombose and embolize, aneurysm. Affected patients should be aggressively treated
processes that lead to digital artery occlusion. with surgical repair of the aneurysm, anticoagulation, and
thoracic outlet decompression.
The diagnosis of neurogenic thoracic outlet syndrome
(most common presentation) is very complex and is primarily
based on clinical presentation and physical findings. Thoracic VA S O S PA S T I C D I S O R D E R S
outlet maneuvers (costoclavicular active, costoclavicular pas-
sive, hyperabduction, Adson, and elevated arm stress tests) are Vasospastic disorders are characterized by episodic color
performed to aid in the diagnosis. These maneuvers induce changes of the skin resulting from intermittent spasm of the
dynamic compression of the axillary-subclavian artery, which small arteries and arterioles of the skin and digits. These vas-
is identified as dynamic obliteration of the radial pulse. Results cular disorders are important because they may be a clue to
of these maneuvers may be positive in up to 30% of the general another underlying disorder, such as arterial occlusive disease,
population; thus, their specificity and positive predictive value connective tissue disorders, arterial injury, neurologic dis-
are limited. Vascular imaging (ultrasonography, CT angiogra- orders, or endocrine disease. Vasospastic disorders may also
phy, and MR angiography) for neurogenic thoracic outlet syn- be caused by toxins and certain medications, particularly
drome shows dynamic vascular compression with maneuvers -adrenergic blockers. Ergot preparations, estrogen therapy,
in up to 30% of the general population; thus, the usefulness of chemotherapeutic agents, interferon, cyclosporine, clonidine,
imaging in diagnostic evaluation is limited. narcotics, nicotine, and cocaine use are other possible causes.
110 C A R D I O L O GY
Table 7.4 CHARACTERISTIC CLINICAL FEATURES OF focuses on protection from cold and avoidance of
PRIMARY AND SECONDARY RAYNAUD SYNDROME vasoconstrictive triggers. Calcium channel blockers
and -adrenergic blockers may be used when not
CLINICAL FEATURE PRIMARY SECONDARY
contraindicated.
Symmetry Bilateral Unilateral or bilateral Raynaud phenomenon is due to a fixed digital artery
Pulses Normal Abnormal
obstruction, which may be due to various causes,
including connective tissue disease, vasculitis, embolism,
Skin ulcers Absent May be present atherosclerosis, and drugs. Distribution is typically
Gangrene, tissue loss Absent May be present
asymmetric. Associated findings include pulse deficits and
ischemic changes.
Vascular laboratory finding Vasospasm Fixed obstruction
L I VED O R ET I CU L A R I S
Secondary Raynaud Phenomenon
Livedo reticularis is due to spasm or occlusion of dermal arte-
In contrast to Raynaud disease, patients with secondary rioles leading to a bluish mottling of the skin in a lacy, reticu-
Raynaud phenomenon are more commonly male and older lar pattern (Figure 7.3). Primary livedo reticularis is idiopathic
than 40 years. It is usually unilateral or asymmetric at onset. and not associated with an identifiable underlying disorder.
There is evidence of fixed digital artery obstruction, which Secondary livedo reticularis is suggested by an abrupt, severe
may be due to various causes, including atherosclerosis, vasculi- onset of symptoms, ischemic changes, and systemic symptoms.
tis, connective tissue diseases, hypothenar hammer syndrome, Most commonly, it is the result of atheroembolism from a prox-
embolism, or drugs (especially -adrenergic blockers and imal aneurysm or from proximal atheromatous plaques. The
ergotamine). Distribution of symptoms is asymmetric with appearance of livedo reticularis in a patient older than 50 years
involvement of few digits. Associated pulse deficits, ischemic should suggest atheroembolism. Other causes of secondary
changes (including digital ulcerations), and systemic signs and livedo reticularis include connective tissue disease, antiphos-
symptoms are often present. Identification of the underlying pholipid antibody syndrome, vasculitis, myeloproliferative
cause is essential to allow appropriate treatment. disorders, dysproteinemias, reflex sympathetic dystrophy, cold
injury, and an adverse effect of amantadine hydrochloride
Raynaud disease (primary) most commonly affects women, therapy.
and age at onset is younger than 40 years.
Secondary Raynaud phenomenon is more common in men Livedo reticularis is due to spasm or occlusion of
older than 40 years. dermal arterioles leading to the pathognomonic skin
appearance.
Raynaud disease is typically bilateral involving multiple
digits. Arterial occlusion and digital ulcerations are Primary livedo reticularis is idiopathic with no identifiable
rare. Cause is unknown, and typically symptoms and cause, whereas secondary livedo reticularis is due to an
signs of systemic disease are not present. Treatment underlying condition and should be further evaluated.
7. VA S C U L A R D I S E A S E S 111
EDEMA
LY M P H E D E M A
The primary form is idiopathic and is managed by avoiding Bilateral Occasional Always
warm temperatures and using aspirin therapy. Nonselective
-adrenergic blockers may also be helpful. Foot involved + +
112 C A R D I O L O GY
Table 7.6 CLINICAL FEATURES OF THE 4 MOST COMMON TYPES OF LEG ULCER
TYPE OF ULCER
Location Medial aspect of leg Toe, heel, foot Lateral, posterior aspect of leg Plantar
diagnosis of lymphedema can be evaluated noninvasively with Therapy includes edema reduction therapy using
lymphoscintigraphy. wrapping, followed by daily compression elastic support in
combination with manual lymphatic drainage, skin care,
Patients with obstructive lymphedema should be evaluated and exercise.
for a malignancy.
Appropriate management of lymphedema leads to reduction
in excess limb volume and improved quality of life.
Medical management of lymphedema includes edema
reduction therapy using bandage wrapping, followed by Treatment of dermatophytosis with antifungal agents is
daily use of custom-fitted, graduated compression (usually necessary.
4050 mm Hg) elastic support. Manual lymphatic drain-
Weight reduction in obese patients is helpful.
age is a type of massage used in combination with skin care,
support and compression therapy, and exercise to manage
lymphedema. A combined multimodality approach may sub-
stantially reduce excess limb volume and improve quality of LEG ULCER
life. Dermatophytosis, if present, should be treated with anti-
fungal agents. Weight reduction in obese patients is beneficial. The cause of lower extremity ulceration usually can be deter-
Surgical treatment of lymphedema (eg, lymphaticovenous mined by a careful clinical examination. Clinical features
anastomosis, lymphedema reduction) may be helpful in care- of the 4 most common types of leg ulcer are summarized in
fully selected patients. Table 7.6.
7. VA S C U L A R D I S E A S E S 113
8.
HYPERTENSION
114
Table 8.1 CLASSIFICATION OF BLOOD PRESSURE FOR initial laboratory studies should focus on detection of second-
ADULTS 18 YEARS OR OLDER a ary causes. Medications that can aggravate or cause hyperten-
BLOOD PRESSURE, mm hg sion are listed in Table 8.4.
CATEGORY Systolic Diastolic
Target Organ Damage
Normal <120 & <80
Target organ damage that can occur as a result of hyperten-
Prehypertension 120139 or 8089 sion is summarized in Table 8.5. Organs typically involved
Hypertension include the heart, brain, kidney, arteries, and eye. Physical
examination should focus on these organs, looking for signs
Stage 1 140159 or 9099 of left ventricular hypertrophy, heart failure, atheroscle-
Stage 2 160 or 100 rosis, stroke, peripheral arterial disease, and retinopathy.
Initial laboratory evaluation should include identifica-
a
Not taking antihypertensive drugs and not acutely ill. When a patients systolic tion of target organ damage, including chest radiography,
and diastolic blood pressures are in different categories, the higher category should
be selected to classify the blood pressure status. electrocardiography, urinalysis with microalbumin, and
Adapted from Chobanian AV, Bakris GL, Black HR, Cushman WC, Green
determination of serum creatinine, sodium, potassium, and
LA, Izzo JL Jr, et al; Joint National Committee on Prevention, Detection, calcium values.
Evaluation, and Treatment of High Blood Pressure. National Heart, Lung, and
Blood Institute; National High Blood Pressure Education Program Coordinating
Committee. Seventh report of the Joint National Committee on Prevention,
Detection, Evaluation, and Treatment of High Blood Pressure. Hypertension. Table 8.3 SECONDARY CAUSES OF HYPERTENSION
2003 Dec;42(6):120652. Epub 2003 Dec 1. Used with permission.
CAUSE KEY FEATURES
Cardiac
Coarctation of the Examine for weak, delayed, or absent femoral
Table 8.2 FOLLOW-UP RECOMMENDATIONS BASED aorta pulse
ON SCREENING BLOOD PRESSURE IN ADULTS Rib notching on chest radiography
SCREENING Obstructive sleep Presents in overweight persons with loud
BLOOD PRESSURE FOLLOW-UPa apnea snoring, large neck circumference, morn-
ing headaches, & daytime sleepiness
Confirm diagnosis with polysomnography
Normal Recheck in 2 y
Renal
Prehypertension Recheck in 1 y
Renal artery stenosis Presents in smokers, persons with CAD, or
Hypertension new-onset HTN after age 50 years
Examine for high-pitched systolic-diastolic
Stage 1 Confirm within 2 mo abdominal bruit
Stage 2 Confirm within 1 mo; if blood pressure >180/110 Fibromuscular Presents in females, usually younger than age
mm Hg, confirm within 1 wk or treat immedi- dysplasia 30 years without family history of HTN
ately, depending on clinical situation Renal parenchymal Check creatinine value & results of urinalysis
disease
a
Modify the follow-up schedule on the basis of knowledge of previous blood pres-
sure measurement, other cardiovascular risk factors, or target organ disease. Abbreviations: CAD, coronary artery disease; HTN, hypertension.
Adapted from Chobanian AV, Bakris GL, Black HR, Cushman WC, Green Adapted from Chobanian AV, Bakris GL, Black HR, Cushman WC, Green
LA, Izzo JL Jr, et al; Joint National Committee on Prevention, Detection, LA, Izzo JL Jr, et al; Joint National Committee on Prevention, Detection,
Evaluation, and Treatment of High Blood Pressure. National Heart, Lung, and Evaluation, and Treatment of High Blood Pressure. National Heart, Lung, and
Blood Institute; National High Blood Pressure Education Program Coordinating Blood Institute; National High Blood Pressure Education Program Coordinating
Committee. Seventh report of the Joint National Committee on Prevention, Committee. Seventh report of the Joint National Committee on Prevention,
Detection, Evaluation, and Treatment of High Blood Pressure. Hypertension. Detection, Evaluation, and Treatment of High Blood Pressure. Hypertension.
2003 Dec;42(6):120652. Epub 2003 Dec 1. Used with permission. 2003 Dec;42(6):120652. Epub 2003 Dec 1. Used with permission.
8. H Y P E RT E N S I O N 115
Table 8.4 DRUGS THAT CAN INCREASE BLOOD Table 8.5 HYPERTENSIVE TARGET ORGAN INJURY
PRESSURE TARGET
DRUG MECHANISM ORGAN INJURY CLINICAL MARKER/DIAGNOSIS
Oral contraceptives (with Induce sodium retention & increase Heart Left ven- S4 gallop, forceful & prolonged apical
high estrogenic activity) renin substrate tricular thrust
Facilitate action of catecholamines hypertrophy Displacement of point of maximal
intensity
Alcohol (>30 mL daily) Activates sympathetic nervous system Chest radiography, ECG,
Increases cortisol secretion echocardiography
Increases intracellular calcium levels Angina History, ECG
Prior myo-
Sympathomimetics & Increase peripheral vascular resistance cardial
amphetamine-like sub- infarction
stances (eg, cold formulas, Prior revascu-
allergy medications, diet larization
pills) Heart failure History
(systolic or Lung rales
Nonsteroidal Induce sodium retention
diastolic) S3 gallop
anti-inflammatory drugs
Edema
Corticosteroids Iatrogenic Cushing disease Chest radiography, echocardiography
116 C A R D I O L O GY
Table 8.6 EFFECT OF LIFESTYLE MODIFICATIONS ON American, obese, or elderly, the antihypertensive effect of
SYSTOLIC BLOOD PRESSURE many medications is enhanced by sodium restriction.
EXPECTED DECREASE Restriction of daily alcohol intake to less than 30 mL of
IN SYSTOLIC BLOOD ethanol (15 mL for women) is associated with a decrease in
MODIFICATION RECOMMENDATION PRESSURE, mm Hg a blood pressure. Because complications of coronary artery
disease are the most common causes of death in hyperten-
Adopt DASH Consume a diet rich 814 sive persons, all risk factors for cardiovascular disease must be
eating plan in fruits, veg-
etables, & low-fat addressed. This includes smoking cessation and treatment of
dairy products the metabolic syndrome.
with a reduced
content of satu- Lifestyle modifications are the initial step for any patient
rated & total fat found to have prehypertension, stage 1 hypertension, or
Reduce weight Normal body weight 520 (per 10 kg) stage 2 hypertension.
(BMI, 18.524.9)
8. H Y P E RT E N S I O N 117
Lifestyle
modifications
Initial
drug choices
Not at goal
blood pressure
Figure 8.1 Algorithm for Treatment of Hypertension. ACEI indicates angiotensin-converting enzyme inhibitor; ARB, angiotensin receptor blocker;
BB, E-blocker; CCB, calcium channel blocker; DBP, diastolic blood pressure; SBP, systolic blood pressure. (Adapted from Chobanian AV, Bakris
GL, Black HR, Cushman WC, Green LA, Izzo JL Jr, et al; Joint National Committee on Prevention, Detection, Evaluation, and Treatment of
High Blood Pressure. National Heart, Lung, and Blood Institute; National High Blood Pressure Education Program Coordinating Committee.
Seventh report of the Joint National Committee on Prevention, Detection, Evaluation, and Treatment of High Blood Pressure. Hypertension. 2003
Dec;42[6]:120652. Epub 2003 Dec 1. Used with permission.)
in blood pressure, and when hypertension is refractory to Options for the management of renovascular hyperten-
treatment. sion include interventional therapies when feasible and
medical therapy for persons who are not candidates for
interventional therapy. Percutaneous transluminal angio-
R E N O VA S C U L A R H Y P E RT E N S I O N
plasty is the treatment of choice for amenable lesions caused
Renovascular hypertension is a potentially curable form of by fibromuscular dysplasia and is an option in some cases
secondary hypertension. Generally, renovascular hyperten- of atherosclerotic renovascular disease. Stent-supported
sion can be grouped into 1) renal artery stenosis and 2) fibro- angioplasty is the best option for most persons with athero-
muscular dysplasia. sclerotic renal artery stenosis, especially for orificial disease.
Clues that suggest renovascular hypertension include lack Recurrent stenosis is common. Surgical intervention is the
of a family history of hypertension, onset of hypertension treatment of choice in patients with aneurysmal or severe
before age 30 years (consider fibromuscular dysplasia, espe- atherosclerotic disease of the aorta requiring concomitant
cially in white women), onset of hypertension after age 50 aortic reconstruction and in patients in whom percutaneous
years (consider atherosclerotic renovascular disease, especially intervention has failed. The role of interventional therapy
in a smoker or a person with coronary or peripheral arterial for preservation of renal function in ischemic nephropathy
disease), or presentation with accelerated hypertension. is uncertain.
The most important physical finding is an abdominal bruit, The medical treatment of renovascular hypertension is
especially a high-pitched systolic-diastolic bruit in the upper similar to that of essential hypertension. The presence of
abdomen or flank. However, 50% of persons with renovascu- severe bilateral renal artery stenosis (ischemic nephropathy) is
lar hypertension do not have this finding. suggested by an acute decline in renal function either after the
118 C A R D I O L O GY
initiation of therapy with an angiotensin-converting enzyme hypokalemia or marked hypokalemia precipitated by usual
inhibitor or an angiotensin receptor blocker. doses of diuretics.
Screening for primary aldosteronism is done using the
Renovascular hypertension can be grouped into 1) renal
aldosterone-renin ratio.
artery stenosis and 2) fibromuscular dysplasia.
Think of bilateral renal artery stenosis in a patient with
acute decline in renal function after starting therapy P H EO C H RO MO C Y TO M A
with an angiotensin-converting enzyme inhibitor or an
angiotensin receptor blocker. Pheochromocytoma is a tumor that causes hypertension
due to excess catecholamines. Tumors can be present in the
adrenal medulla (pheochromocytomas) or sympathetic gan-
R E NA L PA R E N C H Y M A L D I S E A S E glia (extra-adrenal pheochromocytomas or paragangliomas).
Pheochromocytoma is rare; its incidence is 2 to 8 cases per
Renal parenchymal disease is a common secondary cause of million persons per year. The prevalence is 0.5% among per-
hypertension. Moreover, hypertension in patients with renal sons with hypertension.
parenchymal disease is associated with a more rapid loss of A rule of 10 describes the typical locations of pheochro-
renal function. The major mechanisms of hypertension in renal mocytomas: 10% are extra-adrenal; 10% of extra-adrenal gland
disease include volume expansion from impaired renal elimi- tumors are extra-abdominal; 10% occur in children; 10% are
nation of salt and water, oversecretion of renin, and decreased multiple or bilateral; 10% recur after the initial resection; 10%
production of renal vasodilators. Angiotensin-converting are malignant; 10% are found in persons without hyperten-
enzyme inhibitors reduce proteinuria and high glomerular sion; and 10% are familial.
transcapillary pressures, slowing further loss of renal function. Patients can present with paroxysms of hypertension,
However, they can cause hyperkalemia and an acute decline but most have sustained hypertension. Paroxysms can be
in renal function. Modest acute decreases in renal function associated with headache, diaphoresis, and palpitations. The
(<30%) should be tolerated because they are often followed presentation of pheochromocytoma corresponds to 5 Ps: pres-
by stabilization and preservation of renal function. Calcium sure, pain, palpitations, perspiration, and pallor. Patients can
channel blockers are effective blood pressurelowering agents also present with symptoms mimicking an anxiety attack.
in persons with chronic kidney disease. Nondihydropyridine Additionally, pheochromocytomas can be discovered as an
calcium channel blockers reduce proteinuria, but dihydropyri- incidental adrenal mass on an imaging study.
dine calcium channel blockers do not. Pheochromocytoma is associated with multiple endo-
crine neoplasia (MEN) type 2a (medullary thyroid carci-
P R I M A RY A L D O S T E RO N I S M
noma, pheochromocytoma, and parathyroid tumors), MEN
type 2b (medullary thyroid cancer, pheochromocytoma, and
The syndrome of primary aldosteronism is characterized by neuroma), neurofibromatosis, von Hippel-Lindau disease
clinical and laboratory consequences of autonomous over- (pheochromocytoma, retinal hemangiomatosis, cerebellar
production of aldosterone by the adrenal glands. These hemangioblastomas, epididymal cystadenoma, renal and pan-
consequences are hypertension, hypokalemia, alkalosis, hyper- creatic cysts, and renal cell carcinoma), and familial paragan-
glycemia, and increased aldosterone levels. Prevalence esti- glioma syndrome.
mates range from 2% to 15% of the hypertensive population. Investigations for pheochromocytoma should be selec-
Primary aldosteronism should be suspected in hyperten- tive and based on results of history and examination. Initial
sive patients who have spontaneous hypokalemia or marked studies involve measurement of catecholamine metabolites.
hypokalemia precipitated by usual doses of diuretics. However, Plasma or urine measures of catecholamines alone lack diag-
in many patients with primary aldosteronism, the potassium nostic accuracy. Measurement of plasma free metanephrines
level is normal. Additionally, it should be suspected in those is considered the test of choice by some because of its high
with an adrenal mass, a history of early-onset hypertension, or sensitivity. Measurement of plasma free metanephrines should
a first-degree relative with primary aldosteronism. be strongly considered if a familial syndrome is suspected, if
Screening for primary aldosteronism is done using the the person has a previous history of pheochromocytoma, or
aldosterone-renin ratio. This should be measured when the if clinical suspicion is high. A negative result for either the
patient is not taking any aldosterone-blocking medications. plasma test or the urine test excludes the diagnosis in most
In essential hypertension, the average value of the ratio is 5.5. cases.
A ratio more than 15 to 20 suggests the diagnosis of primary Because of the low prevalence of pheochromocytoma,
aldosteronism. false-positive results outnumber true-positive results during
Treatment of primary aldosteronism can involve spirono- screening for this disorder. Diet, medications, and physiologic
lactone, eplerenone, other antihypertensive medications, or stresses can interfere with the tests.
surgery. Computed tomography or magnetic resonance imaging of
the abdomen and pelvis is the initial test used to locate a tumor
Primary aldosteronism should be suspected in any after biochemical testing has confirmed the presence of the
hypertensive person who presents with spontaneous disorder. Treatment is surgical. Preoperatively, administration
8. H Y P E RT E N S I O N 119
of a phenoxybenzamine is needed to control blood pressure Gestational hypertension is increased blood pressure that
and cardiac rhythm. Because pheochromocytomas can recur develops for the first time during pregnancy without findings
in 10% of cases, long-term biochemical follow-up is required. of preeclampsia. If gestational hypertension does not evolve
into preeclampsia by delivery, and if blood pressure normal-
Pheochromocytomas are tumors that cause hypertension izes within 12 weeks post partum, the hypertension is called
due to excess catecholamines. transient hypertension of pregnancy. This is a predictor of the
future development of essential hypertension. If blood pres-
Investigation should be stepwise, with biochemical testing sure remains increased, it is recognized retrospectively as
preceding imaging. chronic hypertension that was previously undiagnosed and
masked by the decrease in blood pressure that occurs during
C OA RC TAT I O N O F T H E AO RTA early pregnancy.
Preeclampsia is defined as a blood pressure greater than
Coarctation of the aorta is a constriction of the vessel usu-
140/90 mm Hg and proteinuria (24-hour urine protein excre-
ally just beyond the takeoff of the left subclavian artery. It
tion greater than 0.3 g) that develops after the 20th week of
is usually detected in childhood when blood pressure in the
gestation. Eclampsia is defined by seizures that occur in the
upper extremities is increased and blood pressure in the lower
presence of preeclampsia and cannot be attributed to other
extremities is low. Weak or delayed lower extremity pulses can
causes. Patients with preeclampsia can also have headache,
also be present. Patients can experience signs of lower extrem-
blurry vision, epigastric pain, nephrotic-range proteinuria
ity claudication. Dilated collateral vessels can cause bruits and
(>3.5 g in 24 hours), oliguria, creatinine level greater than
characteristic rib notching on chest radiography. Treatment is
1.2 mg/dL, low platelet count, evidence of microangiopathic
surgical repair.
hemolytic anemia (abnormal blood smear or increased lactate
dehydrogenase value), increased liver transaminase values, and
O B S T RU C T I VE S L E E P A P N E A pulmonary edema.
Preeclampsia occurs more commonly in African American
Obstructive sleep apnea is associated with hypertension that
women, the relatively young (<18 years), the relatively old
may be severe and resistant to control. Upper body obesity
(>35 years), first pregnancies, twin pregnancies, obese women,
is a risk factor for obstructive sleep apnea and is common in
diabetic patients, and women with a personal or family history
hypertensive persons. Consider the diagnosis of obstructive
of preeclampsia. Preeclampsia that develops before the 20th
sleep apnea in persons who are overweight, snore loudly, have
week of gestation suggests molar pregnancy, fetal hydrops,
a large neck circumference, and complain of morning head-
thalassemia, or renal disease.
aches and daytime sleepiness.
The HELLP syndrome (hemolysis, elevated liver enzymes,
and low platelet count) occurs when intravascular coagulation
OT H E R C AUS E S O F H Y P E RT E NS I O N and liver ischemia develop in preeclampsia. The HELLP syn-
drome can rapidly develop into a life-threatening disorder of
Cushing syndrome should be considered in the hypertensive
liver failure and worsening thrombocytopenia in the presence
person who has impaired fasting glucose and unexplained
of only mild or moderate hypertension. The most serious com-
hypokalemia.
plication of the HELLP syndrome is liver rupture, which is
Hypothyroidism is associated with diastolic hyperten-
associated with high maternal and fetal mortality.
sion due to decreased cardiac output and contractility. Tissue
The oral agent of choice is methyldopa. If methyldopa is
perfusion is maintained by an increase in peripheral vascular
ineffective or not tolerated, other drugs can be considered.
resistance mediated by increased activity of the sympathetic
Except for angiotensin-converting enzyme inhibitors, angio-
nervous system.
tensin receptor blockers, and direct renin inhibitors, none of
Hyperparathyroidism may increase blood pressure directly
the currently available drugs are known to increase perinatal
via hypercalcemia, which increases peripheral vascular resis-
morbidity or mortality. Magnesium sulfate is the treatment
tance, and indirectly by increasing vascular sensitivity to
of choice for impending eclampsia or for preventing recurrent
catecholamines.
seizures. The only definitive treatment of eclampsia and the
HELLP syndrome is delivery.
S P E C I A L C A S E S O F H Y P E RT E N S I O N
Blood pressure typically decreases early in pregnancy (first
1618 weeks) and then gradually increases.
P R E G NA N C Y
Preeclampsia is defined as a blood pressure greater than
Blood pressure typically decreases early in pregnancy (first
140/90 mm Hg and proteinuria (24-hour urine protein
1618 weeks) and then gradually increases. Hypertension dur-
excretion >0.3 g) that develops after the 20th week of
ing pregnancy is defined as a systolic blood pressure of 140
gestation.
mm Hg or greater or diastolic blood pressure of 90 mm Hg
or greater. Hypertension during pregnancy is associated with Eclampsia is defined by seizures that occur in the presence
increased neonatal morbidity and mortality. of preeclampsia and cannot be attributed to other causes.
120 C A R D I O L O GY
The oral agent of choice for hypertension in pregnancy is that decreases both preload and afterload. Toxicity is related
methyldopa. to the metabolism of nitroprusside to cyanide in erythrocytes.
Thiocyanate levels should be monitored.
Other medications can be used to reduce blood pressure in
patients with hypertensive emergency on the basis of the clini-
H Y P E RT E N S I O N A N D B R E A S T FE E D I N G
cal scenario, such as angiotensin-converting enzyme inhibitor
Increased blood pressure may persist for 6 to 12 weeks after in scleroderma renal crisis.
delivery in women who have preeclampsia or gestational
hypertension. Most antihypertensive drugs are compat- Hypertensive urgency is severe hypertension without
ible with breastfeeding, and all studied drugs are excreted evidence of acute target organ injury.
into breast milk. Methyldopa and hydralazine have been
Hypertensive emergency is severe hypertension with
shown to be safe. Propranolol and labetalol are the preferred
evidence of acute injury to target organs.
E-blockers. Angiotensin-converting enzyme inhibitors and
angiotensin receptor blockers should be avoided because Sodium nitroprusside is the drug of choice for hypertensive
their use may be associated with adverse neonatal renal emergency.
effects. Diuretics may suppress milk volume. Regardless of
the drug chosen, the infant should be carefully monitored
for adverse effects. S U M M A RY
H Y P E RT E NS I VE C R I S I S
Initial evaluation of hypertension should focus on
Hypertensive crisis can be subdivided into hypertensive 1) determination of lifestyle and cardiovascular risk
urgency and emergency. Hypertensive urgency is severe hyper- factors, 2) identifying and treating secondary causes of
tension without evidence of acute target organ injury. It should hypertension, and 3) identifying target organ damage.
be treated to decrease blood pressure to safer levels over 24 to
48 hours. This decrease can usually be achieved in the outpa- Treat stage 1 hypertension with a single medication.
tient setting with oral agents. Hypertensive emergency is severe Treat stage 2 hypertension with a 2-drug combination.
hypertension with evidence of acute injury to target organs. Use compelling indications, if present, to help select a
It implies the need for hospitalization to immediately lower medication for hypertension.
blood pressure with parenteral therapy. Look for secondary causes of hypertension when there
Sodium nitroprusside is the drug of choice for hyperten- is an unusual age at onset or a sudden change in blood
sive emergency. It is a balanced arterial and venous dilator pressure or when hypertension is refractory to treatment.
8. H Y P E RT E N S I O N 121
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PA RT I I
G A S T R O E N T E R O L O GY A N D H E PATO L O GY
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9.
COLON
Conor G. Loftus, MD
125
Eye lesions occur in 5% of patients. The lesion is usually In patients with active inflammation, avoid potential
episcleritis or uveitis (or both). Episcleritis usually mirrors precipitants of toxic megacolon.
inflammatory bowel disease activity, but uveitis does not.
Patients with episcleritis typically present with a painless red T R E AT M E N T O F U L C E R AT I V E C O L I T I S
eye, whereas those with uveitis often present with a painful
red eye. Uveitis is an indication for emergent ophthalmologic Sulfasalazine and other aminosalicylates can induce remis-
evaluation. sion in 80% of patients with mild or moderate ulcerative coli-
Renal lithiasis occurs in 5% to 15% of patients. In Crohn tis and are effective maintenance therapy for 50% to 75% of
disease with malabsorption, calcium oxalate stones occur. In patients with ulcerative colitis. The active agent of sulfasala-
ulcerative colitis, uric acid stones due to dehydration and loss zine, 5-aminosalicylic acid (5-ASA), is bound to sulfapyridine
of bicarbonate in the stool lead to acidic urine. (the vehicle). Colonic bacteria break the bond and release
Liver disease occurs in 5% of patients. Primary scleros- 5-ASA, which is not absorbed but stays in contact with the
ing cholangitis is more common in ulcerative colitis than in mucosa and exerts its anti-inflammatory action. The efficacy
Crohn disease. If the alkaline phosphatase level is increased in of 5-ASA may be related to its ability to inhibit the lipoxy-
a patient with inflammatory bowel disease, the evaluation for genase pathway of arachidonic acid metabolism or to func-
primary sclerosing cholangitis may include ultrasonography, tion as an oxygen free radical scavenger. It is effective in acute
endoscopic retrograde cholangiopancreatography, and possi- disease and in maintaining remission. The side effects include
bly liver biopsy. reversible sterility in men, malaise, nausea, pancreatitis, rashes,
headaches, hemolysis, impaired folate absorption, hepatitis,
Peripheral joint symptoms mirror bowel activity. aplastic anemia, and exacerbation of colitis. They are related
to the sulfapyridine moiety and occur in 30% of patients who
Axial joint symptoms, such as those of ankylosing take sulfasalazine.
spondylitis and sacroiliitis, can develop and have a The 5-ASAs are a group of drugs that deliver 5-ASA to
progressive course independent of bowel activity. the intestine in various ways. They eliminate sulfa toxicity but
The skin lesions seen most commonly are erythema are more expensive than sulfasalazine. Two of these drugs are
nodosum, pyoderma gangrenosum, and aphthous ulcers of mesalamine and olsalazine. Mesalamine can be given topically
the mouth. (Rowasa suppositories and Rowasa enema) or orally (Asacol,
which is 5-ASA coated with an acrylic polymer that releases
Patients who have inflammatory bowel disease and 5-ASA in the terminal ileum, and Pentasa, which has an eth-
a painful red eye (uveitis) should be referred to an ylcellulose coating that releases 50% of the 5-ASA in the small
ophthalmologist without delay. bowel). Olsalazine consists of 2 molecules of 5-ASA conju-
If a patients alkaline phosphatase level increases with gated with each other. Bacteria break the bond, releasing
inflammatory bowel disease, evaluate for primary sclerosing 5-ASA into the colon.
cholangitis. Aminosalicylates are used for mild to moderately active
ulcerative colitis and for Crohn disease. Topical forms are use-
Central (axial) arthritis, pyoderma gangrenosum, primary ful for proctitis or left-sided colitis; systemic forms are used for
sclerosing cholangitis, and uveitis usually follow a course pancolitis. Of the patients who do not tolerate sulfasalazine,
that is independent of bowel disease activity. 80% to 90% tolerate oral 5-ASA preparations. Side effects
include hair loss, pancreatitis (often in patients in whom
pancreatitis developed while they were taking sulfasalazine),
I N D I C AT I O N S F O R C O L O N O S C O P Y reversible worsening of underlying renal disease, and exacerba-
Colonoscopy is indicated for evaluating the extent of the disease, tion of colitis.
performing biopsies, and evaluating strictures and filling defects.
It is also indicated for differentiating Crohn disease from ulcera- Sulfasalazine and other aminosalicylates can induce
tive colitis when they are otherwise indistinguishable. Another remission in 80% of patients with mild or moderate
indication is monitoring with surveillance biopsies (typically, a ulcerative colitis and are effective maintenance therapy for
total of 32 biopsies) for the development of dysplasia or can- 50%75% of patients with ulcerative colitis.
cer in patients who have had ulcerative colitis (involving colon Sulfasalazine may cause reversible sterility in male patients.
proximal to the rectum) or Crohn colitis for more than 8 years.
Patients who have ulcerative colitis limited to the rectum (ulcer- Other aminosalicylates are equally effective but more
ative proctitis) are not at increased risk of dysplasia and colon expensive; they are useful in 80%90% of patients
cancer; they do not require surveillance colonoscopy. intolerant of sulfasalazine.
126 G A S T R O E N T E R O L O GY A N D H E PATO L O GY
the attacks. Up to 50% of the dose can be absorbed. Oral retardation in pediatric patients, cancer prophylaxis, or inabil-
preparations (prednisone, 40 mg daily) are indicated in active ity to taper a regimen to low doses of corticosteroid (ie, <15
pancolonic disease that is of moderate severity and is unre- mg daily) over 2 to 3 months.
sponsive to aminosalicylates. Prednisolone, the active metab-
olite, is the preferred form of drug for patients with cirrhosis Surgical treatment is curative in ulcerative colitis.
(these patients may not be able to convert inactive prednisone
to prednisolone). For patients who have a prompt response
to oral corticosteroids, the dose may be tapered gradually at T R E AT M E N T O F C RO H N D I S E A S E
a rate not to exceed a 5-mg decrease in the total dose every The use of sulfasalazine is discussed above (see Treatment of
7 days. In severely ill patients, intravenous preparations Ulcerative Colitis subsection). This drug is more effective for
should be given (methylprednisolone, 4060 mg daily) for colonic disease than for small-bowel disease, although 5-ASA
up to 7 to 10 days. If improvement occurs at that time, ther- products designed to be released and activated in the small
apy should be converted to oral corticosteroids (40 mg daily). bowel may prove to be effective in the colon. Sulfasalazine
If improvement does not occur, infliximab (discussed in the does not have an additive effect or a steroid-sparing effect
Treatment of Crohn Disease subsection) may be consid- when given with corticosteroids, nor does it maintain remis-
ered for induction of remission. If there is no improvement, sion in Crohn disease as it does in ulcerative colitis. None of
surgical intervention (colectomy) is required. Because corti- the 5-ASA products are effective for the prophylaxis of Crohn
costeroids are not thought to prevent relapse, they should not disease.
be prescribed after the patient has complete remission and is
free of symptoms. Sulfasalazine is more effective for colonic disease than for
small-bowel disease.
Prescribe topical preparations for patients with active mild
or moderate disease that is limited to the distal colon. It does not have an additive effect or a sparing effect when
given with corticosteroids.
Oral corticosteroids should be added to the regimen of
patients with more proximal disease if aminosalicylates It does not maintain remission in Crohn disease.
have not controlled the attacks.
The use of corticosteroids is discussed above (see
Oral preparations (corticosteroids) are useful in active Treatment of Ulcerative Colitis subsection). Corticosteroids
pancolonic disease of moderate severity. are the agents that are most effective at controlling an acute
Intravenous corticosteroids are given to severely ill patients. exacerbation of Crohn disease. They are the most useful drugs
for treating acute small-bowel Crohn disease and for achiev-
Corticosteroids are useful in remission induction for ing rapid remission. Budesonide is favored for the treatment
ulcerative colitis but are not effective in maintenance of of mild to moderate small-bowel and proximal colonic Crohn
remission. disease since it has limited systemic toxicity owing to first-pass
hepatic metabolism. Budesonide is ineffective for more distal
Total parenteral nutrition does not alter the clinical course colonic Crohn disease.
of an ongoing attack. Indications for its use include severe Azathioprine and 6-mercaptopurine (the active metabolite
dehydration and cachexia with marked fluid and nutrient of azathioprine) have steroid-sparing effects. These immuno-
deficits, excessive diarrhea that has not responded to stand- modulating medications are effective for maintaining remis-
ard therapy for ulcerative colitis, and debilitation in patients sion but not for treating acute disease flares because they have
undergoing colectomy. Use of opiates (or their synthetic deriv- a gradual onset of action (68 weeks). Their use should be
atives) and anticholinergic agents should be limited in ulcera- reserved for patients who are taking corticosteroids for active
tive colitis because they can contribute to the development of disease and whose corticosteroid dose needs to be decreased
toxic megacolon. (or a given dose needs to be maintained in the face of worsen-
ing disease activity).
Total parenteral nutrition does not alter the clinical course
of an ongoing attack. 6-Mercaptopurine is the active metabolite of azathioprine.
Use of opiates and anticholinergic agents should be limited Azathioprine and 6-mercaptopurine are effective as
in ulcerative colitis. maintenance therapy for Crohn disease. Both agents have a
steroid-sparing effect.
Surgical treatment is curative in ulcerative colitis.
Indications for colectomy include severe intractable disease, Metronidazole (at a dose of 20 mg/kg) is effective for
acute life-threatening complications (perforation, hemor- treating perianal Crohn disease. Six weeks may be needed
rhage, or toxic megacolon unresponsive to treatment), symp- for the therapeutic effect to become manifest. Recurrences
tomatic colonic stricture, and suspected or documented colon are frequent when the drug dose is tapered or discontin-
cancer. Other indications are intractable moderate or severe ued, leading to long-term therapy. It is less effective for
colitis, refractory uveitis or pyoderma gangrenosum, growth colonic and small-bowel disease. Side effects include glossitis,
9. C O L O N 127
metallic taste, vaginal and urethral burning sensation, neutro- The anastomotic site is the most likely location for disease
penia, dark urine, urticaria, disulfiram (Antabuse) effect, and recurrence.
paresthesias.
128 G A S T R O E N T E R O L O GY A N D H E PATO L O GY
type A) inclusions in multinucleated cells and is confirmed Histoplasma capsulatum
with isolation of the virus from biopsies. Treatment is acyclo-
vir given orally or intravenously. Histoplasma capsulatum causes an important opportunis-
tic infection in AIDS patients who reside in areas where the
organism is endemic. Colonic involvement is more common
Adenovirus than small-bowel involvement. Symptoms include diarrhea,
Adenovirus reportedly causes diarrhea. The organ affected is weight loss, fever, and abdominal pain. Diagnosis is established
the colon. The main symptom is watery, nonbloody diarrhea. by culture. Colonoscopy may show inflammation and ulcer-
Diagnosis is based on culture and biopsy. There is no treatment. ations, and histologic examination with Giemsa stain shows
intracellular yeast-like H capsulatum within lamina propria
macrophages. Treatment is with amphotericin or itraconazole.
BAC T E R I A L PAT H O G E N S
Mycobacterium avium-intracellulare P ROTO Z OA N PAT H O G E N S
Mycobacterium avium-intracellulare causes infection of the Cryptosporidium
gut in patients with disseminated disease. The small intestine
is affected more commonly than the colon. Symptoms include Cryptosporidium is among the most common enteric patho-
fever, weight loss, diarrhea, abdominal pain, and malabsorp- gens, occurring in 10% to 20% of patients who have AIDS and
tion. Diagnosis is based on finding acid-fast organisms in the diarrhea in the United States and in 50% of those in devel-
stool and tissue, with confirmation from culture of stool and oping countries. The organs affected are the small and large
biopsy specimens. Treatment is multiple drug therapy with intestines and the biliary tree. Symptoms include volumi-
ethambutol, rifampin, and isoniazid. nous watery diarrhea, severe abdominal cramps, weight loss,
anorexia, malaise, and low-grade fever. Biliary tract obstruc-
tion has been reported. Diagnosis is based on microscopic
Other Bacteria identification of organisms in stool specimens with modi-
Other important bacteria include the following: fied acid-fast staining or stains specific for Cryptosporidium.
Organisms may also be identified in biopsy specimens or in
1. Salmonella ser Typhimurium and Salmonella duodenal fluid aspirates. Treatment is with paromomycin,
ser EnteritidisTreatment is with amoxicillin, which improves the diarrhea.
trimethoprim-sulfamethoxazole, or ciprofloxacin.
2. Shigella flexneriTreatment is with Cystoisospora belli
trimethoprim-sulfamethoxazole, ampicillin, or Cystoisospora belli is the most common cause of diarrhea in
ciprofloxacin. developing countries. The small intestine is primarily affected,
3. Campylobacter jejuniTreatment is with erythromycin or but the organisms can be identified throughout the gut and
ciprofloxacin. in other organs. Symptoms include watery diarrhea, cramp-
ing abdominal pain, weight loss, anorexia, malaise, and fever.
AIDS patients with Salmonella, S flexneri, or C jejuni have Diagnosis is based on identifying oval oocysts in stool with
a substantially higher incidence of intestinal infection, bacter- a modified Kinyoun carbolfuchsin stain. Biopsy specimens
emia, and prolonged or recurrent infections because of antibi- from the small intestine may show organisms in the lumen
otic resistance or compromised immune function, or both. or within cytoplasmic vacuoles in enterocytes. Although
C belli oocysts resemble Cryptosporidium oocysts, C belli
oocysts contain 2 sporoblasts. Cryptosporidium oocysts are
F U N G A L PAT H O G E NS small and round and contain 4 sporozoites. Treatment is with
Candida albicans trimethoprim-sulfamethoxazole.
9. C O L O N 129
Other Protozoa PSEUDOMEMBR ANOUS
ENTEROCOLITIS
1. Entamoeba histolyticaTreatment is with metronidazole.
2. Giardia lambliaTreatment is with metronidazole. Pseudomembranous enterocolitis is a necrotizing inflamma-
tory disease of the intestines characterized by the formation of
3. Blastocystis hominisBecause there is no evidence a membrane-like collection of exudate overlying a degenerat-
that B hominis is pathogenic, it does not need to be ing mucosa. Precipitating factors include colon obstruction,
treated. uremia, ischemia, intestinal surgery, and all antibiotics (except
vancomycin).
The rates of symptomatic infection with E histolytica,
G lamblia, or B hominis are not markedly higher than in
patients who do not have AIDS. In most patients with AIDS, A N T I B I OT I C C O L I T I S
E histolytica is a nonpathogenic commensal. Giardiasis may
require prolonged treatment, as in other immunocompetent The symptoms of antibiotic colitis are fever, abdominal
persons. pain, and diarrhea (mucus and blood), which usually occur
1 to 6 weeks after antibiotic therapy. Sigmoidoscopy shows
pseudomembranes and friability. Biopsy specimens show
D I AG N O S T I C EVA LUAT I O N O F PAT I E N T S inflammation and microulceration with exudation. The
WIT H A I D S WH O H AVE D I A R R H E A condition usually remits, but it recurs in 15% of patients.
When patients with AIDS have diarrhea, initial studies Complications include perforation and megacolon. The
include the following: pathogenesis begins with the antibiotic altering the colonic
a. Examination for stool leukocytes flora, resulting in an overgrowth of C difficile. The toxin pro-
duced by C difficile is cytotoxic, causing necrosis of the epithe-
b. Stool cultures for Salmonella species, S flexneri, and C lium and exudation (pseudomembranes). Diagnosis is based
jejuni (t3 specimens) on a stool toxin assay. Enzyme-linked immunosorbent assay
c. Stool examination for ova and parasites (use of saline, (ELISA)-based stool testing has a sensitivity of 70% when a
iodine, trichrome, and acid-fast preparations) single stool sample is examined. The sensitivity increases to
90% when 2 stool samples are examined. Polymerase chain
d. Stool assay for Clostridium difficile toxin reaction (PCR)-based stool testing has a sensitivity of 95%
Additional studies include the following: when a single stool sample is examined. Proctoscopic find-
ings may be normal or show classic pseudomembranes. The
a. Gastroscopy to inspect tissue, to aspirate luminal treatment is to discontinue the use of antibiotics and provide
material, and to obtain biopsy specimens general supportive care (eg, fluids). Avoid use of antimotility
agents. Metronidazole (500 mg 3 times daily) is 80% effec-
b. Examination of duodenal aspirate for parasites and
tive and inexpensive and is recommended in patients with
culture
mild disease (white blood cell [WBC] count <15.0u10 9/L
c. Culture of duodenal biopsy specimens for and normal serum creatinine). Vancomycin (125 mg 4 times
cytomegalovirus and mycobacteria daily) is recommended for patients with more severe disease
(WBC count t15.0u10 9/L and elevated serum creatinine).
d. Colonoscopy to inspect tissue and to obtain biopsy
For a first recurrence, the same antibiotic can be used or
specimens
the drug can be switched. For multiple recurrences, add
e. Culture of biopsy specimens for cytomegalovirus, cholestyramine and prolong the course of treatment with
adenovirus, mycobacteria, and herpes simplex virus antibiotics.
f. Staining biopsy specimens with hematoxylin-eosin for
protozoa and viral inclusion cells, with methenamine Antibiotic colitis: symptoms include fever,
silver or Giemsa stain for fungi, and with the Fite abdominal pain, and diarrhea 16 weeks after
method for mycobacteria antibiotic therapy.
ELISA-based stool testing has a sensitivity of 70%.
Whether further evaluation is needed if the studies listed
above do not yield a diagnosis is a matter of controversy. PCR-based stool testing has a sensitivity of 95%.
Most experts advocate empirical treatment with loperamide Metronidazole is the initial treatment of mild
(Imodium). Others recommend that biopsy specimens from disease.
the duodenum be examined with electron microscopy for
Microsporida or from the colon for adenovirus. Empirical Antibiotic colitis recurs in 15% of patients.
treatment with loperamide is favored because there is no treat- Vancomycin may be used for patients with more severe
ment for either Microsporida or adenovirus. disease and recurrent disease.
130 G A S T R O E N T E R O L O GY A N D H E PATO L O GY
R A D I AT I O N C O L I T I S There are several syndromes. Acute mesenteric isch-
emia is due to embolic obstruction of the superior mesen-
Irradiation injury usually affects both the colon and the small teric artery in 80% of patients. Most emboli (95%) lodge
bowel. Endothelial cells of the small submucosal arterioles are in this artery because of laminar flow, vessel caliber, and
very radiosensitive and respond to large doses of irradiation the angle it takes off from the aorta. This syndrome may
by swelling, proliferating, and undergoing fibrinoid degenera- result in a loss of small bowel and produce short-bowel
tion. The result is obliterative endarteritis. syndrome. Radiography shows ileus, small-bowel obstruc-
Acute disease occurs during or immediately after irradia- tion, and, later, gas in the portal vein. The treatment is
tion; the mucosa fails to regenerate, and there is friability, embolectomy.
hyperemia, and edema. Subacute disease occurs 2 to 12 months Ischemic colitis is due to a transient decrease in perfusion
after irradiation. Obliterative endarteritis produces progressive pressure with chronic, diffuse mesenteric vascular disease.
inflammation and ulceration. Chronic disease consists of fistu- This decrease occurs in severe dehydration or shock and
las, abscesses, strictures, and bleeding from intestinal mucosal results in ischemia of the gastrointestinal tract. It commonly
vessels. Predisposing factors include other diseases that pro- involves areas of the colon between adjacent arteries (ie,
duce microvascular insufficiency (eg, hypertension, diabetes watershed areas) such as the splenic flexure and the recto-
mellitus, atherosclerosis, heart failure) because they accelerate sigmoid. Patients with this syndrome present with abdomi-
the development of vascular occlusion, total irradiation dose nal pain and rectal bleeding. The characteristic radiographic
of 40 to 50 Gy, previous chemotherapy, adhesions, previous feature is thumbprinting of watershed areas. The treatment
surgical procedure and pelvic inflammatory disease, and older is supportive, with administration of intravenous fluids to
age. The elderly are more susceptible. Radiography during maintain adequate tissue perfusion and consideration of
acute disease shows fine serrations of the bowel, and radiog- antibiotics if clinically significant leukocytosis or fever is
raphy during chronic disease shows stricture of the rectum, present. If the condition deteriorates, surgical resection may
which is involved most commonly. Endoscopy shows atrophic be necessary.
mucosa with telangiectatic vessels. Endoscopic coagulation is Nonocclusive ischemia is due to poor tissue perfusion caused
effective treatment for bleeding, but surgery may be required by inadequate cardiac output. It can involve both small and
for fistulas, strictures, or abscesses. large bowels. Its distribution does not conform to an area sup-
plied by a major vessel. It occurs in patients with cardiac failure
Radiation colitis involves both the colon and the small or anoxia and in patients who are in shock.
bowel.
The diagnosis of ischemic colitis is based on the
The endothelial cells of the small submucosal arterioles are
radiographic finding of thumbprinting of watershed areas.
very radiosensitive.
The result is obliterative endarteritis.
C H RO N I C M E S E N T E R I C I S C H E M I A
Predisposing factors: hypertension, diabetes mellitus, ( I N T E S T I NA L A N G I NA)
atherosclerosis, chemotherapy, and >40 Gy of irradiation.
Chronic mesenteric ischemia is uncommon. Symptoms include
The rectum is involved most commonly. postprandial pain and fear of eating, with secondary weight
loss. At least 2 of 3 major splanchnic vessels must be occluded.
Chronic mesenteric ischemia is associated with hypertension,
ISCHEMIA diabetes mellitus, and atherosclerosis. An abdominal bruit is a
clue to the diagnosis. Noninvasive imaging may be performed,
R EV I EW O F VA S CU L A R A NATO MY
including duplex ultrasonography or computed tomography
(CT) or magnetic resonance angiography. The primary treat-
The celiac trunk supplies the stomach and duodenum. The ment options are angiography with possible stent placement
superior mesenteric artery supplies the jejunum, ileum, and or surgical revascularization.
right colon. The inferior mesenteric artery supplies the left Occlusion of the superior mesenteric vein accounts for
colon and rectum. approximately 10% of the cases of bowel ischemia. Risk fac-
tors include hypercoagulable states such as polycythemia vera,
liver disease, pancreatic cancer, intra-abdominal abscess, and
ACU T E I S C H E M I A portal hypertension. Patients present with abdominal pain
The symptoms of acute ischemia are sudden severe abdominal that gradually becomes severe. Diagnosis is based on nonin-
pain, vomiting, and diarrhea (with or without blood). Early in vasive imaging studies such as duplex ultrasonography or CT
the course of ischemia, physical examination findings are normal scan.
despite complaints of severe abdominal pain. Risk factors include
severe atherosclerosis, congestive heart failure, atrial fibrillation Chronic mesenteric ischemia is associated with
(source of emboli), hypotension, and oral contraceptives. hypertension, diabetes mellitus, and atherosclerosis.
9. C O L O N 131
Mesenteric venous thrombosis occurs with interactions of the intestine, the psyche, and, possibly, lumi-
hypercoagulable states. nal factors. Most patients have abdominal pain that is relieved
with defecation or associated with a change in the frequency or
consistency of the stool. Other associated symptoms include
AMEBIC COLITIS abdominal bloating and passage of excessive mucus with the
stool.
The colon is the usual initial site of amebic colitis. Symptoms Patients with irritable bowel syndrome usually have a long
vary from none to explosive bloody diarrhea with fever, duration of symptoms, symptoms associated with situations
tenesmus, and abdominal cramps. Proctoscopy shows dis- of stress, and no weight loss, no intestinal bleeding, and no
crete ulcers with undermined edges and normal adjacent associated organic symptoms (eg, arthritis or fever). Irritable
mucosa. If an exudate is present, swab and make wet mount bowel syndrome is a diagnosis of exclusion: the diagnosis is
preparations for trophozoites. Indirect hemagglutination confirmed by an appropriate medical evaluation that does not
is useful for invasive disease. Radiography shows concen- reveal any organic illness. Always ask whether the patients
tric narrowing of the cecum in 90% of the cases. Treat with symptoms are related to ingestion of dairy foods because
metronidazole. The only pathogenic ameba in humans is E lactase deficiency must be ruled out. Patients who have upper
histolytica. abdominal discomfort and bloating may require an ultrasono-
graphic examination of the abdomen and esophagogastrodu-
Proctoscopy shows discrete ulcers with undermined edges. odenoscopy. Patients who have lower abdominal discomfort
or a change in bowel habits may require stool studies, procto-
Radiography shows concentric narrowing of the cecum in scopic examination, or colonoscopy.
90% of the cases. The treatment of irritable bowel syndrome is reassurance,
The only pathogenic ameba in humans is E histolytica. stress reduction, and a high-fiber diet or the use of fiber supple-
ments. The use of antispasmodics to control abdominal pain
or antimotility agents to control diarrhea should be reserved
for patients who do not have a response to a high-fiber diet.
TUBERCULOSIS
132 G A S T R O E N T E R O L O GY A N D H E PATO L O GY
anorectal inhibitory reflex. Treatment is with sphincter-saving In the evaluation of lower gastrointestinal tract bleeding,
operations. stabilize the patients condition, perform proctoscopy to rule
out rectal outlet bleeding (due to hemorrhoids or anal fis-
Congenital megacolon: increased incidence with Down sure), and obtain a nasogastric tube aspirate or use esophago-
syndrome. gastroduodenoscopy to rule out upper gastrointestinal tract
bleeding. A radionuclide-tagged red blood cell scan may help
If the diagnosis is made when the patient is an adult, the determine whether bleeding is occurring, but it may not pre-
patient usually has a history of chronic constipation. cisely localize the bleeding site. If bleeding stops or occurs at
Radiography of the colon shows a characteristically a slow rate, perform colonoscopy. If the patient is young, per-
narrowed distal segment and a dilated proximal colon. form a Meckel scan. For persistent bleeding that is not amena-
ble to endoscopic therapy, angiography may be used to localize
Rectal biopsy shows aganglionosis. the bleeding site; infusion of vasopressin or embolization may
Evaluation of anorectal motility shows an absence of the be useful. If colonoscopy demonstrates bleeding, injection of
anorectal inhibitory reflex. epinephrine, electrocoagulation, or laser coagulation may be
useful. If bleeding is massive or if marked bleeding continues,
management is surgical.
L OW E R G A S T R O I N T E S T I N A L T R AC T
BLEEDING A N G I O DYS P L A S I A
The evaluation of acute rectal bleeding should begin with a digi- Angiodysplasia is a common cause of lower gastrointestinal
tal rectal examination, anoscopy, and proctosigmoidoscopy. If a tract bleeding, usually involving the cecum and ascending
definitive diagnosis cannot be made, colonoscopy is necessary. colon, in elderly patients. It is associated with cardiac disease
The inability to cleanse the colon appropriately during active (especially aortic stenosis), advanced age, and chronic renal
bleeding makes colonoscopy sometimes difficult to perform insufficiency. There are no associated skin or visceral lesions.
and interpret. Some advocate the use of nuclear scanning if the Colon radiography is of no diagnostic value, but angiography
extent of bleeding is uncertain. If clinically significant active localizes the extent of involvement. Colonoscopy may show
bleeding cannot be treated endoscopically, angiography may lesions, and cautery application may be effective.
be necessary. Colonoscopy is not useful if bleeding in the lower
gastrointestinal tract is torrential, but it may be of some benefit Acquired vascular ectasias are associated with aging, aortic
with a slower rate of bleeding. Colonoscopy is valuable for eval- stenosis, and chronic renal insufficiency.
uating patients who have unexplained rectal bleeding and per- Angiodysplasia usually involves the cecum and ascending
sistently positive findings on tests for occult blood in the stool. colon.
Important causes of lower gastrointestinal tract bleeding Colonoscopy may show lesions. Apply cautery.
are the following:
a. Angiodysplasiausually involves the right colon and D I VE RT I C U L A R D I S E A S E O F T H E C O L O N
small bowel and may respond to endoscopic treatment
b. Diverticular diseaseusually bleeding without other DEFINITIONS
symptoms
Diverticula are acquired herniations of the mucosa and sub-
c. Inflammatory bowel disease (colitis)5% of patients mucosa through the muscular layers of the colonic wall.
present with it Diverticulosis is the mere presence of uninflamed diverticula
d. Ischemic colitispainful and bloody diarrhea of the colon. Diverticulitis is the inflammation of 1 or more
diverticula. The diagnosis and management of the complica-
e. Cancerrarely causes marked bleeding tions of diverticular disease are outlined in Table 9.1.
f. Meckel diverticulumthe commonest cause of lower
gastrointestinal tract bleeding in young patients; it is D I V E RT I CU L I T I S
usually painless
Microperforation or macroperforation of the diverticulum
g. Internal hemorrhoidspainless with small volume of with subsequent peridiverticular inflammation is necessary to
outlet-type bleeding produce diverticulitis. The severity of the clinical symptoms
depends on the extent of the inflammation. Free perforation
h. External hemorrhoidspain with small volume of
is infrequent (diverticula are invested with longitudinal mus-
outlet-type bleeding
cle and mesentery). Local perforations may dissect along the
i. Anal fissurevery painful defecation associated with colonic wall and form intramural fistulas. The clinical presen-
small volume of outlet-type bleeding and often tation is left lower quadrant pain, fever, abdominal distention,
coexisting with constipation change in bowel habits, and, occasionally, a palpable tender
9. C O L O N 133
Table 9.1 DIAGNOSIS AND MANAGEMENT OF COMPLICATIONS OF DIVERTICULAR DISEASE
Diverticulitis Pain, fever, & constipation or diar- Palpable tender colon, leukocytosis Liquid diet (with or without antibiotics) or
rhea (or both) elective surgery
Pericolic abscess Pain, fever (with or without tender- Tender mass, guarding, leukocytosis, Nothing by mouth, intravenous fluids,
ness), or pus in stools soft tissue mass on abdominal films antibiotics, early surgical treatment with
or ultrasonograms colostomy
Fistula Depends on site: dysuria, pneuma- Depends on site: fistulogram, meth- Antibiotics, clear liquids, colostomy; later,
turia, fecal discharge on skin or ylene blue resection
vagina
Perforation Sudden severe pain, fever Sepsis, leukocytosis, free air Antibiotics, nothing by mouth, intravenous
fluids, immediate surgical treatment
Liver abscess Right upper quadrant pain, fever, Tender liver, tender bowel or mass, Antibiotics, surgical drainage, operation
weight loss leukocytosis, increased serum for bowel disease
alkaline phosphatase, lumbosacral
scan (filling defect)
Bleeding Bright red or maroon blood or clots Blood on rectal examination, Conservative; blood transfusion if needed,
sigmoidoscopy, colonoscopy, with or without operation
angiography
mass. Treatment includes resting the bowel or using a low-fiber shows an adenomatous polyp, perform colonoscopy to look for
diet and antibiotics and obtaining an early surgical consulta- additional polyps and to perform polypectomy if necessary.
tion. Indications for surgical treatment include generalized
peritonitis, an enlarging inflammatory mass, fistula formation, Adenomatous polyps are the only neoplastic
colonic obstruction, inability to rule out carcinoma in an area (premalignant) polyp.
of stricture, or recurrent episodes of diverticulitis.
The risk of cancer with any adenomatous polyp depends on
2 features: size >1 cm and the presence of villous elements.
The clinical symptoms of diverticulitis depend on the
extent of inflammation.
Free perforation is infrequent. H E R E D I TA RY P O LY P O S I S S Y N D RO M E S
A S S O C I AT E D WI T H R I S K O F C A N C E R
Clinical presentation is left lower quadrant pain, fever,
abdominal distention, change in bowel habits, and, Only the polyposis syndromes associated with adenomatous
occasionally, a palpable tender mass. polyps carry a risk of cancer.
Treatment includes resting the bowel, administering
antibiotics, and obtaining a surgical consultation. Familial Adenomatous Polyposis
Familial adenomatous polyposis (FAP) is characterized by ade-
nomatous polyps of the colon. Colorectal carcinoma develops
C O L O N I C P O LY P S
in more than 95% of patients, typically by age 40, if prophylac-
tic colectomy is not performed. There are no extra-abdominal
Three types of epithelial polyps are benign: hyperplastic,
manifestations except for bilateral congenital hypertrophy of
hamartomatous, and inflammatory polyps. Hyperplastic
the retinal pigment epithelium. Diagnosis is based on family
polyps are metaplastic, completely differentiated glandular
history and documentation of adenomatous polyps. Screening
elements. Hamartomatous polyps are a mixture of normal
is indicated for all family members, and colectomy is indicated
tissues. Inflammatory polyps are an epithelial inflammatory
before malignancy develops. The inheritance is autosomal
reaction.
dominant; however, the phenotypic expression may vary con-
The fourth type of epithelial polyp, adenomatous pol-
siderably. The second most common malignancy in patients
yps, results from failed differentiation of glandular elements.
with FAP is cancer of the duodenum.
Adenomatous polyps are the only neoplastic (premalignant)
polyps. The 3 types of adenomatous polyps are tubular adenoma,
Colorectal carcinoma develops in more than 95% of
mixed (tubulovillous) adenoma, and villous adenoma. The risk
patients with FAP.
of cancer with any adenomatous polyp depends on 2 features:
size larger than 1 cm and the presence of villous elements. If a There are no extra-abdominal manifestations except for
polyp is found on flexible sigmoidoscopy and biopsy shows a bilateral congenital hypertrophy of the retinal pigment
hyperplastic polyp, no further work-up is needed. If biopsy epithelium.
134 G A S T R O E N T E R O L O GY A N D H E PATO L O GY
The second most common malignancy in patients with C O L O R E C TA L C A N C E R
FAP is cancer of the duodenum.
Colectomy is indicated before malignancy develops. E P I D E M I O L O GY
Colorectal cancer is the second most common cancer in
Gardner Syndrome the United States, with 100,000 new cases and 60,000
In Gardner syndrome, adenomatous polyps involve the deaths annually. Colon cancer eventually develops in 6% of
colon, although rarely the terminal ileum and proximal Americans, and the mortality rate has not decreased since the
small bowel are involved. Colorectal cancer develops in 1930s. The incidence, which varies widely among different
more than 95% of patients. Extraintestinal manifestations populations, is highest in westernized countries. Compared
include congenital hypertrophy of the retinal pigment epi- with past rates, as percentages of the total cases of colorec-
thelium; osteomas of the mandible, skull, and long bones; tal cancer, the rates for cancer of the right colon and sigmoid
supernumerary teeth; soft tissue tumors; thyroid and adre- colon have increased, but the rates for cancer of the rectum
nal tumors; and epidermoid and sebaceous cysts. Screening have decreased: cecum or ascending colon, 25%; sigmoid,
is indicated for family members, and colectomy should be 25%; rectum, 20%; transverse colon, 12%; rectosigmoid,
performed before malignancy develops. The inheritance is 10%; and descending colon, 6%.
autosomal dominant.
Colorectal cancer is the second most common cancer in
Colorectal cancer develops in more than 95% of patients the United States.
with Gardner syndrome. Rates for cancer of the right colon and sigmoid colon have
Gardner syndrome includes extraintestinal increased.
manifestations.
Screening is indicated for family members. ET I O L O GY
The role of the environment as a cause of colorectal cancer is
Turcot Syndrome supported by regional differences and migration studies of
incidence. A high-fat diet increases the risk and may enhance
In Turcot syndrome, adenomatous polyps of the colon are the cholesterol and bile acid content of bile, which is con-
associated with malignant gliomas and other brain tumors. verted by colonic bacteria to compounds that may promote
The inheritance is likely autosomal dominant but with vari- tumors. A high-fiber diet is protective. Increased stool bulk
able penetrance. may dilute carcinogens and promoters and decrease exposure
by decreasing transit time. Fiber components may bind car-
Only the polyposis syndromes associated with cinogens or decrease bacterial enzymes that form toxic com-
adenomatous polyps carry a risk of cancer. pounds. Charbroiled meat or fish and fried foods contain
Perform colectomy for diffuse polyposis only if the polyps possible mutagens. Antioxidants (vitamins A and C), sele-
are adenomatous. nium, vitamin E, yellow-green vegetables, and calcium may
protect against cancer.
Screening is indicated for patients with heritable polyposis
syndromes only if the polyps are adenomatous. A high-fat diet increases the risk of colorectal cancer.
A high-fiber diet has a protective effect.
H E R E D I TA RY P O LY P O S I S SY N D RO M E S Charbroiled meat or fish and fried foods contain possible
N OT A S S O C I AT E D WIT H R I S K O F mutagens.
CANCER
Peutz-Jeghers Syndrome
G E N ET I C FAC TO R S
In Peutz-Jeghers syndrome, hamartomas occur in the small
Certain oncogenes amplify or alter gene products in colon
intestine and, less commonly, in the stomach and colon.
cancer cells, and aneuploidy is characteristic of more aggres-
Pigmented lesions of the mouth, hands, and feet are associ-
sive tumors. The carbohydrate structure of colonic mucus is
ated with ovarian sex cord tumors and tumors of the proximal
altered in colon cancer. Cell-cell interaction possibly has a role
small bowel. The inheritance is autosomal dominant.
in cancer development.
Genetic predisposition has a role in many patients with
Peutz-Jeghers syndrome is characterized by hamartomas of
colon cancer. Inheritance of FAP syndromes is autosomal
the small intestine.
dominant, and most colon cancer arises in adenomatous
Pigmented lesions of the mouth, hands, and feet are polyps. Hereditary nonpolyposis colon cancer (Lynch syn-
associated with ovarian sex cord and proximal small-bowel drome) is an autosomal dominant disease that may account
tumors. for up to 5% of cases of colon cancer. Genetic susceptibility
9. C O L O N 135
in the general population also has a role; for example, there is the portal vein to the liver. The surgical-pathologic stage of the
a 3-fold increased risk of colorectal cancer in first-degree rela- primary tumor describes the depth of invasion and the extent
tives of patients with sporadic colorectal cancer. of regional lymph node involvement, which are important in
determining prognosis.
Aneuploidy is characteristic of more aggressive tumors.
Genetic predisposition to cancer exists in many patients Modified Dukes Classification
with colon cancer.
Survival is determined by the extent of the invasion, which is
Inheritance of FAP is autosomal dominant. categorized according to the modified Dukes classification:
There is a 3-fold increased risk of colorectal cancer in
A: mucosa, submucosa (5-year survival, 95%)
first-degree relatives of patients with sporadic colorectal
cancer. B1: into, not through, the muscularis propria without
nodal involvement (85%)
B2: through the bowel wall without regional nodal
R I S K FAC TO R S F O R C O L O R EC TA L C A N C E R involvement (70%85%)
The risk factors for colorectal cancer include the following: C1: as in B1 but with regional nodes involved (45%55%)
a. Age older than 40The risk increases sharply at age 40, C2: as in B2 but with regional nodes involved (20%30%)
doubles each decade until age 60, and peaks at age 80. D: distant metastases (<1%)
b. Personal history of adenoma or colon cancerThe
risk increases with the number of adenomas; 2%6%
of patients with colon cancer have synchronous colon Regional Node Involvement and Prognosis
cancer, and 1.1%4.7% have metachronous colon cancer.
The extent of regional node involvement and prognosis are as
c. Inflammatory bowel diseaseDysplasia precedes follows: 1 to 4 nodes, 35% recur; more than 4 nodes, 61% recur.
cancer; the cancer rate begins to increase after 8 years of
ulcerative colitis and increases 10% per decade of disease.
After 25 years, the risk is 15%20%. The risk is greatest Other Pathologic Features and Prognosis
for pancolitis. The risk of colon cancer is not increased An ulcerating or infiltrating tumor is worse than an exophytic
in patients with ulcerative proctitis (involvement of the or polypoid tumor. Poorly differentiated histologic features
rectum only). Cancer risk is not related to the severity of are worse than highly differentiated ones. Venous or lymphatic
the first attack, disease activity, or age at onset. The rate of invasion has a poor prognosis, as does aneuploidy.
colon cancer is also increased 420 times in Crohn disease
or ileocolitis. A family history of colon cancer is a risk
factor, and a personal history of female genital or breast Clinical Features and Prognosis
cancer carries a 2-fold increased risk of colon cancer. A high preoperative level of carcinoembryonic antigen is asso-
Colorectal cancer risk increases among persons older than 40. ciated with a high recurrence rate and a shorter time before
recurrence. The prognosis is poor if obstruction or perforation
Risk increases with the number of adenomas. is present. The prognosis is worse for younger patients than
Among patients with colon cancer, 2%6% have for older patients. The depth of invasion and the extent of
synchronous colon cancer, and 1.1%4.7% have regional lymph node involvement are important in determin-
metachronous colon cancer. ing prognosis.
Cancer rate begins to increase after 8 years of chronic A high preoperative level of carcinoembryonic antigen is
ulcerative colitis. associated with a high recurrence rate and a shorter time
After 25 years, the risk is 15%20%. before recurrence.
The risk is greatest for pancolitis. The prognosis is poor if obstruction or perforation is present.
In Crohn disease, the rate of colon cancer is increased 420 The prognosis is worse for younger patients than for older
times. patients.
PAT H O L O GY A N D P RO G N O S T I C I N D I C ATO R S D I AG N O S I S
Cancer arises in the epithelium and invades transmurally to The clinical presentation is a slow growth pattern. Disease may
penetrate the bowel wall; it then enters the regional lymphat- be present for 5 years before symptoms appear. The symptoms
ics to reach distant nodes. Hematogenous spread is through depend on the location of the disease. Patients with a tumor
136 G A S T R O E N T E R O L O GY A N D H E PATO L O GY
in the proximal colon may present with symptoms of anemia, 1 year, 3 years, and every 5 years thereafter if there has been no
abdominal discomfort, or a mass. Patients with a tumor in the evidence of recurrence.
left colon, which is narrower, may present with obstructive Adjuvant chemotherapy with 5-fluorouracil and levamisole
symptoms, a change in bowel habits, and rectal bleeding. If decreases recurrence by 41% and mortality by 33% in colonic
cancer is suspected, perform a colonoscopy. stage C; it may be beneficial for stage B2. Radiotherapy plus
A metastatic survey includes physical examination, evalua- 5-fluorouracil decreases the recurrence rate in rectal cancer
tion of liver-associated enzymes, chest radiography, and CT scan stages B2 and C, but it is not clear whether there is any sur-
of the abdomen. The preoperative level of carcinoembryonic vival advantage.
antigen is helpful for assessing prognosis and for follow-up.
A single colonoscopy is preferred to exclude synchronous
Symptoms of patients with a tumor in the proximal colon lesions; if the findings are negative, colonoscopy is
may be related to anemia, abdominal discomfort, or a mass. performed at 1 year, 3 years, and every 5 years thereafter.
Tumor in the left colon is characterized by obstructive The use of 5-fluorouracil and levamisole decreases
symptoms, change in bowel habits, and rectal bleeding. recurrence by 41% and mortality by 33% in colonic stage C.
Preoperative level of carcinoembryonic antigen is helpful
for assessing prognosis and for follow-up. P R EV E N T I O N O F C O L O R E C TA L C A RC I N O M A
Primary Prevention
T R E AT M E N T
The steps to be taken in primary prevention are not known,
For most cases, surgical resection is the treatment of choice. although epidemiologic data suggest that a high-fiber, low-fat
This includes wide resection of the involved segment (5-cm diet is a reasonable recommendation.
margins), with removal of lymphatic drainage. In rectal car-
cinoma, a low anterior resection is performed if an adequate
distal margin of at least 2 cm can be achieved; this rectal Secondary Prevention
sphinctersaving operation does not make the prognosis Secondary prevention involves identifying and eradicating
worse in comparison with abdominal perineal resection. The premalignant lesions and detecting cancer while it is still cur-
tumor may require resection to prevent obstruction or bleed- able. Screening includes occult blood screening and colon-
ing even if distant metastases are present. oscopy. With occult blood screening, lesions are detected
at an earlier stage, but this has not decreased mortality. The
For most cases, surgical resection is the treatment of choice. Hemoccult test has a positive predictive value of 20% to 30%
for adenomas and 5% to 10% for carcinomas. With colonos-
copy, earlier-stage lesions are detected and removed.
P O S TO P E R AT I V E M A NAG E M E N T WH E N T H E R E
A R E N O A P PA R E N T M ETA S TA S E S
Recommendations for Screening
A single colonoscopy either preoperatively or within 6 to
12 months postoperatively is needed to exclude synchronous Colon cancer screening recommendations are outlined in
lesions. If the findings are negative, colonoscopy is repeated at Tables 9.2 and 9.3. For average-risk patients (ie, anyone not
FREQUENCY OF SUBSEQUENT
PATIENT RISK AGE AT INITIAL SCREENING SCREENING IF FINDINGS ARE NORMAL
Increased risk
Family history of colon cancer when younger 40 y or 10 y younger than age of relative at Every 5 y
than 60 y cancer diagnosis
Risk of hereditary nonpolyposis colorectal 25 y or 5 y younger than age of relative at Every 2 y until age 40 y; then annually
cancer diagnosis
Risk of familial adenomatous polyposis Flexible sigmoidoscopy at 1012 y Flexible sigmoidoscopy annually until
age 40 y; then colonoscopy every 35 y
Ulcerative colitis or Crohn colitis 810 y after diagnosis of pancolitis or 15 y after Colonoscopy every 13 y
left-sided colitis only; if patient has primary
sclerosing cholangitis, start immediately
Data from ASGE guideline: colorectal cancer screening and surveillance. Gastrointest Endosc. 2006 Apr;63(4):54657 and Winawer SJ, Zauber AG, Fletcher RH,
Stillman JS, OBrien MJ, Levin B, et al. Guidelines for colonoscopy surveillance after polypectomy: a consensus update by the U.S. Multi-Society Task Force on Colorectal
Cancer and the American Cancer Society. Gastroenterology. 2006 May;130(6):187285.
9. C O L O N 137
Table 9.3 COLON CANCER SCREENING with hereditary nonpolyposis colorectal cancer (HNPCC)
RECOMMENDATIONS: FOLLOW-UP INTERVALS FOR syndromes, colonoscopy should be performed at age 25 and
AVERAGE-RISK PATIENTS IF POLYPS ARE FOUND then every 2 years until age 40 and then annually thereafter.
For patients with FAP, annual sigmoidoscopy should be per-
FINDING NEXT COLONOSCOPY
formed beginning at puberty until polyposis is diagnosed, and
then colectomy should be performed. For patients with ulcer-
Hyperplastic polyps only 10 y
ative colitis or Crohn colitis, of more than 8 years duration,
1 or 2 diminutive (<1 cm) tubular 510 y colonoscopy and multiple biopsies are recommended every
adenomas 1 to 2 years; dysplasia indicates the need for more frequent
t3 diminutive polyps; any polyp t1 3 y (if normal findings at endoscopic follow-up and may lead to colectomy.
cm; any villous features; high-grade follow-up, increase interval to
dysplasia every 5 y)
Data from Winawer SJ, Zauber AG, Fletcher RH, Stillman JS, OBrien MJ, Levin
Chronic inflammation on biopsy is the key factor for
B, et al. Guidelines for colonoscopy surveillance after polypectomy: a consen- diagnosing inflammatory bowel disease.
sus update by the U.S. Multi-Society Task Force on Colorectal Cancer and the
American Cancer Society. Gastroenterology. 2006 May;130(6):187285. Sulfasalazine is more effective for colonic disease than for
small-bowel disease, it does not have an additive effect or a
sparing effect when given with corticosteroids, and it does
in the high-risk group), colonoscopy every 10 years after age not maintain remission in Crohn disease.
50 has generally become the diagnostic standard; however, The majority of AIDS patients with diarrhea have 1 or
an annual occult blood test plus sigmoidoscopy every 3 to more identifiable pathogens.
5 years after age 50 is still an alternative. For patients with 1
or 2 small adenomas (<10 mm), surveillance colonoscopy is The diagnosis of ischemic colitis is based on the
recommended in 5 years. For patients with multiple polyps, radiographic finding of thumbprinting of watershed areas.
a polyp larger than 10 mm, or polyps with villous histologic
The clinical symptoms of diverticulitis depend on the
features, surveillance colonoscopy is recommended in 3 years.
extent of inflammation. Clinical presentation is left lower
If a patient has more than 10 polyps, a surveillance colonos-
quadrant pain, fever, abdominal distention, change in
copy is generally recommended in 1 year. For patients with
bowel habits, and, occasionally, a palpable tender mass.
previous colon carcinoma, a single colonoscopy either preop-
Treatment includes resting the bowel, administering
eratively or within 6 to 12 months postoperatively is needed
antibiotics, and obtaining a surgical consultation.
to exclude synchronous lesions. If the findings are negative,
colonoscopy is repeated at 1 year, 3 years, and every 5 years Symptoms of patients with a tumor in the proximal colon
thereafter if there has been no evidence of recurrence. For may be related to anemia, abdominal discomfort, or a mass.
patients with a first-degree relative who has colorectal cancer, Tumor in the left colon is characterized by obstructive
colonoscopy should be performed every 5 years beginning at symptoms, change in bowel habits, and rectal bleeding.
age 40 or at the age that is 10 years younger than the young- For most cases of colorectal cancer, surgical resection is the
est age at which a relative received a diagnosis. For patients treatment of choice.
138 G A S T R O E N T E R O L O GY A N D H E PATO L O GY
10.
PANCREAS
Conor G. Loftus, MD
139
enalapril, erythromycin, metronidazole, and nonsulfa-linked degree of hypoxemia, usually from pulmonary shunting.
aminosalicylate derivatives such as 5-aminosalicylic acid Patients often have atelectasis and may have pleural effusions.
and interleukin 2.
Other causes include hypertriglyceridemia, which may Fever >38.3C suggests infection.
cause pancreatitis if the triglyceride level is greater than
1,000 mg/dL. Look for types I, IV, and V hyperlipoproteinemia
and for associated oral contraceptive use. Hypertriglyceridemia D I AG N O S I S O F AC U T E PA N C R E AT I T I S
may mask hyperamylasemia. Hypercalcemia may also cause pan- Serum Amylase
creatitis; look for underlying multiple myeloma, hyperparathy-
roidism, or metastatic carcinoma. In immunocompetent patients, Determining the serum level of amylase is the most useful test
mumps and coxsackievirus cause acute pancreatitis. In AIDS for diagnosing acute pancreatitis. The level of amylase increases
patients, acute pancreatitis has been reported with cytomegalovi- 2 or 3 hours after an attack and remains increased for 3 or 4
rus infection. Pancreas divisum, or incomplete fusion of the dor- days. The magnitude of the increase does not correlate with the
sal and ventral pancreatic ducts, may predispose some people to clinical severity of the attack. Serum amylase levels may be nor-
acute pancreatitis, although this is a controversial matter. mal in some patients (<10%) because of alcohol consumption
or hypertriglyceridemia. A persistent increase suggests a com-
In nonalcoholic patients with acute pancreatitis, review all plication such as pseudocyst, abscess, or ascites. Serum amylase
medications, check lipid and calcium levels, and rule out is cleared by the kidney. The urinary amylase level remains ele-
gallstones. vated after the serum amylase level returns to normal. Isoenzyme
identification may aid in distinguishing between salivary (ie,
Significant elevation (>3 times normal) of AST or ALT nonpancreatic) and pancreatic sources. Serum lipase levels may
in a patient with acute pancreatitis generally indicates that help distinguish between pancreatic hyperamylasemia and
gallstones are the cause. an ectopic source (lung, ovarian, or esophageal carcinoma).
Several medications can cause acute pancreatitis. Lipase levels are also increased for a longer time than amylase
levels after acute pancreatitis. Computed tomographic (CT)
imaging of the abdomen may be useful. If the amylase level is
C L I N I C A L P R E S E N TAT I O N mildly elevated and there is a history of vomiting but no signs
of obstruction, one should consider performing an esophago-
Pain gastroduodenoscopy to rule out a penetrating ulcer.
Pain may be mild to severe; it is usually sudden in onset and
persistent. Typically, the pain is located in the upper abdomen If the presentation for pancreatitis is classic but the amylase
and radiates to the back. Relief may be obtained by bending value is normal, repeat the amylase test, check urinary
forward or sitting up. The ingestion of food or alcohol com- amylase and serum lipase levels, and scan the abdomen.
monly exacerbates the pain. Patients without pain have a poor Persistent hyperamylasemia suggests a complication.
prognosis because they usually present with shock.
If the amylase level is mildly elevated and there is a history
of vomiting but no signs of obstruction, perform an
Fever esophagogastroduodenoscopy to rule out a penetrating ulcer.
Fever, if present, is low grade, rarely exceeding 38.3C in the
absence of complications. (Fever >38.3C suggests infection.) Nonpancreatic Hyperamylasemia
Nonpancreatic hyperamylasemia may result from parotitis;
Volume Depletion renal failure; macroamylasemia; intestinal obstruction, infarc-
Most patients are hypovolemic because fluid accumulates in tion, or perforation; ruptured ectopic pregnancy; diabetic
the abdomen. ketoacidosis; drugs (eg, morphine); burns; pregnancy; and
neoplasms (lung, ovary, or esophagus).
Jaundice
Physical Findings
Patients with pancreatitis may have a mild increase in the total
Physical findings include tachycardia, orthostasis, fat necrosis, and
bilirubin level, but they usually are not clinically jaundiced.
xanthelasmas of the skin. The Grey Turner sign (flank discolora-
When jaundice is present, it generally results from obstruction
tion) and the Cullen sign (periumbilical discoloration) suggest
of the common bile duct by stones, compression by pseudo-
retroperitoneal hemorrhage. The abdominal findings often are less
cyst, or inflamed pancreatic tissue.
impressive than the amount of pain the patient is experiencing.
140 G A S T R O E N T E R O L O GY A N D H E PATO L O GY
Imaging Studies Analgesics
Chest Radiography Common practice has been to use meperidine (Demerol)
An isolated left pleural effusion strongly suggests pancre- (75125 mg given intramuscularly every 34 hours) instead
atitis; infiltrates may indicate aspiration pneumonia or acute of morphine because meperidine purportedly causes less
respiratory distress syndrome. spasm of the sphincter of Oddi. Meperidine has potentially
toxic metabolites, though, so it has been removed from many
Abdominal Plain Film hospital formularies, and the in vivo link between meperi-
Look for the sentinel loop sign (a dilated loop of bowel dine and sphincter spasm is unclear. Standard methods of
over the pancreatic area) and the colon cutoff sign (abrupt analgesia can generally be used with impunity. The efficacy
cutoff of gas in the transverse colon); pancreatic calcifications of antisecretory drugs (eg, H2 receptor antagonists, anti-
indicate chronic pancreatitis. cholinergic agents, somatostatin, glucagon) has not been
documented.
Ultrasonography
Ultrasonographic examination is the procedure of choice Nutrition
for helping to determine the cause of acute pancreatitis. Patients with severe pancreatitis may require supplemental
Although ultrasonography gives information about the pan- nutrition. This should be provided by means of a nasoenteric
creas and is the best method for delineating gallstones, it is not tube. Total parenteral nutrition is unnecessary in most cases of
a good method if the patient is obese. pancreatitis and should be considered only when enteral feed-
ing has failed or is not feasible.
Computed Tomography
CT is indicated for critically ill patients to rule out necro-
tizing pancreatitis. CT scans are not required for patients with Antibiotics
documented mild interstitial acute pancreatitis. Antibiotics are indicated for prophylaxis of gram-negative
sepsis in patients with necrotizing pancreatitis but not for
Endoscopic Retrograde Cholangiopancreatography patients with nonnecrotizing pancreatitis.
ERCP has no role in the diagnosis of acute pancreatitis
and should be avoided because it may cause infection. Supportive care is the backbone of treatment of acute
pancreatitis.
Endoscopic Papillotomy Eliminate medications that may cause pancreatitis.
Endoscopic papillotomy is indicated when acute pancrea-
titis is associated with jaundice and cholangitis. The use of a nasogastric tube does not shorten the course
or severity of pancreatitis.
An isolated left pleural effusion on chest radiography is Antibiotics are indicated for patients with necrotizing
strongly suggestive of acute pancreatitis. pancreatitis.
On an abdominal plain film, look for the sentinel loop
sign, the colon cutoff sign, and pancreatic C O M P L I C AT I O N S
calcifications.
A local complication is pancreatic phlegmon, a mass of inflamed
CT is indicated for critically ill patients to rule out pancreatic tissue. It may resolve. Pseudocyst, a fluid collection
necrotizing pancreatitis. within a nonepithelial-lined cavity, should be suspected if
ERCP has no role in the diagnosis of acute pancreatitis. there is persistent pain and persistent hyperamylasemia. In
50% to 80% of patients, this resolves within 6 weeks with-
out intervention. A pancreatic abscess develops usually 2 to
T R E AT M E N T
4 weeks after the acute episode and causes fever (>38.3C),
Supportive care is the backbone of treatment, with monitor- persistent abdominal pain, and persistent hyperamylasemia.
ing for complications and treating them when they occur. If a pancreatic abscess is not drained surgically, the mortal-
ity rate is virtually 100%. Give antibiotics that are effective
for gram-negative and anaerobic organisms. Jaundice results
Fluids
from obstruction of the common bile duct. Pancreatic asci-
Restore and maintain intravascular fluid volume; usually this tes results from disruption of the pancreatic duct or a leaking
can be accomplished with crystalloids and peripheral intrave- pseudocyst.
nous catheters. Monitor blood pressure, pulse, urine output, A well-recognized systemic complication of acute pancre-
daily intake and output, and weight. Eliminate medications atitis is acute respiratory distress syndrome. Circulating leci-
that may cause pancreatitis. The use of a nasogastric tube does thinase probably splits fatty acids off lecithin, producing a
not shorten the course or severity of pancreatitis, but it should faulty surfactant. Pleural effusion occurs in approximately 20%
be used for ileus or severe nausea and vomiting. of patients with acute pancreatitis. Aspirate analysis shows a
10. PA N C R E A S 141
high amylase content. Fat necrosis may be due to increased Hereditary pancreatitis is caused by a mutation in the
levels of serum lipase. cationic trypsinogen gene, which is inherited as an autoso-
mal dominant trait with variable penetrance. Onset is before
A local complication of pancreatitis should be suspected age 20, although 20% of patients may present later than this.
if fever, persistent pain, or persistent hyperamylasemia Hereditary pancreatitis is marked by recurring abdominal
occurs. pain, positive family history, and pancreatic calcifications. It
may increase the risk of pancreatic cancer.
Acute respiratory distress syndrome is a complication of Trauma with pancreatic ductal disruption causes
acute pancreatitis. chronic pancreatitis. Protein calorie malnutrition is the
Pleural effusion occurs in approximately 20% of patients most common cause of chronic pancreatitis in Third World
with acute pancreatitis; the fluid has a high amylase countries.
content.
Chronic pancreatitis is commonly caused by alcohol but
A S S E S S M E N T O F S EVE R IT Y
seldom by gallstones or hyperlipidemia.
Most patients with acute pancreatitis recover without any Hereditary pancreatitis occurs in young people with a
sequelae. The overall mortality rate of acute pancreatitis is positive family history and pancreatic calcifications.
5% to 10%, and death is due most often to hypovolemia and Protein calorie malnutrition is the most common cause of
shock, respiratory failure, pancreatic abscess, or systemic sep- chronic pancreatitis in Third World countries.
sis. The Ranson criteria (Box 10.1) and the Acute Physiology
and Chronic Health Evaluation (APACHE) criteria are reli-
able for predicting mortality in acute pancreatitis. Predicted T R I A D O F C H RO N I C PA N C R E AT I T I S
mortality is calculated as follows: less than 3 Ranson criteria,
1%; 3 or 4 criteria, 15%; 5 or 6 criteria, 40%; and 7 or more Patients with chronic pancreatitis present with abdominal
criteria, more than 80%. pain. In addition, the triad of chronic pancreatitis consists
of pancreatic calcifications, steatorrhea, and diabetes melli-
Most patients with acute pancreatitis recover without any tus. Diffuse calcification of the pancreas is due to hereditary
sequelae. pancreatitis, alcoholic pancreatitis, or malnutrition. Local
calcification is due to trauma, islet cell tumor, or hyper-
calcemia. By the time steatorrhea occurs, 90% of the pan-
C H R O N I C PA N C R E AT I T I S creas has been destroyed and lipase output has decreased
by 90%.
Long-term alcohol use (t10 years of heavy consump-
tion) is the most common cause of chronic pancreatitis. Patients with chronic pancreatitis present with abdominal
Gallstones and hyperlipidemia usually do not cause chronic pain, pancreatic calcifications, steatorrhea, and diabetes
pancreatitis. mellitus.
For steatorrhea to occur, 90% of the gland must be
Box 10.1 RANSON CRITERIA
damaged.
On admission
Age > 55 y L A B O R ATO RY D I AG N O S I S
White blood cell count >15u109/L Serum amylase and lipase levels may be normal, and stool fat
Serum glucose >200 mg/dL may be normal. If malabsorption is present, stool fat is more
Serum aspartate aminotransferase >250 U/L than 10 g in 24 hours during a 48- to 72-hour stool collection
Serum lactate dehydrogenase >350 U/L while the patient is consuming a diet with 100 g of fat.
At 48 h after admission For the secretin-cholecystokinin (CCK) test of pancreatic
Pao2 <60 mm Hg function, secretin and CCK are injected intravenously and
Hematocrit decrease >10% then the contents of the small bowel are aspirated and the con-
Serum albumin <3.2 g/dL centration of pancreatic enzymes is determined.
Serum urea nitrogen increase >5 mg/dL In the bentiromide test, p-aminobenzoic acid (PABA) con-
Serum calcium <8 mg/dL jugated with N-benzoyl tyrosine (bentiromide) is given orally.
Estimated fluid sequestration >4 L If chymotrypsin activity is adequate, the molecule is cleaved
and PABA is absorbed and excreted in the urine. This test
Abbreviation: U, units.
requires a normal small intestine (normal d-xylose test) and is
Adapted from Ranson JHC. Acute pancreatitis: surgical management. In: Go
VLW, Gardner JD, Brooks FP, Lebenthal E, DiMagno EP, Scheele GA, editors.
useful only in severe steatorrhea.
The exocrine pancreas: biology, pathobiology, and diseases. New York (NY): CT shows calcifications, an irregular pancreatic contour,
Raven Press; c1986. p. 50311. Used with permission. a dilated duct system, or pseudocysts. ERCP shows protein
142 G A S T R O E N T E R O L O GY A N D H E PATO L O GY
plugs, segmental duct dilatation, and alternating stenosis and overlooked until pain or jaundice develop. Two signs associ-
dilatation, with obliteration of branches of the main duct. ated with pancreatic cancer are the Courvoisier sign (painless
jaundice with a palpable gallbladder) and the Trousseau sign
Serum amylase and lipase levels may be normal, but (recurrent migratory thrombophlebitis). Recent-onset diabe-
evidence for structural disease or endocrine or exocrine tes and nonbacterial (thrombotic) marantic endocarditis may
insufficiency is present. be associated with pancreatic cancer.
10. PA N C R E A S 143
prolapse occurs in 20% of patients, and a distal small-bowel Insulinoma: most common islet cell tumor.
obstruction from thick secretions occurs in 15% to 20%. Focal
Pancreatic cholera: pancreatic tumor that produces VIP,
biliary cirrhosis develops in 20% of patients.
which causes secretory diarrhea.
Exocrine pancreatic insufficiency occurs in 85%90% of Octreotide prevents hormone release and antagonizes
patients with cystic fibrosis. hormonal effects.
PA N C R E AT I C E N D O C R I N E T U M O R S
S U M M A RY
Zollinger-Ellison syndrome is a nonbeta islet cell tumor of the
pancreas that produces gastrin and causes gastric acid hyperse- If the presentation for pancreatitis is classic but the amylase
cretion. This results in peptic ulcer disease (see Peptic Ulcer value is normal, repeat the amylase test, check urinary
Disease subsection in Chapter 11). amylase and serum lipase levels, and scan the abdomen.
Insulinoma is the most common islet cell tumor. It is a beta Persistent hyperamylasemia suggests a complication. If
islet cell tumor that produces insulin and causes hypoglyce- the amylase level is mildly elevated and there is a history
mia. The diagnosis is based on finding increased fasting plasma of vomiting but no signs of obstruction, perform an
levels of insulin and hypoglycemia. CT, EUS, or arteriography esophagogastroduodenoscopy to rule out a penetrating
may be useful in localizing the tumor. ulcer.
Glucagonoma is an alpha islet cell tumor that produces gluca-
An isolated left pleural effusion on chest radiography is
gon. Patients present with diabetes mellitus, weight loss, and a clas-
strongly suggestive of acute pancreatitis. On an abdominal
sic skin rash (migratory necrolytic erythema). The diagnosis is based
plain film, look for the sentinel loop sign, the colon cutoff
on finding increased glucagon levels and on finding that the blood
sign, and pancreatic calcifications.
glucose level does not increase after an injection of glucagon.
Pancreatic cholera is a pancreatic tumor that produces vaso- Supportive care is the backbone of treatment of acute
active intestinal polypeptide (VIP), which causes watery diar- pancreatitis. Antibiotics are indicated for patients with
rhea (see Secretory Diarrhea subsection in Chapter 12). necrotizing pancreatitis.
Somatostatinoma is a delta islet cell tumor that produces somat-
ostatin, which inhibits insulin, gastrin, and pancreatic enzyme Patients with chronic pancreatitis present with abdominal
secretion. The result is diabetes mellitus and diarrhea. The diag- pain, pancreatic calcifications, steatorrhea, and diabetes
nosis is based on finding increased plasma levels of somatostatin. mellitus.
Octreotide is useful in treating pancreatic endocrine tumors For patients with chronic pancreatitis, abstinence from
except for somatostatinomas. Octreotide prevents the release of alcohol may relieve the pain. A 1- or 2-month trial of
hormone and antagonizes hormonal effects on target organs. pancreatic enzyme replacement is worthwhile; women
are more likely to have a response. Surgical treatment
Zollinger-Ellison syndrome: nonbeta islet cell tumor of should be considered only after conservative measures
the pancreas. have failed.
144 G A S T R O E N T E R O L O GY A N D H E PATO L O GY
11.
ESOPHAGUS AND STOMACH
Amy S. Oxentenko, MD
G OA L S N O R M A L M OT I L I T Y
Immediately after a person swallows, the UES relaxes, allowing
Distinguish between the 3 main forms of dysphagia on the a food bolus to pass from the oropharynx into the esophagus.
basis of clinical history, and recognize the differences in the A peristaltic wave then passes through the body of the esopha-
evaluation of each. gus, and within 2 seconds after the swallow, the LES relaxes
Describe the stepwise diagnostic evaluation of a patient and stays relaxed until the wave of peristalsis passes through
with gastroesophageal reflux disease (GERD). it. The LES then contracts and maintains resting tone. If the
esophagus cannot perform its 2 main functions, 2 major symp-
List the common causes of peptic ulcer disease (PUD), tom complexes result: dysphagia (transport dysfunction) and
and describe the differences between the invasive and reflux (LES dysfunction).
noninvasive tests for Helicobacter pylori infection.
Recognize the appropriate order of staging tests for the Dysphagia results from oropharyngeal or esophageal
evaluation of both esophageal cancer and gastric cancer. transport dysfunction.
Reflux results from LES dysfunction.
E S O P H AGU S
DYS P H AG I A
E S O P H AG E A L F U N C T I O N Dysphagia results from defective transport of food and is
usually described as difficulty swallowing or food stick-
The main functions of the esophagus are to transport food
ing. The 3 causes of dysphagia must be distinguished: 1)
and prevent reflux. To transport food from the mouth to
oropharyngeal (faulty transfer of a food bolus from the
the stomach, the esophagus must work against a pressure
oropharynx into the esophagus), 2) mechanical (structural
gradient, with negative pressure in the chest and positive
abnormality of the esophageal lumen), and 3) motor (motil-
pressure in the abdomen. The lower esophageal sphincter
ity disorder). Answers to 3 questions frequently suggest the
(LES) helps to prevent reflux of gastric contents back into
diagnosis (Figure 11.1): 1) What types of food produce the
the esophagus.
dysphagia (solids or liquids)? 2) What is the time course of
The upper esophageal sphincter (UES) (or cricopharyn-
the dysphagia (intermittent or progressive)? 3) Is there asso-
geal muscle) and the muscle of the proximal one-third of the
ciated heartburn? Esophagogastroduodenoscopy (EGD) is
esophagus are striated muscle under voluntary control. A tran-
the first test that should be done in the evaluation of dys-
sition from skeletal to smooth muscle occurs in the midesoph-
phagia unless there are features of oropharyngeal dysphagia
agus, with the distal one-third of the esophagus composed
(see below).
of smooth muscle under involuntary control. The LES is a
zone of circular muscle located in the distal 2 to 3 cm of the
The 3 types of dysphagia are oropharyngeal, mechanical,
esophagus.
and motor.
The main functions of the esophagus are to transport food The cause of dysphagia is strongly suggested by the
and prevent reflux of gastric contents. triggering foods, time course, and associated symptoms.
The esophagus transports food from the mouth to the EGD is the initial test of choice for the evaluation of
stomach against a pressure gradient. dysphagia unless oropharyngeal dysphagia is suspected.
145
Dysphagia
Figure 11.1 Diagnostic Scheme for Dysphagia. The answers to 3 questions (see text) often suggest the most likely diagnosis. (Adapted from MKSAP
VI: part 1:44, 1982. American College of Physicians. Used with permission.)
146 G A S T R O E N T E R O L O GY A N D H E PATO L O GY
beak) tapering at the LES. The motility pattern is char- studies may demonstrate simultaneous contractions in the
acterized by the following: 1) incomplete relaxation of body of the esophagus during symptoms. A trial of acid sup-
the LES, 2) hypertensive LES, and 3) aperistalsis of the pression should be considered because acid reflux may precip-
esophageal body. All patients with features of achalasia itate esophageal spasm in some persons. Medical treatment
require an EGD because cancer infiltrating near the esoph- (nitrates, anticholinergic agents, and nifedipine) has unpre-
agogastric junction may have the same radiographic and dictable results.
manometric pattern of achalasia (termed pseudoachalasia).
Patients with pseudoachalasia tend to be older, have more Diffuse esophageal spasm usually causes chest pain.
rapid onset of symptoms (months rather than years), and
have more profound weight loss. Treatment of achalasia Esophageal spasm may be aggravated by stress, hot or cold
includes surgical methods (myotomy), injection of botu- liquids, and carbonated beverages.
linum toxin into the LES, or pneumatic dilation. Healthy Barium imaging may show a corkscrew esophagus during
patients who can undergo surgery should be considered symptoms.
for a myotomy. Botulinum toxin injection into the LES
decreases lower esophageal pressure for 3 to 12 months;
given the short-term relief of symptoms, it should be con-
Mechanical Dysphagia
sidered for elderly patients and for those with high surgi-
cal risk. In Brazil, the parasite Trypanosoma cruzi (which Dysphagia can result when there is compromise of the
causes Chagas disease) produces a neurotoxin that destroys esophageal lumen to a diameter of less than 12 mm. This
the myenteric plexus and leads to esophageal dilatation type of dysphagia usually begins with solid foods, but it may
identical to that of achalasia. progress to involve liquids with further luminal narrowing.
Depending on the cause, such as malignancy, weight loss
Clinical features of achalasia include chronic, progressive may occur.
dysphagia to both solids and liquids with regurgitation of
undigested food. Patients with mechanical abnormalities of the esophagus
present with solid food dysphagia, which may progress to
Radiographic features of achalasia can include an air-fluid
involve liquids.
level in the esophagus on chest radiography and a dilated
esophagus with bird beak tapering with barium imaging.
A peptic stricture results from esophageal reflux of acid. It
The manometric pattern in achalasia includes 1) failed LES is usually a short (<2 cm in length) narrowing in the distal
relaxation, 2) increased or hypertensive LES resting tone, esophagus immediately at or above the esophagogastric junc-
and 3) aperistalsis of the esophageal body. tion. Management includes esophageal dilation and acid sup-
pression; proton pump inhibitor (PPI) therapy after dilation
All patients with features of achalasia require an EGD to
of a peptic stricture decreases recurrence.
rule out pseudoachalasia.
Treatment of achalasia includes surgery, pneumatic A peptic stricture results from acid reflux and is located
dilation, or botulinum toxin injection. in the distal esophagus; dilation and acid suppression are
recommended.
Esophageal involvement with scleroderma is associated
with the presence of Raynaud phenomenon and is part of the Alkali is more injurious to the esophagus than acid.
CREST syndrome. Patients have chronic, progressive dyspha- Alkali-induced strictures can occur in patients after a total gas-
gia with both solids and liquids, along with severe heartburn trectomy (stricture due to alkaline reflux) or after lye inges-
and reflux. Barium swallow fluoroscopy may show a rigid tion. Inducing emesis after lye ingestion is contraindicated
esophagus and a widely patent LES. Although motility testing since the caustic substance can further injure the esophagus
shows aperistalsis in the body of the esophagus similar to acha- with subsequent exposure. Lye-induced strictures tend to be
lasia, there is decreased tone of the LES in scleroderma, which long (compared with peptic strictures). Repeated dilation or
differentiates the 2 conditions. temporary stenting of the esophagus is often required after an
alkali-induced stricture has occurred. Patients with lye-induced
Although patients with achalasia and scleroderma share strictures have an increased incidence of squamous cell cancer
some clinical and manometric findings, the presence of of the esophagus.
decreased LES tone in patients with scleroderma helps to
distinguish the condition from achalasia. Both postgastrectomy alkaline reflux and lye ingestion can
produce alkali-induced strictures.
Patients with diffuse esophageal spasm usually present
Inducing emesis after lye ingestion is contraindicated.
with chest pain, but they may have intermittent dyspha-
gia with solids or liquids, or both; symptoms may be aggra- Lye-induced strictures are associated with an
vated by stress, hot or cold liquids, and carbonated beverages. increased incidence of squamous cell cancer of the
Barium imaging may show a corkscrew esophagus. Motility esophagus.
148 G A S T R O E N T E R O L O GY A N D H E PATO L O GY
infection, endoscopy may show small discrete ulcers. Diagnosis Most patients with GERD describe classic heartburn or
is based on finding intranuclear inclusions with surrounding regurgitation. Atypical symptoms of GERD include noncar-
halos and multinucleated giant cells in biopsy specimens from diac chest pain, asthma, chronic cough, hoarseness, and enamel
an edge of the ulcer. Treatment is with acyclovir. In cytomega- defects. Reflux is the most common cause of noncardiac chest
loviral infection, endoscopy may show large, irregular ulcers. pain; however, cardiac status must be evaluated before chest
Histologic examination of biopsy specimens from the ulcer pain is attributed to reflux. Asthmatic patients with coexisting
base shows owls eye intranuclear inclusions and enlarged reflux should receive therapy for reflux because it may improve
areas of cytoplasm. Treatment is with ganciclovir or foscarnet control of respiratory symptoms. Reflux should be considered
(if resistant to ganciclovir). in asthmatic patients who have postprandial or nocturnal
wheezing.
Odynophagia in an immunosuppressed patient is For patients who are younger than 50 years with classic
typically due to an opportunistic infection with Candida, symptoms of reflux and no alarm features (weight loss, ane-
herpesvirus, or cytomegalovirus. mia, dysphagia, odynophagia, or family history of cancer in
the upper gastrointestinal tract), an empirical trial of PPI
If a patient presents with odynophagia and has evidence of therapy is warranted. However, testing should be performed
thrush, empirical therapy with oral fluconazole should be if patients have new-onset symptoms after age 50, atypical fea-
started. tures, refractory or long-standing symptoms, or alarm features.
The initial test in the evaluation of these symptoms would be
Medication-Induced Esophagitis an EGD; if an EGD does not show esophagitis or other fea-
tures to support the diagnosis of reflux, a 24-hour ambulatory
Patients with medication-induced esophagitis present with pH probe can be used to document esophageal acid exposure
odynophagia (or, less frequently, dysphagia). Medication- and symptom correlation.
induced esophagitis may occur if esophageal motility or anat-
omy is abnormal, but it can happen if medications are not
For most patients, the medical history is sufficiently typical
taken with adequate fluids or if patients assume a supine pos-
to warrant a trial of PPI therapy without tests.
ition immediately after taking them. Medications commonly
associated with esophagitis include tetracycline, doxycycline, An EGD is recommended for patients with reflux-type
quinidine, potassium supplements, bisphosphonates, ferrous symptoms if they have new-onset symptoms after age 50,
sulfate, and ascorbic acid. The use of these medications should atypical features, refractory or long-standing symptoms, or
be avoided if possible in patients with known esophageal stric- alarm features.
tures or symptoms of dysphagia.
Atypical symptoms of GERD include noncardiac chest
pain, asthma, chronic cough, hoarseness, and enamel
Medicines responsible for medication-induced esophagitis
defects.
include tetracycline, doxycycline, quinidine, potassium
supplements, bisphosphonates, ferrous sulfate, and ascorbic Complications of gastroesophageal reflux include
acid. esophagitis, bleeding, stricture formation, aspiration,
Barrett esophagus, and adenocarcinoma of the esophagus.
G A S T RO E S O P H AG E A L R E FLUX D I S E A S E
Reflux Barrett Esophagus
The LES is the major barrier to prevent esophageal reflux of Barrett esophagus is a complication of chronic gastroesopha-
gastric contents. Swallowing causes the sphincter pressure to geal reflux in which the normal esophageal squamous mucosa
decrease promptly within 1 to 2 seconds and remain relaxed is replaced by columnar epithelium or intestinal metaplasia.
until the peristaltic wave passes over it. The sphincter then Patients with Barrett esophagus are at increased risk of ade-
contracts and maintains the increased resting pressure that nocarcinoma. Although considerable controversy exists about
prevents reflux. the benefits of performing screening endoscopy to evaluate for
GERD is typically caused by inappropriate relaxation of Barrett esophagus, most experts recommend screening endos-
the LES or by intragastric pressure that exceeds LES pressure. copy for high-risk patients (obese white men older than 50
GERD can lead to tissue damage and ulceration, known as years) who have had chronic reflux for more than 5 years. If
esophagitis. Factors that determine whether reflux esopha- mucosal changes are seen endoscopically, biopsies are needed
gitis occurs include the frequency of transient relaxations of to confirm the diagnosis and to look for dysplasia. The surveil-
the LES, the rate of gastric emptying (if delayed, reflux may lance frequency is based on the presence and degree of dyspla-
develop), the potency of the refluxate (acid, pepsin, and bile), sia found during the previous study. If there is no dysplasia,
the efficiency of esophageal clearance (motility and salivary surveillance should occur every 3 years. If low-grade dyspla-
bicarbonate), and the resistance of esophageal tissue to injury. sia is identified, surveillance should be yearly. If high-grade
Complications of reflux include esophagitis, bleeding, stric- dysplasia is identified (and confirmed by 2 pathologists), the
ture formation, aspiration, Barrett esophagus, and adenocar- patient may elect to undergo an esophagectomy or be consid-
cinoma of the esophagus. ered for an ablative therapy, such as photodynamic therapy.
Ambulatory 24-hour pH monitoring allows a physiologic All patients with chest pain should be thoroughly evaluated to
evaluation of reflux during daily activities and is valuable rule out a potential cardiac cause before other diagnoses are con-
for patients who have a nondiagnostic EGD or atypical or sidered. GERD is the most common cause of noncardiac chest
refractory symptoms. pain, but esophageal pain may be due to a motor disorder (eg,
spasm) or esophageal inflammation (eg, infection or injury).
Esophageal spasm can closely mimic angina. EGD is used to
Esophageal impedance testing can be used to detect the rule out mucosal disease (eg, inflammation, neoplasm, or chem-
presence of nonacidic reflux in patients who are receiving ical injury). A 24-hour ambulatory pH probe can be used to
PPI therapy or who have achlorhydria or bile reflux, since this document the presence of reflux and its correlation with chest
test detects the presence of a fluid column, regardless of pH. pain. Therapy for noncardiac chest pain includes avoidance of
Esophageal manometry is reserved for patients with suspected precipitants. Antacids, H2 receptor antagonists, and PPIs may
esophageal motility disorders; it is not useful for the evalua- be beneficial for patients with reflux. Sublingual nitroglycerin
tion of reflux. or calcium channel blockers are sometimes helpful in motor dis-
orders, but their efficacy is unproven. If appropriate, reassurance
Esophageal impedance testing can be used to evaluate that cardiac disease is not present may be all that is necessary.
nonacid reflux.
For all chest pain, first rule out cardiac disease.
Esophageal manometry is reserved for suspected
esophageal motility disorders. GERD is the most common cause of noncardiac chest pain.
150 G A S T R O E N T E R O L O GY A N D H E PATO L O GY
EGD is useful to detect mucosal disease that may account nonsteroidal anti-inflammatory drugs (NSAIDs), including
for chest pain. aspirin; or 3) miscellaneous causes. At least 90% of peptic
ulcers are due to either H pylori or NSAIDs. Miscellaneous
A 24-hour ambulatory pH probe documents reflux and its
causes include gastrinomas (Zollinger-Ellison syndrome),
correlation with symptoms.
Crohn disease, malignancy, drugs (cocaine), and viral infec-
Acid suppression can be helpful in alleviating chest pain by tions (such as those caused by cytomegalovirus). There is no
controlling reflux disease. evidence that smoking or corticosteroids cause PUD, but
either can result in decreased ulcer healing and increased
complications.
OT H E R E S O P H AG E A L P RO B L E M S Infection with H pylori causes more duodenal ulcers than
gastric ulcers. Although NSAIDs tend to cause more gastric
Mallory-Weiss Tear
ulcers than duodenal ulcers, H pylori infection is still more
A Mallory-Weiss tear is a mucosal laceration at the esophago- likely to account for gastric ulcer disease in general.
gastric junction. It accounts for about 10% of the cases of upper Certain medical conditions may predispose to
gastrointestinal tract bleeding; most patients have a history of stress-induced peptic injury; these include ventilator use,
retching or vomiting before the bleeding begins. In 90% of underlying coagulopathy, significant burns, and central ner-
the patients, the bleeding stops spontaneously, but endoscopic vous system injury. Patients with these conditions should be
hemostatic techniques can be used if needed. considered candidates for prophylactic therapy.
A Mallory-Weiss tear is a mucosal laceration at the More than 90% of peptic ulcers are caused by either H
esophagogastric junction; the laceration usually occurs pylori infection or NSAID use.
after a bout of retching or vomiting.
Risk factors for stress ulcerations include ventilator use,
A Mallory-Weiss tear accounts for about 10% of the cases coagulopathy, burns, and central nervous system injury.
of upper gastrointestinal tract bleeding; bleeding stops
spontaneously in 90%.
HE LICOBACTE R PY LO RI
The Organism
Esophageal Perforation
A gram-negative, spiral-shaped bacillus, H pylori is commonly
Esophageal perforation most commonly occurs after dilation
acquired through oral ingestion and transmitted among those
of a strictured area or with stenting of an esophageal cancer.
in close living quarters. This fastidious organism resides and
Spontaneous perforation of the esophagus (Boerhaave syn-
multiplies beneath and within the mucous layer of the gastric
drome) occurs after violent retching, often after an alcohol
mucosa and produces several enzymes, such as urease, impor-
binge. It has been reported after heavy lifting, seizures, and
tant for its survival and pathogenic effects.
strenuous childbirth. The most common site of perforation is
Helicobacter pylori infection can lead to a spectrum from
the left posterior aspect of the distal esophagus. If pleural fluid
acute to chronic gastritis, and it can lead to PUD, atrophic
is present, it may have an increased concentration of amylase.
gastritis, mucosa-associated lymphoid tissue (MALT) lym-
The cervical esophagus may be perforated if a Zenker diver-
phoma, or gastric malignancy.
ticulum is inadvertently intubated for an EGD.
Noninvasive tests
Serology Easy to perform Prevalence dependent
Good negative predictive value Indicates only past infection (not used for eradication testing)
Stool antigen Indicates active infection Stool collection
Useful for primary or eradication testing
Urea breath test Indicates active infection False-negative results with antibiotics, acid suppression, or bismuth
Useful for primary or eradication testing
Invasive tests
Rapid urease test Quick results Expense of endoscopy to perform the test
False-negative results with antibiotics, acid suppression, or bismuth
Histology Allows evaluation for histologic changes Expense of endoscopy to perform the test
(dysplasia, etc) Dependent on expertise of pathologist
152 G A S T R O E N T E R O L O GY A N D H E PATO L O GY
serologic antibody, stool antigen, or urea breath testing can elderly patients and patients with a previous history of PUD
be performed. Because many symptomatic patients undergo are at highest risk.
endoscopy, histologic examination or rapid urease testing can The first step in the treatment of an NSAID-induced ulcer
be done. The best tests for determining eradication are the is to discontinue use of the drug if feasible. PPIs are most
stool antigen test and the urea breath test. effective in healing and preventing ulcers and have few side
effects. H2 receptor antagonists and sucralfate are less effec-
Serologic tests for H pylori infection are prevalence tive in preventing gastric ulcers and in decreasing the fre-
dependent and remain positive over time, which limits quency of NSAID-induced mucosal erosions. The synthetic
their usefulness for previously treated patients. prostaglandin agonist misoprostol decreases the incidence of
NSAID-induced gastric ulcers; however, its usefulness is lim-
Recent therapy with PPIs, antibiotics, or bismuth can ited by the side effect of diarrhea and its role as an abortifa-
lead to false-negative results for most H pylori tests except cient (avoid using it in women of childbearing age).
serology.
The best tests for determining eradication are the stool The risk of gastrointestinal tract injury related to NSAID
antigen test and the urea breath test since a positive result use increases with higher doses of NSAIDs, combinations
indicates active infection. of 2 or more agents (including low-dose aspirin), elderly
patients, and patients with a prior history of PUD.
Treatment For both prevention and treatment of NSAID-induced
ulcers, PPI therapy is most often used.
With an H pyloripositive duodenal or gastric ulcer, the treat-
ment goal is to heal the ulcer and eradicate the bacteria. All
patients who are infected with H pylori should receive combi-
Z O L L I N G E R-E L L I S O N S Y N D RO M E
nation therapy. PPI-based triple therapy (usually in combina-
tion with amoxicillin and clarithromycin) for 10 to 14 days is Zollinger-Ellison syndrome is characterized by acid hypersecre-
the most commonly used initial therapy; metronidazole can be tion and the triad of peptic ulceration, esophagitis, and diar-
used in place of amoxicillin in patients who have a penicillin rhea (since excess acid inactivates pancreatic lipase) caused
allergy. Because of emerging patterns of resistance to clarithro- by a gastrin-producing tumor. The tumor usually is located
mycin and metronidazole, these agents should be avoided if in the gastrinoma triangle, which includes the head of the
subsequent treatment is necessary and they were used as ini- pancreas and the duodenal wall. Two-thirds of gastrinomas
tial therapy. If the first course of therapy fails to eradicate the are malignant and can metastasize. One-fourth of gastrinomas
organism, quadruple therapy can be considered (PPI, metro- are related to multiple endocrine neoplasia type 1 (MEN-1)
nidazole, bismuth, and tetracycline). syndrome and are associated with pituitary adenomas and
hyperparathyroidism.
PPI-based triple therapy (usually in combination with Zollinger-Ellison syndrome should be considered in the
amoxicillin and clarithromycin) for 1014 days is the most person with H pylorinegative, NSAID-negative PUD, espe-
commonly used initial therapy for H pylori infection. cially when there are multiple ulcers, ulcers in unusual loca-
tions (postbulbar duodenum), and refractory ulcers. Increased
serum gastrin levels (>1,000 pg/mL) in patients who produce
N S A I D -I N D U C E D U L C E R S
gastric acid are essentially diagnostic of gastrinoma. Increased
NSAIDs inhibit gastroduodenal prostaglandin synthesis, serum gastrin levels may also be present in patients who are
which results in decreased secretion of mucus and bicarbonate, receiving PPI therapy (the most common reason), or who
reduced mucosal blood flow, and stimulated acid production. have atrophic gastritis (the next most common reason), perni-
NSAID-induced ulcers occur more commonly in the stomach cious anemia, postvagotomy states, or gastric outlet obstruc-
(typically in the antrum) than in the duodenum. tion. Basal and stimulated gastric acid studies should be
The risk of PUD with NSAIDs is dose-dependent. performed for all patients who have increased levels of gastrin
Higher doses of NSAIDs or the combination of 2 or more to see whether there is acid hypersecretion. When the labora-
NSAIDs (including low-dose aspirin) increases the risk tory results are equivocal, a secretin test should be performed;
of gastrointestinal tract injury. Selective cyclooxygenase this test produces a paradoxical increase in the serum level of
(COX)-2 inhibition has been shown to decrease the rate of gastrin in patients with gastrinoma.
PUD and ulcer complications such as bleeding, perforation, An octreotide scan (Octreoscan) can be used to localize a
and pain. However, data suggest that even low-dose aspirin gastrinoma owing to the presence of somatostatin receptors.
can reduce or eliminate any protective benefit of selective Endoscopic ultrasonography has been very successful in local-
COX-2 drugs (celecoxib). In most cases, acetaminophen izing gastrinomas because the pancreas and duodenal wall can
can be substituted for the NSAID. For patients who require be easily viewed with this test.
NSAID therapy, the lowest possible dose should be used Since 50% of patients with gastrinomas have metastatic
and combination NSAID therapy avoided. The risk of PUD disease, curative surgery is not always feasible. Patients who
with NSAID use is maximal in the first month of treatment are not candidates for surgery can be managed with high-dose
(ulcers may occur shortly after treatment is begun), and acid suppression. Those with MEN-1 syndrome are usually
154 G A S T R O E N T E R O L O GY A N D H E PATO L O GY
Treatment and Prognosis Box 11.2 CONDITIONS CAUSING GASTROPARESIS
For localized disease, resection for tumor-free margins often
requires total gastrectomy. For disseminated disease, surgical Acute conditions
treatment is necessary only for palliation. Response to che- Anticholinergic drug use
motherapy is generally poor. Five-year survival is 90% if the Hyperglycemia
tumor is confined to the mucosa and submucosa, 50% if the Hypokalemia
tumor is through the serosa, and 10% if the tumor involves Morphine use
regional lymph nodes. Pancreatitis
Surgical procedures
Trauma
G A S T R I C P O LY P S Chronic conditions
Gastric polyps are common and are typically found inciden- Amyloidosis
tally. There are 3 types of polyps: cystic fundic gland, hyper- Diabetes mellitus
plastic, and adenomatous. Cystic fundic gland polyps are the Gastric dysrhythmias
most common gastric polyps and are not premalignant except Pseudo-obstruction
in association with familial adenomatous polyposis (FAP). No Scleroderma
additional therapy is needed unless FAP is known or suspected Vagotomy
to be present. Hyperplastic polyps may occur with chronic gas-
tritis, so patients should be tested for H pylori. Hyperplastic Management of gastroparesis includes 1) dietary alter-
polyps rarely have malignant potential. Adenomatous polyps are ations, 2) antiemetic agents, and 3) prokinetic drugs, if
deemed premalignant and need to be fully removed (like colon needed. Metoclopramide is a dopamine antagonist and a
polyps). cholinergic agonist that increases the rate and amplitude
There are 3 types of carcinoid tumors, which may man- of antral contractions. It crosses the blood-brain barrier
ifest as an incidentally noted gastric polyp. Type 1 gas- and can cause drowsiness and galactorrhea (from increased
tric carcinoids are associated with autoimmune gastritis, release of prolactin). The most feared complication of
whereas type 2 gastric carcinoids are associated with MEN-1 this medication is tardive dyskinesia, which can be irre-
syndrome; both forms tend to follow an indolent course. versible. Erythromycin stimulates both cholinergic and
Type 3 gastric carcinoids tend to be sporadic and behave motilin receptors, but because tachyphylaxis occurs with
aggressively. long-term use, it is most often used transiently in hospital-
ized patients.
Cystic fundic gland polyps are the most common types of
gastric polyps and tend to be benign except in association Metoclopramide can be used for gastroparesis, but
with FAP. it carries a risk of tardive dyskinesia, which may be
Adenomatous polyps are premalignant and need to be irreversible.
removed. Because long-term use of erythromycin can lead to
tachyphylaxis, it is usually used for only short periods.
G A S T RO D U O D E NA L DY S M OT I L I T Y
S Y N D RO M E S D U M P I N G S Y N D RO M E
156 G A S T R O E N T E R O L O GY A N D H E PATO L O GY
12.
DIARRHEA, MALABSORPTION, AND
SMALL-B OWEL DISORDER S
Seth R. Sweetser, MD
Diarrhea is a symptom or sign, not a disease. As a symptom, Osmotic diarrhea occurs when a poorly absorbed substance
it can manifest as a decrease in consistency, an increase in remains in the intestinal lumen and causes water retention that
fluidity, an increase in number or volume of stools, or any maintains an intraluminal osmolality equal to that of body flu-
combination thereof. A stool frequency of 3 or more times ids (approximately 290 mOsm/kg). This occurs because, unlike
daily is considered abnormal; however, most people consider the kidney, neither the small intestine nor the colon maintains
increased fluidity of stool as the essential characteristic of diar- an osmotic gradient. Osmotic diarrhea follows ingestion of an
rhea. As a sign, diarrhea is an increase in stool weight or vol- osmotically active substance and stops with fasting. Stool vol-
ume of more than 200 g or 200 mL per 24 hours for a person ume is less than 1 L daily, and the stool osmotic gap (SOG),
eating a Western diet. Although stool weight is often used as calculated as follows, is greater than the sum of the measured
the objective definition of diarrhea, diarrhea should not be concentrations of sodium (NA) and potassium (K) (the sum is
strictly defined by stool weight because the amount of dietary doubled to account for their associated anions):
fiber influences the water content of the stool. Therefore, stool
weight can vary considerably depending on fiber intake. In the SOG = 290 mOsm/kg 2 u (Stool [Na] + Stool [K]).
United States, normal daily stool weight or volume is less than
200 g or 200 mL daily because of lower fiber intake (compared A normal stool osmotic gap is less than 50 mOsm/kg.
with up to 400 g or 400 mL daily in rural Africa). However, with an osmotically active substance in the bowel,
Because diarrhea has multiple causes, its evaluation is often sodium and potassium levels will decrease (keeping stool
complex and time consuming. An understanding of the basic osmotically neutral with the body). The calculated stool osmo-
pathogenic mechanisms leading to diarrhea can help facili- lality decreases, resulting in a gap (typically >100 mOsm/kg).
tate its evaluation and management. The basic mechanism of Clinical causes of osmotic diarrhea include carbohydrate mal-
all diarrheal diseases is incomplete absorption of fluid from absorption, lactase deficiency, sorbitol-sweetened foods, saline
luminal contents. Each day, approximately 10 L of fluid passes cathartics, and magnesium-based antacids. In carbohydrate
into the proximal small intestine (2 L from diet; 8 L from malabsorption (most commonly lactase deficiency), stool pH
endogenous secretions). The small bowel absorbs most of the is often less than 6.0 because of colonic fermentation of the
fluid (9 L), and the colon absorbs about 90% of the remain- undigested sugars.
ing 1 L, so that only about 1% of the original fluid entering
the small intestine is excreted in the stool. A normal stool is In osmotic diarrhea, stool volume is <1 L daily.
approximately 75% water and 25% solids, with a normal fecal
Osmotic diarrhea stops with fasting.
water output of 60 mL daily. An increase in fecal water out-
put of only 100 mL is enough to cause increased stool fluidity The stool osmotic gap is typically >100 mOsm/kg.
157
Causes of osmotic diarrhea: lactase deficiency, sorbitol, and The volume of feces is small and the stools may be bloody.
antacids. Examples include invasive bacterial pathogens (eg, Shigella
and Salmonella) and inflammatory bowel disease. In motil-
The term secretory diarrhea is used to indicate disor- ity disorders, both rapid transit (inadequate time for chyme
dered intestinal epithelial electrolyte transport (ie, the to contact the absorbing surface) and delayed transit (bacte-
intestine secretes electrolytes and fluid rather than absorb- rial overgrowth) can cause diarrhea. Rapid transit occurs after
ing them) even though it is more commonly caused by gastrectomy or intestinal resection and with hyperthyroidism
reduced absorption than by net secretion. Stool volume or carcinoid syndrome. Delayed transit occurs with structural
is more than 1 L daily. The stool composition is predomi- defects (strictures, blind loops, and small-bowel diverticula)
nantly extracellular fluid, so there is no stool osmotic gap. or with underlying illnesses that cause visceral neuropathy
Secretory diarrhea persists despite fasting. Causes of secre- (diabetes mellitus) or myopathy (scleroderma), resulting in
tory diarrhea include bacterial toxins, neuroendocrine pseudo-obstruction.
tumors, surreptitious ingestion of laxative, bile acid diar-
rhea, and fatty acid diarrhea. Evaluation of chronic watery diarrhea requires
distinguishing between secretory diarrhea and osmotic
In secretory diarrhea, stool volume is >1 L daily. diarrhea.
There is no stool osmotic gap. Exudative diarrhea: abnormal membrane permeability and
a stool volume that is typically small.
Secretory diarrhea persists despite fasting.
Causes of exudative diarrhea: invasive bacterial pathogens
Causes of secretory diarrhea: bacterial toxins,
and inflammatory bowel disease.
neuroendocrine tumors, surreptitious ingestion of laxative,
bile acid diarrhea, and fatty acid diarrhea. Rapid transit: diarrhea results from malabsorption.
A useful method to evaluate chronic watery diarrhea Delayed transit: diarrhea results from bacterial overgrowth.
is to distinguish secretory diarrhea from osmotic diarrhea
(Table 12.1) by measuring the concentrations of sodium and C L I N I C A L A P P ROAC H TO D I A R R H E A
potassium in stool water (calculate the stool osmotic gap) and
observing the patients response to fasting. Knowing the stool volume is potentially useful to distinguish
Many disease processes cause diarrhea by more than 1 between diarrhea arising from the small bowel or ascending
mechanism. For example, generalized malabsorption, such as colon (right-sided diarrhea) and diarrhea arising from the
in celiac disease, has osmotic components (from carbohydrate distal colon (left-sided diarrhea) (Table 12.2). The distal left
malabsorption) and secretory components (unabsorbed fatty colon acts as a distensible reservoir that collects stool until
acids cause secretion in the colon). defecation. With inflammation of the left colon, the reser-
In exudative diarrhea, membrane permeability is abnor- voir becomes spastic and its ability to accommodate normal
mal and serum proteins, blood, or mucus is exuded into the volumes of stool is impaired. As a result, left-sided diarrhea is
bowel from sites of inflammation, ulceration, or infiltration. characterized by frequent, small-volume stools and tenesmus
with evidence of inflammation (blood or pus) in the stools.
Table 12.1 FEATURES DIFFERENTIATING OSMOTIC
DIARRHEA FROM SECRETORY DIARRHEA
Table 12.2 FEATURES THAT DISTINGUISH
OSMOTIC SECRETORY RIGHT-SIDED DIARRHEA FROM LEFT-SIDED
FEATURE DIARRHEA DIARRHEA
DIARRHEA
Daily stool volume, L <1 >1
RIGHT-SIDED LEFT-SIDED
Effect of 48-h fasting Diarrhea stops Diarrhea (SMALL-BOWEL) (COLONIC)
continues FEATURE DIARRHEA DIARRHEA
158 G A S T R O E N T E R O L O GY A N D H E PATO L O GY
Proctosigmoidoscopic examination usually confirms mucosal Always consider lactase deficiency in suspected irritable
inflammation. bowel syndrome.
Right-sided diarrhea is characterized by large-volume
Differentiate organic diarrhea from functional diarrhea.
stools (due to normal distensibility of the rectum) and a mod-
est increase in the number of stools. Symptoms attributed to
inflammation of the rectosigmoid are absent, and proctoscopic
examination findings are normal. Left-sided diarrhea usually P H YS I O L O GY O F N U T R I E N T A B S O R P T I O N
suggests an exudative mechanism, whereas the mechanism for The sites of nutrient, vitamin, and mineral absorption are
right-sided diarrhea is nonspecific. the following: The duodenum absorbs iron, calcium, folate,
water-soluble vitamins, and monosaccharides. The jeju-
ACU T E D I A R R H E A num absorbs fatty acids, amino acids, monosaccharides, and
Acute diarrhea is abrupt in onset and usually resolves in 3 to 10 water-soluble vitamins. The ileum absorbs monosaccharides,
days. It is self-limited, and the cause (often viral) usually is not fatty acids, amino acids, fat-soluble vitamins (A, D, E, and K),
found. No evaluation is necessary unless an invasive infection is vitamin B12, and conjugated bile salts. The distal small bowel
suspected (eg, bloody stools, fever, travel history, or a common can adapt to absorb nutrients. The proximal small bowel can-
source outbreak). If these conditions exist, do not treat with not adapt to absorb vitamin B12 or bile salts.
antimotility agents. Begin the evaluation with stool studies
for bacterial pathogens, ova, and parasites and proctosigmoi- The distal small bowel can adapt to absorb nutrients.
doscopy. Recognize the common situations that predispose to The proximal small bowel cannot adapt to absorb vitamin
specific infections (see Noninvasive (Toxicogenic) Bacterial B12 or bile salts.
Diarrhea subsection).
Fat absorption is the most complex process. Dietary
For acute diarrhea, no evaluation is necessary unless an fat consists mostly of long-chain triglycerides that must
invasive infection is suspected. be digested by pancreatic lipase, which cleaves 2 of the 3
Do not administer antimotility agents if infection is long-chain fatty acids from the glycerol backbone. The result-
suspected. ant free fatty acids and monoglycerides are solubilized by
micelles for absorption. The fatty acids and monoglycerides
are re-esterified by intestinal epithelial cells into chylomicrons
C H RO N I C D I A R R H E A
that are absorbed into the circulation via lymphatic vessels.
Chronic diarrhea is defined as diarrhea lasting longer than 4 Conversely, medium-chain triglycerides are absorbed directly
weeks. The most common cause of chronic diarrhea is irritable into the portal venous system and do not require micellar
bowel syndrome, but lactase deficiency should always be con- solubilization.
sidered. Several features help differentiate organic diarrhea Mechanisms of fat malabsorption are summarized in
from functional diarrhea (Table 12.3). Table 12.4. Malabsorption should be suspected if the medical
history suggests steatorrhea or if diarrhea occurs with weight
The most common cause of chronic diarrhea is irritable loss (especially if intake is adequate), chronic diarrhea of inde-
bowel syndrome. terminate nature, or nutritional deficiency.
Table 12.3 FEATURES THAT DISTINGUISH ORGANIC DIARRHEA FROM FUNCTIONAL DIARRHEA
Quantity of stool Variable but usually large (>200 g in 24 h) Usually small (<200 g in 24 h)
Adapted from Matseshe JW, Phillips SF. Chronic diarrhea: a practical approach. Med Clin North Am. 1978 Jan;62(1):14154. Used with permission.
12 . D I A R R H E A , M A L A B S O R P T I O N, A N D S M A L L -B OW E L D I S O R D E R S 159
Table 12.4 MECHANISMS OF FAT MALABSORPTION
Impaired micelle formation Duodenal bile salt concentration Common duct obstruction or cholestasis
160 G A S T R O E N T E R O L O GY A N D H E PATO L O GY
Table 12.6 FEATURES THAT SUGGEST MALABSORPTION CONDITIONS
FEATURE CONDITION
Diarrhea with iron deficiency anemia (evaluation for blood loss is Proximal small-bowel malabsorption (eg, celiac disease)
negative)
Diarrhea with metabolic bone disease Proximal small-bowel malabsorption (from decreased calcium & pro-
tein levels)
Hypoproteinemia with normal fat absorption Protein-losing enteropathy (with eosinophilia, eosinophilic gastroen-
teritis; with lymphopenia, intestinal lymphangiectasia)
Oil droplets (neutral fat) or muscle fibers (undigested protein) present Pancreatic insufficiency (maldigestion)
in stool
Normal (usually) serum levels of calcium, magnesium, & iron Pancreatic insufficiency (serum levels of albumin may also be normal)
FEATURE SUGGESTED CAUSE Arthritis Ulcerative colitis, Crohn disease, Whipple dis-
ease, Yersinia infection
Age Youth: lactase deficiency, inflammatory bowel disease,
or sprue Marked weight loss Malabsorption, inflammatory bowel disease,
cancer, thyrotoxicosis
Travel Parasites or toxicogenic agents (exposure to contami-
nated food or water) Eosinophilia Eosinophilic gastroenteritis, parasitic disease
Drugs Laxatives, antacids, antibiotics, colchicine, or lactulose Lymphadenopathy Lymphoma, Whipple disease
Family Celiac sprue, inflammatory bowel disease, polyposis Neuropathy Diabetic diarrhea, amyloidosis
history coli, or lactase deficiency
Postural hypotension Diabetic diarrhea, Addison disease, idio-
pathic orthostatic hypotension, autonomic
terminal ileum. There is episodic facial flushing (lasting up dysfunction
to 10 minutes), watery diarrhea, wheezing, right-sided val- Flushing Malignant carcinoid syndrome
vular disease (endocardial fibrosis), and hepatomegaly. If the
gut is normal, look for bronchial tumors or gonadal tumors. Proteinuria Amyloidosis
Dietary tryptophan is converted into serotonin (which causes Peptic ulcers Zollinger-Ellison syndrome
diarrhea, abdominal cramps [intestinal hypermotility], nau-
sea, and vomiting), histamine (responsible for flushing), and Hyperpigmentation Whipple disease, celiac disease, Addison
disease, pancreatic cholera, eosinophilic
other chemicals (bradykinin and corticotropin). Persons gastroenteritis
with intestinal tumors are usually asymptomatic because
the mediators have high first-pass clearance in the liver.
Adapted from Fine KD. Diarrhea. In: Feldman M, Scharschmidt BF, Sleisenger
Carcinoid syndrome arises when these mediators are released MH, editors. Sleisenger & Fordtrans gastrointestinal and liver disease: pathophys-
into the systemic bloodstream; this suggests that liver metas- iology, diagnosis, management. 6th ed. Vol. 1. Philadelphia (PA): WB Saunders
tases or bronchial tumors are present. The diagnosis of car- Company; c1998. p. 12852. Used with permission.
cinoid syndrome is made by finding increased urinary levels
of 5-hydroxyindoleacetic acid and by performing liver biopsy. Laxative Abuse and Surreptitious Laxative Ingestion
Treatment is with octreotide. Of the population older than 60 years, 15% to 30% admit
that they take laxatives regularly. With the concealed inges-
Pancreatic cholera: massive diarrhea, dehydration, and tion of laxatives (surreptitious laxative ingestion), patients
hypokalemia. complain of diarrhea but do not admit that they take laxatives.
In referral centers, this is a common cause of chronic watery
Patients may have multiple endocrine tumors.
diarrhea. Colonoscopy may show melanosis coli, which is a
Diarrhea is associated with a nonbeta islet cell tumor of brown discoloration of the mucosa due to lipofuscin pigment
the pancreas. accumulating in lamina propria macrophages. Melanosis coli
12 . D I A R R H E A , M A L A B S O R P T I O N, A N D S M A L L -B OW E L D I S O R D E R S 161
is caused by anthraquinone laxatives (senna, cascara, and aloe). bacterial overgrowth is the deconjugation of bile acids by
This benign condition is reversible with discontinuation of bacteria that normally do not occur in the proximal intes-
laxative use. A high degree of awareness is required to detect tine. Deconjugation of bile acids changes the ionization
this condition. When surreptitious laxative ingestion is sus- coefficient, and the deconjugated bile acids can then be
pected, stool water can be analyzed for laxatives by chemical passively absorbed in the proximal small bowel. Normally,
or chromatographic methods. Patients who ingest laxatives conjugated bile acids are actively absorbed distally in the
surreptitously often have underlying emotional problems that ileum. As a result, the critical micellar concentration is not
should be addressed. reached, and mild steatorrhea results from the intraluminal
deficiency of bile acids.
In patients using laxatives, colonoscopy may demonstrate Clinical features of bacterial overgrowth are steator-
melanosis coli. rhea (typically >20 g daily), vitamin B12 malabsorption
(macrocytic anemia), increased serum folate levels from
Anthraquinone laxatives cause melanosis coli. bacterial production, and positive duodenal or jejunal cul-
Address underlying emotional problems. tures. Conditions associated with small intestinal bacte-
rial overgrowth include postoperative conditions (blind
loops, enteroenterostomy, or gastrojejunocolic fistula),
Bile Acid Malabsorption structural abnormalities (diverticula, strictures, or fistu-
las), motility disorders (diabetes mellitus, scleroderma, or
Bile acid malabsorption is caused by ileal resection or disease.
pseudo-obstruction), achlorhydria (atrophic gastritis or gas-
Diarrhea due to bile acid malabsorption may produce 2 clini-
tric resections; achlorhydria is corrected with antibiotics),
cal syndromes, each requiring a different treatment.
and impaired immunity. Two examples of impaired immu-
With a limited resection (d100 cm of small intestine), mal-
nity are hypogammaglobulinemic sprue (in small-bowel
absorbed bile acids enter the colon and stimulate secretion.
biopsy specimens, no plasma cells are seen in the lamina
Liver synthesis can compensate, so bile acid concentration
propria and the villi are flat) and nodular lymphoid hyper-
in the upper small bowel is sufficient to achieve the critical
plasia associated with IgA deficiency, which predisposes to
micelle concentration and allow for normal fat absorption.
Giardia lamblia infection.
The excess bile acids irritate the colon mucosa, causing a secre-
tory diarrhea with minimal fat malabsorption. Treatment of
Deconjugated bile acids can be absorbed passively in the
the diarrhea is with cholestyramine, which binds excess bile
jejunum.
acids.
With an extensive resection (>100 cm of small intestine), Steatorrhea results from the intraluminal deficiency of bile
bile acid malabsorption is severe and enterohepatic circula- acids.
tion is interrupted. This limits synthesis, and the liver cannot
compensate. Bile acid concentration is decreased in the upper Diarrhea, vitamin B12 deficiency with normal or elevated
small bowel, micelles cannot be formed, and fat malabsorp- folate levels, postoperative or structural conditions,
tion results. The malabsorbed fatty acids themselves stimu- motility disorders, achlorhydria, and impaired immunity
late secretion in the colon. Fat-soluble vitamins (A, D, E, and suggest bacterial overgrowth.
K) may be malabsorbed. Additionally, excess fatty acids bind
intestinal calcium; this allows an increase in oxylate absorp- Noninvasive (Toxicogenic) Bacterial Diarrhea
tion, which increases the risk of oxylate renal stones. The treat-
ment of this bile acid malabsorption is a low-fat diet (<50 g Toxicogenic bacterial diarrhea, characterized by watery stools
daily) rich in medium-chain triglycerides. Cholestyramine without fecal leukocytes, is caused by several organisms
would further decrease bile acid concentration and worsen (Table 12.9).
the steatorrhea.
Staphylococcus aureus
Limited resection (d100 cm of small intestine): treat with Diarrhea caused by S aureus is of rapid onset and lasts
cholestyramine. for 24 hours. There is no fever, vomiting, or cramps. The
toxin is ingested with egg products, cream, and mayonnaise.
Extensive resection (>100 cm of small intestine): treat with Treatment is supportive.
a low-fat diet and medium-chain triglycerides.
Clostridium perfringens
The toxin of C perfringens (the buffet pathogen) is
Bacterial Overgrowth
ingested with precooked foods, usually beef and turkey, that
The proximal small intestine normally has low bacte- have been kept warm under heating lamps in buffet lines.
rial counts because it has several major defenses against Heat-stable spores produce toxins. Although the bacteria are
excess small intestinal bacterial proliferation: intestinal killed and the toxin is destroyed, the spores survive. When
peristalsis (the most important defense), gastric acid, and food is rewarmed, the spores germinate, producing toxin. The
intestinal IgA. When these defenses are altered, bacte- diarrhea is worse than the vomiting and is later in onset. It lasts
rial overgrowth results. The mechanism of steatorrhea in 24 hours. Treatment is supportive.
162 G A S T R O E N T E R O L O GY A N D H E PATO L O GY
Table 12.9 TOXICOGENIC CAUSES OF BACTERIAL DIARRHEA
MEDIATED BY CYCLIC
ORGANISM ONSET, H AMP FEVER INTESTINAL SECRETION
Staphylococcus aureus 16 + +
Escherichia coli 12 + + +
Bacillus cereus 16 + +
Abbreviations: , absence of feature; +, presence of feature (++++, strong presence); r, feature may be present or absent; AMP, adenosine monophosphate.
12 . D I A R R H E A , M A L A B S O R P T I O N, A N D S M A L L -B OW E L D I S O R D E R S 163
Table 12.10 CAUSES OF INVASIVE BACTERIAL DIARRHEA
ANTIBIOTIC
ORGANISM FEVER BLOODY DIARRHEA BACTEREMIA EFFECTIVENESS
Shigella + + + +
Salmonella +
Vibrio parahaemolyticus + + +a
Escherichia coli + +
Staphylococcus aureus + + r +
(enterocolitis)
Yersinia enterocolitica + + + +
Campylobacter jejuni + + r +
Vibrio vulnificus + + + +
Abbreviations: , absence of feature; +, presence of feature; r, feature may be present or absent.
a
Antibiotics are of questionable value, but erythromycin may be most effective.
can cause sporadic or epidemic illness from contaminated ham- Extraintestinal manifestations are nonsuppurative arthri-
burger and raw milk. Enterohemorrhagic E coli infection should tis and ankylosing spondylitis (associated with HLA-B27).
be suspected when bloody diarrhea occurs after eating ham- Skin manifestations are erythema nodosum and ery-
burger and when bloody diarrhea is complicated by hemolytic thema multiforme. Thyroid manifestations are Graves and
uremic syndrome or thrombotic thrombocytopenic purpura. Hashimoto diseases. Multiple liver abscesses and granulo-
Antibiotic treatment has not been effective and is not recom- mata are present.
mended because it may increase the risk of development of Treatment is with aminoglycosides or trimethoprim-
hemolytic uremic syndrome or thrombotic thrombocytopenic sulfamethoxazole. The bacteria are variably sensitive to tet-
purpura from the rapid release of toxin during bacterial death. racycline and chloramphenicol. -Lactamases are frequently
produced, making penicillin resistance common.
Invasive bacterial diarrhea: fever, bloody stools, and fecal
leukocytes. Yersinia enterocolitica: enteritis with acute abdominal pain
(differential diagnosis includes appendicitis and Crohn
Shigella: bloody diarrhea.
disease).
Salmonella typhimurium: bloody diarrhea may be present;
Fecal-oral transmission in water and milk.
treat with antibiotics only if blood cultures are positive.
Manifestations include nonsuppurative arthritis and
Vibrio parahaemolyticus: undercooked shellfish; bloody
ankylosing spondylitis (associated with HLA-B27).
diarrhea.
Escherichia coli: bloody stools, abdominal pain with
fever; occurs after eating contaminated hamburger and Campylobacter jejuni
may cause hemolytic uremic syndrome or thrombotic The comma-shaped C jejuni organisms are motile,
thrombocytopenic purpura. microaerophilic gram-negative bacilli. Transmission is linked
to infected water, unpasteurized milk, poultry, sick dogs, and
infected children. The incubation period is 2 to 4 days before
Yersinia enterocolitica invasion of the small bowel or colon. Infection results in the
The spectrum of disease caused by Y enterocolitica includes presence of blood and leukocytes in the stool. It may mimic
acute and chronic enteritis. Acute enteritis is similar to granulomatous or idiopathic ulcerative colitis. It also may
shigellosis and usually lasts 1 to 3 weeks. It is characterized mimic small-bowel secretory diarrhea, with explosive, frequent
by fever, diarrhea, leukocytosis, and fecal leukocytes. Chronic watery diarrhea due to many C jejuni strains that produce a
enteritis occurs especially in children with diarrhea, failure to cholera-type toxin. The diarrhea usually lasts 3 to 5 days but
thrive, hypoalbuminemia, and hypokalemia. Other features may recur. Antibiotic treatment is with a macrolide antibiotic
are acute abdominal pain (mesenteric adenitis), right lower when severe, but treatment often is not needed. Postdiarrheal
quadrant pain, tenderness, nausea, and vomiting. The disease illnesses are hemolytic uremic syndrome and postinfectious
mimics appendicitis or Crohn disease. This gram-negative rod arthritis.
is hardy and can survive in cold temperatures. It grows on spe-
cial cold-enriched medium. It is an invasive pathogen, with Campylobacter jejuni: transmission is linked to infected water,
fecal-oral transmission in water and milk. unpasteurized milk, poultry, sick dogs, and infected children.
164 G A S T R O E N T E R O L O GY A N D H E PATO L O GY
Infection may mimic granulomatous or idiopathic antibody testing is negative, another diagnosis should be
ulcerative colitis. considered. Small-bowel biopsy findings are not diagnos-
tic. Diagnosis requires response to a gluten-free diet. If
Diarrhea usually lasts 35 days but may recur.
the patient has no response to the diet, the diet should be
reviewed for inadvertent gluten ingestion. If symptoms recur
after 10 to 15 years of successful dietary management, con-
Vibrio vulnificus
sider enteropathy-associated T-cell lymphoma, which is a
Noncholera V vulnificus organisms are extremely inva-
characteristic complication of CD, especially if there is asso-
sive and produce necrotizing vasculitis, gangrene, and shock.
ciated abdominal pain and weight loss.
They are routinely isolated from seawater, zooplankton, and
shellfish along the Gulf of Mexico and both coasts of the
United States, especially in the summer. The 2 clinical syn- CD: iron deficiency anemia is the most common
dromes are 1) wound infection, cellulitis, fasciitis, or myositis manifestation in adults.
after exposure to seawater or cleaning shellfish and 2) septi- Splenic atrophy and an abnormal blood smear with
cemia after the ingestion of raw shellfish (oysters). Patients Howell-Jolly bodies may be clues to the diagnosis in
at high risk of septicemia include those with liver disease, 10%-15% of patients.
congestive heart failure, diabetes mellitus, renal failure, an
immunosuppressive state, or hemochromatosis. Treatment is Enteropathy-associated T-cell lymphoma is a characteristic
with tetracycline. complication of CD.
12 . D I A R R H E A , M A L A B S O R P T I O N, A N D S M A L L -B OW E L D I S O R D E R S 165
Thus, the primary diagnostic approach to a patient with Although the c-kit gene is mutated, the tyrosine kinase inhibi-
clinically suspected Whipple disease is upper endoscopy with tor, imatinib mesylate, is not an effective treatment.
mucosal biopsy. Intestinal biopsy specimens show the char-
acteristic finding of macrophages with periodic acid-Schiff Systemic mastocytosis causes urticaria pigmentosa.
(PAS)-staining particles that represent T whipplei bacilli.
Polymerase chain reaction assays may assist in detecting T Characteristic gastrointestinal tract manifestations include
whipplei DNA in the intestinal mucosa. Whipple disease peptic ulcer disease and diarrhea.
should be suspected in patients who have recurrent arthritis, Bath pruritus is a clue to the diagnosis.
pigmentation, adenopathy, or CNS symptoms (dementia,
myoclonus, ophthalmoplegia, visual disturbances, coma, or
I N T E S T I NA L LY M P H A N G I E C TA S I A
seizures). Treatment is with trimethoprim-sulfamethoxazole
for 1 year. Intestinal lymphangiectasia is caused by lymphatic obstruc-
tion that results in dilatation of intestinal lymphatic channels
Suspect Whipple disease in patients who have recurrent with subsequent lacteal rupture and leakage of chylomicrons
arthritis, adenopathy, or CNS symptoms. and protein-rich fluid into the intestine. The clinical fea-
tures are edema (often unilateral leg edema), chylous perito-
Oculomasticatory myorhythmia is pathognomonic of
neal or pleural effusions, and steatorrhea or protein-losing
Whipple disease.
enteropathy. Laboratory findings include lymphocytopenia
Small-bowel biopsy specimens show PAS-positive granules (average lymphocyte count, 0.6109/L) due to enteric loss.
in macrophages. Levels of all serum proteins, including immunoglobulins, are
decreased. Small-bowel radiographs show edematous folds,
Treatment: trimethoprim-sulfamethoxazole for 1 year.
and small-bowel biopsy specimens show dilated lacteals and
lymphatics in the lamina propria that may contain lipid-laden
macrophages. The same biopsy findings are seen in obstruc-
E O S I N O P H I L I C G A S T RO E N T E R IT I S tion of mesenteric lymph nodes (lymphoma, Whipple disease,
and Crohn disease) and obstruction of venous inflow to the
Patients with eosinophilic gastroenteritis have a history of heart (constrictive pericarditis and severe right heart failure).
allergies (eg, asthma), food intolerances, and episodic symp- Diagnosis is based on abnormal small-bowel biopsy findings
toms of nausea, vomiting, abdominal pain, and diarrhea. and enteric protein loss documented by finding increased 1-
Laboratory findings include peripheral eosinophilia, iron antitrypsin levels in the stool. Treatment is with a low-fat diet
deficiency anemia, and steatorrhea or protein-losing enteropa- and medium-chain triglycerides (they enter the portal blood
thy. Small-bowel radiographs show coarse folds and filling rather than the lymphatics). Occasionally, surgical excision of
defects, and biopsy specimens show infiltration of the mucosa the involved segment is useful if the lesion is localized.
by eosinophils and, occasionally, the absence of villi. Parasitic
infection should be ruled out. Treatment with corticosteroids Intestinal lymphangiectasia: unilateral lymphedema of the
produces a rapid response. leg and chylous peritoneal or pleural effusions.
Eosinophilic gastroenteritis: allergies, food intolerances, Lymphocytopenia is characteristic.
eosinophilia, and episodic intestinal symptoms. Decreased levels of serum proteins.
Rule out parasitic infection. Biopsy specimens of the small intestine show dilated
Corticosteroids produce a rapid response. lymphatic channels.
Treatment: low-fat diet and medium-chain triglycerides.
S Y S T E M I C M A S TO C Y TO S I S
A MY L O I D O S I S
Systemic mastocytosis is a clonal proliferation of mast cells
with activating mutations in the c-kit gene. It is characterized Amyloidosis is characterized by diffuse deposition of amor-
by mast cell infiltration of tissues, including those in the bone phous eosinophilic extracellular protein in the tissue.
marrow, spleen, liver, and gastrointestinal tract. The charac- Gastrointestinal tract involvement can occur with AL amyloi-
teristic dermatologic finding is urticaria pigmentosa. Typical dosis, AA amyloidosis, and hereditary amyloidosis. The main
symptoms include pruritus, flushing, tachycardia, asthma, sites of amyloid deposition are the walls of blood vessels and
and headache caused by the release of histamine from mast the mucous membranes and muscle layers of the intestine. Any
cells. Gastrointestinal tract manifestations include diarrhea portion of the gut may be involved. Amyloid damages tissues
and peptic ulcer disease. Symptoms may be provoked by heat; by infiltration (muscle and nerve infiltration causes motility
hence, bath pruritus (ie, itching after a hot bath) is a clue to disorders and malabsorption) and ischemia (obliteration of
the diagnosis. Treatment includes histamine receptor block- vessels causes ulceration and bleeding). Intestinal dysmotil-
ers, anticholinergics, cromoglycate, and glucocorticoids. ity can produce diarrhea, constipation, pseudo-obstruction,
166 G A S T R O E N T E R O L O GY A N D H E PATO L O GY
megacolon, and fecal incontinence. Clinical findings in amy- of a graft into the intestinal lumen on endoscopy), emergent
loidosis include macroglossia, hepatomegaly, cardiomegaly, surgery is indicated.
proteinuria, and peripheral neuropathy. Pinch (posttraumatic)
purpura or periorbital purpura after proctoscopic examina- If a patient presents with massive bleeding, do not attempt
tion may occur. Small-bowel radiography shows symmetri- endoscopy or arteriography. Instead, emergency surgery is
cal, sharply demarcated thickening of the plicae circulares. indicated.
Histologic examination of duodenal biopsy specimens shows
amyloid deposits in up to 100% of patients. It is the diagnostic C H RO N I C I N T E S T I NA L
test of choice when amyloid is suspected as a cause of gastro- P S EU D O - O B S T RU C T I O N
intestinal tract symptoms. Amyloid deposits may not be seen
on routine histologic stains; Congo red staining is required. Pseudo-obstruction is a syndrome characterized by the clin-
Subcutaneous fat pad aspirate stained with Congo red can be ical findings of mechanical bowel obstruction but with-
used to make the diagnosis in 80% of patients. out occlusion of the lumen. The 2 types are primary and
secondary.
The primary type, also called idiopathic pseudo-obstruction,
M I S C E L L A N E O U S S M A L L -B OW E L is a visceral myopathy or neuropathy. It is associated with recur-
DISORDER S rent attacks of nausea, vomiting, cramping abdominal pain, dis-
tention, and constipation, which are of variable frequency and
duration. If the cause is familial, the patient has a positive family
M E C K E L D I VE RT I CU LUM
history and the condition is present when the patient is young.
A Meckel diverticulum results from persistence of the vitelline Esophageal motility is abnormal (achalasia) in most patients;
duct, which is the communication between the intestine and occasionally, urinary tract motility is abnormal. Diarrhea or
the yolk sac. It is the most frequent congenital abnormality of steatorrhea results from bacterial overgrowth. Upper gastroin-
the small intestine and is an antimesenteric outpouching of the testinal tract and small-bowel radiographs show dilatation of
ileum usually occurring within 100 cm of the ileocecal valve. A the bowel and slow transit (not mechanical obstruction).
Meckel diverticulum contains all layers of the intestinal wall and
so is a true diverticulum. It may contain ectopic gastrointestinal Idiopathic pseudo-obstruction is due to a familial cause or
tract mucosa, including gastric (most commonly), duodenal, bil- to a sporadic visceral myopathy or neuropathy.
iary, colonic, or pancreatic tissue. The most common manifesta-
tion is painless, maroon stools, with peptic ulceration being the Recurrent attacks have variable frequency and duration.
cause of bleeding secondary to acid production by the ectopic Esophageal motility is abnormal in most patients.
gastric mucosa within the Meckel diverticulum. Other mani-
festations include intestinal obstruction due to intussusception Steatorrhea is caused by bacterial overgrowth.
or volvulus around the band that fixes the diverticulum to the
bowel wall. Diverticulitis of a Meckel diverticulum can occur Secondary pseudo-obstruction occurs in the presence of
and mimic acute appendicitis. The diagnostic test of choice is a underlying systemic disease or precipitating causes, including
Meckel scan (a technetium Tc 99m pertechnetate nuclear scan the following:
with mucous cells of gastric mucosa concentrating technetium),
but false-positive and false-negative results can occur. Diseases involving the intestinal smooth muscle:
amyloidosis, scleroderma, systemic lupus erythematosus,
Meckel diverticulum is the most common congenital myotonic dystrophy, and muscular dystrophy.
abnormality of the small intestine. Neurologic diseases: Parkinson disease, Hirschsprung
The most common manifestation is painless, maroon disease, Chagas disease, and familial autonomic
stools, and this diagnosis must be considered when young dysfunction.
adults present with lower gastrointestinal tract bleeding. Endocrine disorders: hypoparathyroidism.
Drugs: antiparkinsonian medications (levodopa),
AO RTO E N T E R I C FI S T U L A
phenothiazines, tricyclic antidepressants, ganglionic
A history of gastrointestinal tract bleeding in a patient who blockers, clonidine, and narcotics.
has had a previous aortic graft demands immediate evaluation
to rule out an aortoenteric fistula. If the patient presents with Approach to the Patient With Chronic Intestinal
massive bleeding, do not attempt endoscopy or arteriography. Pseudo-Obstruction
Emergency surgery is indicated.
Management of a smaller bleeding episode is more contro- If a patient has chronic intestinal pseudo-obstruction, first
versial, and urgent computed tomography or extended upper rule out a mechanical cause for the obstruction. Second, look
endoscopy has been suggested as a possible alternative to sur- for an underlying precipitating cause such as metabolic abnor-
gical exploration. If the presence of a graft fistula is confirmed malities, medications, or an underlying associated disease.
(by air in the vessel wall on computed tomography or erosion If a familial idiopathic cause is suspected, assess esophageal
12 . D I A R R H E A , M A L A B S O R P T I O N, A N D S M A L L -B OW E L D I S O R D E R S 167
motility. Suspect scleroderma if intestinal radiography shows In exudative diarrhea, membrane permeability is abnormal
large-mouth diverticula of the small intestine. Suspect amyloi- and stool volume is typically small. Causes of exudative
dosis if the skin shows palpable purpura and if proteinuria and diarrhea: invasive bacterial pathogens and inflammatory
neuropathy are present. bowel disease.
Noninvasive (toxicogenic) bacterial diarrhea, characterized
Secondary pseudo-obstruction is due to an underlying
by watery stools without fecal leukocytes. Invasive bacterial
systemic disease or precipitating cause.
diarrhea is characterized by fever, bloody stools, and fecal
Patients with scleroderma present with large-mouth leukocytes.
diverticula of the intestine.
CD: iron deficiency anemia is the most common
Patients with amyloidosis present with palpable purpura, manifestation in adults.
proteinuria, and neuropathy.
Tropical sprue: diarrhea and megaloblastic anemia after
travel to the tropics.
S U M M A RY Suspect Whipple disease in patients who have recurrent
arthritis, adenopathy, or CNS symptoms.
In osmotic diarrhea, stool volume is <1 L daily. Causes of
Eosinophilic gastroenteritis: allergies, food intolerances,
osmotic diarrhea: lactase deficiency, sorbitol, and antacids.
eosinophilia, and episodic intestinal symptoms. Rule out
In secretory diarrhea, stool volume is >1 L daily. Causes parasitic infection.
of secretory diarrhea: bacterial toxins, neuroendocrine
Intestinal lymphangiectasia: unilateral lymphedema of the
tumors, surreptitious ingestion of laxative, bile acid
leg and chylous peritoneal or pleural effusions.
diarrhea, and fatty acid diarrhea.
168 G A S T R O E N T E R O L O GY A N D H E PATO L O GY
13.
LIVER AND BILIARY TRACTa
John J. Poterucha, MD
A L K A L I N E P H O S P H ATA S E
I N T E R P R ETAT I O N O F A B N O R M A L L I VE R Alkaline phosphatase is found on the hepatocyte membrane
T E S T R E S U LT S that borders the bile canaliculi (the smallest branches of
the bile ducts). Because alkaline phosphatase is also found
The evaluation of patients who have abnormal liver test in bone and placenta, an isolated increase in the serum level
results includes many clinical factors: the patients chief of this enzyme should prompt further testing to determine
complaints, age, risk factors for liver disease, personal whether the increase is from the liver or other tissues. One
or family history of liver disease, medications, and physi- method of further testing is to determine alkaline phospha-
cal examination findings. Designing a standard algorithm tase isoenzyme levels. Another method is to determine the
for the evaluation of abnormal liver test results has been level of J-glutamyltransferase (GGT), an enzyme of intra-
challenging. Nevertheless, with some basic information, hepatic biliary canaliculi that is more specific than alkaline
abnormalities can be evaluated in an efficient, cost-effective phosphatase. Other than to confirm the hepatic origin of
manner. an increased level of alkaline phosphatase, GGT has little
role in the diagnosis of diseases of the liver because its syn-
thesis can be induced by many medications, thus reducing
C O M M O N LY U S E D L I VE R T E S T S its specificity for clinically important liver disease.
169
as hemolysis or resorption of a hematoma, are character- Table 13.1 COMMON CAUSES OF A MARKED ACUTE
ized by hyperbilirubinemia that is less than 20% conjuga- INCREASE IN ALT
ted. Hepatocyte dysfunction or impaired bile flow produces
hyperbilirubinemia that is usually more than 50% conjuga- DISEASE CLINICAL CLUE DIAGNOSTIC TEST
ted bilirubin. Because conjugated bilirubin is water soluble
and may be excreted in the urine, patients with liver disease Hepatitis A Exposure history IgM anti-HAV
and hyperbilirubinemia have dark urine. In these patients, the Hepatitis B Risk factors HBsAg, IgM anti-HBc
stools have a lighter color because of the absence of bilirubin
pigments. Drug-induced Compatible medication Improvement after with-
hepatitis or timing drawal of the agent
Hyperbilirubinemia is usually <20% conjugated bilirubin Alcoholic History of alcohol excess, Clinical improvement
in diseases characterized by overproduction of bilirubin. hepatitis AST:ALT >2, AST with abstinence
<400 U/L
Hyperbilirubinemia is usually >50% conjugated bilirubin
with hepatocyte dysfunction or impaired bile flow. Hepatitic History of hypotension & Rapid improvement of
ischemia heart disease aminotransferase
levels
Acute biliary Abdominal pain, fever Cholangiography
P ROT H RO M B I N T I M E A N D A L BU M I N obstruction
Prothrombin time (PT), expressed as the international nor-
malized ratio (INR), and serum level of albumin are markers Abbreviations: ALT, alanine aminotransferase; AST, aspartate aminotransferase;
HAV, hepatitis A virus; anti-HBc, antibody to hepatitis B core antigen; HBsAg,
of liver synthetic function. Abnormalities of PT and albumin hepatitis B surface antigen; U, units.
imply severe liver disease and should prompt an immediate
evaluation. INR is a measure of the activity of coagulation fac-
tors II, V, VII, and X, all of which are synthesized in the liver.
Because these factors are also dependent on vitamin K for syn-
jaundice. ALT and AST levels are usually greater than 500
thesis, deficiencies of vitamin K also produce abnormalities of
U/L. Common causes of a marked acute increase in ALT are
INR. Vitamin K deficiency can result from the use of antibiot-
listed in Table 13.1.
ics during a period of prolonged fasting, small-bowel mucosal
The level and pattern of aminotransferase elevation may be
disorders such as celiac disease, and severe cholestasis, with an
helpful in the differential diagnosis of acute hepatitis. Acute
inability to absorb fat-soluble vitamins. True hepatocellular
hepatitis due to viruses or drugs generally produces mark-
dysfunction is characterized by an inability to synthesize clot-
edly elevated levels of aminotransferases, often in the thou-
ting factors even when stores of vitamin K are adequate. A sim-
sands (units per liter). In general, the concentration of ALT is
ple way to distinguish between vitamin K deficiency and liver
higher than that of AST. An ALT concentration greater than
dysfunction in a patient with a prolonged PT is to administer
5,000 U/L is usually caused by acetaminophen hepatotoxic-
vitamin K. A 10-mg dose of oral vitamin K for 3 days or 10 mg
ity, hepatic ischemia (shock liver), or unusual viruses such
of subcutaneous vitamin K normalizes the PT within 48 hours
as herpes simplex virus. Hepatic ischemia typically occurs
in a vitamin Kdeficient patient, but it has no effect on the PT
in patients with preexisting cardiac disease after an episode
in a patient with decreased liver synthetic function.
of hypotension. Aminotransferase levels are very high but
Because albumin has a half-life of 21 days, serum levels do
decrease considerably within a few days. Another cause of
not decrease suddenly with liver dysfunction. However, the
transient elevations of aminotransferase levels is transient bile
serum level of albumin can decrease relatively quickly in a
duct obstruction, usually from a stone. These elevations can
severe systemic illness such as bacteremia. This rapid decrease
be as high as 1,000 U/L, but they decrease within 24 to 48
most likely results from the release of cytokines and the accel-
hours. In patients with pancreatitis, a transient increase in the
erated metabolism of albumin. A chronic decrease of albumin
AST or ALT concentration suggests gallstone pancreatitis.
in a patient without overt liver disease should prompt a search
Alcoholic hepatitis is characterized by more modest increases
for albumin in the urine.
in aminotransferase levels, which are always less than 400 U/L
and, at times, near normal. In patients with alcoholic hepatitis,
PT and albumin are markers of liver synthetic function.
usually the AST:ALT ratio is greater than 2:1. Finally, patients
with alcoholic hepatitis frequently have a markedly elevated
level of bilirubin that is out of proportion to the aminotrans-
H E PATO C E L LU L A R D I S O R D E R S ferase elevations.
Diseases that produce a sustained (>3 months) increase in
Hepatocellular disorders are diseases that primarily affect aminotransferase levels are in the category of chronic hepa-
hepatocytes and are characterized predominantly by increases titis. The increase (usually 2-fold to 5-fold) in aminotrans-
in aminotransferases. The disorders are best considered as ferase levels is more modest than in acute hepatitis. Patients
acute (generally <3 months) or chronic. Acute hepatitis may are usually asymptomatic but occasionally complain of fatigue
be accompanied by malaise, anorexia, abdominal pain, and and right upper quadrant pain. The differential diagnosis of
170 G A S T R O E N T E R O L O GY A N D H E PATO L O GY
Table 13.2 COMMON CAUSES OF CHRONIC HEPATITIS Table 13.3 COMMON CAUSES OF CHOLESTASIS
DISEASE CLINICAL CLUE DIAGNOSTIC TEST DISEASE CLINICAL CLUE DIAGNOSTIC TEST
Hepatitis C Risk factors Anti-HCV, HCV RNA Primary biliary Middle-aged woman Antimitochondrial
cirrhosis antibody
Hepatitis B Risk factors HBsAg
Primary sclerosing Association with Cholangiography
Nonalcoholic Obesity, Steatosis on liver imaging, cholangitis ulcerative colitis (ERCP or MRCP)
steatohepatitis diabetes mellitus, liver biopsy
hyperlipidemia Large bile duct Jaundice or pain Ultrasonography,
obstruction (or both) ERCP, or MRCP
Alcoholic liver History, AST:ALT Clinical liver biopsy
disease >2 Drug-induced Compatible medica- Improvement after
cholestasis tion or timing withdrawal of the
Autoimmune ALT 2001,500 Strongly positive antinuclear agent
hepatitis U/L, usually or antismooth muscle
female, other antibody (or both), hyper- Infiltrative disorder Other clinical features Ultrasonography, com-
autoimmune gammaglobulinemia, liver or malignancy of malignancy, puted tomography,
disease biopsy sarcoidosis, or liver biopsy
amyloidosis
Abbreviations: ALT, alanine aminotransferase; AST, aspartate aminotransferase; Inflammation- Symptoms of underly- Blood cultures, appro-
HBsAg, hepatitis B surface antigen; HCV, hepatitis C virus; U, units. associated ing inflammatory priate antibody
cholestasis state tests
chronic hepatitis is relatively lengthy; the more important and Abbreviations: ERCP, endoscopic retrograde cholangiopancreatography; MRCP,
common disorders are listed in Table 13.2. magnetic resonance cholangiopancreatography.
13. L I VE R A N D B I L I A RY T R AC T 171
Conjugated hyperbilirubinemia
Sepsis
Elevated alkaline phosphatase
Persistently high ALT Dubin-Johnson syndrome
Transient increase in ALT
Rotor syndrome
Figure 13.1 Evaluation of Conjugated Hyperbilirubinemia. ALT indicates alanine aminotransferase; CT, computed tomography; ERCP, endoscopic
retrograde cholangiopancreatography; MRCP, magnetic resonance cholangiopancreatography; US, ultrasonography. (Adapted from Poterucha JJ.
Approach to the patient with abnormal liver tests and fulminant liver failure. In: Hauser SC, editor. Mayo Clinic gastroenterology and hepatology
board review. 3rd ed. Rochester [MN]: Mayo Clinic Scientific Press and Florence [KY]: Informa Healthcare USA; c2008. p. 28392. Used with
permission of Mayo Foundation for Medical Education and Research.)
A L G O R I T H M S F O R PAT I E N T S W I T H liver test results that are less than 3 times the normal value
A B N O R M A L L I VE R T E S T R E S U LT S can be observed unless the patient is symptomatic or the
albumin level, INR, or bilirubin concentration is abnormal.
Algorithms for patients with abnormal liver test results are Persistent abnormalities should be evaluated. Algorithms
at best only guidelines and at worst misleading. The patients for the management of patients with increased levels of ALT
clinical presentation should be considered when interpret- or alkaline phosphatase are shown in Figures 13.2 and 13.3,
ing abnormal results. In general, patients with abnormal respectively.
Abnormal ALT
Duration <3 mo
Persistent increase,
Elevation <3-fold
symptomatic patient, or
No symptoms
impaired liver function
Good liver function
Figure 13.2 Evaluation of Abnormal Alanine Aminotransferase (ALT) Levels. A1AT indicates D1-antitrypsin; ANA, antinuclear antibody;
anti-HAV, hepatitis A virus antibody; anti-HBc, antibody to hepatitis B core antigen; anti-HCV, hepatitis C virus antibody; HBsAg, hepatitis B
surface antigen; HCV, hepatis C virus; US, ultrasonography. (Adapted from Poterucha JJ. Approach to the patient with abnormal liver tests and
fulminant liver failure. In: Hauser SC, editor. Mayo Clinic gastroenterology and hepatology board review. 3rd ed. Rochester [MN]: Mayo Clinic
Scientific Press and Florence [KY]: Informa Healthcare USA; c2008. p. 28392. Used with permission of Mayo Foundation for Medical Education
and Research.)
172 G A S T R O E N T E R O L O GY A N D H E PATO L O GY
Alkaline phosphatase increased
Figure 13.3 Evaluation of Increased Levels of Alkaline Phosphatase. GGT indicates -glutamyltransferase; MRCP, magnetic resonance
cholangiopancreatography; US, ultrasonography. (Adapted from Poterucha JJ. Approach to the patient with abnormal liver tests and fulminant liver
failure. In: Hauser SC, editor. Mayo Clinic gastroenterology and hepatology board review. 3rd ed. Rochester [MN]: Mayo Clinic Scientific Press and
Florence [KY]: Informa Healthcare USA; c2008. p. 28392. Used with permission of Mayo Foundation for Medical Education and Research.)
HAV is transmitted by ingestion of contaminated food or Jaundice rarely lasts >4 weeks.
water or contact with an infected person.
A brief guide to the interpretation of serologic markers
The incubation period is 1550 days. of hepatitis B is shown in Table 13.4. Viral markers in the
IgM anti-HAV is present during the acute illness. blood during a self-limited infection with HBV are shown
in Figure 13.4. Note that IgM antibody to hepatitis B core
The prognosis is excellent and chronic liver disease does antigen (anti-HBc) is nearly always present during acute
not develop. hepatitis B.
Five percent of patients who acquire HBV as adults and
90% of those infected as neonates do not clear hepatitis B
Hepatitis B
surface antigen (HBsAg) from the serum within 6 months
Hepatitis B virus (HBV) is a DNA virus that is transmit- and, thus, become chronically infected. The natural history of
ted by exposure to blood or contaminated body fluids. In chronic infection is illustrated in Figure 13.5.
13. L I VE R A N D B I L I A RY T R AC T 173
Table 13.4 HEPATITIS B SEROLOGIC MARKERS e antigen (HBeAg), and very high HBV DNA levels. Liver
histology shows ground glass hepatocytes but otherwise
INTERPRETATION OF POSITIVE
TEST RESULTS
minimal changes. Treatment is not recommended. The
immune-tolerant phase evolves under immune pressure into
Hepatitis B surface antigen Current infection the HBeAg-positive chronic hepatitis B phase, character-
(HBsAg) ized by elevated ALT, the presence of HBeAg, more than 10 4
IU/mL of HBV DNA, and active inflammation and often
Antibody to hepatitis B sur- Immunity (immunization or resolved
face (anti-HBs) infection)
fibrosis on liver biopsy. This phase is generally considered to
lead to progressive liver damage, including cirrhosis and an
IgM antibody to hepatitis B Usually recent infection; occasionally increased risk of hepatocellular carcinoma. At a rate of about
core (IgM anti-HBc) reactivation of chronic infection 10% per year, patients mount an immune response that is suf-
IgG antibody to hepatitis B Remote infection ficient to achieve a decrease in ALT, clearance of HBeAg,
core (IgG anti-HBc) development of antibody to hepatitis B e antigen (anti-HBe)
(seroconversion), and a decrease of HBV DNA levels to less
Hepatitis B e antigen Active viral replication
(HBeAg) or HBV DNA
than 2,000 IU/mL. This inactive carrier phase is generally
>104 IU/mL not accompanied by progressive liver damage. Most patients
remain in this phase for many years and have a better prog-
Antibody to hepatitis B e Remote infection nosis than patients with active liver inflammation and viral
(anti-HBe)
replication. Sixty percent of patients with chronic hepatitis
B infection are in the inactive carrier phase.
Abbreviations: HBV, hepatitis B virus; IU, international units. About one-third of inactive carriers have a recurrence of
Adapted from Poterucha JJ. Chronic viral hepatitis. In: Hauser SC, editor. Mayo chronic hepatitis characterized by an abnormal ALT level and
Clinic gastroenterology and hepatology board review. 4th ed. Rochester (MN):
Mayo Clinic Scientific Press and New York (NY): Oxford University Press; c2011. an increased HBV DNA level. This may be associated with a
p. 26979. Used with permission of Mayo Foundation for Medical Education and recurrence of the HBeAg-positive state, although more com-
Research. monly it is due to a precore or core promoter variant that pro-
duces HBeAg-negative chronic hepatitis B. This phase, similar
Patients who are infected perinatally, typically those from to the HBeAg-positive phase, is associated with a progression
Asia, generally go through an immune-tolerant phase that of liver disease.
lasts until early adulthood. The immune tolerant phase is Patients with chronic hepatitis B and cirrhosis are at high
characterized by normal ALT, the presence of hepatitis B risk of hepatocellular carcinoma, and liver ultrasonography
should be performed every 6 to 12 months. After neonatal
or early childhood acquisition of hepatitis B, hepatocellu-
Clinical lar carcinoma may develop even in the absence of cirrhosis,
hepatitis
and surveillance is advised for the following patients: Asian
men older than 40 years, Asian women older than 50 years,
Africans older than 20 years, patients with a family history of
hepatocellular carcinoma, and patients with persistent eleva-
HBsAg
Anti-HBc
tions of ALT and HBV DNA.
Figure 13.4 Viral Markers in Blood During Self-limited Hepatitis B Patients with chronic hepatitis B, an abnormal ALT level,
Virus Infection. Anti-HBc indicates hepatitis B core antibody; anti-HBe, and HBV DNA >104 IU/mL are candidates for therapy.
hepatitis B e antibody; anti-HBs, hepatitis B surface antibody; HBeAg, Treatment options are compared and contrasted in Table 13.5.
hepatitis B e antigen; HBsAg, hepatitis B surface antigen; part, particle; Treatment with peginterferon alfa results in a 30% response
pol, polymerase. (Adapted from Robinson WS. Biology of human
hepatitis viruses. In: Zakim D, Boyer TD, editors. Hepatology: a rate as measured by the loss of HBeAg, the suppression of HBV
textbook of liver disease. Vol 2. 2nd ed. Philadelphia [PA]: WB Saunders DNA, and the appearance of anti-HBe. Rarely, patients also
Company; c1990. p. 890945. Used with permission.) clear HBsAg. Patients more likely to respond to peginterferon
174 G A S T R O E N T E R O L O GY A N D H E PATO L O GY
Immune
tolerance
Positive HBeAg
DNA
Normal ALT
HBeAg-negative HBeAg-positive
chronic hepatitis chronic hepatitis
Progression to
Negative HBeAg cirrhosis Positive HBeAg
DNA DNA
Abnormal ALT Abnormal ALT
Inactive
Precore carrier HBeAg
mutation seroconversion
Negative HBeAg
DNA
Normal ALT
Figure 13.5 Phases of Chronic Hepatitis B Virus Infection. Black arrows represent histopathologic changes; gray arrows represent changes in serologic
markers between phases; thin arrows represent an increase or decrease in DNA level (n, low increase; nn, moderate increase; pp, moderate decrease;
nnn, high increase). ALT indicates alanine aminotransferase; HBeAg, hepatitis B e antigen. (Adapted from Pungpapong S, Kim WR, Poterucha
JJ. Natural history of hepatitis B virus infection: an update for clinicians. Mayo Clin Proc. 2007 Aug;82[8]:96775. Used with permission of Mayo
Foundation for Medical Education and Research.)
include those with high serum levels of aminotransferases, low resistance rates, entecavir and tenofovir are the preferred
active hepatitis without evidence of cirrhosis on biopsy, and oral drugs of choice for the treatment of hepatitis B.
low serum levels of HBV DNA. Patients with HBV infec- Hepatitis B immune globulin should be given to house-
tion who have a response to peginterferon therapy may have hold and sexual contacts of patients with acute hepatitis
a transient increase in aminotransferase levels after about 8 B. Infants should receive hepatitis B vaccine. The marker
weeks of treatment. An acute hepatitis syndrome may be pre- of immunity is hepatitis B surface antibody (anti-HBs).
cipitated, and peginterferon is generally not given to patients Neonates often acquire hepatitis B perinatally if the mother
with cirrhosis. Tenofovir, entecavir, lamivudine, adefovir, and is infected. Because infected neonates are at high risk of
telbivudine are oral agents that decrease HBV DNA levels and chronic infection, all pregnant women should be tested
may result in clinical improvement, even in the presence of for HBsAg. If a pregnant woman is HBsAg-positive, the
decompensation. The oral drugs are safer than peginterferon infant should receive both hepatitis B immunoglobulin and
for patients with cirrhosis because flares of hepatitis and infec- hepatitis B vaccine. This strategy may not be effective when
tious complications are uncommon. Resistance is a concern HBV DNA is high in the mother, and some have advised
with the oral agents; the highest rates of resistance occur with administration of lamivudine or tenofovir during the third
lamivudine, intermediate rates with adefovir and telbivudine, trimester in women who have an HBV DNA level of more
and low rates with entecavir and tenofovir. Because of their than 10 7 U/mL.
HBeAg seroconversion, % 27 20 12 21 22 20
Resistance None 12%15% yearly 1%4% yearly 1%2% yearly 22% at 2 y None
13. L I VE R A N D B I L I A RY T R AC T 175
Patients who are HBsAg-positive and are receiving immu- Table 13.6 INTERPRETATION OF ANTI-HCV RESULTS
nosuppressive therapy should also receive hepatitis B treat-
ANTI-HCV BY ANTI-HCV BY
ment, even if they do not meet the other recommendations for
ELISA RIBA INTERPRETATION
therapy. Treatment of those patients decreases the risk of hepa-
titis B flares that can be precipitated by immune suppression. Positive Negative False-positive ELISA; patient does
not have true antibody
Hepatitis D virus (HDV), or delta agent, is a small RNA par- Positive Indeterminate Uncertain antibody status
ticle that requires the presence of HBsAg to cause infection.
HDV infection can occur simultaneously with acute HBV Abbreviations: ELISA, enzyme-linked immunosorbent assay; anti-HCV, antibod-
ies to hepatitis C virus; RIBA, recombinant immunoblot assay.
infection (coinfection) or HDV may infect a patient with
a
chronic hepatitis B (superinfection). Infection with HDV Anti-HCV does not necessarily indicate current hepatitis C infection (see text).
should be considered only for patients with HBsAg; it is diag-
nosed by anti-HDV seroconversion.
Common modes of transmission are illicit drug use and
HDV requires the presence of HBsAg to cause infection. transfusion of blood products before 1990.
HDV infection is diagnosed by anti-HDV seroconversion. The presence of HCV RNA is used to diagnose HCV
infection.
176 G A S T R O E N T E R O L O GY A N D H E PATO L O GY
HCC
1.4% yearly
60%85% 20%30%
Acute hepatitis C Chronic infection Cirrhosis
15%40%
Death
Resolution
10 y 20 y 30 y
Figure 13.6 Natural History of Hepatitis C. Values are percentages of patients. HCC indicates hepatocellular carcinoma. (Adapted from Poterucha
JJ. Chronic viral hepatitis. In: Hauser SC, editor. Mayo Clinic gastroenterology and hepatology board review. 4th ed. Rochester [MN]: Mayo Clinic
Scientific Press and New York [NY]: Oxford University Press; c2011. p. 26979. Used with permission of Mayo Foundation for Medical Education
and Research.)
The risk of hepatocellular carcinoma complicating hepa- is increasingly reported in patients who have not visited these
titis C with cirrhosis is 1% to 4% per year. Surveillance with areas. Clinically, hepatitis E resembles hepatitis A.
liver imaging every 6 to 12 months is advised for patients
who are potential candidates for treatment with liver trans-
plant, percutaneous ablation, transarterial chemoemboliza- Other Viral Causes of Hepatitis
tion, or radioembolization. Patients with HCV infection Epstein-Barr virus, cytomegalovirus, and herpesvirus may all
and decompensated cirrhosis should be considered for liver cause hepatitis as part of a clinical syndrome. Infections with
transplant. these agents are most serious in immunocompromised patients.
Immunocompetent patients with infectious mononucleosis
Symptomatic, clinically recognized acute hepatitis C is syndromes commonly have abnormal liver test results and
unusual. mild increases in bilirubin levels, although clinically recog-
Of the patients who acquire HCV, 60%85% remain nized jaundice is unusual. Herpes hepatitis generally occurs in
chronically infected. immunosuppressed or pregnant patients and is characterized
by fever, mental status changes, absence of jaundice, and AST
Treatment of hepatitis C results in sustained clearance and ALT levels greater than 5,000 U/L.
of HCV RNA in approximately 70%90% of patients;
response rates are highest in those infected with genotype
2 or 3. AU TO I M MU N E H E PAT I T I S
Patients with cirrhosis due to hepatitis C are at increased Autoimmune hepatitis was previously called autoimmune
risk of hepatocellular carcinoma, particularly if they have a chronic active hepatitis because the diagnosis required 3 to
history of alcohol excess. 6 months of abnormal liver enzyme test results. However,
40% of patients with autoimmune hepatitis present with
a clinical acute hepatitis. Autoimmune hepatitis can affect
Hepatitis E patients of any age, predominantly females. By definition,
patients with autoimmune hepatitis should not have a
Hepatitis E virus is an enterically transmitted RNA virus history of drug-related hepatitis, HBV, HCV, or Wilson
that causes acute hepatitis primarily in patients who have disease. Immunoserologic markers, such as antinuclear anti-
lived or traveled in areas where the virus is endemic (India, body (ANA), smooth muscle antibody, soluble liver anti-
Pakistan, Mexico, and Southeast Asia); however, hepatitis E gen antibodies, or antibodies to liver-kidney microsomal
13. L I VE R A N D B I L I A RY T R AC T 177
(LKM) antigens, are usually detected. Patients with auto- Mallory bodies), and an inflammatory infiltrate of
immune hepatitis may have other autoimmune diseases, neutrophils.
including Hashimoto thyroiditis. Aminotransferase lev-
Common symptoms include anorexia, nausea, vomiting,
els are generally 4 to 20 times the reference value, and
abdominal pain, and weight loss.
most patients have an increased level of gamma globulin.
Corticosteroids (3060 mg daily) produce improvement Common signs are hepatomegaly, ascites, jaundice, fever,
in most patients, and the improvement in liver test results splenomegaly, and encephalopathy.
and gamma globulin levels is often dramatic. Azathioprine
is often used to allow the use of lower doses of prednisone. The level of AST is almost always <400 U/L in patients
Immunosuppressive doses should be decreased to control with alcoholic hepatitis.
symptoms and to maintain the serum level of aminotrans- The AST:ALT ratio is frequently >2.
ferases less than 5 times the reference value. Even after an
excellent response to corticosteroids, relapse often occurs Leukocytosis occurs in severely ill patients.
and the control of autoimmune hepatitis usually requires
maintenance therapy. Poor prognostic markers of alcoholic hepatitis include
encephalopathy, spider angiomata, ascites, renal failure,
Autoimmune hepatitis is a chronic condition, but patients prolonged PT, and a bilirubin concentration greater than
may present with acute hepatitis. 20 mg/dL. Many patients have disease progression, particu-
larly if alcohol intake is not curtailed. Corticosteroid therapy
Drug-related hepatitis, HBV, HCV, and Wilson disease may be beneficial as an acute treatment of alcoholic hepati-
should be excluded before making a diagnosis of tis in patients with severe disease characterized by encephal-
autoimmune hepatitis. opathy and a markedly prolonged PT. Pentoxifylline is a safe
Immunoserologic markers are usually detected. agent that has shown benefit in a single randomized controlled
study. A discriminant function (DF) greater than 32 helps to
Most patients have improvement with corticosteroid identify patients with a poor prognosis:
therapy, and the improvement in liver test results and
gamma globulin levels is often dramatic. DF = 4.6(PTpatient PTcontrol) + bilirubin (mg/dL).
The control of autoimmune hepatitis usually requires
Poor prognostic markers of alcoholic hepatitis:
maintenance therapy.
encephalopathy, ascites, renal failure, prolonged PT, and
bilirubin >20 mg/dL.
Corticosteroid therapy may be beneficial in severe disease.
A L C O H O L I C L I VE R D I S E A S E
Alcoholic Hepatitis Alcoholic Cirrhosis
Long-term, excessive use of alcohol (>20 g daily for women Cirrhosis is defined histologically by septal fibrosis with
and >40 g daily for men) can produce advanced liver disease. nodular parenchymal regeneration. Only 60% of patients
Alcoholic hepatitis is characterized histologically by fatty with alcoholic cirrhosis have signs or symptoms of liver dis-
change, degeneration and necrosis of hepatocytes (with or ease, and most patients with alcoholic cirrhosis lack a clini-
without Mallory bodies), and an inflammatory infiltrate of cal history of alcoholic hepatitis. Liver enzyme levels may
neutrophils. Almost all patients have fibrosis, and they may be relatively normal in cirrhosis without alcoholic hepatitis.
have cirrhosis. Clinically, patients with alcoholic hepatitis may The prognosis of alcoholic cirrhosis depends on whether
be asymptomatic or icteric and critically ill. Common symp- patients continue to consume alcohol and whether there are
toms include anorexia, nausea, vomiting, abdominal pain, and signs (jaundice, ascites, or gastrointestinal tract bleeding) of
weight loss. The most common sign is hepatomegaly, which chronic liver disease. For patients who do not have ascites,
may be accompanied by ascites, jaundice, fever, splenomegaly, jaundice, or variceal bleeding and who abstain from alcohol,
and encephalopathy. The level of AST is increased in 80% to the 5-year survival rate is 89%; for patients who have any of
90% of patients, but it is almost always less than 400 U/L. those complications and continue to consume alcohol, it is
The AST:ALT ratio is frequently greater than 2. Leukocytosis 34%. Liver transplant is an option for patients with end-stage
is commonly present, particularly in severely ill patients. alcoholic liver disease if they demonstrate that they can main-
Although the constellation of symptoms may mimic biliary tain abstinence from alcohol. The outcome of liver transplant
disease, the clinical features are characteristic in an alcoholic for alcoholic liver disease is similar to that of transplant for
patient. Because cholecystectomy carries a high morbidity other indications.
among patients with alcoholic hepatitis, the clinical distinc-
tion is important.
Only 60% of patients with alcoholic cirrhosis have signs or
symptoms of liver disease.
Alcoholic hepatitis is characterized by fatty change,
degeneration and necrosis of hepatocytes (with or without Liver enzyme levels may be relatively normal.
178 G A S T R O E N T E R O L O GY A N D H E PATO L O GY
The 5-year survival for patients with alcoholic cirrhosis sicca complex. Biochemical features include increased levels of
who abstain from alcohol is 89%. alkaline phosphatase and IgM. When PBC is advanced, the
concentration of bilirubin is high, the serum level of albumin
The 5-year survival for those who have signs and continue
is low, and PT is prolonged. Steatorrhea may occur because
to consume alcohol is 34%.
of progressive cholestasis. Fat-soluble vitamin deficiencies and
Liver transplant is an option for patients who can metabolic bone disease are common.
demonstrate a pattern of abstinence from alcohol. Antimitochondrial antibodies are present in 90% to 95%
of patients with PBC. The classic histologic lesion is granu-
lomatous infiltration of septal bile ducts. Ursodiol treatment
N O NA L C O H O L I C FAT T Y L I VE R D I S E A S E benefits patients who have this disease by improving survival
Nonalcoholic fatty liver disease (NAFLD) is a common cause and delaying the need for liver transplant. Cholestyramine
of abnormal levels of liver enzymes. A subset of NAFLD is and rifampin may be beneficial in the management of
nonalcoholic steatohepatitis (NASH), which is charac- pruritus.
terized histologically by fatty change and inflammation.
Characteristically, patients with NAFLD have at least 1 of PBC primarily affects middle-aged women.
the following risk factors: obesity, hyperlipidemia, and diabe- Common early symptoms: pruritus and fatigue.
tes. The aminotransferase levels are mildly abnormal, and the
alkaline phosphatase level is increased in about one-third of Alkaline phosphatase and IgM levels increase.
patients. When advanced cirrhosis develops, fat may not be Fat-soluble vitamin deficiencies and metabolic bone disease
recognizable in liver tissue, and NASH most likely accounts are common.
for some cases of cryptogenic cirrhosis. The pathogenesis of
NAFLD is unknown, and the effect of weight loss and con- Antimitochrondrial antibodies are present in 90%95% of
trol of hyperlipidemia and hyperglycemia is variable. In 10% patients.
of patients, NAFLD progresses to cirrhosis. The risk factors Classic histologic lesion: granulomatous infiltration of
for more advanced disease are advanced age, marked obesity, septal bile ducts.
and diabetes mellitus. Other than to control risk factors, there
is no approved therapy for NAFLD. In patients with fat in the Treatment: ursodiol.
liver, it is important to rule out other diseases that result in
steatosis, including hepatitis C, celiac disease, Wilson disease,
and alcoholic liver disease.
Primary Sclerosing Cholangitis
Aggressive treatment of obesity, hyperlipidemia, and diabe-
tes is indicated in patients with NAFLD. The weight loss that Primary sclerosing cholangitis (PSC) is a chronic chole-
occurs after bariatric surgery improves the histologic features static liver disease characterized by obliterative inflamma-
of NAFLD. Vitamin E has been shown to improve liver test tory fibrosis of extrahepatic and intrahepatic bile ducts.
results and histologic features in patients with NAFLD. Use An immune mechanism has been implicated. Patients
of agents such as pioglitazone and rosiglitazone has resulted may have an asymptomatic increase in the alkaline phos-
in biochemical and histologic improvement but also in weight phatase level or progressive fatigue, pruritus, and jaundice.
gain. For treatment of hyperlipidemia, the statin drugs are Bacterial cholangitis may occur in patients with dominant
safe in patients with NAFLD. For patients with NAFLD who strictures or in whom instrumentation has been performed.
are given potentially hepatotoxic medications, liver enzymes Cholangiography, with either endoscopic retrograde cholan-
should be monitored regularly and use of the medications can giopancreatography (ERCP) or magnetic resonance cholan-
continue as long as liver enzyme levels are less than 5-fold the giopancreatography (MRCP), establishes the diagnosis of
reference value and liver function is preserved. PSC, showing short strictures of bile ducts with intervening
segments of normal or slightly dilated ducts. This cholang-
There is no approved therapy for NAFLD other than risk iographic appearance may be mimicked by human immuno-
factor control. deficiency virus (HIV)-associated cholangiopathy (due to
cytomegalovirus or Cryptosporidium), ischemic cholangiop-
athy after intra-arterial infusion of fluorodeoxyuridine, and
C H RO N I C C H O L E S TAT I C L I VE R D I S E A S E S IgG4-associated cholangitis.
Primary Biliary Cirrhosis
PSC: obliterative inflammatory fibrosis of extrahepatic and
Primary biliary cirrhosis (PBC) is a chronic, progressive, chole-
intrahepatic bile ducts.
static liver disease that primarily affects middle-aged women.
Its cause is unknown but appears to involve an immunologic Asymptomatic increase in the alkaline phosphatase level.
disturbance resulting in small bile duct destruction. In many
Cholangiography establishes the diagnosis.
patients, the disease is identified by an asymptomatic increase
in alkaline phosphatase. Common early symptoms are pruri- HIV-associated cholangiopathy mimics the
tus and fatigue. Patients may have Hashimoto thyroiditis or cholangiographic appearance of PSC.
13. L I VE R A N D B I L I A RY T R AC T 179
Seventy percent of patients with PSC have ulcerative coli- the patients with hemochromatosis, 80% to 90% are homozy-
tis (UC), which may antedate, accompany, or even follow gous for C282Y. Heterozygotes for C282Y generally do not
the diagnosis of PSC. Treatment of UC has no effect on the have the disease. Patients who are C282Y heterozygote and
development or clinical course of PSC. Patients with PSC are H63D heterozygote (compound heterozygosity) may have
at higher risk of cholangiocarcinoma; its development may be iron overload.
manifested by rapid clinical deterioration, jaundice, weight Liver biopsy in patients with abnormal iron tests is done
loss, and abdominal pain. There is no effective medical ther- only if patients are negative for C282Y or if there is a con-
apy for PSC. Treatment of PSC is generally supportive, and cern about cirrhosis. The knowledge of cirrhosis is important
many patients have progressive liver disease and require liver because of the increased risk of hepatocellular carcinoma.
transplant. Endoscopic balloon dilatation of bile duct stric- Generally, hepatic iron levels in hemochromatosis are greater
tures may offer palliation, especially in patients with recurrent than 10,000 g/g dry weight. A diagnostic algorithm is shown
cholangitis. in Figure 13.7.
UC occurs in 70% of patients with PSC. Iron overload is more common in men.
Treatment of UC has no effect on the development or Clinical features: arthropathy, hepatomegaly, skin
clinical course of PSC. pigmentation, diabetes mellitus, cardiac dysfunction, and
hypogonadism.
Patients with PSC are at higher risk of
cholangiocarcinoma. Iron saturation and serum levels of ferritin are high.
Standard tests for making the diagnosis: genetic testing
H E R E D I TA RY L I VE R D I S E A S E S and liver biopsy with quantification of hepatic iron
concentration.
Genetic Hemochromatosis
Genetic hemochromatosis is an autosomal recessively trans- Patients with hemochromatosis should be treated with
mitted disorder characterized by iron overload. The physi- phlebotomy if the ferritin level is high. Those with C282Y
ologic defect appears to be an inappropriately high absorption homozygosity and a normal ferritin level can be observed every
of iron from the gastrointestinal tract. The HFE gene for 2 to 3 years without treatment. The standard for phlebotomy
genetic hemochromatosis has been identified. In the general is to remove 500 mL weekly to achieve a ferritin level less than
population, the heterozygote frequency is 10%. Only homozy- 50 g/L or iron saturation less than 50%. A maintenance pro-
gotes manifest progressive iron accumulation. gram of 4 to 8 phlebotomies annually is then required. When
initiated in the precirrhotic stage, removal of iron can render
Genetic hemochromatosis is a disorder of iron metabolism. the liver normal and may improve cardiac function and con-
trol of diabetes. Treatment does not reverse arthropathy or
Transmission is autosomal recessive. hypogonadism, nor does it eliminate the increased risk (30%)
Only homozygotes have progressive iron accumulation. of hepatocellular carcinoma if cirrhosis has already developed.
All first-degree relatives of patients should be evaluated for
Patients often present with end-stage disease, although an hemochromatosis.
increased sensitivity to screening is aiding in earlier diagnosis.
The peak incidence of clinical presentation is between the ages Hemochromatosis is treated with repeated phlebotomies.
of 40 and 60 years. Iron overload is manifested more often and Treatment does not reverse arthropathy or hypogonadism
earlier in men than in women because women are protected or eliminate the increased risk of hepatocellular
by the iron losses of menstruation and pregnancy. Although carcinoma.
hemochromatosis is now usually diagnosed from screening
iron test results, clinical features include arthropathy, hepato- First-degree relatives should be tested for
megaly, skin pigmentation, diabetes mellitus, cardiac dys- hemochromatosis.
function, and hypogonadism. Hemochromatosis should be
considered in patients presenting with symptoms or diseases
Wilson Disease
such as arthritis, diabetes, cardiac arrhythmias, or sexual dys-
function. Routine liver biochemistry studies generally show Wilson disease is an autosomal recessive disorder character-
few abnormalities, and complications of portal hypertension ized by increased amounts of copper in tissues. The basic
are unusual. Transferrin saturation greater than 50% is the defect involves an inability of the liver to prepare copper
earliest biochemical iron abnormality in hemochromatosis. for biliary excretion. The liver is chiefly involved in children
High serum levels of ferritin indicate tissue iron overload in and adolescents, whereas neuropsychiatric manifestations
patients with hemochromatosis. Increased levels of iron and are more prominent in older patients. The Kayser-Fleischer
ferritin may occur in other liver diseases, particularly advanced ring is a brownish pigmented ring at the periphery of the
cirrhosis of any cause. Testing for mutations in the HFE gene cornea. It is not invariably present and is seen more com-
is the standard method for diagnosing hemochromatosis. Of monly in patients with neurologic manifestations. Hepatic
180 G A S T R O E N T E R O L O GY A N D H E PATO L O GY
Fasting, morning transferrin
No Stop
saturation >50%?
Yes
Yes
No
Yes
Yes No
Yes No
Phlebotomy Follow
Figure 13.7 Diagnostic Algorithm for Genetic Hemochromatosis. Causes of secondary iron overload include anemias with ineffective erythropoiesis,
multiple blood transfusions, and oral or parenteral iron supplementation. AST indicates aspartate aminotransferase. (Adapted from Brandhagen DJ,
Fairbanks VF, Batts KP, Thibodeau SN. Update on hereditary hemochromatosis and the HFE gene. Mayo Clin Proc. 1999 Sep;74[9]:91721. Used
with permission of Mayo Foundation for Medical Education and Research.)
forms of Wilson disease include acute liver failure (often basis of a low level of ceruloplasmin and an increased urinary or
accompanied by hemolysis and renal failure), chronic hepa- hepatic concentration of copper. Ceruloplasmin levels may be
titis, steatohepatitis, and insidiously developing cirrho- misleadingthey may be increased by inflammation or biliary
sis. The development of hepatocellular carcinoma is rare. obstruction and decreased by liver failure of any cause. High
Neurologic signs include tremor, rigidity, altered speech, concentrations of copper in the liver are found in Wilson dis-
and changes in personality. Fanconi syndrome and prema- ease, although similarly high values can also occur in cholestatic
ture arthritis may occur. syndromes. Genetic testing for Wilson disease is developing but
is currently most reliable for screening among first-degree rela-
Wilson disease: an autosomal recessive disorder tives when a specific mutation in the proband has been identi-
characterized by increased amounts of copper in tissues. fied. Standard treatments for Wilson disease are penicillamine,
which chelates and increases the urinary excretion of copper,
Kayser-Fleischer ring is a brownish pigmented ring at the and trientine. Zinc inhibits absorption of copper by the gastro-
periphery of the cornea. intestinal tract and can be used as adjunctive therapy. All sib-
Hepatocellular carcinoma is rare. lings of patients should be evaluated for Wilson disease. Liver
transplant corrects the metabolic defect of the disease.
Neurologic signs: tremor, rigidity, altered speech, and
changes in personality.
Diagnosis: low ceruloplasmin level and increased urinary
Evidence of hemolysis (total bilirubin increased out of pro- or hepatic concentration of copper.
portion to direct bilirubin), a low or normal level of alkaline
Treatment: penicillamine or trientine; zinc.
phosphatase, and a low serum level of uric acid (due to uricosu-
ria) suggest Wilson disease. The diagnosis is established on the Liver transplant corrects the metabolic defect.
13. L I VE R A N D B I L I A RY T R AC T 181
D1-Antitrypsin Deficiency acute liver failure due to other causes. Poor prognostic mark-
ers include a drug-induced cause (other than acetaminophen),
D1-Antitrypsin is synthesized in the liver. The gene is on chro- older age, grade 3 or 4 encephalopathy, acidosis, and INR
mosome 14. M is the common normal allele, and Z and S are greater than 3.5. Treatment is supportive, and patients should
abnormal alleles. Patients with the ZZ phenotype are at high- be transferred to a medical center where liver transplant is
est risk of liver disease. Inability to excrete the abnormally available.
folded mutant protein results in intrahepatic accumulation
of D1-antitrypsin. Patients with D1-antitrypsin deficiency may Acute liver failure is hepatic failure with encephalopathy
have a history of jaundice during the first 6 months of life. In developing <8 weeks after the onset of jaundice in patients
later childhood or adulthood, cirrhosis may develop. Patients with no history of liver disease.
with D1-antitrypsininduced liver disease often lack clinically
important lung disease, and infusions of D1-antitrypsin do not Poor prognostic markers include a drug-induced cause
protect against hepatic involvement. The prevalence of cirrho- (other than acetaminophen), older age, grade 3 or 4
sis in patients with the MZ phenotype is likely increased, but encephalopathy, and INR >3.5.
the risk is small. Hepatocellular carcinoma may complicate
D1-antitrypsin deficiency when cirrhosis is present, especially
in males. D1-Antitrypsin deficiency is diagnosed by determin-
D RU G -I N D U C E D L I V E R I N J U RY
ing the D1-antitrypsin phenotype or genotype. The serum levels
of D1-antitrypsin may vary and be unreliable. Liver transplant Drugs cause toxic effects in the liver in different ways,
corrects the metabolic defect and changes the recipients phe- often mimicking liver disease from other causes. With the
notype to that of the donor. notable exception of acetaminophen hepatotoxicity, most
drug-induced liver disorders are idiosyncratic and not
Intrahepatic accumulation of D1-antitrypsin causes liver dose-related. Drug-induced liver injury accounts for 2% of
disease. the cases of jaundice in hospitalized patients and 50% of the
cases of acute liver failure. Consequently, all drugs that have
The diagnosis is made by determining the D1-antitrypsin
been used by a patient presenting with liver disease must be
phenotype or genotype.
identified.
Hepatocellular carcinoma can complicate D1-antitrypsin Acetaminophen toxicity is the most common cause of
deficiency, especially in males. acute liver failure. Toxicity may occur at relatively low doses
(eg, 3 g daily) in alcoholics because alcohol induces hepatic
Liver transplant corrects the metabolic defect.
microsomal cytochrome P450 enzymes, which metabolize
acetaminophen to its toxic metabolite. Acetaminophen hepa-
AC U T E L I VE R FA I LU R E totoxicity is characterized by aminotransferase values greater
than 5,000 U/L and often by renal failure. N-acetylcysteine
Acute liver failure is hepatic failure that includes encephalopa-
should be given to any patient with acute liver failure in whom
thy developing less than 8 weeks after the onset of jaundice in
acetaminophen toxicity is suspected.
patients with no history of liver disease. The common causes
Valproic acid, tetracycline, and zidovudine may cause
are listed in Box 13.1. Acute liver failure due to acetaminophen
severe microvesicular steatosis associated with enceph-
hepatotoxicity or hepatitis A carries a better prognosis than
alopathy. Hepatotoxicity due to amiodarone may have
histologic features that mimic those of alcoholic hepati-
tis or NAFLD. Antituberculous agents, including isoni-
Box 13.1 COMMON CAUSES OF ACUTE LIVER FAILURE
azid, rifampin, and ethambutol, may cause acute hepatitis.
Antibiotics are frequently associated with acute hepatitis.
Infective
Amoxicillin-clavulanate is a relatively common cause of
Hepatitis virus A, B, C (rare), D, and E
drug-induced liver injury and may result in prolonged
Herpesvirus
cholestasis that can mimic large bile duct obstruction.
Drug reactions and toxins
Nitrofurantoin and minocycline can mimic autoimmune
Acetaminophen hepatotoxicity
hepatitis. The chance of hepatotoxicity from lipid-lowering
Idiosyncratic drug reaction
agents is extremely remote, even in patients with preexisting
Vascular
liver disease.
Ischemic hepatitis (shock liver)
Acute Budd-Chiari syndrome
Most drug-induced liver disorders are idiosyncratic, not
Metabolic
dose-related.
Wilson disease
Fatty liver of pregnancy Drugs cause 2% of the cases of jaundice (in hospitalized
Miscellaneous patients) and 50% of the cases of acute liver failure.
Massive malignant infiltration
In alcoholics, acetaminophen toxicity may occur at lower
Autoimmune hepatitis
doses than in nonalcoholics.
182 G A S T R O E N T E R O L O GY A N D H E PATO L O GY
Antibiotics are a common cause of drug-induced liver discovered liver mass lesions, although they can present with
injury. acute right upper quadrant pain and hemodynamic compro-
mise because of bleeding. Avoidance of estrogens is advised for
Amiodarone may cause hepatotoxicity that histologically
patients with hepatic adenomas.
mimics alcoholic hepatitis or NAFLD.
Statins may cause mild liver test abnormalities but only
rarely cause significant liver injury. Cavernous Hemangioma
Cavernous hemangioma is the most common benign tumor of
L I VER T UMO R S the liver. CT or MRI with intravenous contrast is often diag-
nostic, demonstrating peripheral enhancement of the lesion.
Hepatocellular Carcinoma Cavernous hemangiomas generally require no treatment and
In the United States, 90% of hepatocellular carcinoma are not estrogen dependent.
(HCC) cases occur in patients with cirrhosis. The level
of D-fetoprotein is increased in only 50% of patients with Focal Nodular Hyperplasia
HCC; however, a level of D-fetoprotein greater than 400
ng/mL in a cirrhotic patient with a liver mass is essentially Focal nodular hyperplasia (FNH) is a benign liver lesion that
diagnostic of HCC. A lesion that enhances on the hepatic is probably a reaction to aberrant arterial flow to the liver.
arterial phase with washout on the portal venous phase on These lesions are typically discovered incidentally, although
computed tomography (CT) or magnetic resonance imaging large lesions that stretch the liver capsule may cause abdominal
(MRI) in a patient with cirrhosis is very suggestive of HCC, pain. Diagnosis can usually be made with imaging; the char-
and biopsy is often not necessary for diagnosis. Common acteristic findings are intense vascular enhancement on the
metastatic sites are lymph nodes, lung, bone, and brain. hepatic arterial phase and a central scar. Bleeding from FNH is
Liver transplant is an option for patients with 3 or fewer rare and malignant transformation does not occur; therefore,
lesions (largest <3 cm) or a single lesion smaller than 5 cm. resection is not necessary. Similar to cavernous hemangioma,
Transplant is advised particularly for patients with cirrhosis FNH is not estrogen dependent.
who may not tolerate resection because of poor liver reserve.
Transarterial chemoembolization, radioembolization, and
percutaneous ablative techniques, such as alcohol injection Metastases
or radiofrequency ablation, may be useful as primary or neo- Metastases are more common than primary tumors of the
adjuvant therapy. liver. Frequent primary sites are the colon, stomach, breast,
lung, and pancreas. Surgical resection of isolated colon cancer
The D-fetoprotein level is increased in d50% of patients metastases has a limited effect on long-term survival.
with HCC.
Usually, imaging is characteristic and biopsy is not C O M P L I C AT I O N S O F E N D -S TAG E L I VE R
necessary for diagnosis. DISEASE
Common metastatic sites: lymph nodes, lung, bone, and Most of the complications of cirrhosis are due to the develop-
brain. ment of portal hypertension. The mechanism of portal hyper-
Treatment options: liver transplant, hepatic resection, tension is related to increases in both portal vein blood flow
transarterial chemoembolization, radioembolization, and and intrahepatic resistance to flow. Increased flow is related
percutaneous ablation. to splanchnic vasodilatation. Increased resistance is related
to sinusoidal narrowing from fibrous tissue and regenerative
nodules as well as active vasoconstriction from alterations in
Cholangiocarcinoma
production of endothelin and nitric oxide.
The incidence of cholangiocarcinoma is increasing in the
United States. Recognized risk factors are PSC, chronic
Ascites
biliary infection, and a history of choledochal cysts.
Cholangiocarcinoma may be difficult to diagnose, especially The pathogenesis of ascites involves stimulation of the
in patients with PSC. For most patients, surgical resection is renin-angiotensin-aldosterone system, resulting in inappro-
the treatment of choice, although resection is not possible in priate renal sodium retention with expansion of plasma vol-
many patients. At some centers, liver transplant is considered ume. Pleural effusion (hepatic hydrothorax) occurs in 6% of
in select patients with cholangiocarcinoma. patients with cirrhosis and is right-sided in 67%. Edema usu-
ally follows ascites and is related to hypoalbuminemia and
Adenoma possibly to increased pressure on the inferior vena cava by
the intra-abdominal fluid. The sudden onset of ascites should
Adenomas are associated with the use of oral contraceptives or raise the possibility of hepatic venous outflow obstruction
estrogen. Patients most commonly present with incidentally (Budd-Chiari syndrome).
13. L I VE R A N D B I L I A RY T R AC T 183
Table 13.7 USE OF THE SERUM-ASCITES ALBUMIN Pleural effusion occurs in 6% of patients with cirrhosis and
GRADIENT (SAAG) AND ASCITES PROTEIN TO is right-sided in 67%.
DETERMINE THE CAUSE OF ASCITES
The sudden onset of ascites raises the possibility of hepatic
ASCITES PROTEIN venous outflow obstruction (Budd-Chiari syndrome).
SAAG, g/dL <2.5 g/dL ASCITES PROTEIN t 2.5 g/dL
A SAAG t1.1 g/dL almost always indicates portal
1.1 Portal hypertension Portal hypertension due to hypertension.
due to cirrhosis hepatic venous outflow Patients with cirrhotic ascites generally have a low
obstruction (including right
heart failure) concentration of urinary sodium.
<1.1 Nephrotic syndrome Malignancy, tuberculosis The mainstay of treatment is sodium restriction and
diuretics; large-volume paracentesis is safe and well
tolerated.
Paracentesis is indicated at presentation to confirm the
cause of ascites. Tests most useful for determining the cause of
ascites are measurements of total protein and the serum-ascites Spontaneous Bacterial Peritonitis
albumin gradient (SAAG), which is calculated as
Spontaneous bacterial peritonitis (SBP) occurs in 10% to 20%
of patients with cirrhosis who have ascites. SBP is a bacterial
SAAG = [serum albumin] [ascitic fluid albumin]. infection of ascitic fluid without an intra-abdominal source
of infection. Fever, abdominal pain, and abdominal tender-
A SAAG of 1.1 g/dL or more indicates portal hyperten- ness are classic symptoms; however, many patients have few or
sion. Ascites due to portal hypertension induced by congestive no symptoms. SBP should be considered in any patient with
heart failure can be distinguished from cirrhotic ascites because cirrhotic ascites, particularly if there has been clinical deterio-
congestive heart failure (and other conditions associated with ration. For all patients presenting with ascites, diagnostic para-
hepatic venous outflow obstruction such as Budd-Chiari syn- centesis is advisable as an initial step. Unless severe (INR >2.5
drome) usually has an ascitic fluid protein level of 2.5 g/dL or or platelets <10u109/mL), coagulopathy and thrombocytope-
more. Ascites from peritoneal carcinomatosis or tuberculosis nia are not contraindications for diagnostic paracentesis. A
generally has an ascitic fluid protein level of 2.5 g/dL or more cell count and culture of ascitic fluid should be performed for
and a SAAG of less than 1.1 g/dL (Table 13.7). all patients in whom SBP is being considered. Bedside inocu-
The treatment of ascites involves dietary sodium restric- lation of blood culture bottles with ascitic fluid increases the
tion and diuretics. Spironolactone (100200 mg daily) and diagnostic yield of fluid cultures. SBP is more common in
furosemide (2040 mg daily) are usually used initially. The patients with large-volume ascites and in patients with a low
goal is to increase the concentration of urinary sodium and ascitic fluid protein concentration (<1.0 g/dL). Also, blood
to allow the loss of 1 L of ascitic fluid (1 kg of body weight) from all patients with SBP should be cultured because almost
per day. Paracentesis should be performed therapeutically in 50% of these cultures are positive. Variants of SBP are listed
patients with tense ascites or with respiratory compromise in Table 13.8.
from abdominal distention. Large-volume or even total para-
centesis in combination with 6 to 8 g of albumin for each liter
Table 13.8 VARIANTS OF SPONTANEOUS BACTERIAL
of ascitic fluid removed is safe and well tolerated. Refractory
PERITONITIS
ascites is uncommon. Patients with cirrhotic ascites have
a low concentration of urinary sodium (<10 mEq/mL on a ASCITIC FLUID
random specimen) despite maximal diuretic therapy. Those
Polymorpho- Culture
who do not adhere to dietary sodium restriction excrete more CONDITION nuclear cells/mL Results MANAGEMENT
than 80 mEq in 24 hours. For patients with refractory or
resistant ascites, most physicians advocate therapeutic para- Spontaneous >250 Positive Antibiotics
centesis as needed. A transjugular intrahepatic portosystemic bacterial
shunt (TIPS) is effective in some patients with refractory peritonitis
ascites and is particularly useful for cirrhotic patients with
Culture-negative >250 Negative Antibiotics
pleural effusion as the main manifestation of fluid retention. neutrocytic
Peritoneovenous shunts are complicated by disseminated ascites
intravascular coagulation and shunt malfunction and are
Bacterascites <250 Positive Treat if symptoms
rarely performed. of infection are
present; oth-
The pathogenesis of ascites involves stimulation of erwise, repeat
the renin-angiotensin-aldosterone system, resulting in paracentesis
inappropriate renal sodium retention with expansion of for cell count
and cultures
plasma volume.
184 G A S T R O E N T E R O L O GY A N D H E PATO L O GY
SBP and culture-negative neutrocytic ascites should patients with low blood pressure. After liver transplant, renal
be treated, usually with a third-generation cephalosporin. function usually improves, although this is confounded by
Albumin should also be given (1.5 g/kg on day 1 and 1 g/kg on the renal toxicity of the antirejection drugs tacrolimus and
day 3). Polymicrobial infection of ascitic fluid should prompt cyclosporine.
a search for an intra-abdominal focus of infection; SBP nearly
always involves only 1 organism. Patients with a prior episode Hepatorenal syndrome: renal failure with normal tubular
of SBP are at high risk of recurrence, and daily prophylactic function in a patient with portal hypertension.
therapy (usually with norfloxacin) is recommended.
It is difficult to differentiate from prerenal azotemia.
SBP occurs in 10%20% of patients with cirrhosis who After liver transplant, renal function usually improves.
have ascites.
Classic symptoms: fever, abdominal pain, and abdominal
tenderness. Portal Systemic Encephalopathy
Many patients have few or no symptoms. Portal systemic encephalopathy is a reversible decrease in the
Bedside inoculation of blood culture bottles with ascitic level of consciousness of patients with severe liver disease.
fluid increases the diagnostic yield. Disturbed consciousness, personality change, intellectual
deterioration, and slowed speech are common manifesta-
SBP is more common in patients with large-volume tions. Patients often have asterixis (flapping tremor). The
ascites and in patients with a low ascitic fluid protein sudden development of portal systemic encephalopathy in
concentration (<1.0 g/dL). patients with stable cirrhosis should prompt a search for
Secondary prophylaxis is advised for patients with a bleeding, infection (especially SBP), or electrolyte distur-
previous episode of SBP. bances; however, simple precipitating events are increased
dietary protein, constipation, or sedatives. Serum and arte-
rial levels of ammonia are usually increased but are not nec-
essary for diagnosis. Lactulose decreases the nitrogenous
Hepatorenal Syndrome compounds presented to the liver and is the first-line treat-
Hepatorenal syndrome is renal failure in the absence of under- ment for hepatic encephalopathy. Oral nonabsorbable anti-
lying renal pathologic abnormalities in patients with portal biotics such as rifaximin or neomycin are given to patients
hypertension. The differential diagnosis is given in Table who do not respond to or tolerate lactulose. Dietary protein
13.9. In cirrhotic patients presenting with renal insufficiency, restriction is advised only for patients with no response to
hepatorenal syndrome is difficult to differentiate from pre- medical therapy.
renal azotemia; thus, a brief trial of volume expansion with
albumin is indicated. Treatment is supportive, although vaso- Portal systemic encephalopathy: reversible decrease in the
constrictors such as midodrine or norepinephrine are used in level of consciousness of patients with severe liver disease.
Patients often have asterixis.
Table 13.9 DIFFERENTIAL DIAGNOSIS FOR If portal systemic encephalopathy develops suddenly, look
HEPATORENAL SYNDROME for bleeding, infection, or electrolyte disturbances.
PRERENAL HEPATORENAL ACUTE RENAL Treatment: lactulose or nonabsorbable antibiotics.
VARIABLE AZOTEMIA SYNDROME FAILURE
13. L I VE R A N D B I L I A RY T R AC T 185
EGD
Medium or
No varices Small varices
large varices
Child A Child B or C Child A with no red Child B or C or red Child A Child B or C or red
marks on varices marks on varices marks on varices
Repeat EGD in 3 y Repeat EGD in 1 y Repeat EGD in 2 y Nonselective Nonselective -Blockers or
-blockers -blockers variceal ligation
Figure 13.8 Prophylaxis of Esophageal Variceal Bleeding in Patients With Cirrhosis. Child indicates Child-Pugh class (A, B, or C, in order of
increasing severity of cirrhosis); EGD, esophagogastroduodenoscopy.
Bleeding from esophageal varices is generally massive. For Recurrent bleeding occurs in 80%100% of patients.
patients with acute bleeding, early endoscopy is indicated for
Patients with refractory bleeding are candidates for TIPS.
diagnosis and treatment. Endoscopic therapy consists of band
ligation or, less commonly, sclerotherapy. Octreotide decreases The incidence of portal systemic encephalopathy after
portal venous pressure and may also be given for acute variceal TIPS is 10%40%.
bleeding. All patients with cirrhosis who are hospitalized for
gastrointestinal tract bleeding should receive prophylactic
antibiotics. B I L I A RY T R AC T D I S E A S E
186 G A S T R O E N T E R O L O GY A N D H E PATO L O GY
without gallbladder stones have undergone cholecystectomy Malignant Biliary Obstruction
because of a decrease in gallbladder ejection fraction noted on
radionuclide biliary scan. Most of these patients do not have Malignant biliary obstruction is usually the result of carci-
resolution of pain, and therefore a decreased gallbladder ejec- noma of the head of the pancreas, bile duct cancer, or meta-
tion fraction should be interpreted with caution since often static malignancy to hilar nodes. If the disease is unresectable,
the patients symptoms are unrelated to the finding. palliative endoscopic stenting is as effective as surgical bypass.
Patients with malignant biliary obstruction and impending
duodenal obstruction are usually considered for palliative
Ultrasonography is 90%97% sensitive for detecting surgery, although endoscopic techniques can be attempted by
gallstones. expert endoscopists.
Radionuclide biliary scanning helps diagnose cystic duct
obstruction with cholecystitis. Gallbladder Carcinoma
Asymptomatic patients with gallstones require Gallbladder carcinoma has a strong association with calcified
no therapy. gallbladder wall (porcelain gallbladder); therefore, prophylac-
tic cholecystectomy is advised. Most patients with gallblad-
der carcinoma present at an advanced stage and have a poor
Bile Duct Stones prognosis.
Most bile duct stones originate in the gallbladder, although
a few patients, such as those with preexisting biliary dis- S U M M A RY
ease (eg, PSC), have primary duct stones. CT and ultra-
sonography are relatively insensitive for common bile duct Aminotransferases are markers of liver cell injury or
stones, and diagnosis generally requires MRCP, ERCP, or hepatocellular disease.
endoscopic ultrasonography. ERCP also offers therapeutic
potential for patients with bile duct stones and is the test Hyperbilirubinemia is usually <20% conjugated
of choice when clinical suspicion is high. Patients with bile bilirubin in diseases characterized by overproduction
duct stones can have minimal or no symptoms, or they can of bilirubin. Hyperbilirubinemia is usually >50%
have life-threatening cholangitis with abdominal pain, fever, conjugated bilirubin with hepatocyte dysfunction or
and jaundice. Common bile duct stones should be removed; impaired bile flow.
in nearly all patients, this can be accomplished with ERCP.
HAV is transmitted by ingestion of contaminated food
The urgency of the procedure depends on the clinical pre-
or water or contact with an infected person. HBV is
sentation. Patients with minimal symptoms can have elective
transmitted by exposure to blood or contaminated body
ERCP, but those with cholangitis and fever unresponsive to
fluids. HCV is a parenterally transmitted virus and a
antibiotics should have urgent endoscopic treatment. Patients
common cause of chronic hepatitis.
with gallbladder stones who have a sphincterotomy and clear-
ance of their duct stones have only a 10% chance of having Autoimmune hepatitis is a chronic condition, but patients
additional problems with their gallbladder stones; thus, may present with acute hepatitis. Drug-related hepatitis,
cholecystectomy can be avoided in patients who are at high HBV, HCV, and Wilson disease should be excluded before
risk of complications with surgery. making a diagnosis of autoimmune hepatitis.
Genetic hemochromatosis is a disorder of iron metabolism.
Most bile duct stones originate in the gallbladder.
Transmission is autosomal recessive.
Diagnosis of bile duct stones generally requires MRCP,
Wilson disease: an autosomal recessive disorder
ERCP, or endoscopic ultrasonography.
characterized by increased amounts of copper in tissues.
Common bile duct stones should be removed.
Diagnosis of bile duct stones generally requires MRCP,
Urgent endoscopic treatment is needed if cholangitis and ERCP, or endoscopic ultrasonography. Common bile duct
fever are unresponsive to antibiotics. stones should be removed.
13. L I VE R A N D B I L I A RY T R AC T 187
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PA RT I I I
P U L M O N A RY D I S E A S E S
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14.
CRITICAL CARE MEDICINE
J. Christopher Farmer, MD
191
Box 14.1 PREDICTORS OF DIFFICULT MASK Recognition of impending respiratory failure is not always
VENTILATION AND INTUBATION straightforward.
Successful management is predicated on assessment of risk
Difficult mask ventilation factors and proper preparation and planning.
Age >55 y
BMI >26 A backup method to direct laryngoscopy should be readily
Edentulous available.
Male Use muscle relaxants with extreme caution.
Mallampati class IV
Beard
History of snoring
Difficult intubation R E S P I R ATO RY FA I LU R E
Short thick neck Effective functioning of the respiratory system requires 1)
Limited neck flexion or extension normal central nervous system control, 2) intact neuromus-
Thyromental distance <3 finger breadths cular transmission and bellows function, and 3) normal gas
Long upper incisors exchange at the alveolar-capillary level. Respiratory failure
Presence of overbite may result from physiologic impairment or disease at any of
Inability to jut mandibular incisors anterior to upper incisors these levels. Respiratory failure is typically classified as hypox-
Inability to open mouth >3 cm emic or hypercapnic. Board examination questions typically
Mallampati class III or IV focus on the following:
High arched palate
Abbreviation: BMI, body mass index (calculated as weight in kilograms divided 1. Ability to recognize impending respiratory failure:
by height in meters squared). oxygenation, ventilation, and the work of breathing are no
longer sustainable without mechanical intervention
medicine certification examination. However, the risk of 2. Ability to discern the type of respiratory failure
using a depolarizing muscle relaxant (eg, succinylcholine) in hypoxemic or hypercapnicand the specific type of
some patients can be substantial, and these risks should be support that is medically indicated.
known:
3. Ability to calculate values for common physiologic
perturbations that indicate the presence of respiratory
1. Risk of causing a precipitous, life-threatening
failure, such as the alveolar-arterial (A-a) gradient
hyperkalemia in patients with significant burn injuries,
spinal cord injuries, demyelination syndromes, crush
The determination of impending respiratory failure is based
injuries, and renal failure
on clinical findings (arterial blood gas findings may be normal
2. Risk of inducing a mechanical circumstance leading to an initially). Thus, it is important to assess the patients breath-
inability to intubate or ventilate (refractory upper airway ing work (ie, effort), the presence or absence of worsening
obstruction) tachycardia and tachypnea, the presence or absence of altered
Figure 14.1 Mallampati Classification. The Mallampati classification is based on the structures visualized with maximal mouth opening and tongue
protrusion in the sitting position. (This test was originally described without phonation, but some have suggested that Mallampati Classification with
or without phonation correlates with intubation difficulty: higher Mallampati scores are more likely to indicate greater intubation difficulty.)
192 P U L M O N A RY D I S E A S E S
Box 14.2 ELEMENTS AND EQUIPMENT REQUIRED FOR The A-a gradient = Pao2 Pao2, where Pao2 indicates
SUCCESSFUL ENDOTRACHEAL INTUBATION partial pressure of oxygen in the alveoli. Normally, the A-a
gradient is less than 10 torr in a young adult; it increases by 10
Adequate personnel
torr every decade thereafter.
Proper patient positioning
Pulmonary shunt is defined as alveoli that are perfused but
Oxygen (100%)
not ventilated. The absence of ventilation is caused by alveolar
Well-fitting bag valve mask
collapse (eg, atelectasis, loss of surfactant) or alveolar flood-
Suctioning equipment
ing (eg, alveolar capillary leak). Clinically, pulmonary shunt
Nasal & oral airways
occurs when Pao2 does not appropriately increase even with
Working laryngoscope
increased supplemental oxygen administration, as is common
Various types & sizes of laryngoscope blades
in patients with acute respiratory distress syndrome (ARDS)
Endotracheal tubes with intact cuffs
as discussed below.
Tube stylet
Treatment of hypoxemic respiratory failure requires
Syringe (10 mL)
correction of hypoxia. For patients who have pulmonary
Head rest
shunting, this likely means the use of either invasive or nonin-
Working intravenous line
vasive mechanical ventilation (discussed in the Mechanical
Induction drugs
Ventilation section). In addition to the use of mechani-
Vasoconstrictor drugs
cal ventilation, recognition and treatment of underlying
End-tidal carbon dioxide detector
causes, such as pneumonia and heart failure, is extremely
Method to secure tube
important.
14 . C R I T I C A L C A R E M E D I C I N E 193
Acute Respiratory Distress Syndrome management. Recently, in prospective controlled trials, a strat-
egy of mechanical ventilation with reduced tidal volumes was
Board examination questions related to ARDS typically focus associated with improved survival (discussed below).
on 1) diagnosis of ARDS, 2) causes of ARDS, and 3) gen-
eral principles of therapy. Board examinations must focus on Pathophysiology
settled science, and there are many treatment areas related to The pathophysiology of ARDS is related to damage of
ARDS that are still in flux and are therefore difficult to test. alveolar-capillary units. Early changes include endothelial cell
swelling and capillary leak, followed by interstitial edema and
Description parenchymal inflammation. Mononuclear inflammation, loss of
ARDS is diffuse lung injury that causes acute hypoxic alveolar type I cells, and hyaline membrane formation typically
respiratory failure. Acute lung injury (ALI) is a frequent pri- develop within 2 or 3 days after an initial insult (eg, sepsis).
mary cause of critical illness and may occur as a complication Fibrosis may subsequently develop within days to weeks
or as a coexisting feature of multisystem disease. ARDS is after the initial insult that caused ARDS. Damage to type
commonly defined as diffuse ALI with the following major II alveolar cells leads to the loss of surfactant production.
features: Ultimately, alveolar filling and. alveolar collapse develop, and
.
intrapulmonary shunting and V/Q mismatch with hypoxemia
1. Diffuse (bilateral) pulmonary infiltratesinfiltration in 3 are clinically apparent.
or 4 quadrants on the chest radiograph
2. Abnormal ratio of Pao2 to Fio2 (P/F ratio)in ALI Treatment
<300, and in ARDS <200 Respiratory support for ARDS can be summarized as
follows: Excessive mechanical ventilation amplitude varia-
3. Normal volume statuspulmonary artery occlusion tion is bad. After an initial insult, lung injury is exacerbated
pressure <18 mm Hg, and lack of evidence of left by high-pressure distention of alveoli and alveolar cycling
atrial hypertension or volume overload (eg, on (repeated opening and closing of alveolar sacs, leading to shear
echocardiogram) injury, also known as alveolar recruitment and derecruitment).
Both processes (overdistention and alveolar cycling) further
Several conditions are associated with ARDS (Table 14.1). increase the proinflammatory cascade response in the lungs,
Mortality from ARDS has averaged about 50%. For the which worsens the endothelial capillary leak and loss of sur-
first 30 years after ARDS was described, no single therapy was factant and increases the rate of fibrosis. Treatment involves
shown to alter the outcome, although gradual improvement mechanical ventilation strategies (ie, lung-protective ventila-
in overall mortality was attributed to multidisciplinary ICU tory strategies) that allow for lung healing. This concept is
graphically depicted for an ARDS patient in Figure 14.2.
In 2000, a multicenter group of investigators affiliated
Table 14.1 CONDITIONS ASSOCIATED WITH ACUTE with the ARDS Network showed improved survivorship
RESPIRATORY DISTRESS SYNDROME (ARDS) a among patients receiving a tidal volume of 6 mL/kg (based on
ideal body weight) compared with a control group receiving a
DISORDER tidal volume of 12 mL/kg (based on ideal body weight). The
OR TYPE OF smaller tidal volumes were used to maintain plateau airway
DISORDER CAUSE
194 P U L M O N A RY D I S E A S E S
pressures below 30 cm water. This is the only specific therapy is cycled to exhalation by either volume (ie, tidal volume deliv-
for ARDS that has been shown to decrease mortality. ery) or pressure (ie, pressure control).
In patients treated with a lung-protective ventilatory strat- Internal medicine board examination questions related to
egy, the resulting level of alveolar ventilation may increase mechanical ventilation are basic and do not involve complex
Paco2 (referred to as permissive hypercapnia) but does not management decisions. As already mentioned, these examina-
appear to be harmful and may even decrease the degree of tions must focus on settled science, and there is much about
ventilator-induced lung injury. In other words, in patients who mechanical ventilation that reflects individual and institu-
have ARDS or increased pulmonary dead space, the pressure tional preferences (eg, the use of synchronized intermittent
cost required to achieve a normal Pco2 often exceeds any mandatory ventilation [SIMV] or controlled mechanical ven-
benefit and may actually exacerbate ALI. tilation [CMV]). Therefore, typical question content areas
Finally, many clinicians use an open-lung ventilatory strat- might include the following:
egy, in which incremental positive end-expiratory pressure
(PEEP) levels are used to maintain alveolar recruitment and 1. Recognition of complications caused by mechanical
to prevent alveolar cycling and derecruitment. . . ventilation (eg, barotrauma or pneumothorax,
Patients with ARDS progress beyond simple V/Q mismatch auto-PEEP)
to pulmonary shunt. The clinical hallmark is that increasing
the Fio2 as a single maneuver does not improve oxygenation. 2. A plan for the next step (eg, if a patient with specified
PEEP is required to recruit alveoli; the goal is to improve oxy- blood gas results is mechanically ventilated, what should
genation. A common board examination question asks what be done next?)
should be done next for a patient who has ARDS and inade- 3. Selection of noninvasive or invasive mechanical
quate oxygenation (Fio2 >0.40.5). PEEP is the first choice. In ventilation approaches for patients with specific
addition, patients with ARDS may have some alveoli (and lung conditions (eg, COPD, pneumonia, or ARDS)
segments) that are slow to open or recruit (the physiologic term
is prolonged alveolar time constant). Besides providing PEEP for 4. Recognition of complications of mechanical ventilation
these patients, lengthening the duration of inspiration may be (eg, barotrauma, high pressure ventilator alarm)
beneficial to allow for additional time for alveolar recruitment. 5. Indications for weaning a patient from mechanical
How to improve alveolar recruitment is also a common ARDS ventilation
subject area for board examination questions.
Because increased capillary permeability allows for larger Mechanical ventilation is necessary for many patients who
volumes of intravascular fluid, a conservative fluid strategy have loss of respiratory control, neuromuscular or respiratory
to maintain adequate systemic perfusion is preferred and was pump failure, and severe disorders of gas exchange that do
recently validated in a large study. Supplemental nutrition not respond to lesser levels of support. Patients who require
(enteral feeding) is recommended throughout the course of mechanical ventilation usually meet the criteria for ventilator
critical illness if tolerated (both acute and chronic). Patient support listed in Table 14.2.
mobilization with ambulation and ventilator weaning are also
initiated as early as possible for all patients with ARDS.
The role of corticosteroids in patients with ARDS remains Table 14.2 TYPICAL PHYSIOLOGIC CRITERIA FOR
controversial. Nitric oxide and other vasodilating agents in
MECHANICAL VENTILATOR SUPPORT
ARDS provide short-term improvement in oxygenation but
no mortality benefit. Prone positioning has been used in an VARIABLE VALUE
attempt
. . to open flooded dependent alveoli and improve
V/Q matching and oxygenation; it has resulted in nonsustain- Respiratory rate, breaths/min >2530
able improvements in oxygenation with no effect on mortality Minute ventilation, L/min >1015
and an increase in dislodgment and obstruction of endotra-
cheal tubes. Maximal inspiratory pressure <20
(force), cm water
ARDS is defined as a P/F ratio <200 with bilateral Vital capacity, mL/kg <10
pulmonary infiltrates and a normal volume status.
Pao2, mm Hg <60 when Fio2 >0.60
A lowtidal volume strategy is the only ARDS treatment
that has improved survival. Pao2/Fio2 <200
M EC H A N I C A L VE N T I L AT I O N Vd/Vt >0.60
The goals of mechanical ventilation are 1) correct hypoxia, 2) pH <7.20 (with a predominant respira-
tory component)
support ventilation, 3) decrease the work of breathing, and 4)
support lung injury healing. All modern forms of mechanical Abbreviations: Fio2, fraction of inspired oxygen; Pao2Pao2, alveolar-arterial gra-
ventilation use positive pressure during inspiration. Inspiration dient in partial pressure of oxygen; Vd, dead space volume; Vt, tidal volume.
14 . C R I T I C A L C A R E M E D I C I N E 195
Modes of Mechanical Ventilation due to VAP can be decreased by prevention with use of a
VAP bundle, as recommended by the Institute for Healthcare
Modes of mechanical ventilation refers to how a positive-pressure Improvement (IHI). The IHI Ventilator Bundle includes the
machine breath is delivered and its relation to the spontaneous following:
breaths of the patient (eg, assist/control mode, intermittent
mandatory ventilation [IMV], and pressure support ventila-
1. Elevation of the head of the bed
tion). Table 14.3 outlines basic ventilator modes and basic ini-
tial invasive mechanical ventilation settings for a patient with 2. Daily sedation vacations and assessment of readiness to
respiratory failure. extubate
3. Peptic ulcer disease prophylaxis
Volume Preset Assist/Control Mode Ventilation
In this mode, a machine-assisted breath is delivered for every 4. Deep vein thrombosis prophylaxis
inspiratory effort by the patient. If no spontaneous breaths occur
5. Daily oral care with chlorhexidine
during a preset time interval, a controlled breath of predetermined
volume is delivered by the ventilator. The backup rate determines
the minimum minute ventilation the patient will receive. Implementing the IHI Ventilator Bundle can prevent VAP.
The advantage of assist/control mode ventilation is that it
allows maximal rest for the patient and maximal control of ven-
tilation. The disadvantage is that hyperventilation or air trapping Intrinsic PEEP
(or both) can occur in patients making rapid inspiratory efforts. Intrinsic PEEP, or auto-PEEP, is an important complica-
tion of positive pressure ventilation. Inadequate time during
Pressure Support Ventilation the expiratory phase of the respiratory cycle results in a new
Pressure support ventilation may be used to assist sponta- machine breath being delivered before the previous breath is
neously breathing patients, with or without IMV breaths. For completely exhaled. This may worsen hyperinflation, increase
each inspiratory effort by the patient, the ventilator delivers a intrathoracic pressure, reduce venous return, and worsen asso-
high rate of flow of inspired gas, up to a preset pressure limit. ciated complications (eg, barotrauma). Intrinsic PEEP may
This pressure support occurs only during the spontaneous occur in spontaneously breathing patients with obstructive
inspiratory effort, so that the rate and pattern of respiration are airway disease, but the effect is most important in mechani-
determined by the patient. cally ventilated patients. Treatment typically involves optimiz-
ing bronchodilator therapy and altering the ventilator cycle to
Volume Preset IMV allow maximal expiratory time.
Volume preset IMV allows a preset number of
machine-assisted breaths of a given tidal volume. Between Auto-PEEP can be treated by allowing maximal expiratory
machine breaths, patients may breathe spontaneously. The time and by optimizing bronchodilator therapy.
IMV mode was developed as a weaning mode so that the num-
ber of mechanical breaths could be decreased gradually, allow-
Oxygen Toxicity
ing for increasing spontaneous ventilation. However, recent
Pulmonary oxygen toxicity appears to be the result of
trials have shown that this mode of weaning is inferior to
direct exposure to high tensions of inspired oxygen or alveo-
weaning with T-piece trials or pressure support ventilation.
lar oxygen. For adults, oxygen toxicity is not believed to be of
clinical concern if the Fio2 is less than 0.40 to 0.50. Higher
Positive End-Expiratory Pressure levels of inspired oxygen may be associated with acute tracheo-
PEEP is intended to increase functional residual capac- bronchitis (most likely an irritant effect). After several days
ity, recruit partially. collapsed
. alveoli, improve lung compli- of exposure, a syndrome of diffuse alveolar damage and lung
ance, and improve V/Q matching. It decreases atelectrauma injury may develop with pathologic features resembling those
(recruitment and derecruitment of alveoli). An adverse effect of ARDS.
of PEEP is an excessive increase in intrathoracic pressure
with decreased cardiac output. Overdistention of lung units Oxygen toxicity is of concern with Fio2 levels greater than
may also worsen gas exchange because of ventilator-induced 0.50.
lung injury. At levels of PEEP greater than 10 to 15 cm water,
barotrauma is of concern. The optimal PEEP may be defined
as the lowest level of PEEP needed to achieve satisfactory oxy- Tracheostomy
gen delivery at a nontoxic Fio2 (<0.60). Prolonged invasive mechanical ventilation increases the
risk of tracheal injury and stenosis, bleeding, tracheoesopha-
Complications of Mechanical Ventilation geal fistula, and, possibly, increased bronchial or pulmonary
infections. For patients who require prolonged mechanical
Ventilator-Associated Pneumonia ventilation or airway support, the timing of tracheostomy is
Ventilator-associated pneumonia (VAP) is a serious pre- controversial. ARDS patients who receive a tracheostomy
ventable complication of mechanical ventilation. Mortality early in their clinical course have demonstrably improved
196 P U L M O N A RY D I S E A S E S
Table 14.3 BASIC VENTILATOR MODES AND SETTINGS
A/C, also Active inhalation Vt is delivered up to a volume threshold & not a pressure threshold
called CMV Exhalation is passive; after the Vt is delivered, the machine releases & exhalation is driven by chest wall & lung elastance
(recoil)
Patient initiates the respiratory cycle (unless apneic or paralyzed)
Machine senses inspiratory effort & then delivers machine-defined Vt for every breath
Does not allow patient to breathe spontaneously (ie, patient-defined Vt)
Machine rate (eg, CMV = 8/min) defines the minimum number of Vt breaths a patient will receive per minute
A patient who initiates more breaths per minute than the defined rate will receive those breaths at the machine-defined Vt
SIMV Active inhalation Vt is delivered up to a volume threshold & not a pressure threshold
Exhalation is passive; after the Vt is delivered, the machine releases & exhalation is driven by chest wall & lung elastance
(recoil)
Patient initiates the respiratory cycle (unless apneic or paralyzed)
Machine senses inspiratory effort & then delivers machine-defined Vt for only the rate of machine breaths
Machine rate (eg, SIMV =8/min) defines the actual number of Vt breaths a patient will receive per minute
A patient who initiates more breaths per minute than the defined rate will receive those breaths at the patient-defined Vt (ie, the
Vt of the spontaneous breaths can be different from the Vt of the machine breaths)
Pressure Control Modes
CPAP This is a spontaneous breathing mode (ie, Vt & rate are not provided by the mechanical ventilator)
Continous positive pressure is delivered while a patient breathes spontaneously
This pressure is continuous, meaning that both inspiratory & expiratory phases of respiration are supplemented with positive
pressure
CPAP may be delivered invasively (ie, through an endotracheal tube) or noninvasively (ie, with a tight-fitting mask or with high
gas flow nasal prongs)
PSV PSV augments spontaneous breaths with a machine-defined amount of positive pressure that is delivered only during
inspiration
The purpose of PSV mode is to improve patient-machine synchrony (comfort) & to decrease the patient work of breathing; in
some patients this may facilitate weaning from mechanical ventilation
PSV inspiratory positive flow continues while the patient inhales & then stops when the patients flow decreases to less than a
threshold value (usually <25% of the initial inspiratory flow rate)
Patients determine their spontaneous Vt during PSV breaths by controlling their flow rate. When they have had enough, they
simply stop inspiring
Initial Invasive Mechanical Ventilation Settings
Tidal volume Standard: 810 mL/kg ideal body weight (less is preferred)
ARDS: 6 mL/kg ideal body weight
Abbreviations: A/C, assist/control; ARDS, acute respiratory distress syndrome; CMV, controlled mechanical ventilation; CPAP, continuous positive airway pressure;
Fio2, fraction of inspired oxygen; PCV, pressure control ventilation; PEEP, positive end-expiratory pressure; PSV, pressure support ventilation; SIMV, synchronized inter-
mittent mandatory ventilation; Ti, inspiratory time; Vm, minute ventilation; Vt, tidal volume.
14 . C R I T I C A L C A R E M E D I C I N E 197
mortality. Tracheostomy has the advantages of decreased chapter topics in which critical care and cardiology substan-
laryngeal injury, increased patient comfort, ease of suction- tially overlap and are commonly included as board examina-
ing, and, in certain patients, allowance for oral ingestion and tion questions.
speech. Tracheostomy is commonly considered for patients
who have needed or are expected to need intubation and
SHOCK
mechanical ventilation for more than 2 to 4 weeks.
Shock is defined as the inadequate provision of oxygen and
Tracheostomy is considered for patients requiring metabolic substrate to the tissues. Vital signs are typically not
mechanical ventilation for >24 weeks. part of the definition; thus, hypotension is not necessary to
establish a diagnosis of shock. Many patients present to criti-
cal care units with undifferentiated shock (ie, the cause may
Weaning (Liberation From Mechanical Ventilation)
not be readily apparent). Initial assessment is aimed at deter-
Patients are candidates for weaning from mechanical ventilation mining the cause of shock. The following classification system
when they are hemodynamically stable, underlying pathophysi- is widely used (Table 14.4): 1) hypovolemic (hemorrhagic),
ologic processes (both pulmonary and nonpulmonary) are 2) distributive, 3) cardiogenic, and 4) obstructive.
resolving, and they have adequately recovered from respira-
tory failure. It is important to identify these patients in order Given systemic vascular resistance, cardiac output, and
to decrease costs, ICU lengths of stay, and infectious and other central venous pressure, be able to differentiate between
complications of mechanical ventilation. The most effective and different types of shock.
consistent way to wean patients is to use a protocol that involves
a nurse or respiratory therapist. What seems to be most impor- When patients present to an ICU or emergency depart-
tant is a daily spontaneous breathing trial after the patient seems ment with undifferentiated shock and life-threatening hypo-
ready for weaning, preceded by a daily interruption of sedation. perfusion, time matters. Thus, instead of proceeding in a linear
This is typically done each morning with a T-piece system, or by fashion (history first, and then examination, laboratory and
using continuous positive airway pressure (CPAP) or pressure imaging studies, and finally treatment), diagnosis and treat-
support ventilation (PSV) mode for 30 minutes to 2 hours. A ment must occur simultaneously. This is because failure to
weaning protocol is presented in Figure 14.3. promptly restore perfusion status (within a few hours) results
in secondary tissue damage from proinflammatory mediators
Daily spontaneous breathing trials are helpful for patients (possibly leading to multiple organ failure). A typical sequence
who seem ready for weaning. of events (amplification) is depicted in Figure 14.4.
In 2001, a landmark article was published on rapid resus-
citation of patients who had shock caused by severe sepsis
(Figure 14.5). There has been ongoing controversy about the
C A R D I AC C R I T I C A L C A R E end points of resuscitation and specific therapies used in that
study. Nevertheless, the principles of the study are highly
Cardiac-specific topics are largely covered in the Cardiology relevant: early recognition and treatment of hypoperfusion
section of this book. Therefore, the present chapter focuses on can decrease the ensuing inflammatory response to shock.
Spontaneous respirations
Good cough
No pressors
No paralytics
No coronary ischemia
No Yes
Fio2 <0.50
Spo2 >90%
f/Vt 105
Mean arterial pressure >65 mm Hg
Heart rate <110 beats per minute
Continue mechanical
2-h T-piece trial
ventilation
198 P U L M O N A RY D I S E A S E S
Table 14.4 CLASSIFICATION OF SHOCK a
SYSTEMIC
PRELOAD (CENTRAL WEDGE VASCULAR CARDIAC
SHOCK TYPE VENOUS PRESSURE) PRESSURE RESISTANCE OUTPUT EXAMPLES OF CAUSES
Hypovolemic Bleeding
(hemorrhagic) Vomiting, diarrhea
Diuretic use (excess)
Diabetes mellitus
Burns, exudative skin lesions
Diabetes insipidus
Distributive Sepsis
Hyperthyroidism
Liver disease
Anaphylaxis
Thiamine deficiency
Spinal cord injury (neurogenic shock)
a
Arrows indicate increase (), decrease (), or no change ().
14 . C R I T I C A L C A R E M E D I C I N E 199
focus on the need to obtain additional hemodynamic moni- SEPSIS
toring data to sort out the type of shock and complications of
Description
these invasive procedures, or the examination provides hemo-
dynamic results and then asks a question about next steps. Sepsis is an exaggerated inflammatory response to a noxious
Peripheral veins are the preferred access sites in patients (infectious) stimulus and is characterized by a severe catabolic
who require intravenous therapy. Indications for central reaction, widespread endothelial dysfunction, and release of
venous access are lack of adequate peripheral veins, need for innate inflammatory response components. To achieve a common
hypertonic or phlebitic medications or solutions, need for terminology, systemic inflammatory response syndrome (SIRS)
long-term access, need for measuring central pressures, and was introduced for findings of fever or hypothermia, tachycar-
access for procedures (hemodialysis and cardiac pacing). The dia, hyperventilation, and leukocytosis or leukopenia regardless
most common locations for central access are the internal jug- of cause. Not all SIRS is infection mediated. Sepsis is defined as
ular, subclavian, and femoral veins. SIRS with a known or presumed source of infection, and severe
Relative contraindications include procedural inexperi- sepsis is defined as sepsis associated with organ system dysfunc-
ence of the practitioner, significant coagulopathy, inability tion and systemic effects, including hypotension, decreased urine
to identify landmarks, infection or burn at the entry site, and output, or metabolic acidosis. Septic shock refers to persistent signs
thrombosis of the proposed central venous site. At most insti- of organ hypoperfusion despite adequate fluid resuscitation.
tutions today, central venous catheters are inserted with the The mortality of patients with sepsis and multiorgan failure
help of direct ultrasonographic visualization. may be greater than 70% to 90%. Adverse risk factors include
Complications of central venous catheterization include age older than 65 years, continued systemic signs of sepsis, per-
bloodstream infections, cardiac arrhythmias, pneumothorax, sistent deficit in oxygen delivery, and preexisting renal or liver
air embolism, vascular injury, catheter or guidewire embolism, failure. Physiologic scoring systems (eg, Acute Physiology and
catheter knotting, bleeding, and other potential complica- Chronic Health Evaluation [APACHE]) may predict out-
tions of needle or catheter misplacement. come more accurately for subgroups of patients.
The IHI has identified prevention of catheter-related
bloodstream infections (CR-BSIs) with use of the IHI Central
Complications
Line Bundle as a key element in improving patient outcomes
and preventing morbidity. The key components of the Central Multisystem organ failure, or multiple-organ dysfunction syn-
Line Bundle are 1) hand hygiene; 2) maximal barrier precau- drome (MODS), is usually defined as acute dysfunction of 2
tions upon insertion; 3) chlorhexidine skin antisepsis; 4) or more organ systems lasting more than 2 days. Sepsis is the
optimal catheter site selection, with avoidance of the femoral most common cause. Corticosteroids have no known benefit
vein for central venous access in adult patients; and 5) daily and may cause adverse effects in patients with sepsis syndrome.
review of line necessity, with prompt removal of unnecessary The exception is patients who have a documented adrenal
lines. CR-BSIs are usually attributed to the migration of bac- insufficiency and severe sepsis; they may benefit from low
teria from the skin along the catheter tract. CR-BSI is usually doses of hydrocortisone or methylprednisolone.
defined as more than 15 colony-forming units per milliliter on
semiquantitative culture of the catheter tip. Catheter-related
Treatment
bacteremia is defined as bacterial growth and blood cultures
that are positive for the same organism as on the catheter The Surviving Sepsis Campaign is a group of organizations
tip. Risk factors include infected catheter site or cutaneous and professional societies that have created guidelines for the
breakdown, multiple manipulations, the number of catheter treatment of sepsis. These have been modified and updated at
lumens, and the duration of use of the same site (particularly intervals. The use of activated protein C is no longer recom-
after 3 or 4 days). Treatment of CR-BSIs should include cath- mended. Primary therapies are described below.
eter removal and replacement at another site if necessary.
Antibiotics
The Central Line Bundle is important in preventing Use of antibiotics includes the following steps:
CR-BSIs.
1. Collect samples for blood cultures before antibiotics are
Treatment of CR-BSIs includes prompt catheter removal. given
2. Obtain other cultures and imaging studies as indicated
INFECTIOUS DISE ASES AND CRITICAL 3. Administer appropriate antibiotics within 1 hour of ICU
ILLNESS admission (within 3 hours of emergency department
admission)
Critical caredirected board examination questions typically
4. Select specific antibiotics after 72 hours as appropriate and
focus on sepsis recognition and management, appropriate
continue their use for 10 days
antibiotic selection for serious or life-threatening infections
(see the Infectious Diseases section of this book), and infec- 5. Control the source of the infection, and drain it if
tion control (eg, Central Line Bundle, VAP prevention). indicated
200 P U L M O N A RY D I S E A S E S
Resuscitation Intensive Care EvaluationSurvival Using Glucose Algorithm
Prompt resuscitation and correction of systemic hypo- Regulation (NICE-SUGAR) trial.
perfusion is critical (within 6 hours of initial presentation to
the hospital). The most common error during resuscitation of Intensive glucose management is associated with
medical patients with sepsis is inadequate administration of frequent hypoglycemia, and more lenient goals should
intravenous fluids during the first few hours after ICU admis- be targeted.
sion. Use of blood products and inotropic support should also
be considered as indicated. The early goal-directed therapy
protocol (Figure 14.5) is not strictly endorsed as an absolute
approach in this chapter because of lingering controversies (as G A S T R O E N T E R O L O GY A N D C R I T I C A L
mentioned above). ILLNESS
1. Presence of coagulopathy
G LU C O S E M A NAG E M E N T
2. Presence of shock
Two large randomized studies of intensive insulin therapy in
surgical and medical ICUs in Belgium showed mortality ben- 3. Presence of hypothermia
efit, but they raised questions of both internal and external
4. Use of medications that exacerbate GI bleeding or inhibit
validity and sparked debate in this area. It is generally agreed
clotting
that allowing blood glucose levels to increase to 200 mg/dL or
more is unacceptable. Conversely, maintaining strict normo- 5. Active alcohol ingestion
glycemia (110 mg/dL) is associated with frequent episodes
6. Active non-GI comorbidities that worsen the outcome
of hypoglycemia and may increase mortality. A blood glucose
maintenance target of 140 to 180 mg/dL is currently encour- 7. Prior history of GI hemorrhage that required ICU
aged, most recently in the multicenter Normoglycemia in admission
14 . C R I T I C A L C A R E M E D I C I N E 201
Table 14.5 Classification of Blood Loss
CLASS
FEATURE I II III IV
Pulse, beats per minute 100 100120 >120 (thready) >120140 (very thready)
8. Presence of severe liver disease coronary ischemia and its use should be carefully considered
before administration.
9. Recent GI surgery that can be associated with GI
The treatment of acute lower GI hemorrhage is largely
bleeding
supportive. Resuscitate the patient, administer blood, cor-
10. Prior history of conditions such as peptic disease, polyps, rect coagulopathy, and involve other providers with the
and diverticular disease care plan early on (eg, gastroenterology department, surgery
department). Identifying the source of bleeding can be dif-
ficult because active bleeding can be intermittent and elusive.
Many patients presenting to an ICU with lower GI hemor-
Management rhage have had a previous episode. The role of emergent
The following are management priorities: colonoscopy, especially in an unprepped patient, is not clearly
defined. Various studies have reported widely disparate diag-
1. Administer necessary fluid and blood resuscitation nostic yields with this test when performed under these cir-
cumstances. Other diagnostic adjuncts, such as arteriography
2. Correct coagulopathy or nuclear medicine scans, may be needed to more precisely
3. Reverse adverse medications if possible (eg, identify the source of bleeding.
anticoagulants)
Identify and treat shock in patients with GI hemorrhage.
4. Notify the gastroenterology department about the patient
and the possible need for emergent endoscopy Notify and involve gastroenterology specialists early.
202 P U L M O N A RY D I S E A S E S
4. Intracranial pressure monitoring and therapies when and left ventricles results in stiff walls and impaired relax-
obtundation and evidence of intracranial pressure ation). These derangements result in reduced stroke volume
elevation are present that is only partly compensated for by increases in heart rate
and contractility. The Starling curve is thus shifted down and
5. Maintenance of the perfusion status of other vital organs,
to the right, and cardiac output continues to decrease with
such as the kidneys
progressive elevation of IAP. These derangements are exac-
erbated by the frequent coexistence of hypovolemia or a sys-
Seek reversible causes of fulminant hepatic failure and treat temic inflammatory condition, resulting in vasodilatation.
supportively. Hence, diuresis is not appropriate since it would further
reduce venous return and cardiac output. Decompression of
the abdominal cavity results in nearly immediate reversal of
A B D O M I NA L C O M PA RT M E N T SY N D RO M E respiratory failure.
Primary abdominal compartment syndrome (ACS) is asso-
ACS is defined as IAP >20 mm Hg.
ciated with abdominopelvic injury or disease that frequently
requires early surgical or interventional radiologic interven- Elevated intra-abdominal pressure causes both respiratory
tion. Secondary ACS does not originate from the abdomi- dysfunction and cardiac dysfunction.
nopelvic region. Risk factors for ACS are severe penetrating
and blunt abdominal trauma, ruptured abdominal aortic Decompression of the abdominal cavity is the
aneurysm, retroperitoneal hemorrhage, pneumoperitoneum, treatment.
neoplasm, pancreatitis, massive ascites, liver transplant,
abdominal wall burn eschar, abdominal surgery, high-volume
fluid resuscitation (>3,500 mL in 24 hours), ileus, and pul- H E M ATO L O G I C D I S O R D E R S A N D
monary, renal, or liver dysfunction. CRITICAL ILLNESS
Normal intra-abdominal pressure (IAP) (ie, the pressure
within the abdominal cavity) is approximately 5 to 7 mm Hg Critical carefocused internal medicine board examination ques-
in critically ill adults. Intra-abdominal hypertension is defined tions in this content domain typically focus on the following:
by a sustained or repeated elevation of IAP (12 mm Hg) and
is graded as follows: 1. Most common causes of bleeding in ICU patients
2. Primary hematologic syndromes in the ICU with
Grade I: IAP 1215 mm Hg. associated bleeding
Grade II: IAP 1620 mm Hg. 3. ICU treatment of these disorders
Grade III: IAP 2125 mm Hg.
Grade IV: IAP >25 mm Hg. I CU-R E L AT E D B L E E D I N G D I S O R D E R S
14 . C R I T I C A L C A R E M E D I C I N E 203
Similarly, coagulopathy develops in many ICU patients. S U M M A RY
Most commonly, prothrombin time is prolonged. In general
the causes are the same causes of coagulopathy in other care Major causes of hypercapnic respiratory failure include
environments. inadequate alveolar ventilation, increased pulmonary dead
space, and failure of the respiratory bellows.
1. Clinically significant bleeding develops Important concepts in sepsis include identification of the
source of infection, early administration of antibiotics, and
2. An invasive procedure, which may cause bleeding, is needed fluid resuscitation.
Identify and treat shock in patients with GI
Drug-induced thrombocytopenia is very common in ICU hemorrhage. Notify and involve gastroenterology
patients; heparin is 1 of the most important causes. specialists early.
204 P U L M O N A RY D I S E A S E S
15.
INTER STITIAL LUNG DISEASES
Fabien Maldonado, MD, and Timothy R. Aksamit, MD
Understand the diagnostic approach to interstitial lung 1. ILDs of known cause (eg, drug-induced lung
diseases. disease, connective tissue diseaserelated ILD
Identify key features and differentiating characteristics of [CTD-ILD])
interstitial lung diseases. 2. Idiopathic interstitial pneumonias (Box 15.2)
3. Granulomatous ILDs (eg, sarcoidosis, hypersensitivity
pneumonitis [HP])
O VE RVI EW
4. Other ILDs (usually readily recognizable owing to
characteristic findings)
Interstitial lung diseases (ILDs), better described as diffuse
parenchymal lung diseases, encompass a group of heteroge-
neous lung conditions characterized by various etiologies, The strategy for diagnosing ILD should follow a stepwise
clinical and radiologic manifestations, clinical courses, and approach, including comprehensive history and thorough
responses to treatment. In this chapter, we use the American physical examination, pulmonary function tests (PFTs),
Board of Internal Medicine designation ILDs. Although more radiologic studies (usually including high-resolution com-
than 100 distinct entities have been described, the vast major- puted tomography [HRCT]), and, if needed, bronchoscopic
ity are rare enough to be considered clinical oddities. Prompt or surgical (or both) lung biopsy (Figure 15.1). It is important
recognition of ILD and initiation of appropriate therapy can to realize that for the majority of patients all tests are not nec-
result in significant improvement of otherwise potentially essary and the diagnosis may be achieved without histologic
life-threatening respiratory conditions. confirmation.
Some ILDs are characterized by suggestive or even
pathognomonic findings, but the majority are best diagnosed
D I AG N O S I S
through a dynamic interaction between clinicians, radiolo-
gists, and pathologists. ILDs are thought to affect 1 in 3,000
to 1 in 4,000 persons in the general population and represent H I S TO RY
approximately 15% of all consultations for the general pul-
A detailed history is the most important step in the diagno-
monologist. Although there is no widely accepted definition
sis of ILD (Table 15.1). Environmental (eg, pets, organic or
for ILDs, they share the common feature of diffuse involve-
mineral dust) or occupational exposures should be compre-
ment of the lung parenchyma and may affect the pulmonary
hensively investigated.
interstitium. By convention, infections, pulmonary edema,
lung malignancies, and emphysema are excluded, but they
The use of amiodarone, methotrexate, nitrofurantoin,
should be carefully considered as part of the differential diag-
chemotherapy, or radiotherapy should suggest iatrogenic
nosis (Box 15.1).
lung disease.
Most ILDs need an integrated approach between Insulation work or ship building should suggest
clinicians, radiologists, and pathologists for accurate asbestos-related disease; mining or sandblasting may be
diagnosis. associated with silicosis.
205
Box 15.1 CAUSES OF INTERSTITIAL LUNG DISEASE Box 15.2 IDIOPATHIC INTERSTITIAL LUNG DISEASE
Collagen vascular
Dermatomyositis Idiopathic pulmonary fibrosisusual interstitial pneumonia
Rheumatoid arthritis (IPF-UIP)
Scleroderma Nonspecific interstitial pneumonia (NSIP)
Systemic lupus erythematosus Sarcoidosis
Drug-induced Bronchiolitis obliterans with organizing pneumonia/crypto-
Chemotherapy genic organizing pneumonia (BOOP/COP)
Drug therapy Eosinophilic lung diseases
Radiotherapy Lymphocytic interstitial pneumonia (LIP)
Genetic Alveolar microlithiasis
Hermansky-Pudlak syndrome Lymphangioleiomyomatosis (LAM)
Metabolic storage disease Langerhans cell histiocytosis/eosinophilic granulomatosis
Neurofibromatosis Pulmonary alveolar proteinosis
Tuberous sclerosis Acute respiratory distress syndrome/acute lung injury
Idiopathic Others
Infectious
Chronic mycobacterial
diffusing capacity of lung for carbon monoxide (Dlco) is also
Chronic mycoses
reduced. When Dlco is reduced out of proportion to the
Malignant
rest of the PFTs, concurrent pulmonary hypertension or com-
Bronchoalveolar cell carcinoma
bined emphysema may be present. Some patients with ILD
Lymphangitic metastases
may present with mixed obstructive-restrictive disease, such as
Lymphoma
sarcoidosis, PLCH, lymphangioleiomyomatosis (LAM), HP,
Occupational or inhalational
and chronic eosinophilic pneumonia.
Asbestosis
Coal workers pneumoconiosis
Hypersensitivity I M AG I N G S T U D I E S
Silicosis Although chest radiography (CXR) has been largely sup-
Toxic gas planted by HRCT, several characteristic findings are worth
Vasculitides mentioning:
Churg-Strauss syndrome
Giant cell arteritis 1. Alveolar opacities suggest potentially reversible diseases
Wegener granulomatosis (caused by inflammation, edema, or alveolar hemorrhage)
as opposed to reticular findings (more likely associated
with irreversible fibrosis).
Idiopathic pulmonary fibrosis (IPF), desquamative
interstitial pneumonia, and pulmonary Langerhans cell Suspected interstitial lung disease
histiocytosis (PLCH) are more common in smokers;
sarcoidosis and HP are more common in nonsmokers.
Complete history, physical examination, CXR, PFTs, blood tests
(Should include previous CXRs & drug, radiation, occupational/exposure history)
P H Y S I C A L E X A M I NAT I O N +
Rales (dry or Velcro crackles) suggest fibrosis, but they are
Stop & treat HRCT
nonspecific. Clubbing of the digits can be associated with IPF (eg, EAA: eliminate exposure +
and asbestosis but is rare otherwise. Clubbing should raise & treat with corticosteroids)
concerns for alternative diagnoses (eg, lung or pleural malig-
Stop & treat Consider BAL/TBBx
nancies, chronic suppurative lung diseases, right-to-left shunt, +
liver disease, inflammatory bowel diseases). Careful attention
should be paid to extrapulmonary manifestations of systemic Stop & treat VATS-OLBx
diseases such as musculoskeletal pain, sicca syndrome, esopha-
geal dysmotility, and Raynaud phenomenon.
Diagnosis & treatment
Clubbing is rare in ILD aside from IPF and asbestosis.
Figure 15.1 Strategy for Diagnosing Interstitial Lung Disease. BAL
indicates bronchoalveolar lavage; CXR, chest radiography; EAA,
P U L MO NA RY F U N C T I O N S T U D I E S extrinsic allergic alveolitis; HRCT, high-resolution computed
tomography; OLBx, open lung biopsy; PFT, pulmonary function test;
The typical pattern is that of restriction, as evidenced by TBBx, transbronchial biopsy; VATS, video-assisted thoracoscopy; +,
decreased lung volumes and preservation of flows. The positive findings; , negative findings.
206 P U L M O N A RY D I S E A S E S
Table 15.1 INTERSTITIAL LUNG DISEASES ground-glass infiltrates) suggest reversible disease, while
DISTINGUISHED BY HISTORY reticular fibrotic infiltrates are less likely to resolve.
Honeycombing, traction bronchiectases, and basal predom-
EXPOSURE OR FEATURE DISEASE
inance are typical for usual interstitial pneumonia (UIP), a
pattern necessary for the diagnosis of IPF (see section on
Amiodarone, methotrexate, Drug-induced or iatrogenic lung
nitrofurantoin, chemotherapy, disease IPF below). Thin-walled cysts suggest PLCH (upper lobe
radiotherapy predominance) or LAM (diffuse lung involvement). A
crazy-paving pattern (ground-glass infiltrates with septal
Insulation work, ship building, Pneumoconioses
thickening) is seen in PAP.
mining, sandblasting
Micronodular infiltrates may be clustered around the bron-
Birds, indoor hot tubs, moldy Hypersensitivity pneumonitis chovascular bundles and subpleural areas (as in sarcoidosis and
humidifiers lymphangitic carcinomatosis) or randomly distributed (as in
Acute onset of disease Acute eosinophilic pneumonia or hematogenously spread diseases such as miliary tuberculosis).
organizing pneumonia Centrilobular infiltrates (sparing subpleural spaces and bron-
Virtually rules out IPF and chovascular bundles) may have a tree-and-bud pattern (fungal
asbestosis (which evolve over or mycobacterial infections) or they may not (HP and PLCH).
months to years)
Current smoker Desquamative interstitial Bilateral hilar lymphadenopathy is common in silicosis and
pneumonia, IPF, pulmonary sarcoidosis, but infections (fungal or mycobacterial) and
Langerhans cell histiocytosis lymphoma should be excluded.
Former smoker, never smoker Sarcoidosis, hypersensitivity Bat wing distribution on CXR and crazy-paving
pneumonitis
pattern on HRCT are typical of PAP.
Abbreviation: IPF, idiopathic pulmonary fibrosis. A photographic negative of pulmonary edema is seen in
chronic eosinophilic pneumonia.
2. Distribution of the infiltrates may provide guidance. Use Thin-walled cysts are seen in PLCH and LAM.
the mnemonic CHAPS to remember predominant upper
lung opacities:
a. Cystic fibrosis, chronic eosinophilic pneumonia L A B O R ATO RY S T U D I E S
b. HP, histiocytosis (PLCH) Laboratory studies are rarely helpful in the diagnosis of
ILD. Useful tests include a complete blood cell count with
c. Allergic bronchopulmonary aspergillosis, ankylosing a differential blood count and liver and renal function tests.
spondylitis Subsequently, hepatitis and human immunodeficiency virus
d. Pneumoconioses (HIV) serologies may be indicated. Other laboratory studies
can be considered depending on the clinical picture:
e. Sarcoidosis
3. Lower lung diseases include IPF, asbestosis, and aspiration. 1. Serologies for connective tissue disease are often obtained,
particularly in the case of organizing pneumonia (OP)
4. Bilateral hilar lymphadenopathy should suggest and nonspecific interstitial pneumonia (NSIP), the most
sarcoidosis, silicosis, or, rarely, berylliosis (however, fungal common patterns seen in CTD-ILD.
or mycobacterial infections and lymphoma should be
excluded). 2. Serum protein electrophoresis may be ordered if
amyloidosis is a consideration.
5. Alveolar infiltrates in a bat wing distribution are typical
of pulmonary alveolar proteinosis (PAP) (or cardiogenic 3. HP antibody testing is usually limited to a few common
pulmonary edema). offenders and is rarely helpful in practice.
6. Peripheral opacities (photographic negative of 4. The angiotensin-converting enzyme level, classically used
pulmonary edema) have been described in chronic to follow patients with sarcoidosis, is neither sensitive nor
eosinophilic pneumonia. specific.
7. Pneumothorax may be the clinical manifestation of 5. One notable exception is that of cytoplasmic
PLCH and LAM. antineutrophil cytoplasmic autoantibody (c-ANCA)
proteinase 3 antibodies, which are both sensitive and
specific for Wegener granulomatosis.
HRCT has revolutionized the diagnosis of ILD and
often obviates the need for histopathologic examina-
tion. Several characteristic features should narrow the dif- Laboratory studies are rarely helpful in ILD, except for the
ferential diagnosis. Alveolar opacities (consolidation or diagnosis of Wegener granulomatosis.
15. I N T E R S T I T I A L LU N G D I S E A S E S 207
H I S TO PAT H O L O G I C D I AG N O S I S I L D S O F K N OW N C AU S E
Bronchoscopic or surgical lung biopsy have limited roles.
It is important to realize that the histopathologic diagnosis C O N N E C T I V E T I S S U E D I S E A S E R E L AT E D
may only support a presumptive diagnosis without establish- I N T E R S T I T I A L LU N G D I S E A S E S
ing it.
Bronchoscopy is relatively simple and safe. The main risks Virtually all connective tissue diseases may affect the lungs.
are pneumothorax (up to 5%) and bleeding (up to 2%). It is CTD-ILDs are more common in females, with the exception
used primarily to exclude infection or malignancy; the biopsy of rheumatoid arthritis (RA), which is more common in men.
samples are too small to establish a confident diagnosis in The typical histopathologic patterns seen in CTD-ILD are
ILD. In selected cases, the findings can be diagnostic. For NSIP and OP. In fact, these histopathologic diagnoses should
instance, a profusion of nonnecrotizing granulomas should suggest the possibility of a connective tissue disease limited to
suggest sarcoidosis (as opposed to necrotizing granulomas the lungs in otherwise asymptomatic patients.
seen in fungal and mycobacterial infections and Wegener
granulomatosis). Treat the underlying cause. These ILDs tend to respond
Bronchoalveolar lavage (BAL) can be done safely in to treatment of the underlying inflammatory conditions
nearly all patients (including anticoagulated patients) with corticosteroids or other immunosuppressive agents as
and can exclude infection. On occasion, it may offer some indicated.
guidance:
R H EU M ATO I D A RT H R I T I S
1. A predominance of lymphocytes on the BAL is
Differences between RA-ILD and other CTD-ILDs include
consistent with sarcoidosis (with a classically inverted
the following:
CD4:CD8 ratio, typically >4) or HP (normal
CD4:CD8 ratio).
RA-ILD is more common in males.
2. Eosinophilic predominance is seen with acute and chronic
eosinophilic pneumonia. A UIP pattern is typically seen in RA-ILD, which is less
responsive to treatment.
3. Hemosiderin-laden macrophages are seen in diffuse
alveolar hemorrhage. RA is commonly associated with pleural effusions, pul-
4. Lipid-laden macrophages are seen in aspiration monary nodules, and fibrosis (RA-ILD) but may affect any
pneumonia and, less commonly, in lipoid part of the respiratory system. Arytenoid arthritis may cause
pneumonia. central airway obstruction, and in patients with RA, bron-
chiectases or constrictive bronchiolitis may develop. The pos-
5. A CD1a+ (a marker of Langerhans histiocytes) sibility of drug-induced lung disease (sarcoidosis-like reaction
cell count greater than 5% suggests PLCH as a with methotrexate; Goodpasture syndrome or constrictive
possibility. bronchiolitis with penicillamine) should be considered.
208 P U L M O N A RY D I S E A S E S
various malignancies, primarily in Hodgkin disease. The toxic-
ity is cumulative (and therefore subacute or chronic), resulting
in progressive fibrosis that may be indistinguishable from IPF.
Lung toxicity may be exacerbated by concurrent radiotherapy,
renal failure, and high fractions of inspired oxygen. Rarely, the
onset may be acute and associated with eosinophilia.
Methotrexate
Methotrexate may cause a hypersensitivity reaction that
occurs early in the treatment. The typical manifestation is
sarcoidosis-like, with bilateral hilar lymphadenopathy and dif-
fuse lung infiltrates. Eosinophilia is present in 50% of the cases.
Bronchoscopic lung biopsies may reveal ill-defined granulo-
mas, and the cell count and differential count on BAL are sim-
ilar to those in sarcoidosis with lymphocytic predominance.
Sometimes the CD4:CD8 ratio is increased. Opportunistic
Figure 15.2 Dermatomyositis. Mechanics hands are characterized by infections should be excluded.
roughening and fissures of the skin on the lateral and palmar areas of
the fingers. (Adapted from Khambatta S, Wittich CM. Amyopathic
dermatomyositis. Mayo Clin Proc. 2010 Nov;85[11]:e82. Used with Nitrofurantoin
permission of Mayo Foundation for Medical Education and Research.)
Nitrofurantoin is an antibiotic used to treat and prevent uri-
nary tract infections. It may cause potentially life-threatening
S C L E RO D E R M A
acute forms of lung toxicity (eosinophilic pneumonia) in 1 in
Scleroderma (systemic sclerosis) is associated with fibrosis 500 to 1 in 5,000 patients. A chronic form, similar in presenta-
(NSIP, OP, or less commonly UIP) and pulmonary hyper- tion to IPF, occurs in 1 in 50,000 patients. Discontinuing use
tension (in up to 25% of the patients), particularly in lim- of the drug is mandatory.
ited scleroderma or CREST syndrome. Scleroderma may
also cause recurrent aspiration due to esophageal dysmotility. Amiodarone
Lymphocytic interstitial pneumonia (thought to represent a
low-grade lymphoproliferative disorder) is a classic manifesta- Amiodarone, a drug commonly used in cardiovascular medi-
tion of Sjgren lung disease. cine, can cause lung toxicity, which is cumulative in the major-
ity of cases after exposure to amiodarone at a dosage of more
RA-ILD affects more men than women and tends to have a than 400 mg daily for 3 to 6 months. One particular radiologic
UIP pattern. characteristic of amiodarone lung toxicity is the presence of
high-attenuation infiltrates on non-contrast HRCT, owing to
Acute lupus pneumonitis has a poor prognosis. the high iodine content of amiodarone. Treatment consists of
Limited scleroderma is associated with pulmonary discontinuing use of the drug, but because of its long half-life
hypertension, while systemic sclerosis is associated with (23 months), clinical improvement may be delayed.
pulmonary fibrosis.
Illicit Substances
The use of illicit substances should be investigated. Opiate
D RU G - A N D T H E R A P Y-I N D U C E D LU N G products cause pulmonary edema, and crack cocaine causes
DISEASES various lung manifestations, including eosinophilic pneumo-
Various pharmacologic agents may cause drug-induced lung nia (crack lung), HP, bronchospasm, and diffuse alveolar
disease. Discontinuing use of the drug is mandatory and usu- hemorrhage.
ally results in prompt clinical improvement. The use of cor-
ticosteroids is often recommended, but the evidence for this
Chemotherapy and Radiotherapy
practice is anecdotal at best. The drugs discussed below should
be presumed to be responsible for lung disease until proven A history of chemotherapy or radiotherapy (or both) should sug-
otherwise. gest the possibility of iatrogenic lung disease. Radiation pneu-
monitis typically occurs within 6 to 12 weeks of treatment and is
usually limited to the field of radiation, but it may also affect other
Bleomycin Lung Toxicity areas (including the contralateral lung, owing to OP). Treatment
Bleomycin lung toxicity is the prototype of drug-induced with corticosteroids may help, but progression toward chronic
lung disease. This antibiotic chemotherapeutic agent is used in fibrosis may become evident months after treatment.
15. I N T E R S T I T I A L LU N G D I S E A S E S 209
Bleomycin toxicity is exacerbated by radiotherapy, uremia, 3. Silicosis may be an independent risk factor for lung
and high fractions of inspired oxygen. cancer, although to a much lesser extent than asbestos
exposure.
Methotrexate lung disease resembles sarcoidosis.
Lung infiltrates in females with recurrent urinary tract
Asbestos exposure may result in pleural effusions, rounded
infections should suggest nitrofurantoin lung toxicity.
atelectasis, fibrosis (asbestosis), mesothelioma, and
High-attenuation lung infiltrates suggest amiodarone lung bronchogenic carcinoma.
toxicity.
Silicosis resembles sarcoidosis radiologically.
Silicosis is associated with mycobacterial infections,
connective tissue diseases, and lung cancer.
P N EU M O C O N I O S E S
Asbestos-Related Lung Diseases
I D I O PAT H I C I N T E R S T I T I A L
Asbestos-related lung diseases should be suspected in patients PNEUMONIAS
with high-risk occupations (eg, insulation work, ship build-
ing, mining). Most pulmonary manifestations occur after a
prolonged dormant period of 20 to 40 years, except for benign I D I O PAT H I C P U L M O NA RY F I B RO S I S
asbestos-related pleural effusion, which may occur within 10 IPF is the most common idiopathic interstitial pneumo-
years of exposure. Calcified pleural (or pericardial) plaques are nia, and it affects males and females older than 50 years. The
a marker for asbestos exposure, but they do not generally cause pathophysiology remains elusive but is thought to be second-
symptoms. Other lung manifestations include the following: ary to poor wound healing of the lung characterized by exuber-
ant fibrosis without underlying inflammation. No treatment
Asbestosis: has been effective; corticosteroids should not be used. Lung
a. An ILD with similarities to IPF, but asbestosis carries transplant is an option for selected patients.
a better prognosis UIP is a histopathologic diagnosis necessary for the diag-
nosis of IPF, but it may be seen in other diseases (eg, asbes-
b. Treatment is supportive; corticosteroids are not tosis, drug-induced lung disease, HP, CTD-ILD). Either a
indicated radiologic diagnosis (HRCT) or a histopathologic diagnosis
Rounded atelectasis: of UIP is acceptable (ie, a surgical lung biopsy is not necessary
if HRCT demonstrates typical IPF with honeycombing, trac-
a. A focal subpleural opacity often confused with lung tion bronchiectases, and basal predominance). Biopsy may
cancer precipitate an acute exacerbation, a life-threatening complica-
Malignancy: tion of IPF. Other complications include pulmonary hyper-
tension and pneumothorax. The prognosis is poor; median
a. Mesothelioma: a primary pleural malignancy with survival is approximately 3 to 5 years. Other conditions asso-
poor prognosis and few therapeutic options ciated with UIP should be excluded, since they may be more
b. Bronchogenic carcinoma: although smoking is not responsive to treatment.
a risk factor for mesothelioma, it acts synergistically
with asbestos exposure and exponentially increases the Corticosteroids are not useful in IPF and should not be
risk of bronchogenic carcinoma used.
A surgical lung biopsy is not needed to diagnose UIP when
HRCT shows typical IPF; surgical lung biopsy may trigger
Silicosis an acute exacerbation.
Silicosis occurs in patients exposed to silica (eg, mining, quar-
rying, sandblasting). The disease is distinct from asbestosis,
and findings include bilateral hilar lymphadenopathy (occa- N O N S P E C I F I C I N T E R S T I T I A L P N EUM O N I A
sionally eggshell calcifications) with clustered micronodu-
lar infiltrates that typically favor the apices of the lungs (as NSIP is the main differential diagnosis for IPF. Patients with
opposed to asbestosis which, like IPF, typically predominates NSIP present at a younger age (<50 years) and females pre-
in the bases). There are 3 characteristic associations: dominate over males (2:1). The frequent presence of autoan-
tibodies suggests that NSIP may be, at least in some cases, an
1. Silicosis is a risk factor for tuberculosis, which should be autoimmune process. Radiologically, NSIP shows homoge-
excluded in patients whose respiratory condition worsens. neous involvement of the lungs, ground-glass opacities, and
limited honeycombing and traction bronchiectases. NSIP
2. An association with connective tissue diseases has been is also a histopathologic diagnosis that may occur in other
described (Caplan syndrome). diseases (eg, CTD-ILD, HP, infections). Treatment with
210 P U L M O N A RY D I S E A S E S
corticosteroids is usually effective, and the 5-year survival ACU T E EO S I N O P H I L I C P N EUMO N I A
(about 80%) is much better than with IPF.
Another rare type of idiopathic ARDS is acute eosinophilic
pneumonia (not to be confused with chronic eosinophilic
NSIP responds to corticosteroids. pneumonia); patients present with acute ARDS and eosino-
philic infiltration of the lungs. The presentation is often dra-
matic and leads to acute respiratory failure and a need for
C RY P TO G E N I C O RG A N I Z I N G P N EUMO N I A mechanical ventilation. Affected persons are young; typically,
Cryptogenic organizing pneumonia (COP) was formerly they recently began smoking. The disease has affected military
known as idiopathic bronchiolitis obliterans with organizing personnel returning from the Middle East. Acute eosinophilic
pneumonia (BOOP). Typically, COP manifests as a recurrent pneumonia responds dramatically to corticosteroids without
flulike illness resistant to antibiotics with migratory infiltrates rebound after discontinued use. Treatment can be short (2
that progress over several months. Histopathologically, it is an weeks). Pulmonary eosinophilia is common, but peripheral
alveolar-filling process (with intra-alveolar plugs of granula- eosinophilia is rare.
tion tissue). The radiologic features include consolidation and
ground-glass infiltrates (usually peripheral), and the pattern AIP, or Hamman-Rich syndrome, is idiopathic ARDS.
on PFTs is that of restriction rather than obstruction. Thus, Acute eosinophilic pneumonia is similar to AIP but is
BOOP is a misnomer (there is little bronchiolar involve- characterized by eosinophilic infiltration of the lungs and a
ment). COP is exquisitely responsive to treatment with cor- dramatic response to corticosteroids.
ticosteroids, which should be administered for 3 to 6 months.
Rebound after discontinuation is common, but COP gener-
ally responds to retreatment with corticosteroids. The absence
of prompt improvement should suggest the possibility of D E S Q UA M AT I V E I N T E R S T I T I A L P N EUM O N I A
secondary OP rather than COP. The most common underly- A N D R E S P I R ATO RY B RO N C H I O L I T I S
ing diagnoses are drug-induced lung disease, CTD-ILD, and I N T E R S T IT I A L LU N G D I S E A S E
hematologic malignancies. Desquamative interstitial pneumonia (DIP) and respira-
tory bronchiolitisinterstitial lung disease (RB-ILD) are
Persistent pneumonia with migratory infiltrates suggests rare. Although classified as idiopathic, they are considered
COP. smoking-related lung diseases. They belong to the same spec-
COP is exquisitely responsive to corticosteroids. trum of disease, with DIP on one end (primarily alveolar dis-
ease) and RB-ILD on the other (bronchiolar disease). Initially
Rebound is frequent after discontinuation of treatment. thought to be secondary to desquamated epithelial cells, the
disease is now understood to result from the accumulation of
Although not considered an idiopathic interstitial pneu- pigment-laden macrophages in the airspaces (DIP) or around
monia, chronic eosinophilic pneumonia manifests much like the bronchioles (RB-ILD) (or both). Smoking cessation is
COP, with recurrent flulike episodes and migratory, periph- warranted and, if achieved, the prognosis is good.
eral infiltrates (typically described as a photographic nega-
tive of pulmonary edema). It is also exquisitely responsive DIP and RB-ILD are smoking-related lung diseases, and
to corticosteroids and, like in COP, rebound is frequent after smoking cessation is recommended.
discontinuation of treatment. The main differences with COP
are the upper lung predominance of the infiltrates and the
eosinophilic infiltration of the lungs (peripheral eosinophilia
is present in two-thirds of the cases). G R A N U L O M ATO U S I L D S
15. I N T E R S T I T I A L LU N G D I S E A S E S 211
increased liver enzyme levels may be noted. Familial clusters H Y P E R S E N S I T I V I T Y P N EUM O N I T I S
of sarcoidosis have been reported. The course of the disease is
HP is an uncommon form of ILD. It is considered an allergic
highly variable, from asymptomatic to life-threatening.
reaction to various organic antigens, including molds, grain
dusts (farmers lung), pets and birds (bird fanciers lung),
Imaging and mycobacterial antigens (hot tub lung). Serum precipi-
Radiographic stage correlates with the severity of pulmonary tins for specific antigens are inconsistently specific and have
disease and prognosis as follows: poor sensitivity for diagnostic purposes. The symptoms and
clinical course are related temporally to antigen exposure.
Stage 0: normal CXR. With acute disease, patients may have dyspnea, cough, fever,
chest pain, headache, malaise, fatigue, and flulike illness.
Stage I: hilar adenopathy. Chronic diffuse fibrotic lung disease may be indistinguish-
Stage II: hilar adenopathy with pulmonary infiltrates. able from IPF.
The histopathologic features of HP show a range of
Stage III: infiltrates without adenopathy. bronchiolar-oriented, ill-defined, noncaseating granulo-
Stage IV: fibrotic lung disease. mas with lymphocytic-predominant centrilobular infil-
trates and varying degrees of fibrosis. A restrictive pattern
CXR may also show characteristic bilateral hilar or medi- is common on PFTs, although an airway component may
astinal lymphadenopathy with occasional eggshell calci- also be present and result in an obstructive component.
fications. Computed tomography of the chest may show Bronchodilators may be needed to treat airflow obstruc-
clustered micronodules with a bronchovascular and subpleu- tion. CXR generally shows reticulonodular changes, and
ral distribution. HRCT often shows nonspecific nodules and ground-glass
opacities predominantly in the upper lobes. Acute symp-
toms generally improve after the patient is no longer
Diagnosis exposed to the antigen. Severe cases require treatment with
In most cases, granulomatous histopathologic features need to corticosteroids.
be identified and other causes of granulomatous inflammation
excluded (primarily fungal, mycobacterial, and other infec- The granulomas in HP are poorly defined.
tions). If hilar adenopathy and parenchymal infiltrates are Treatment consists of avoidance of allergens and,
present, bronchoscopy with biopsy confirms granulomatous sometimes, administration of corticosteroids.
changes in more than 90% of cases. Thus, sarcoidosis must
be considered a diagnosis of exclusion after other causes of
granulomatous disease have been ruled out. The serum levels
of angiotensin-converting enzyme are not sufficiently sensitive OT H E R G R A N U L O M ATO US D I S E A S E S
or specific to be of diagnostic value, but they may be helpful as Other granulomatous diseases include infections such as
a marker of disease activity. fungal or mycobacterial infections. The granulomas are usu-
ally necrotizing, as opposed to those in sarcoidosis and HP.
Treatment Wegener granulomatosis and Churg-Strauss syndrome should
also be in the differential diagnosis. Response to intravenous
Corticosteroids are first-line therapy. However, whether
injection of insoluble material, such as intravenous talcosis (as
immunosuppressive therapy, including corticosteroids, alters
occurs in intravenous drug users), may result in diffuse lung
the natural course of the disease is debated. Other immuno-
granulomas centered on foreign bodies that are birefringent in
suppressive regimens used as second-line therapy for pulmo-
polarized light.
nary sarcoidosis have included methotrexate, azathioprine,
pentoxifylline, and cyclosporine. Treatment is reserved for
severe organ disease (including progressive lung disease). In
OT H E R I L D S
up to 90% of patients with stage I pulmonary sarcoidosis,
the disease is expected to remain stable or to resolve sponta-
neously with no treatment. Stage III pulmonary sarcoidosis P U L M O NA RY L A N G E R H A N S C E L L
is expected to spontaneously remit in only 10% of patients. H I S T I O C Y TO S I S
Pulmonary sarcoidosis is expected to progress within 2 to 5
years after diagnosis, although increased disease activity can PLCH is a rare cystic lung disease mostly affecting young
occur at any time. white smokers. Spontaneous pneumothoraces are common
(25% of cases). CXR shows diffuse interstitial infiltrates with
classic cystic and micronodular changes, predominantly in the
Sarcoidosis affects the lungs in 90% of cases and
upper lobes. The distinctive nodular component and upper
extrapulmonary organs in 30% of cases.
lobe predominance seen on HRCT differentiate PLCH from
Treatment with corticosteroids is indicated for only severe LAM (see below). Restriction is common, but a mixed pat-
manifestations of the disease. tern is also classically described. In the systemic variant of
212 P U L M O N A RY D I S E A S E S
the disease (more common in children), there may be bone Pneumothorax, hemoptysis, chylous pleural effusions,
involvement and pituitary insufficiency (central diabetes and retroperitoneal pain or hemorrhage from ruptured
insipidus). The combination of exophthalmos, diabetes insip- angiomyolipomas are common.
idus, and lytic bone lesions (often in the skull) is known as
Hand-Schller-Christian disease. Aggregates of Langerhans
cells interspersed with normal lung parenchyma are the char-
P U L M O NA RY A LV E O L A R P ROT E I N O S I S
acteristic histopathologic finding. An increase in the number
of Langerhans cells can be detected by staining BAL speci- PAP is a rare, idiopathic form of diffuse lung disease charac-
mens for CD1a (typically >5%), which is overexpressed in terized by the filling of alveoli with proteinaceous material
these cells. Absolute cessation of smoking is mandatory. The consisting mostly of phospholipoprotein (dipalmitoyl leci-
response to abstinence from all tobacco products varies, with thin). A defect in the signaling of granulocyte-macrophage
stabilization or improvement noted in as many as two-thirds colony-stimulating factor (GM-CSF) is thought to contrib-
of patients. Langerhans cell histiocytosis increases the risk ute to the clinical manifestations. Most patients are smokers
of bronchogenic cancer and lymphoma. The success of cor- younger than 50 years, with a male predominance (male to
ticosteroid treatment and chemotherapy has been limited. female ratio, 3:1). Symptoms of dyspnea, cough, and low-grade
Transplant is reserved for advanced, progressive disease. fever are common. Many infectious, occupational, inflamma-
tory, and environmental secondary causes of PAP-like pre-
PLCH is another smoking-related lung disease, and sentations have been recognized. Increased predisposition
cessation of smoking is mandatory. to Nocardia infections has been reported. CXR may show
an alveolar filling pattern infiltrate that resembles bat wings,
Pneumothorax is common in PLCH.
mimicking pulmonary edema. A nonspecific but characteristic
Think of PLCH in a young smoker with pneumothoraces. alveolar filling pattern seen with HRCT, described as a cra-
zy-paving pattern with airspace consolidation and thickened
interlobular septa, is suggestive of PAP. A milky white return
of BAL fluid or lung biopsy findings usually indicate the diag-
LY M P H A N G I O L E I O MYO M ATO S I S
nosis. In addition to smoking cessation, therapy has involved
LAM is a disease of women of childbearing age that may be whole-lung lavage and, more recently, trials of GM-CSF.
associated with tuberous sclerosis (in up to 20% of cases). It is
characterized clinically by a history of recurrent pneumothora- PAP is often due to a deficiency in GM-CSF or to
ces (50%-80%), chylous pleural effusions (30%), diffuse infil- autoantibodies directed against GM-CSF.
trates with hypoxemia, and airflow obstruction. Hemoptysis is
Treatment with whole-lung lavage remains the standard of
common (25%). HRCT typically demonstrates well-defined
care for severe cases, although GM-CSF supplementation
cysts scattered homogeneously throughout the lungs, without
is sometimes effective.
nodules or interstitial fibrosis. Pregnancy or exogenous estro-
gens may worsen the course of the disease. The histopatho-
logic features, similar to those of tuberous sclerosis, include a
distinctive proliferation of atypical interstitial smooth mus- S U M M A RY
cle and thin-walled cysts within the lung. Extrapulmonary
involvement may include uterine leiomyomas and renal Diffuse lung disease includes a wide range of idiopathic and
angiomyolipomas. The response to treatment with hormonal secondary lung disease processes that have various presenta-
manipulation has been limited. Currently, lung transplant is tions and prognoses. A focused, complete medical history
the definitive treatment. Sirolimus appears promising in the and physical examination in combination with judicious use
management of LAM. of laboratory data, PFTs, chest imaging, bronchoscopy, and
open lung biopsy when needed can narrow the differential
Cystic lung disease or recurrent pneumothoraces in young diagnosis, provide important prognostic information, and
females suggest LAM. guide therapeutic interventions.
15. I N T E R S T I T I A L LU N G D I S E A S E S 213
16.
PULMONARY VASCULAR DISEASE, PULMONARY
EMB OLISM, AND PULMONARY HYPERTENSION
Karen L. Swanson, DO
214
A B
Figure 16.1 A, Pulmonary angiography documenting the presence of multiple, large pulmonary arteriovenous malformations. B, After coil
embolization, there is complete lack of flow through the pulmonary arteriovenous malformations.
16. P U L M O N A RY VA S C U L A R D I S E A S E , P U L M O N A RY E M B O L I S M , A N D P U L M O N A RY H Y P E RT E N S I O N 215
who have systemic disease. In active disease, the sensitivity is an obvious cause. In fact, 10% of patients have prominent
91%, and the specificity is 98%; in inactive disease, the sensi- respiratory symptoms. Histopathology shows mononuclear
tivity is 63%, and the specificity is 99.5%. infiltrates with giant cell formation in medium-sized and large
pulmonary arteries. Pulmonary nodules, interstitial infiltra-
Positive c-ANCA without clinical evidence of disease does tions, pulmonary artery occlusion, and aneurysms have been
not establish the diagnosis. described. The response to corticosteroids is favorable.
Some patients with active disease have negative c-ANCA.
Respiratory symptoms are prominent in 10% of patients
c-ANCA may be present in other diseases (eg, hepatitis C, with giant cell arteritis.
microscopic polyangiitis, ulcerative colitis, sulfasalazine
Cough, sore throat, and hoarseness occur in older persons
toxicity).
without an obvious cause.
p-ANCA is positive in various diseases, including inflam-
matory bowel disease, autoimmune liver disease, rheumatoid
arthritis, and other vasculitides. p-ANCA with specificity B E H ET D I S E A S E
against MPO is closely associated with microscopic polyangi- Behet disease is a chronic, relapsing, multisystemic inflam-
itis, leukocytoclastic vasculitis, pauci-immune necrotizing matory disorder characterized by aphthous orogenital ulcer-
crescentic glomerulonephritis, and other vasculitides, includ- ations (in >65% of patients), uveitis, cutaneous nodules or
ing Churg-Strauss syndrome. pustules, synovitis, and meningoencephalitis. Superficial
venous thrombosis, deep vein thrombosis (DVT) of upper and
Positive p-ANCA results occur in other vasculitides and lower extremities, and thrombosis of the inferior and superior
collagen diseases. venae cavae occur in 7% to 37% of patients. Pulmonary vas-
The presence of p-ANCA with specificity for MPO should cular involvement produces severe hemoptysis that is initially
suggest small-vessel vasculitis (microscopic polyangiitis). responsive to corticosteroids but which tends to recur; death
is due to hemoptysis in 39% of patients. CXR may show lung
The combination of corticosteroids and cyclophosphamide infiltrates, pleural effusions, prominent pulmonary arteries,
produces complete remission in more than 90% of patients with and pulmonary artery aneurysms. Aneurysms of the pulmo-
limited GPA. In severe GPA, intravenous corticosteroids and nary artery communicating with the bronchial tree (broncho-
rituximab are recommended. Trimethoprim-sulfamethoxazole vascular anastomosis) should be considered in patients with
is effective in preventing disease relapse. Behet disease and massive hemoptysis. Because of the high
incidence of DVT, PE is common. Corticosteroids and che-
motherapeutic agents have been used. The prognosis is poor if
EO S I N O P H I L I C G R A N U L O M ATO S I S WIT H the patient experiences marked hemoptysis.
P O LYA N G I I T I S (C HU RG -S T R AUS S SY N D RO M E)
Eosinophilic granulomatosis with polyangiitis is characterized Behet disease: aphthous orogenital ulcerations, uveitis,
by pulmonary and systemic vasculitis, extravascular granulo- cutaneous nodules, and meningoencephalitis.
mas, increased levels of IgE, and eosinophilia in patients with Severe hemoptysis is the cause of death in 39% of patients.
asthma or allergy. Allergic rhinitis, nasal polyps, nasal mucosal
crusting, and septal perforation occur in more than 70% of A fistula between the airway and vascular structures is
patients. Almost all patients have refractory asthma. In more common.
than 60% of patients, chest radiography (CXR) shows patchy High incidence of DVT and PE.
and occasionally diffuse alveolar-interstitial infiltrates with
a predilection for the upper two-thirds of the lungs. Pleural
effusions develop in up to one-third. The response to systemic
corticosteroids is dramatic. TA K AYA S U A RT E R I T I S
Takayasu arteritis, also known as pulseless disease, aortic
Features of eosinophilic granulomatosis with polyangiitis arch syndrome, and reversed coarctation, is a chronic inflam-
include refractory asthma, progressive respiratory distress, matory disease of unknown cause affecting the aorta and its
allergic rhinitis, nasal polyps, nasal mucosal crusting, septal major branches, including the proximal coronary arteries,
perforation, tissue and blood eosinophilia, and increased renal arteries, and the elastic pulmonary arteries. The pulmo-
levels of IgE. nary arteries are involved in more than 50% of patients, with
lesions in medium-sized and large arteries. Perfusion lung scans
G I A N T C E L L A RT E R I T I S
show abnormalities in more than 75% of patients; pulmo-
nary angiography shows arterial occlusion in 86%. Takayasu
Giant cell arteritis, also known as temporal arteritis, cranial arteritis is most prevalent in East Asia and more common
arteritis, and granulomatous arteritis, should be considered in women. Corticosteroids induce remission within days to
when older patients have a new cough or throat pain without weeks. Pulmonary involvement signifies a poor prognosis.
216 P U L M O N A RY D I S E A S E S
Takayasu arteritis: pulmonary artery involvement occurs in Patients with anti-GBM antibodymediated nephri-
>50% of patients and portends a poor prognosis. tis demonstrate 2 principal patterns of disease: 1) young
men presenting in their 20s with Goodpasture syndrome
(glomerulonephritis and lung hemorrhage) and 2) elderly
A LV E O L A R H E MO R R H AG E S Y N D RO M E S
patients, especially women, presenting in their 60s with
Diffuse hemorrhage into the alveolar spaces is called alveolar glomerulonephritis alone. In the classic form of Goodpasture
hemorrhage syndrome. Disruption of pulmonary capillaries syndrome (in younger patients), men are affected more often
(capillaritis) may result from any of the following: damage than women (male to female ratio, 7:1) and the average age
caused by different immunologic mechanisms (Goodpasture at onset is approximately 27 years. Recurrent hemoptysis,
syndrome, renal-pulmonary syndromes, glomerulonephritis, pulmonary insufficiency, renal involvement with hema-
and systemic lupus erythematosus), direct chemical or toxic turia and renal failure, and anemia are the classic features.
injury (toxic or chemical inhalation, penicillamine, mitomy- Pulmonary hemorrhage almost always precedes renal mani-
cin, abciximab, all-trans-retinoic acid, trimellitic anhydride, festations. Active cigarette smoking increases the risk of
and smoked crack cocaine), physical trauma (pulmonary con- alveolar hemorrhage.
tusion), and increased vascular pressure within the capillaries
(mitral stenosis and severe left ventricular failure). Pulmonary hemorrhage almost always precedes renal
The severity of hemoptysis, anemia, and respiratory dis- manifestations.
tress depends on the extent and rapidity of bleeding. Alveolar
Active cigarette smoking increases the risk of alveolar
hemorrhage is present if hemosiderin-laden macrophages
hemorrhage.
constitute more than 20% of the total alveolar macrophages
recovered with bronchoalveolar lavage. The risk of alveolar Typical clinical scenario for the classic form: A young man
hemorrhage increases with thrombocytopenia, abnormal has glomerulonephritis and lung hemorrhage.
coagulation variables, renal failure (creatinine 2.5 mg/dL),
and heavy smoking. Treatment is with high-dose intravenous Typical clinical scenario for the form in older patients: An
methylprednisolone or plasma exchange. elderly patient, especially a woman, has glomerulonephritis
alone.
Alveolar hemorrhage syndrome is caused by different
mechanisms. One-third of patients with anti-GBM disease test posi-
tive for p-ANCAMPO; fulminant pulmonary hemorrhage
Hemoptysis is not a consistent feature. is more likely to occur in p-ANCApositive patients than in
those who are p-ANCAnegative. Plasmapheresis is the treat-
Risk increases with thrombocytopenia, other
ment of choice. Although complete recovery can be expected
coagulopathy, creatinine 2.5 mg/dL, and heavy smoking.
in most patients treated with systemic corticosteroids, immu-
Drugs that cause alveolar hemorrhage: penicillamine, nosuppressive agents, or plasmapheresis, relapse occurs in up
abciximab, all-trans-retinoic acid, and mitomycin. to 7%.
16. P U L M O N A RY VA S C U L A R D I S E A S E , P U L M O N A RY E M B O L I S M , A N D P U L M O N A RY H Y P E RT E N S I O N 217
p-ANCAMPO) is detected in 75% of patients who have Yellow nail syndrome consists of lymphedema, yellow
microscopic polyangiitis. dystrophic nails that do not grow, and idiopathic pleural
effusions or recurrent lung infection (or both).
Microscopic polyangiitis: progressive glomerulonephritis is
a major feature.
P U L M O N A RY E M B O L I S M
Pulmonary alveolar hemorrhage is observed in 12%-29% of
patients. PE is the cause of death in 5% to 15% of hospitalized patients.
In 75% of patients, p-ANCAMPO is positive. Poor prognostic factors include age older than 70 years, cancer,
congestive heart failure, chronic obstructive pulmonary disease,
systolic arterial hypotension, tachypnea, and right ventricular
hypokinesis. PE is detected in 25% to 30% of routine autopsies.
I D I O PAT H I C P U L MO NA RY H E MO S I D E RO S I S Antemortem diagnosis is made in less than 30% owing to the
Idiopathic pulmonary hemosiderosis (IPH) is a rare disorder variable and nonspecific presentation of patients with PE.
of unknown cause and is a diagnosis of exclusion. Features
include recurrent intra-alveolar hemorrhage, hemoptysis, PE is a common problem; consider PE in all patients who
transient infiltrates on CXR, and secondary iron deficiency have lung symptoms.
anemia. IPH has been described in association with idiopathic Antemortem diagnosis, made in <30% of cases, requires a
thrombocytopenic purpura, autoimmune hemolytic anemia, high degree of awareness.
and nontropical sprue (celiac disease).
Clinical features are chronic cough with intermittent The risk of death from untreated PE is 8%.
hemoptysis, iron deficiency anemia, fever, weight loss, gen-
eralized lymphadenopathy (25% of patients), hepatospleno- ET I O L O GY
megaly (20%), clubbing (15%), and eosinophilia (10%). The
kidneys are not involved. Treatment is repeated blood trans- The most common cause of PE is DVT of the lower extremi-
fusions, iron therapy, corticosteroids, and, possibly, cytotoxic ties. In approximately 45% of patients with femoral and iliac
agents. A 30% mortality rate within 5 years after disease onset DVT, emboli move to the lungs. Other sources of emboli
has been reported. include thrombi in the upper extremities, right ventricle, and
indwelling catheters. The primary and secondary coagulation
IPH is a diagnosis of exclusion. abnormalities that predispose to the development of DVT
and PE are listed in Box 16.1. The incidence of DVT in vari-
Generalized lymphadenopathy occurs in 25% of patients, ous clinical circumstances is listed in Table 16.1. Idiopathic
hepatosplenomegaly in 20%, and clubbing in 15%. DVT, particularly when recurrent, may indicate the presence
Kidneys are not involved. of neoplasm in 10% to 20% of patients. The presence of vari-
cose veins does not increase the risk of DVT. Compression
Eosinophilia occurs in 10% of patients. ultrasonography, the most commonly used noninvasive test,
has a diagnostic accuracy of 90% to 95% in detecting iliac and
femoral DVT. Serial compression ultrasonography is recom-
P U L MO NA RY LY M P H AT I C D I S O R D E R S
mended for high-risk patients because of a 15% detection rate
of DVT after an initial negative study. Magnetic resonance
Pulmonary lymphatic disorders include lymphangioma, lym- imaging has a high sensitivity and specificity for the diagnosis
phangiomatosis, lymphangiectasis, and pulmonary lymphatic of pelvic DVT.
dysplastic syndromes. Pulmonary lymphatic dysplasia syn-
dromes are a heterogeneous group of disorders. They include DVT is detected in only 40% of cases of PE.
idiopathic lymphedema syndromes, idiopathic recurring chy-
lous effusions, and yellow nail syndrome and are characterized Consider factor V Leiden mutation, the presence of lupus
by obstruction of proximal lymphatic channels with refractory anticoagulant, and deficiencies of antithrombin III, protein
accumulation of chyle. The immunoglobulin loss may result S, and protein C among predisposing factors for DVT
in immunodeficiency and the protein loss in malnutrition. and PE.
Yellow nail syndrome consists of lymphedema, yellow dystro- In idiopathic recurrent DVT, look for an occult neoplasm.
phic nails, and idiopathic pleural effusions or respiratory tract
illness (or both) with bronchiectasis and recurrent pneumo-
nias. The nails usually do not grow, and patients may wonder
D I AG N O S T I C T E S T S
why the nails do not need to be trimmed.
Physical examination, electrocardiography, CXR, blood gas
Pulmonary lymphatic disorders include lymphangioma, abnormalities, troponins, B-type natriuretic peptide (BNP),
lymphangiomatosis, lymphangiectasis, and lymphatic and increased plasma D-dimer level have low specificity and
dysplasia syndromes. sensitivity for the diagnosis of PE but, when considered
218 P U L M O N A RY D I S E A S E S
Box 16.1 COAGULATION DISORDERS PREDISPOSING Table 16.1 INCIDENCE OF DEEP VEIN THROMBOSIS
TO THE DEVELOPMENT OF DEEP VEIN THROMBOSIS (DVT) IN VARIOUS CLINICAL CIRCUMSTANCES
AND PULMONARY EMBOLISM
CLINICAL CIRCUMSTANCE INCIDENCE OF DVT, %
16. P U L M O N A RY VA S C U L A R D I S E A S E , P U L M O N A RY E M B O L I S M , A N D P U L M O N A RY H Y P E RT E N S I O N 219
High-probability scan: 90% probability of PE. Heparin therapy is necessary after thrombolytic therapy.
Intermediate-probability scan: 30% probability of PE. Thrombolytic therapy: 1% risk of intracranial bleeding.
Low-probability scan: 15% probability of PE.
Inferior Vena Cava Interruption
Normal scan excludes PE in 100% of cases.
Inferior vena cava interruption is indicated if anticoagulant
CT angiography permits ultrafast scanning of pulmonary therapy is contraindicated, complications result from antico-
arteries during contrast injection. Sensitivity and specificity agulant therapy, anticoagulant therapy fails, a predisposition
rates greater than 95% have been reported. Spiral CT has the to bleeding is present, chronic recurrent PE and secondary
greatest sensitivity in the diagnosis of PE in the main, lobar, pulmonary hypertension occur, or surgical pulmonary throm-
or segmental arteries. Ventilation-perfusion scanning is pre- boendarterectomy has been performed or is intended to be
ferred for patients with possible chronic thromboembolic performed. After the filter has been inserted, anticoagulant
disease owing to the distal nature of the thrombotic mate- therapy is aimed at preventing DVT at the insertion site, infe-
rial. Magnetic resonance imaging may have the advantage of rior vena cava thrombosis, cephalad propagation of a clot from
detecting both DVT and PE. Dysfunction of the right ven- an occluded filter, and propagation or recurrence of lower
tricle (frequently seen in submassive, massive, and recurrent extremity DVT. PE occurs in 2.5% of patients despite inferior
PE) can be detected with transthoracic Doppler echocardiog- vena cava interruption.
raphy. Echocardiography is not necessary for all PE patients,
especially those with normal BNP; however, it is extremely Inferior vena cava interruption does not replace long-term
useful for the clinically unstable patient. anticoagulant therapy.
PE occurs in 2.5% of patients despite inferior vena cava
Spiral CT has the greatest sensitivity in the diagnosis of
interruption.
acute PE.
Ventilation-perfusion scan is helpful in assessing chronic
thromboembolic disease. P U L M O N A RY H Y P E RT E N S I O N
Pulmonary angiography is the gold standard but has been Elevation of pulmonary pressure (ie, PH) can be caused by
largely replaced by CT angiography. It should be performed an elevated pulmonary capillary wedge pressure, a high-flow
within 24 to 48 hours after the diagnosis has been considered. state (increased cardiac output), or a true elevation in pulmo-
After pulmonary angiography, major complications occur in nary vascular resistance (ie, pulmonary arterial hypertension
1% of patients, and minor complications in 2%; mortality [PAH]). PAH is present when the mean pulmonary arterial
from the procedure is 0.5%. pressure (MPAP) is greater than 25 mm Hg at rest (or >35 mm
Hg with exercise), the pulmonary capillary wedge pressure is
T R E AT M E N T less than 15 mm Hg, and the pulmonary vascular resistance is
more than 3 Wood Units (>240 dynes.s.cm5). Pathologically,
Goals of short-term treatment are to prevent recurrence
PAH is characterized by vasoconstriction, pulmonary vascular
of venous thromboembolism (extension and fatal PE)
remodeling, and thrombosis in situ that leads to progressive
and to prevent long-term complications (late recurrence,
increases in pulmonary vascular resistance, right-sided heart
post-thrombotic syndrome, chronic thromboembolic pulmo-
failure, and death. There are many causes of PH; a revised
nary hypertension). Therapy, including drug choice and dura-
clinical classification categorizes the causes into 5 groups
tion, are discussed in detail in Hematology: Thrombosis
(Box 16.2).
(Chapter 36).
PH may be caused by an increased volume (elevated wedge
Thrombolytics pressure), a high-flow state (high cardiac output), or a true
elevation in pulmonary vascular resistance (PAH).
In massive PE or PE with hemodynamic instability, throm-
bolytic therapy is recommended. The use of thrombolytics A revised clinical classification of PH defines 5 groups.
in submassive, hemodynamically stable PE is controversial.
Ideally, thrombolytic agents should be administered within The clinical presentation of PH is nonspecific, and patients
24 hours after PE. Heparin infusion is begun or resumed if the complain of progressive dyspnea, lower extremity edema, and
activated partial thromboplastin time is less than 80 seconds fatigue. Blood testing, which may be helpful for identifying
after thrombolytic therapy. The risk of intracranial bleeding a cause for PH, includes connective tissue serologies, BNP,
in patients who have PE treated with thrombolytic drugs is thyroid studies, liver enzymes, testing for human immunode-
about 1%. ficiency virus, and a complete blood cell count. Full pulmo-
nary function testing and overnight oximetry are essential to
Thrombolytic agents should be administered within exclude pulmonary causes of PH. The diagnosis of PE needs to
24 hours after PE. be excluded in all patients undergoing evaluation for PH.
220 P U L M O N A RY D I S E A S E S
Box 16.2 UPDATED CLINICAL CLASSIFICATION OF Blood tests and pulmonary evaluation are essential to
PULMONARY HYPERTENSION (DANA POINT, 2008) a determine the cause of PH.
PE needs to be excluded in all patients with PH.
1. Pulmonary arterial hypertension
1.1. Idiopathic Typically, a diagnosis of PH is suggested by an increased
1.2. Heritable right ventricular systolic pressure on transthoracic Doppler
1.2.1. BMPR2 echocardiography and is confirmed with right-heart catheter-
1.2.2. ALK1, endoglin (with or without hereditary hemor- ization. Hemodynamic measurements at right-heart catheter-
rhagic telangiectasia) ization are important to exclude PH due to fluid overload or
1.2.3. Unknown contributions from a high cardiac output (such as in liver dis-
1.3. Drug- and toxin-induced ease, thyroid disease, or anemia). Patients who show vasore-
1.4. Associated with activity at right-heart catheterization (a decrease in MPAP or
1.4.1. Connective tissue diseases pulmonary vascular resistance by 20% with vasodilator chal-
1.4.2. HIV infection lenge) may benefit from a trial of calcium channel blockers.
1.4.3. Portal hypertension
1.4.4. Congenital heart diseases Echocardiography is a good screening test; however,
1.4.5. Schistosomiasis right-heart catheterization is imperative to define
1.4.6. Chronic hemolytic anemia hemodynamic measurements.
1.5. Persistent pulmonary hypertension of the newborn
1'. Pulmonary venoocclusive disease or pulmonary capillary Rarely, patients with positive vasodilator response may
hemangiomatosis (or both) respond to calcium channel blockers.
2. Pulmonary hypertension due to left heart disease
World Health Organization (WHO) functional class is a
2.1. Systolic dysfunction
powerful predictor of survival. Patients in WHO functional
2.2. Diastolic dysfunction
class IV have a median survival of 6 months; in functional class
2.3. Valvular disease
III, 2.5 years; and in functional class I or II, 6 years. Extremes
3. Pulmonary hypertension due to lung disease or hypoxia (or of age, decreased exercise capacity (6-minute walk distance),
both) syncope, and signs of right ventricular failure carry a poor
3.1. Chronic obstructive pulmonary disease prognosis.
3.2. Interstitial lung disease
3.3. Other pulmonary diseases with mixed restrictive and WHO functional class is a powerful predictor of survival.
obstructive pattern
3.4. Sleep-disordered breathing To date, no cure exists. However, several treatment options
3.5. Alveolar hypoventilation disorders have been shown to improve quality of life, the hemodynamic
3.6. Chronic exposure to high altitude profile, and survival. A meta-analysis of 23 randomized con-
3.7. Developmental abnormalities trolled trials involving PAH reported a 43% decrease in mor-
tality and a 61% decrease in hospitalizations compared with
4. Chronic thromboembolic pulmonary hypertension
placebo. Oxygen, diuretics, digoxin, and anticoagulation may
5. Pulmonary hypertension with unclear multifactorial be useful in the treatment of PAH. Other treatment options
mechanisms approved by the US Food and Drug Administration (FDA)
5.1. Hematologic disorders: myeloproliferative disorders, for PAH patients in WHO functional class I include intrave-
splenectomy nous, subcutaneous, and inhaled prostanoids (epoprostenol,
5.2. Systemic disorders: sarcoidosis, pulmonary Langerhans treprostinil, and iloprost); oral endothelin receptor antago-
cell histiocytosis: lymphangioleiomyomatosis, neurofibroma- nists (bosentan and ambrisentan); and oral phosphodiesterase
tosis, vasculitis type 5 inhibitors (sildenafil and tadalafil). Combination
5.3. Metabolic disorders: glycogen storage disease, Gaucher therapy has become the standard of care in PAH, although
disease, thyroid disorders the long-term safety and efficacy data are not well defined. A
5.4. Others: tumoral obstruction, fibrosing mediastinitis, stepwise approach appears beneficial. Drug-drug interactions
chronic renal failure on dialysis are common.
Abbreviations: ALK1, activin receptor-like kinase type 1; BMPR2, bone
morphogenetic protein receptor type 2; HIV, human immunodeficiency FDA-approved medications for PAH have all been shown
virus. to improve quality of life and the hemodynamic profile in
a
randomized controlled trials.
Main modifications to the previous Venice classification are in bold.
Combination therapy in PAH is common.
Adapted from Simonneau G, Robbins IM, Beghetti M, Channick RN,
Delcroix M, Denton CP, et al. Updated clinical classification of pulmonary
hypertension. J Am Coll Cardiol. 2009 Jun 30;54(1 Suppl):S4354. Used Balloon atrial septostomy confers a survival advantage for
with permission. patients with Eisenmenger syndrome and PAH with patent
16. P U L M O N A RY VA S C U L A R D I S E A S E , P U L M O N A RY E M B O L I S M , A N D P U L M O N A RY H Y P E RT E N S I O N 221
foramen ovale. The creation of an interatrial right-to-left Transthoracic Doppler echocardiography can suggest the
shunt can decompress the right heart chambers and increase presence of PH; however, right-heart catheterization is
left ventricular preload and cardiac output. Systemic oxy- diagnostic.
gen therapy improves despite oxygen desaturation. Patients
should be receiving optimal medical therapy before septos- Available treatment options for PAH may improve quality
tomy is considered, however, and this likely serves as a bridge of life and survival.
to transplant.
Disease-specific therapy in PAH has reduced referral for S U M M A RY
lung transplant, but transplant is an important option for
patients not responding to medical therapy. PAH patients with The pulmonary vasculitides are a heterogeneous group
connective tissue disease have the worst prognosis; survival is of disorders. Patients may present with fever, malaise,
better for PAH patients with congenital heart disease. The weight loss, palpable purpura, mononeuritis multiplex,
prognosis is poor for patients with pulmonary venoocclusive arthralgias, renal insufficiency, hemoptysis, stridor, cough,
disease and pulmonary capillary hemangiomatosis due to the and dyspnea.
lack of effective medical therapy. Heart-lung and double-lung
Maintain a high degree of awareness for PE.
transplant have been performed.
Thorough evaluation, including pulmonary function
Consider the diagnosis of PH for patients with new-onset tests and evaluation for PE, is indicated in the diagnostic
dyspnea. workup of PH.
222 P U L M O N A RY D I S E A S E S
17.
COMMON PULMONARY DISORDER S
John G. Park, MD
223
Box 17.1 HISTORY AND PHYSICAL EXAMINATION OF Pleural rub
PATIENTS WITH PULMONARY DISEASE Mediastinal noises (mediastinal crunch)
Heart sounds
History Miscellaneous (muscle tremor, etc)
Smoking
Occupational exposure Abbreviations: CO2, carbon dioxide; COPD, chronic obstructive pulmonary
disease; FEV1, forced expiratory volume in the first second of expiration.
Exposure to infected persons or animals
Hobbies & pets
Family history of diseases of the lung & other organs
Past malignancy b. Infradiaphragmatic abnormalities such as calcifications
Systemic (nonpulmonary) diseases in the spleen, displacement of the gastric bubble and
Immune status (corticosteroid therapy, chemotherapy, cancer) colon, and signs of upper abdominal surgery may
History of trauma indicate the cause of a pleuropulmonary process.
Previous chest radiography
Examination c. Lateral CXRs are important in identifying
Inspection retrocardiac and retrodiaphragmatic abnormalities.
Respiratory rate, hoarseness of voice Initially look at the entire CXR.
Respiratory rhythm (abnormal breathing pattern)
Accessory muscles in action (FEV1 <30%) Look for extrapulmonary abnormalities before focusing on
Postural dyspnea (orthopnea, platypnea, trepopnea) any obvious parenchymal findings.
Intercostal retraction 2. View the skeletal thorax to exclude rib fracture, osteolytic
Paradoxical motions of abdomen or diaphragm and other lesions of the ribs, rib notching, missing ribs,
Cough (type, sputum, blood) and vertebral abnormalities. Changes due to previous
Wheeze (audible with or without stethoscope) thoracic surgical procedures (eg, coronary artery bypass,
Pursed lip breathing or glottic wheeze (patients with COPD) thoracotomy, lung resection, or esophageal surgery) may
Cyanosis (central vs peripheral) provide clues to the pulmonary disease.
Conjunctival suffusion (CO2 retention)
Clubbing 3. Assess the intrathoracic but extrapulmonary structures
Thoracic cage (eg, anteroposterior diameter, kyphoscoliosis, such as the mediastinum (including the great vessels,
pectus carinatum) esophagus, heart, lymph nodes, and thymus). A calcified
Trachea, deviation mass in the region of the thyroid almost always indicates a
Superior vena cava syndrome goiter. An obliterated aortopulmonary window (a notch
Asterixis, central nervous system status below the aortic knob on the left, just above the pulmonary
Cardiac impulse, jugular venous pressure, pedal edema (signs of artery) may indicate a tumor or lymphadenopathy. Right
cor pulmonale) paratracheal and paramediastinal lymphadenopathy can
Palpation be subtle. Hilar regions are difficult to interpret because
Clubbing lymphadenopathy, vascular prominence, or tumor may
Lymphadenopathy make the hila appear larger. The retrocardiac region may
Tibial tenderness (hypertrophic pulmonary osteoarthropathy) show hiatal hernia with an air-fluid level; this may be
Motion of thoracic cage (hand or tape measure) helpful in the diagnosis of reflux or aspiration.
Chest wall tenderness (costochondritis, rib fracture, pulmonary Note changes due to previous surgical procedures.
embolism)
Tracheal deviation, tenderness Assess the mediastinal structures: esophagus, thyroid,
Tactile (vocal) fremitus thymus, and great vessels.
Subcutaneous emphysema 4. Examine the pleural regions for pleural effusion, pleural
Succussion splash (effusion, air-fluid level in thorax) thickening (particularly in the apices), blunting of
Percussion costophrenic angles, pleural plaques or masses, and
Thoracic cage (dullness, resonance) pneumothorax. A lateral decubitus radiograph may
Diaphragmatic motion (normal, 57 cm) be necessary to confirm the presence of free fluid in
Upper abdomen (liver) the pleural space. An air bronchogram depicting the
Auscultation major airways may indicate a large tumor (cut-off of air
Tracheal auscultation bronchogram) or consolidation from an infection.
Normal breath sounds
Bronchial breath sounds 5. Finally, evaluate the lung parenchyma. Notably, about 15%
Expiratory slowing of the pulmonary parenchyma is located behind the heart
Crackles and diaphragm; a lateral CXR is helpful in examining
Wheezes this region. It is important not to overinterpret increased
interstitial lung markings. Generally, bronchovascular
224 P U L M O N A RY D I S E A S E S
Table 17.1 PERCUSSION AND AUSCULTATION FINDINGS IN PULMONARY CONDITIONS
CHEST
CONDITION EXPANSION FREMITUS RESONANCE BREATH SOUNDS EGOPHONY BRONCHOPHONY
Pleural effusiona Decreased Decreased Decreased Decreased Absent >> present Absent >> present
b
Consolidation Decreased Increased Decreased Bronchial Present Present
Atelectasisc Decreased Decreased Decreased Decreased Absent > present Absent > present
Pneumothorax Variable Decreased Increased Decreased Absent Absent
a
The trachea is shifted contralaterally in effusion.
b
Whispered pectoriloquy is present in consolidation.
c
The trachea is shifted ipsilaterally in atelectasis.
markings should be visible throughout the lung diaphragmatic motion and in diagnosing diaphragmatic paral-
parenchyma. The absence of any markings within the lung ysis by the sniff test. Paradoxical motion of the diaphragm sug-
parenchyma suggests a bulla or an air-containing cyst. gests diaphragmatic paralysis (but it is present in up to 6% of
Apical areas should be evaluated carefully for the presence healthy subjects). Bilateral diaphragmatic paralysis diminishes
of pleural thickening, pneumothorax, small nodules, and the sensitivity of the test.
subtle infiltrates.
Fluoroscopy is useful in diagnosing diaphragmatic paralysis
Examine the apices for thickening, pneumothorax,
through the sniff test.
nodules, and subtle infiltrates.
Examine the lung parenchyma behind the heart and
C O M P U T E D TO M O G R A P H Y
diaphragm.
A high-resolution computed tomography (HRCT) scan
Common CXR abnormalities are depicted in Figures 17.1
can show characteristic features of pulmonary Langerhans
through 17.26.
cell granulomatosis, lymphangioleiomyomatosis, idiopathic
pulmonary fibrosis, and lymphangitic pulmonary metas-
F LU O RO S C O P Y tasis. Computed tomograpy (CT) is useful in staging lung
cancer and in evaluating the presence of solitary pulmonary
Fluoroscopy is useful in localizing lesions during biopsy
nodules, multiple lung nodules (metastatic), diffuse lung dis-
and aspiration procedures. It also is valuable in assessing
ease, pleural process, and calcification in nodules. Ultrafast
CT with contrast media is used for diagnosing pulmonary
embolism.
Table 17.2 SYSTEMATIC APPROACH TO EVALUATION
OF A CHEST RADIOGRAPH
HRCT is helpful in the diagnosis of intersitial lung disease.
1. Check for patient identifier
M AG N ET I C R E S O NA N C E I M AG I N G
2. Evaluate extrapulmonary structures
Destructive arthritis Magnetic resonance imaging (MRI) is recommended for the
Absence of breast shadow
Evidence of previous surgery: sternal wires, valvular prosthesis,
initial evaluation of a superior sulcus tumor (Pancoast tumor),
surgical staples demarcating previous lobectomy, etc lesions of the brachial plexus, and paraspinal masses that on
Tracheostomy CXR appear consistent with neurogenic tumors. MRI is supe-
rior to CT in evaluating chest wall masses and searching for
3. Infradiaphragmatic abnormalities small occult mediastinal neoplasms (eg, ectopic parathyroid
4. Skeletal changes: rib fractures, notching, osteolytic lesions, etc adenoma).
5. Intrathoracic, extrapulmonary structures: mediastinum, thyroid MRI is superior to CT in evaluating chest wall masses and
calcification, achalasia, aortopulmonary window, hilum, calcified
adenopathy searching for small occult mediastinal neoplasms.
17. C O M M O N P U L M O N A RY D I S O R D E R S 225
A B
Figure 17.1 Collapsed Left Upper Lobe. A, Posteroanterior chest radiograph (CXR). B, Lateral CXR. The ground-glass haze over the left hemithorax is
typical of a partially collapsed left upper lobe. In more than 50% of patients with collapsed lobes, loss of volume is evidenced by left hemidiaphragmatic
elevation; the mediastinum is shifted to the left and the left hilum is pulled cranially. Also, the left main bronchus deviates cranially. Calcification in
the left hilar mass represents an unrelated, old granulomatous infection. In panel B, the density from the left hilum down toward the anterior portion
of the chest represents the partially collapsed left upper lobe. The radiolucency substernally is the right lung.
detected. Bronchial angiography is used for suspected bron- unilateral and regional pulmonary function in surgical candi-
chial arterial bleeding in massive hemoptysis. Radionuclide dates for lung resection.
lung scans are used in the diagnosis of pulmonary embolism,
although CT angiography is used increasingly more often. Pulmonary angiography, bronchial angiography, and
Quantitative radionuclide scans may be useful in assessing radionuclide scans are useful in diagnosing lung pathology.
A B
Figure 17.2 Collapsed Left Lower Lobe. A, Posteroanterior chest radiograph (CXR). B, Lateral CXR. Note nodule in left midlung field plus collapsed
left lower lobe, seen as a density behind the heart. This entity represents 2 separate primary lung cancers: synchronous bronchogenic carcinomas. Do
not stop with the first evident abnormality, such as the nodule in the midlung field, without looking carefully at all other areas. Panel B shows an
increased density over the lower thoracic vertebrae without an obvious wedge-shaped infiltrate. Over the anterior portion of the hemidiaphragm, the
small wedge-shaped infiltrate is not fluid in the left major fissure because the left major fissure is pulled away posteriorly. Instead, it is an incidental
normal variant of fat pushed up into the right major fissure.
226 P U L M O N A RY D I S E A S E S
A B
Figure 17.3 Collapsed Right Upper Lobe. A, Posteroanterior chest radiograph (CXR). B, Lateral CXR. Panel A shows classic reversed S mass in
the right hilus with partial collapse of the right upper lobe. Loss of volume is evident with the elevation of the right hemidiaphragm. In panel B, the
partially collapsed right upper lobe is faintly seen in the upper anterior portion of the hemithorax (arrow).
P U L MO NA RY F U N C T I O N T E S TS
indicates limitation to full expansion of the lungs (eg, as in
large pleural effusion or disease in the lung parenchyma, chest
The main indication for PFTs is dyspnea. Results of PFTs do wall, or diaphragm). A combination of obstructive and restric-
not provide a diagnosis of lung disease, but they are useful in tive patterns is also possible (eg, as in COPD with pulmonary
assessing the mechanical function of the respiratory system fibrosis). An increase in flow rates (ie, >12% and 200 mL) after
and quantifying lung function. PFTs can be used to distin- bronchodilator therapy suggests reversible component airway
guish obstruction, which indicates airflow limitation (eg, as in disease, although the absence of response does not preclude a
asthma, bronchitis, and emphysema), from restriction, which clinical trial with inhaled bronchodilator medications.
A B
Figure 17.4 Collapsed Right Lower Lobe. A, Posteroanterior chest radiograph (CXR). B, Lateral CXR. This 75-year-old male smoker had hemoptysis
for 1.5 years; his CXR had been read as normal on several occasions. In panel A, note the linear density (arrows) projecting downward and laterally
along the right border of the heart. It projects below the diaphragm and is not a normal line. Also, the right hilum is not evident; it has been pulled
centrally and downward because of carcinoma obstructing the bronchus of the right lower lobe. Note the very slight shift in the mediastinum to
the right, indicative of a loss of volume. In panel B, in spite of a notable collapse of the right lower lobe, this collapse is represented by only a subtle
increased density over the lower thoracic vertebrae.
17. C O M M O N P U L M O N A RY D I S O R D E R S 227
A B
Figure 17.5 Effusion. A, Posteroanterior chest radiograph (CXR). B, Decubitus CXR. In panel A, an elevated right hemidiaphragm is actually an
infrapulmonic (or subpulmonic) effusion, as seen in panel B. For unknown reasons, a meniscus is not formed in some people with infrapulmonic
pleural effusion. Thus, a seemingly elevated hemidiaphragm should be examined with the suspicion that it could be infrapulmonic effusion.
Subpulmonic effusion occurs more frequently in patients with nephrotic syndrome. Decubitus CXR or ultrasonography would disclose the free fluid.
PFTs are useful in distinguishing between obstruction and of expiration (FEV1) from baseline is considered a positive test
restriction. result, although up to 10% of healthy subjects show a positive
response to an inhalational challenge. A negative test is helpful
in ruling out hyperreactive airway disease. A false-positive test
Provocation Inhalational Challenge
can result from airway hyperreactivity from recent infection or
Provocation inhalational challenge with bronchospastic agents inflammation.
(eg, methacholine, exercise, etc) is useful when the diagno-
sis of asthma or hyperreactive airway disease is uncertain. A A positive result with provocation is a 20% decrease in
20% decrease in forced expiratory volume in the first second FEV1 from baseline.
A B
Figure 17.6 Embolism. A, Prepulmonary embolism on normal posteroanterior chest radiograph (CXR). B, Pulmonary embolism. The CXR is read
as normal in up to 30% of patients with angiographically proven pulmonary embolism. In comparison with panel A, panel B shows a subtle elevation
of the right hemidiaphragm. In panel A, the right and left hemidiaphragms are equal. In some series, an elevated hemidiaphragm is the most common
finding with acute pulmonary embolism. Also, note the plumpness of the right pulmonary artery, prominent pulmonary outflow tract on the left
(arrow in panel B), and subtle change in cardiac diameter. The patient was a 28-year-old man who was in shock from massive pulmonary emboli as a
result of major soft tissue trauma produced by a motorcycle accident 7 days earlier.
228 P U L M O N A RY D I S E A S E S
A B
Figure 17.7 Asbestos Exposure. The patient was a 68-year-old asymptomatic man who smoked. A, Abnormal chest radiograph shows areas of
pleural calcification (small arrows), particularly on the right hemidiaphragm. This is a tip-off to previous asbestos exposure. The process in the left
midlung was worrisome (large arrow), perhaps indicating a new process such as bronchogenic carcinoma. B, Computed tomography disclosed
rounded atelectasis (small arrow). The comma extending from this mass is characteristic of rounded atelectasis, which is the result of subacute to
chronic pleural effusion resolving and trapping lung as it heals. Pleural calcification is apparent (large arrow).
17. C O M M O N P U L M O N A RY D I S O R D E R S 229
A B
Figure 17.10 Coarctation. A and B, Posteroanterior chest radiographs showing coarctation with a tortuous aorta mimicking a mediastinal mass. This
occurs in about one-third of patients with coarctation. Rib notching is indicated by the arrows in panel B.
Figure 17.11 Histiocytosis X (or Eosinophilic Granuloma). Extensive Figure 17.12 Sarcoidosis in a 35-Year-Old Patient. This chest
change is predominantly in the upper two-thirds of the lung fields. radiograph shows the predominant parenchymal pattern seen in the
Eventually 25% of the patients have pneumothorax, as seen on this chest upper two-thirds of the lungs in many patients with stage II or III
radiograph (right side). The honeycombing, also described as microcysts, sarcoidosis. The pattern can be interstitial, alveolar (which this one is
is characteristic of advanced histiocytosis X. predominantly), or a combination. There probably is some residual
adenopathy in the hila and right paratracheal area.
230 P U L M O N A RY D I S E A S E S
A
17. C O M M O N P U L M O N A RY D I S O R D E R S 231
A B
Figure 17.16 Kerley B Lines. These 2 examples can be helpful in interpreting chest radiographs. A, Kerley B lines are shown in a 75-year-old man with
colon cancer. B, The Kerley B lines are from metastatic adenocarcinoma of the colon; they were a tip-off that the parenchymal process in this patient
resulted from metastatic carcinoma and not from a primary pulmonary process such as pulmonary fibrosis, which was the working diagnosis.
232 P U L M O N A RY D I S E A S E S
A B
Figure 17.19 Pancoast Tumor. A, Subtle asymmetry at the apex of the right lung. The patients symptoms at the time of the initial chest radiography
were attributed to a cervical disk. B, The asymmetry was more obvious 3.5 years later when the Pancoast lesion (primary bronchogenic carcinoma) was
diagnosed.
A B
Figure 17.20 Bronchial Carcinoid. The adage that not all that wheezes is asthma should be remembered every time a patient with asthma is
encountered and the condition does not seem to improve. A, In this patient, wheezes were predominant over the left hemithorax. B, The forced
expiration film showed air trapping in the left lung. Bronchial carcinoid of the left main bronchus was diagnosed at bronchoscopy.
A B
Figure 17.21 Adenocarcinoma. A, A solitary pulmonary nodule is evident below the right hemidiaphragm, where at least 15% of the lung is obscured.
B, Tomography shows that the nodule has a discrete border but is noncalcified. It was not present 18 months earlier.
17. C O M M O N P U L M O N A RY D I S O R D E R S 233
A B
Figure 17.22 Infiltrate. A, Solitary infiltrate in the left upper lobe with air bronchogram, as evident on tomography or computed tomography. B, Air
bronchogram should be considered a sign of bronchoalveolar cell carcinoma or lymphoma until proved otherwise.
A B
Figure 17.23 Granuloma. A and B, Tomography of solitary pulmonary nodules shows characteristic satellite nodules (arrows).
234 P U L M O N A RY D I S E A S E S
A
17. C O M M O N P U L M O N A RY D I S O R D E R S 235
3. Look at the ratio of FEV1 to forced vital capacity (FVC). tests airflow through major airways and muscle strength.
An FEV1/FVC ratio <70% suggests airflow obstruction. Disproportionately reduced MVV (MVV = FEV1
FEV1 is used to classify the severity of airflow obstruction 35) may be from poor effort, variable extrathoracic
(Table 17.3). obstruction, and respiratory muscle weakness. Respiratory
muscle weakness can be assessed by maximum inspiratory
4. If FEV1/FVC is >70% but FEV1 is reduced, look at total
pressure (Pimax) and maximum expiratory pressure
lung capacity (TLC). Reduced TLC suggests a restrictive
(Pemax). Clinical features should be correlated with the
defect (Table 17.3).
results of PFTs.
5. TLC, functional residual capacity (FRC), and residual
9. Diffusing capacity of lung for carbon monoxide (Dlco)
volume (RV) indicate volumes. TLC = VC (vital
is dependent on the thickness of the alveolocapillary
capacity) + RV. Increases in TLC and RV suggest
membrane (T), the area of the alveolocapillary membrane
hyperinflation (asthma or COPD). If TLC and VC are
(A), and the pressure difference between alveolar gas and
decreased, consider restrictive lung disease (fibrosis) or
venous blood (Pco). Thus, Dlco is represented by the
loss of lung volume (surgery, diaphragmatic paralysis, or
following:
skeletal problems).
6. VC measured during a slow (not forced) expiration is A Pco
Dlco =
not affected by airway collapse in COPD. FVC may be T
low with forced expiration because of airway collapse. In
healthy subjects, VC = FVC. a. Low Dlco
7. FEV1 and forced expiratory flow (FEF) of the 1) Anatomical emphysema (decreased A)
midexpiratory phase (FEF25%-75%) indicate flow rates. Flow 2) Anemia (effectively decreased A) (a decrease in
rates are diminished in COPD, but smaller decreases can hemoglobin by 1 g/dL diminishes Dlco by 7%)
occur if lung volumes are low.
3) Restrictive lung diseases (decreased A or decreased
8. The maximal voluntary ventilation (MVV) test requires T in pulmonary fibrosis or other interstitial lung
rapid inspiratory and expiratory maneuvers and, thus, diseases)
4) Pneumonectomy (decreased A)
Table 17.3 INTERPRETATION OF PULMONARY 5) Pulmonary hypertension (effectively decreased T)
FUNCTION TESTING
6) Recurrent pulmonary emboli (effectively
Obstruction is indicated by FEV1/FVC <70% decreased A)
FEV1, Percentage of Severity of Airflow b. Increased Dlco
Predicted Value Obstruction
1) Supine posture (increased A due to increased
>80 Borderline blood volume in upper lobes)
<80 & >60 Mild 2) Exercise (increased A due to increased blood
<60 & >40 Moderate
volume)
Restriction is indicated by TLC <80% of predicted value (restrictive 4) Obesity (increased A due to increased blood
defect is only suggested by reduced vital capacity; TLC is needed volume)
for confirmation)
5) Left-to-right shunt (increased A)
TLC, Percentage of Predicted Severity of Restrictive
Value Defect 6) Some patients with asthma
<80 & >60 Mild c. Isolated low Dlco (with normal PFT results)
<60 & >50 Moderate 1) Pulmonary hypertension
<50 Severe 2) Multiple pulmonary emboli
Bronchodilator response requires both 12% & 200-mL improvement in 3) Combined diseases such as pulmonary fibrosis
FEV1 after bronchodilator therapy with COPD
Methacholine challenge requires 20% decrease in FEV1 after challenge 4) Anemia
to be considered positive
10. Flow-volume curves are helpful to distinguish
Abbreviations: FEV1, forced expiratory volume in the first second of expiration; between intrathoracic and extrathoracic major airway
FVC, forced vital capacity; TLC, total lung capacity. obstructions. Flattening of the expiratory flow curve with
236 P U L M O N A RY D I S E A S E S
a normal inspiratory flow curve suggests intrathoracic Patient 4
airway obstruction. Flattening of the inspiratory flow As indicated by the FEV1/FVC ratio and FEV1, there is a
curve alone suggests extrathoracic airway obstruction. moderately severe airflow obstruction. The normal TLC and
Flattening of both flow curves suggests fixed airway residual volume suggest an absence of air trapping. The normal
obstruction, and the location cannot be determined. Dlco excludes anatomical emphysema or other parenchymal
problems. Bronchodilator testing elicited improvement in lung
volumes and flow rates. The clinical diagnosis is typical asthma.
Explanations for Table 17.4 Patient 5
Patient 1 This patient has normal lung volumes and flow rates (80%-
The patient has typical features of emphysema. The FEV1/ 120% of predicted normal). A former athlete, he recently noted
FVC ratio indicates obstruction. The FEV1 indicates that the cough and chest tightness after exertion. Previous PFT results
obstruction is severe. The TLC indicates hyperinflation. The were unavailable. The following are important points: 1) In a
reduced Dlco suggests emphysema. The clinical diagnosis is young, otherwise healthy patient, the lung volumes and flow
severe obstructive disease with anatomical emphysema. rates are usually above normal and even higher in an athlete. 2)
This patient may have had very high volumes and flow rates in
Patient 2 the past, but without previous PFT results, no comparison can
The PFT results suggest emphysema. In a young non- be made (if earlier PFT results were available, the new results
smoker, other causes of emphysema must be considered. The might represent a severe decrease in pulmonary function).
clinical diagnosis is severe emphysema caused by familial defi- 3) The history suggests the possibility of exercise-induced
ciency of 1-antitrypsin. asthma; spirometry after an exercise test showed a 28% reduc-
tion in flow rates 5 to 10 minutes after exercise ended. 4) Note
Patient 3 the relatively high Dlco, a phenomenon seen in patients with
Flow rates and lung volumes are decreased only slightly but asthma. The clinical diagnosis is exercise-induced asthma.
are within normal limits. MVV is severely decreased. In this
patient, Pimax and Pemax were severely decreased, suggesting Patient 6
muscle weakness. The clinical diagnosis is severe thyrotoxicosis This patient has a moderately severe decrease in lung vol-
with proximal muscle weakness (ie, thyrotoxic myopathy). This umes and normal flow rates. MVV is normal, but Dlco is
pattern of PFT results can also occur in neuromuscular diseases severely diminished. These results suggest severe restrictive
such as amyotrophic lateral sclerosis and myasthenia gravis. lung disease. The slightly diminished flow rates are the result of
Table 17.4 TRY TO INTERPRET THESE RESULTS OF PULMONARY FUNCTION TESTS BEFORE READING THE
EXPLANATIONS
PATIENT
FEATURE 1 2 3 4 5 6 7 8 9
Age, y/sex 73/M 43/M 53/F 43/M 20/M 58/F 40/M 28/F 44/M
Weight, kg 52 53 50 63 80 59 75 52 148
Tobacco, PY 63 NS NS NS NS NS NS NS NS
FEV1/FVC, % 40 34 80 40 85 88 50 85 78
a
FEF25%-75%,% 18 14 80 35 88 82 24 102 88
Abbreviations: Dlco, diffusing capacity of lung for carbon monoxide; FEF25%-75%, forced expiratory flow of the midexpiratory phase; FEV1, forced expiratory volume in the
first second of expiration; FVC, forced vital capacity; NS, nonsmoker; PY, pack-years of smoking.
a
Percentage of the predicted value. Values of 80% to 120% are considered normal.
17. C O M M O N P U L M O N A RY D I S O R D E R S 237
decreased lung volumes. The clinical diagnosis is biopsy-proven Lung biopsy may be indicated in the evaluation of diffuse
idiopathic pulmonary fibrosis. Patients who have had lung lung disease.
resection also have low lung volumes and decreased Dlco.
Patient 7 O B S T RU C T I VE LU N G D I S E A S E S
The reduction in the FEV1/FVC ratio suggests the presence
of obstructive dysfunction. TLC is also decreased, which sug- Obstructive lung diseases include emphysema, bronchitis,
gests additional restrictive lung disease. MVV is also reduced, asthma, bronchiectasis, CF, bronchiolitis, bullous lung dis-
and Dlco is severely decreased. Compared with patient 6, ease, and airway stenosis. The 3 most prevalent obstructive
this patient has obstructive disease plus severe restrictive lung lung diseases are emphysema, chronic bronchitis, and asthma.
disease. A very low Dlco suggests parenchymal disease. CXR Several features are useful for distinguishing these 3
showed bilaterally diffuse nodular interstitial changes, espe- diseases:
cially in the upper two-thirds of the lungs. Biopsy specimens
of the bronchial mucosa and lung showed extensive endobron- 1. Age at onsetasthma: younger than 30 years;
chial sarcoidosis. The clinical diagnosis is severe restrictive bronchitis: 50 or older; emphysema: 60 or older
lung disease from parenchymal sarcoidosis and obstructive 2. Use of tobaccoasthma: no; bronchitis and
dysfunction caused by endobronchial sarcoidosis. emphysema: yes
Patient 8 3. Patternasthma: paroxysmal; bronchitis and
This patient has normal lung volumes and flow rates. MVV emphysema: chronic and progressive
is slightly decreased but within normal limits. Dlco is very
4. Sputumasthma: absent or minimal; bronchitis:
low. Pao2 is 56 mm Hg. The clinical diagnosis is primary pul-
increased; emphysema: minimal or increased
monary hypertension.
5. CXR findingsasthma: usually normal; bronchitis:
Patient 9 increased lung markings; emphysema: hyperinflation
This extremely obese patient has normal lung volumes and
flow rates. Dlco is abnormally high. Abnormally high Dlco 6. Paco2asthma: normal or decreased during attack;
is reported to be a result of increased VC. The clinical diagno- bronchitis: increased; emphysema: normal or increased
sis is obesity-related pulmonary dysfunction. 7. Pao2asthma: normal or decreased during attack;
bronchitis and emphysema: low
238 P U L M O N A RY D I S E A S E S
Box 17.2 PRACTICAL ASPECTS OF MANAGING COPD BU L L O US LU N G D I S E A S E
Bullous changes may be seen in Marfan and Ehlers-Danlos
Steps in management syndromes, burned-out sarcoidosis, and cadmium exposure,
1. Identify type of COPD although small apical bullae are often present in healthy
2. Identify pathophysiology persons. Bullous lung disease is associated with an increased
3. Assess lung dysfunction risk of lung cancer. Complications include pneumothorax,
4. Eliminate causative or exacerbating factors COPD, infection, formation of lung abscess, bleeding into a
5. Aim drug therapy at underlying pathophysiology bulla, and compression of adjacent normal lung. Surgical ther-
6. Anticipate & treat complications apy may improve lung function by 5% to 10% in 10% to 15%
7. Enroll patient in a rehabilitation program of patients.
8. Educate patient & family
Stepped-care approach
Mild COPD (FEV1/FVC <70%; FEV1 80% of predicted ASTHMA
value): short-acting bronchodilator as needed Asthma is discussed in Chapter 42 (Asthma).
Moderate COPD (FEV1/FVC <70%; 50% FEV1 <80% of
predicted value): scheduled use of long-acting bronchodila-
tor, short-acting bronchodilator as needed, rehabilitation T R E AT M E N T O F C O P D
Severe COPD (FEV1/FVC <70%; 30% FEV1 <50% of pre-
dicted value): scheduled use of bronchodilators with or with-
The therapeutic approach to COPD consists of reducing
out inhaled corticosteroids if repeated exacerbations or lung
risk factors (eg, smoking cessation), identifying the sever-
function response, short-acting bronchodilator as needed,
ity of COPD, quantifying the pulmonary dysfunction and
rehabilitation
response to bronchodilator therapy, selecting appropriate
Very severe COPD (FEV1/FVC <70%; FEV1 <30% of pre-
bronchodilators, anticipating and appropriately treating
dicted value or presence of respiratory failure or right heart
complications, and educating the patient and family about
failure): regular use of bronchodilators with or without
long-term therapy. Proper inhalation technique is essential in
inhaled corticosteroids, rehabilitation, long-term oxygen if
optimal treatment. Practical aspects of managing COPD are
respiratory failure; consider surgical treatments
outlined in Box 17.2.
17. C O M M O N P U L M O N A RY D I S O R D E R S 239
effect lasting 34 hours). The dosage should be tailored Phosphodiesterase Inhibitors
on the basis of clinical features and potential side effects.
Adverse effects include tremor, anxiety, restlessness, tachy- The use of phosphodiesterase inhibitors (eg, theophylline) has
cardia, palpitations, increased blood pressure, and cardiac diminished with the increased use of -agonists because phos-
arrhythmias. Side effects are more likely in the presence of phodiesterase inhibitors have a narrow therapeutic window,
cardiovascular, liver, or neurologic disorders and in elderly wide range of toxic effects (eg, cardiac arrhythmias and grand
patients. Rarely, paradoxical bronchospasm may result from mal seizures), and interactions with other drugs. Nevertheless,
tachyphylaxis (a rapidly decreasing response to a drug after theophylline increases the contractility of respiratory muscles
a few doses) or from exposure to preservatives and propel- in a dose-related fashion. The effects of various substances and
lants. A newer single-isomer -agonist, levalbuterol, binds circumstances on the clearance of theophylline are shown in
to -adrenergic receptors with 100-fold greater affinity than Box 17.3.
albuterol. Metered dose inhalers are just as effective as nebu-
lized medications, but the total dose of medication is higher Theophylline use has substantially decreased owing to
in the nebulized formulation. safety concerns.
240 P U L M O N A RY D I S E A S E S
Oral corticosteroids are useful in acute COPD The most common bacterial respiratory agents in COPD
exacerbations. patients are Haemophilus influenzae, Moraxella catarrhalis,
and Streptococcus pneumoniae.
Inhaled corticosteroids may be indicated for selected
patients with moderate to severe COPD.
C YS T I C F I B R O S I S
17. C O M M O N P U L M O N A RY D I S O R D E R S 241
and lower respiratory tract infections, intensive nutritional C AUS E S A N D A S S O C I AT I O N S O F
support, and conditioning. Poor prognostic factors include B RO N C H I E C TA S I S
female sex, residence in a non-Northern climate, pneumotho-
In adults, many cases of bronchiectasis are related to adeno-
rax, hemoptysis, recurrent bacterial infections, presence of
viral or bacterial infections (measles, influenza, adenovirus,
Burkholderia cepacia, and systemic complications. Respiratory
or pertussis) in childhood. Various infections, including
therapy for CF includes management of obstructive lung
Mycoplasma pneumoniae, nontuberculous mycobacteria, and
disease and respiratory infections, chest physiotherapy, pos-
anaerobic organisms, have also been associated with bron-
tural drainage, immunization against influenza, hydration,
chiectasis. Tuberculosis is a common cause of bronchiectasis,
and deoxyribonuclease therapy. Although systemic gluco-
particularly in the upper lobes. Occasionally, chronic histo-
corticoids are administered during acute exacerbations or to
plasmosis and coccidioidomycosis cause bronchiectasis. In
patients who have allergic bronchopulmonary aspergillosis,
patients with chronic stable bronchiectasis, P aeruginosa is the
routine use has been associated with notable side effects and
predominant organism in respiratory secretions.
is not recommended. If patients with CF have decreased FEV1
Ciliary dyskinesia is also associated with the development
or evidence of chronic airway inflammation, and if sputum
of bronchiectasis. Primary ciliary dyskinesia (PCD), which
examination does not show nontuberculous mycobacteria,
results from abnormal motion of cilia, causes many clinical
treatment with azithromycin (500 mg 3 times weekly) appears
problems, including nasal polyps, sinusitis, inner ear infec-
to improve FEV1 and decrease the frequency of pulmonary
tion or deafness, and chronic bronchitis or bronchiectasis.
exacerbations. The risk of death from CF is 38% to 56% within
Kartagener syndrome, an autosomal recessive disorder, is an
2 years when FEV1 has reached 20% to 30% of the predicted
example of PCD. Acquired ciliary defects occur in smokers,
value. Bilateral lung transplant is an option for patients with
in patients with bronchitis, and in patients who have had
declining lung function. The 5-year survival rate is between
viral infections. Both hypogammaglobulinemia and agamma-
40%-60%. The presence of B cepacia, however, is a contraindi-
globulinemia are also associated with bronchiectasis. Central
cation for transplant.
bronchiectasis is present in 85% of patients with allergic bron-
chopulmonary aspergillosis (ABPA) at the time of the initial
Due to improvement in treatments, the lifespan for diagnosis and has been used as a diagnostic criterion of the dis-
patients with CF has increased. ease. Uncommon causes of bronchiectasis include yellow nail
The 5-year survival rate after bilateral lung transplant is syndrome, 1-antitrypsin deficiency, Felty syndrome, inflam-
40%-60%. matory bowel disease, toxic inhalation, and chronic tracheo-
bronchial stenosis.
242 P U L M O N A RY D I S E A S E S
physiotherapy, humidification, bronchodilators, and cyclic Box 17.4 PRINCIPAL CAUSES OF PLEURAL EFFUSION
antibiotic therapy are effective in many patients. Surgical
treatment is reserved for patients with troublesome symp- Osmotic-hydraulica
toms, localized disease, and severe hemoptysis. High-dose Congestive heart failure
inhaled corticosteroid therapy (fluticasone) is reportedly Superior vena caval obstruction
effective in reducing the sputum inflammatory indices in Constrictive pericarditis
bronchiectasis. Cirrhosis with ascites
Hypoalbuminemia
Treatment of bronchiectasis consists of identifying and Salt-retaining syndromes
treating underlying conditions, controlling symptoms, and Peritoneal dialysis
preventing complications. Hydronephrosis
Nephrotic syndrome
Infectionsb
PLEUR AL EFFUSION Parapneumonic (bacterial) effusions
Bacterial empyema
Excess pleural fluid collects in the pleural space when fluid Tuberculosis
accumulation exceeds removal mechanisms. Hydrostatic, Fungi
oncotic, and intrapleural pressures regulate fluid movement in Parasites
the pleural space. Any of the following mechanisms can pro- Viruses & mycoplasma
duce pleural effusion: Neoplasmsb
Primary & metastatic lung tumors
1. Changes in capillary permeability (inflammation) Lymphoma & leukemia
2. Increased hydrostatic pressure Benign & malignant pleural tumors
Intra-abdominal tumors with ascites
3. Decreased plasma oncotic pressure Vascular diseaseb
4. Impaired lymphatic drainage Pulmonary embolism
Wegener granulomatosis
5. Increased negative intrapleural pressure Intra-abdominal diseasesb
Pancreatitis & pancreatic pseudocyst
6. Movement of fluid (through diaphragmatic pores and
Subdiaphragmatic abscess
lymphatic vessels) from the peritoneum
Malignancy with ascites
Meigs syndromea
The principal causes of pleural effusion are listed in
Hepatic cirrhosis with ascitesa
Box 17.4. The diagnosis may be suggested by certain charac-
Traumab
teristics of the effusion. For example, obvious pus suggests
Hemothorax
empyema; an elevated salivary amylase level with pleural fluid
Chylothorax
acidosis suggests esophageal rupture; and a ratio of pleural
Esophageal rupture
fluid hematocrit to blood hematocrit greater than 0.5 sug-
Intra-abdominal surgery
gests hemothorax. On the basis of clinical suspicion, testing
Miscellaneous
of the effusion should be selective. Despite extensive testing
Drug-induced effusionsb
of pleural fluid, the causes of up to one-third of pleural effu-
Uremic pleuritisb
sions remain unknown.
Myxedemaa
Yellow nail syndromeb
Pleural effusion results when fluid accumulation exceeds
Dressler syndromeb
the bodys removal mechanisms.
Familial Mediterranean feverb
The causes of up to one-third of pleural effusions remain a
Usually a transudate.
unknown, even after extensive testing.
b
Usually an exudate.
D I S T I N GU I S H I N G A N E XU DAT E FRO M A
T R A N S U DAT E 3. Pleural fluid LDH greater than two-thirds of the upper
limit of the reference range for serum LDH
Traditionally, an effusion with any one of the following is con-
sidered an exudate: A meta-analysis found that any one of the following find-
ings can also be used to identify the fluid as an exudate:
1. Ratio of pleural fluid protein to serum protein >0.5
1. Pleural fluid protein >2.9 g/dL
2. Ratio of pleural fluid lactate dehydrogenase (LDH) to
serum LDH >0.6 2. Pleural fluid cholesterol >45 mg/dL
17. C O M M O N P U L M O N A RY D I S O R D E R S 243
3. Pleural fluid LDH >60% of the upper limit of the pancreatitis, pulmonary embolism with infarctions, and other
reference range for serum LDH conditions. A bloody effusion in lung cancer usually denotes
pleural metastasis, even if the cytologic results are negative.
It is not necessary to perform all the above tests to differen- Pleural fluid eosinophilia (>10%) is nonspecific and occurs
tiate a transudate from an exudate. Clinically, it is more useful in trauma, pulmonary infarction, psittacosis, drug-induced
to classify the cause by considering the source (organ system) effusion, pulmonary infiltrate with eosinophilia-associated
of the fluid (Box 17.4). The most common cause of a transu- effusions, benign asbestos pleural effusion, and malignancy.
date is congestive heart failure (pulmonary artery wedge pres- Pleural fluid lymphocytosis occurs in tuberculosis, chronic
sure >25 mm Hg). The most common cause of an exudate is effusions, lymphoma, sarcoidosis, chylothorax, and some col-
pneumonia (parapneumonic effusion). lagenoses (eg, yellow nail syndrome and chronic rheumatoid
pleurisy).
The most common cause of a transudate is congestive heart
failure. Cytology
The most common cause of an exudate is pneumonia. Cytologic examination is an important test in most adults with
an unknown effusion. Positive fluid cytologic findings in pri-
mary lung carcinoma imply unresectability (stage IIIB disease).
P L EU R A L FLU I D PA R A M ET E R S
Glucose and pH Cultures
The pleural fluid glucose concentration and pH usually change In tuberculosis, it is important to culture pleural biopsy speci-
in tandem (ie, if the glucose concentration is low, the pH is mens. Tuberculous effusions yield positive cultures in less
low). Glucose levels are low (fluid glucose <60 mg/dL or ratio than 15% of cases. Pleural biopsy has a higher (>75%) diag-
of fluid glucose to plasma glucose <0.5) in rheumatoid effu- nostic yield in tuberculosis. The adenosine deaminase and
sion, malignant mesothelioma, systemic lupus erythemato- interferon- levels are increased in tuberculous pleural effu-
sus, esophageal rupture, tuberculous pleurisy, and empyema. sion. Cultures have poor yields in viral infections.
Pleural fluid pH is less than 7.30 in empyema, esophageal
rupture, rheumatoid effusion, tuberculosis, malignancy, and
trauma. A parapneumonic effusion with pH less than 7.20 Pleural Biopsy
likely represents empyema, and drainage with a chest tube Pleural biopsy is indicated if tuberculous pleural disease is sus-
should be considered. Empyema caused by Proteus species pected. Pleural biopsy through a thoracoscope improves the
produces a pH greater than 7.8 (because of the production of diagnostic yield of pleural effusions.
ammonia).
If pH is <7.2 and clinical suspicion for infection is high,
Amylase drainage for suspected empyema should be considered.
The concentration of amylase in the pleural fluid is increased Pleural fluid amylase is increased in esophageal rupture.
in esophageal rupture because of leakage of salivary amylase.
A mnemonic for the causes of chylous effusions is 5Ts:
In any unexplained left-sided effusion, consider pancreatitis
thoracic duct, trauma, tumor (lymphoma), tuberculosis,
and measure the amylase level in the pleural fluid.
and tuberous sclerosis (lymphangiomyomatosis).
S L E E P -R E L AT E D B R E AT H I N G D I S O R D E R S
Cell Counts
A hemorrhagic effusion (pleural fluid hematocrit >50% of Sleep-related breathing disorders encompass various abnor-
serum hematocrit) is seen in trauma, tumor, asbestos effusion, mal breathing patterns that occur during sleep. Complications
244 P U L M O N A RY D I S E A S E S
include sleepiness and increased cardiovascular morbidity and OSA has been associated with multisystemic dysfunction
mortality (Box 17.5). (Box 17.5). Several studies suggest that there is an increase
in postoperative complications and overall mortality among
patients with untreated OSA.
O B S T RU C T I V E S L E E P A P N E AH Y P O P N E A
S Y N D RO M E
The diagnosis of OSA is made with overnight
Obstructive sleep apnea (OSA) is defined as periodic cessa- polysomnography.
tion of airflow (duration 10 seconds) due to obstruction
Overnight oximetry is neither sensitive nor specific
of the upper airway during sleep with continued respiratory
for OSA.
effort. Typically, the episode is terminated with a temporary
arousal from sleep and return of normal upper airway pat- Untreated OSA is associated with increased postoperative
ency. Hypopnea is defined as reduction in airflow for at least complications and mortality.
10 seconds, usually with resultant desaturation of at least 4%.
Hypopnea is also typically terminated by an arousal. Such
periodic episodes of apnea and hypopnea usually result in CENTRAL SLEEP APNEA
fragmented sleep and periodic desaturations. OSA should
be suspected in patients who are obese, have increased neck Central sleep apnea (CSA) is defined as periodic cessation of
circumference, are known to snore, and complain of daytime airflow (duration 10 seconds) during sleep in the absence
sleepiness. An overnight polysomnogram is required to make of upper airway obstruction, and presumably it is caused by
the diagnosis of OSA, which is defined as having more than 5 lack of respiratory muscle stimulation. In contrast to OSA,
episodes of apnea and hypopnea per hour of sleep. Although airflow is gradually resumed and is not always associated with
overnight oximetry may suggest the presence of OSA, it is an arousal from sleep. CSA may occur in persons with neu-
neither sensitive enough to rule out the diagnosis nor specific rologic abnormalities (eg, cerebrovascular accident, amyo-
enough to confirm it. trophic lateral sclerosis, and postpolio syndrome), endocrine
dysfunctions (eg, acromegaly and hypothyroidism), conges-
tive heart failure, or narcotic use, or it may be idiopathic.
The respiratory pattern, which cycles between crescendo and
Box 17.5 SYSTEMIC DISORDERS THAT HAVE BEEN decrescendo respirations followed by a pause, is known as
ASSOCIATED WITH SLEEP-RELATED BREATHING Cheyne-Stokes respiration or periodic respiration and is often
DISORDERS seen in persons with congestive heart failure (especially dur-
ing acute exacerbation), at high altitude, and after a cerebro-
Central nervous system vascular event.
Cerebrovascular accidents
Cognitive impairments CSA is periodic cessation of airflow without upper airway
Excessive sleepiness obstruction.
Lower seizure threshold
Recurrent headaches Cheyne-Stokes respiration is associated with congestive
Cardiovascular system heart failure, high altitude, and stroke.
Myocardial infarcts
Hypertension S L E E P H Y P O V E N T I L AT I O N S Y N D RO M E
Cardiac arrhythmia
Acceleration of atherosclerosis Sleep hypoventilation syndrome is characterized by a reduction
Pulmonary hypertension in minute ventilation, resulting in hypercapnia and usually
Endocrine system hypoxemia during sleep. Features include daytime hyper-
Insulin insensitivity capnia, pulmonary hypertension, and cor pulmonale. Most
Suppression of growth hormone release affected persons are obese (obesity-hypoventilation syndrome)
Alteration of progesterone & testosterone release or have severe respiratory or neurologic disease.
Obesity
Gastrointestinal tract
Gastroesophageal reflux disease T R E AT M E N T
Respiratory system Patients with these sleep disorders are treated with nonin-
Hypercapnia vasive positive pressure devices, such as continuous positive
Dyspnea airway pressure (CPAP) and bilevel positive airway pressure
Reduced exercise tolerance (BiPAP) devices. Adequate titration can be achieved during a
Psychiatric polysomnogram, but, in certain circumstances, an autotitrat-
Depression ing CPAP device may be used. In severe cases, tracheostomy
Insomnia may be required. Treatment of CSA may require a special
Nocturnal panic disorders positive airway pressure device such as BiPAP or adaptive
17. C O M M O N P U L M O N A RY D I S O R D E R S 245
servo-ventilator. Weight loss is also helpful in the treatment of bronchodilators, anticipating and appropriately treating
OSA and sleep hypoventilation syndrome in overweight and complications, and educating the patient and family about
obese patients. long-term therapy.
CF is caused by a mutation in CFTR. CF affects
Noninvasive positive pressure devices are used to treat
all exocrine glands except sweat glands. Common
these sleep disorders.
manifestations of CF include sinusitis, nasal polyposis,
Weight loss is recommended for overweight and obese bronchiectasis, obstructive airway disease, pancreatic
patients with OSA and sleep hypoventilation syndrome. insufficiency, biliary disease, and male infertility.
The most common cause of a transudate is congestive heart
failure. The most common cause of an exudate is pneumonia.
S U M M A RY
OSA is diagnosed with overnight polysomnography.
PFTs are useful in distinguishing between obstruction and Overnight oximetry is neither sensitive nor specific
restriction. for OSA. Untreated OSA is associated with increased
postoperative complications and mortality.
The therapeutic approach to COPD consists of reducing
risk factors (eg, smoking cessation), identifying the severity CSA is periodic cessation of airflow without upper airway
of COPD, quantifying the pulmonary dysfunction and obstruction. Cheyne-Stokes respiration is associated with
response to bronchodilator therapy, selecting appropriate congestive heart failure, high altitude, and stroke.
246 P U L M O N A RY D I S E A S E S
PA RT I V
INFECTIOUS DISEASES
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18.
INFECTIONS IN THE IMMUNOCOMPROMISED HOST,
RECOGNITION AND MANAGEMENT OF BIOTERRORISM
INFECTIONS, AND INFECTIOUS SYNDROMES CAUSED BY
SPECIFIC MICROORGANISMS
Pritish K. Tosh, MD, M. Rizwan Sohail, MD, and Elie F. Berbari, MD
249
Bacteremia due to anaerobic organisms is uncommon, Table 18.1 OPPORTUNISTIC INFECTIONS IN SOLID
except in cases of perirectal abscess, gingivitis, or neutropenic ORGAN TRANSPLANT
enterocolitis (typhlitis). Persistent fever and abdominal symp-
MONTH TYPE OF INFECTION AFTER TRANSPLANT
toms in the neutropenic host should raise this consideration.
These infections are managed medically with antimicrobials 1 Bacterial infections (related to wound, intravenous lines,
that cover the anaerobic flora. urinary tract), herpes simplex virus, hepatitis B
Disseminated fungal infections often arise in the setting
of prolonged neutropenia and use of broad-spectrum antibi- 14 Cytomegalovirus, Pneumocystis carinii, Listeria monocyto-
genes, Mycobacterium tuberculosis, Aspergillus, Nocardia,
otics. Candida species should be considered in neutropenic Toxoplasma, hepatitis B, Legionella
persons with nodular or erythematous papular skin lesions,
fluff y white chorioretinal exudates, and fever unresponsive to 26 Epstein-Barr virus, varicella-zoster virus, hepatitis C,
empiric antibacterial agents. In particular, the development Legionella
of fever and an increased alkaline phosphatase level during >6 Cryptococcus neoformans, Legionella
recovery from neutropenia and the finding of microabscesses
in the liver and spleen on computed tomography suggest the
presence of disseminated candidiasis (hepatosplenic candidia- posttransplant time course and serologic status of recipi-
sis). The therapy of hepatosplenic candidiasis requires months ent and donor for certain infections (such as cytomega-
of antifungal therapy, usually with fluconazole. Nonresolving lovirus or toxoplasmosis). Most infections in the first
nodular or consolidative pulmonary infiltrates in the setting month after transplant are common nosocomial infec-
of prolonged antibacterial use and neutropenia suggest inva- tions such as wound infections, urinary tract infections,
sive aspergillosis. Affected patients may have an air crescent and line infections. Cytomegalovirus, a common infection
sign on computed tomography of the chest, and the diagnosis after transplant, can present with fever, viremia, hepatitis,
can be determined from a respiratory or tissue specimen or a colitis, gastritis, retinitis, myocarditis, and pneumonitis.
positive result on serum Aspergillus galactomannan assay. The Cytomegalovirus-seronegative recipients of organs from a
most effective agent for treatment of invasive aspergillosis is seropositive donor are at highest risk for cytomegalovirus
voriconazole. The presence of facial numbness, pain, or sinus disease. The time of occurrence of opportunistic infections
disease in the setting of prolonged neutropenia raises suspi- after solid organ transplant is given in Table 18.1. Pathogens
cion for invasive mucormycosis (due most often to Rhizopus associated with various immunodeficiency states are listed in
or Mucor species) and invasive aspergillosis. These conditions Table 18.2.
are diagnosed by examination of respiratory tract specimens
or endoscopic biopsy and treated with dbridement and intra- The majority of infections in the first month after
venous liposomal amphotericin compounds. transplant are not opportunistic infections. Most
infections are common nosocomial infections such
Streptococcus mitis bacteremia may occur in the setting as wound infections, urinary tract infections, and line
of mucositis and can be associated with sepsis and acute infections.
respiratory distress syndrome, especially in patients with
leukemia. Cytomegalovirus is an important pathogen in patients who
have had a transplant. Presentations can include febrile
The development of fever and an increased alkaline illness with viremia, hepatitis, colitis, gastritis, retinitis,
phosphatase level during recovery from neutropenia myocarditis, and pneumonitis.
and the finding of microabscesses in the liver and spleen
on computed tomography suggest the presence of Cytomegalovirus-seronegative recipients of organs from a
disseminated candidiasis (hepatosplenic candidiasis). seropositive donor are at highest risk for cytomegalovirus
disease.
Nonresolving nodular or consolidative pulmonary
infiltrates in the setting of prolonged antibacterial use and
neutropenia suggest the possibility of invasive aspergillosis. I M MU N O S U P P R E S S I VE M E D I C AT I O N S
Commonly used immunosuppressive agents such as
I N FEC T I O NS I N T R A N S P L A N T R EC I P I E N TS
cyclosporin, tacrolimus, sirolimus, mycophenolate mofetil,
Recipients of hematopoietic stem cell transplants receive and azathioprine, often in combination with corticosteroids,
conditioning chemotherapy that often leads to prolonged are associated with several T-cellmediated opportunistic
neutropenia and mucositis in the early transplant period infections, including Pneumocystis jiroveci pneumonia, nocar-
before engraftment. These patients have complications simi- diosis (pulmonary, brain, and cutaneous), histoplasmosis,
lar to those with febrile neutropenia. Additionally, those who cryptococcosis, coccidioidomycosis, listeriosis, cytomegalo-
receive allogeneic transplants are at risk for graft-vs-host dis- virus, varicella-zoster, and herpes simplex virus (Table 18.2).
ease augmenting the degree of immunosuppression. Alemtuzumab and fludarabine agents frequently used in
In solid organ transplant recipients, the risk for spe- chronic lymphocytic leukemia cause a prolonged impact on T
cific infection can be classified according to the following: cells and are associated with similar T-cellmediated infections.
Neutropenia (<0.5 109/L) Cancer chemotherapy, adverse drug Bacteria: Aerobic gram-negative bacilli (coliforms &
reaction, leukemia pseudomonads, Staphylococcus aureus, viridans streptococci,
coagulase-negative Staphylococcus)
Fungi: Aspergillus, Candida species
Cell-mediated immunity Organ transplant, human immunodefi- Bacteria: Listeria, Salmonella, Nocardia, Mycobacterium (M tuber-
ciency virus infection, lymphoma culosis & M avium), Legionella
(especially Hodgkin disease), Viruses: CMV, herpes simplex, varicella-zoster, JC virus
corticosteroid therapy Parasites: Toxoplasma, Strongyloides stercoralis, Cryptosporidium
Fungi: Candida, Cryptococcus, Histoplasma, Coccidioides,
Pneumocystis jiroveci (formerly Pneumocystis carinii)
Hypogammaglobulinemia or Multiple myeloma, congenital or Bacteria: Streptococcus pneumoniae, Haemophilus influenzae (type B)
dysgammaglobulinemia acquired deficiency, chronic Parasites: Giardia
lymphocytic leukemia Viruses: Enteroviruses
Defective chemotaxis Diabetes, alcoholism, renal failure, lazy S aureus, streptococci, Candida
leukocyte syndrome, trauma, SLE
Defective neutrophilic Chronic granulomatous disease, Catalase-positive bacteria: S aureus, Escherichia coli, Candida
killing myeloperoxidase deficiency species
18. T H E I M MU N O C O M P R O M I S E D H O S T, B I OT E R R O R I S M I N F E C T I O N S , A N D I N F E C T I O U S SY N D R O M E S 251
Table 18.3 TREATMENT FOR INFECTIONS POTENTIALLY CAUSED BY BIOTERRORISM
DISEASE
Botulism Toxin
Smallpox Anthrax ( Clostridium Plague Tularemia
VARIABLE (Variola Major) ( Bacillus Anthracis ) Botulinum ) ( Yersinia Pestis ) ( Francisella Tularensis ) Viral Hemorrhagic Fevers
Lethality High to Very high High without High without treatment Moderate if untreated Variable
moderate respiratory
support
Chemotherapyb Cidofovir (in Cutaneous: CDC biva- Streptomycin 1 g IM twice daily or Streptomycin 1 g IM twice daily or Supportive care.
vitro) Ciprofloxacin 500 mg PO lent equine Gentamicin 5 mg/kg IV once Gentamicin 5 mg/kg daily IV or Ribavirin (arena
every 12 h or antitoxin for daily or Ciprofloxacin 400 mg IV twice viruses or bunyavi-
Doxycycline 100 mg PO serotypes A, B Ciprofloxacin 400 mg IV every daily ruses) 30 mg/kg IV
every 12 h (licensed) & 12 h or 750 mg PO twice Duration: 10 d initial dose, then 16
Duration: 60 d monovalent daily or Doxycycline 100 mg IV twice daily mg/kg every 6 h 4 d,
Inhalational: for serotype Chloramphenicol 25 mg/kg IV 4 or then 8 mg/kg every
Ciprofloxacin 500 mg IV E (investiga- times daily or Chloramphenicol 15 mg/kg IV 4 8 h for 6 d. Passive
every 12 h or tional) Doxycycline 100 mg IV twice daily times daily antibody for AHF,
Doxycycline 100 mg IV Duration: 10 d Duration: 1421 d BHF, Lassa fever,
every 12 h & CCHF
Plus 1 or 2 antimicrobi-
als with demonstrated
susceptibility
Duration: 60 d
Chemoprophylaxis Vaccinia Ciprofloxacin 500 mg PO NA Doxycycline 100 mg PO twice Doxycycline 100 mg PO twice daily NA
immune twice daily or daily or or
globulin 0.6 Doxycycline 100 mg PO Ciprofloxacin 500 mg PO twice Ciprofloxacin 500 mg PO twice
mL/kg IM twice daily daily or daily
(within 3 d Duration: 60 dc Chloramphenicol 25 mg/kg PO 4 Duration: 14 d
of exposure) times daily
Duration: 7 d
Vaccine Calf lymph vac- Anthrax vaccine: 0.5 mL SC DOD pentava- Greer inactivated vaccine (FDA Live attenuated vaccine (IND). AHF candidate #1 vac-
cinia vaccine: at 0, 2, 4 wk, 6, 12, 18 mo, lent toxoid for licensed) Recommended for laboratory cine (cross-protection
1 dose by with annual boosters serotypes A-E Not effective for aerosol exposure. personnel, not for postexposure for BHF) (IND). RVF
scarification (IND): 0.5 mL No longer available prophylaxis inactivated vaccine
deep SC at 0, (IND)
2, 12 wk, then
annual booster
Specimend
Postexposure Nasal swab, Nasal swab, sputum, Nasal swabs, Nasal swab, sputum, induced spu- Nasal swab, sputum, induced spu- Nasal swabs & induced
(024 h) sputum, induced sputum for respiratory tum for culture, FA, & PCR tum for culture, FA, & PCR respiratory secretions
induced culture, FA, & PCR secretions for for RT-PCR & viral
sputum for PCR & toxin culture
culture & assays. Serum
PCR for toxin assays
Clinical illness & Serum for viral Blood for culture & PCR. Nasal swabs, Blood, sputum, & tissue for Gram Blood for culture & PCR. Sputum Serum for viral culture,
convalescence culture. CSF for Gram stain, cul- respiratory stain, culture, FA, F-1 antigen & tissue for Gram stain, culture, acute & convalescent
Drainage ture, & PCR. Tissue for secretion for assays, IHC, & PCR. Acute & FA, IHC, & PCR. Acute & con- antibody assays. Tissue
from skin Gram stain, culture, IHC, PCR & toxin convalescent sera for antibody valescent sera for antibody assays for microscopy, EM,
lesions, & PCR. Acute & conva- assays. Usually assays IHC, PCR
scrapings, lescent sera for toxin & no IgM or IgG
tissue for antibody studies
microscopy,
EM, viral
culture, PCR
Abbreviations: AHF, Argentine hemorrhagic fever ( Junin virus); BHF, Bolivian hemorrhagic fever; CCHF, Congo-Crimean hemorrhagic fever; CDC, Centers for Disease Control & Prevention; CSF, cerebrospinal fluid; DOD,
US Department of Defense; EM, electron microscopy; FA, fluorescent antibody; FDA, US Food & Drug Administration; IgG, immunoglobulin G; IgM, immunoglobulin M; IHC, immunohistochemistry; IM, intramuscularly;
IND, investigational drug; IV, intravenously; NA, not applicable; PO, orally; PCR, polymerase chain reaction; RT-PCR, reverse transcription-polymerase chain reaction; RVF, Rift Valley fever; SC, subcutaneously.
a
A human case of inhalational anthrax developed at 42 days after exposure to the accidental release of B anthracis in Sverdlosk, Russia. This long incubation period may have been due, in part, to the use of postexposure prophylaxis
in that setting or to inaccuracies in information regarding the date of the release (or if there was more than 1). The incubation period for inhalational cases acquired outside this setting (millworkers & others) ranges from 1 to 7 days.
b
Dosages are for adult patients only. See agent-specific recommendations for children & immunocompromised populations.
c
Increased duration because of possibility of concomitant aerosol exposure.
d
Should be obtained only in coordination with infection control, public health, & Laboratory Response Network.
Data from Woods CW, Ashford D. Identifying and managing casualties of biological terrorism. In: Rose BD, editor. UpToDate. Wellesley (MA): UpToDate; c2007. Available from: http://www.uptodate.com.
a skin lesion confirms the diagnosis of anthrax. Sputum rarely illness occur, and airborne isolation is needed for hospitalized
reveals the organism. Nasal swab culture is useful for epide- patients. Treatment is supportive, and exposed persons should
miologic purposes but is not sufficiently sensitive to diagnose be given vaccination.
individual exposures.
Bacillus anthracis organisms are usually susceptible to
VI R A L H E MO R R H AG I C FEVER S
penicillins, tetracycline, clindamycin, vancomycin, rifampin,
and the fluoroquinolones. Inhalational exposures should be Multiple viruses can cause hemorrhagic fever, such as
treated with ciprofloxacin or doxycycline for at least 60 days. Ebola, Marburg, Lassa, Crimean-Congo, and Rift Valley.
Combination therapy with multiple active drugs is preferred The clinical presentation includes multiorgan involvement
for inhalational anthrax. with fever, thrombocytopenia, and bleeding. Treatment
is largely supportive, although intravenous ribavirin may
Widened mediastinum is a characteristic finding in be effective in Lassa fever. Secondary cases occur in viral
inhalational anthrax. hemorrhagic fevers, and airborne isolation precautions are
recommended.
Inhalational anthrax requires prolonged therapy with
multiple active drugs.
I N F E C T I O U S SY N D R O M E S C AU S E D BY
TULAREMIA SPECIFIC MICROORGANISMS
Francisella tularensis infection is spread by tick or deer fly bites,
aerosol droplets, or direct contact with tissues of infected ani- BAC T E R I A
mals (eg, rabbits, muskrats, squirrels, and beavers). Typically,
infection causes an eschar at the site of inoculation, regional Actinomycetes
lymphadenopathy, and high fevers. Pneumonia also can occur. Actinomyces israelii, an anaerobic, gram-positive, branching,
Streptomycin and gentamicin are the most effective therapies. filamentous organism, is the most common cause of human
Tetracycline is also active, but its use is associated with a 10% actinomycosis. Actinomyces israelii is part of the normal flora
relapse rate. Francisella tularensis bacteria have been identified of the mouth. Infections are associated with any condition that
as a potential bioterrorism agent. creates an anaerobic environment (such as trauma with tissue
necrosis, pus). The pathologic characteristic is formation of
Francisella tularensis infection is spread by tick or deer fly sulfur granules, which are clumps of filaments. Infection is
bites, aerosol droplets, or direct contact with tissues of not characterized by granuloma formation.
infected animals.
The pathologic characteristic of actinomycosis is sulfur
P L AGU E
granules (clumps of filaments).
From 1950 to 1991, there were 336 cases of plague in the Lumpy jaw is caused by a perimandibular infection with A
United States. According to the Centers for Disease Control israelii. It is characterized by a chronic draining sinus and may
and Prevention, 10 to 15 human plague cases occur each year, follow a dental extraction. Pulmonary actinomycosis develops
mostly in rural areas. Plague is enzootic in the southwestern when aspirated material reaches an area of lung with decreased
United States. New Mexico has 56% of cases, and 29% of oxygenation (such as in atelectasis). This condition often
cases are among American Indians. Rats and fleas are the vec- occurs in association with poor dental hygiene. A chronic sup-
tors. There is concern that the organism Yersinia pestis could purative pneumonitis may develop and eventually result in a
be used for bioterrorism. Clinical presentations include 1) sinus tract draining through the chest wall. There may be sub-
regional lymphadenopathy with septicemiathe most com- sequent perforation into the esophagus, pericardium, ribs, and
mon formand 2) the pneumonic form (high case-fatality vertebrae. Ileocecal perforation from focal actinomycosis has
rate). Secondary cases of pneumonic plague can occur, and been reported. Appendicitis may be a predisposing factor.
droplet isolation is recommended for hospitalized patients.
Treatment is with streptomycin or tetracycline. Lumpy jaw is caused by a perimandibular infection with A
israelii. It is characterized by a chronic draining sinus and
may follow a dental extraction.
S M A L L P OX
Because of global efforts at eradication, the last case of small- Actinomyces israelii also may be found in culture of
pox in the world was in 1977. However, the possibility remains tubo-ovarian abscesses and other pelvic infections. It is espe-
for this virus to be used as a bioterrorism agent. The rash of cially associated with pelvic inflammatory disease developing
this illness is classically described as being pustular, firm, and in a woman with an intrauterine device.
umbilicated. The lesions start in the throat and mouth and
then progress to the face, trunk, and extremities. The lesions A prolonged course of penicillin is the preferred treatment
commonly affect the palms and soles. Secondary cases of this of actinomycosis.
18. T H E I M MU N O C O M P R O M I S E D H O S T, B I OT E R R O R I S M I N F E C T I O N S , A N D I N F E C T I O U S SY N D R O M E S 255
the United States, 200 to 300 cases still occur annually, mostly penicillin G if culture results are positive. They should also be
in elderly persons who have never been immunized. immunized with diphtheria-tetanus toxoid.
The first muscles affected by tetanus are controlled by cra-
nial nerves, resulting in trismus. Eye muscles (cranial nerves Nonimmune persons exposed to diphtheria should be
III and IV) rarely are involved. As the disease progresses, other evaluated and treated with erythromycin or penicillin G if
muscles become involved (generalized rigidity, spasms, and culture results are positive.
opisthotonos). Sympathetic overactivity is common (labile
hypertension, hyperpyrexia, and arrhythmias). The diagnosis Cutaneous infection with C diphtheriae can occur in indi-
of tetanus is based on clinical findings, although a characteris- gent persons and alcoholics. Preexisting dermatologic disease
tic electromyogram is suggestive. (most often in the lower extremities) is a risk factor. Lesions
may appear punched-out and filled with a membrane, but
The diagnosis of tetanus is based primarily on clinical they may be indistinguishable from other infected ulcers.
findings, which are induced by a neurotoxin. Toxin-mediated complications (such as myocarditis and
neuropathy) are uncommon. Diagnosis is established with
Treatment of tetanus includes supportive care, proper methylene blue staining and culture of the lesion with Lffler
wound management, and administration of antiserum (human medium.
tetanus immune globulin). Penicillin G or metronidazole
should be administered to eradicate vegetative organisms in Cutaneous diphtheria is reported in indigent persons and
the wound. Active tetanus does not induce protective immu- alcoholics.
nity. Therefore, a primary tetanus immunization series should
be given after an episode of tetanus.
18. T H E I M MU N O C O M P R O M I S E D H O S T, B I OT E R R O R I S M I N F E C T I O N S , A N D I N F E C T I O U S SY N D R O M E S 257
lymphocytic meningitis, encephalitis, chorea, myelitis, radicu- to 21 days, or intravenous penicillin G 20 million units a day
litis, and peripheral neuropathy). Carditis (reversible atrioven- for 14 to 21 days. Lyme meningitis, radiculopathy, or encepha-
tricular block) occurs in 5% to 10% of patients. Conduction litis should be treated parenterally.
abnormalities are mostly reversible, and permanent heart
block is rare. Temporary pacing is necessary in approximately In Lyme carditis, the outcome is usually favorable.
30% of patients, but a permanent pacemaker is not indicated.
Dilated cardiomyopathy has been reported, and conjunctivitis The outcome in patients with facial palsy is also usually
and iritis also occur. favorable. In one series, 105 of 122 affected patients completely
recovered. Corticosteroids have no role. If only facial nerve
During stage 2 of Lyme disease, 10%-15% of patients have palsy is present (no symptoms of meningitis or radiculoneu-
neurologic abnormalities. ritis), oral therapy with doxycycline or amoxicillin is used.
Patients with Lyme disease may have bilateral facial palsy. The
Carditis occurs in 5%-10% of patients with Lyme disease.
therapy used if other neurologic manifestations are present is
described below.
Stage 3, although uncommon, can develop months to years
after initial infection. Monarticular or oligoarticular arthritis
The outcome in patients with facial palsy due to Lyme
occurs in 50% of patients who do not receive effective therapy.
disease is usually favorable.
It becomes chronic in 10% to 20%. Chronic arthritis is more
common in those with HLA-DR2 and HLA-DR4. Other
manifestations are acrodermatitis chronica atrophicans (pri- If Lyme meningitis is present, ceftriaxone, 2 g a day for
marily with European strains), progressive, chronic encepha- 14 to 28 days, or intravenous penicillin G, 20 million units
litis, and dementia (rare). Most patients will have detectable a day for 14 to 28 days, should be given. Radiculoneuritis
serum antibodies against B burgdorferi. Magnetic resonance and peripheral neuropathy may have a greater tendency for
imaging may show demyelination. chronicity and often occur with meningitis. Treatment is the
same as that for Lyme-associated meningitis. The regimens for
encephalopathy and encephalomyelitis are identical to those
Diagnosis for meningitis.
Anti-B burgdorferi antibodies can be detected by
enzyme-linked immunosorbent assay after the first 2 to 6 weeks Radiculoneuritis and peripheral neuropathy may have
of illness. The Western blot test is the confirmatory serologic a greater tendency for chronicity and often occur with
test for the diagnosis when the antibody response of screening meningitis.
enzyme-linked immunosorbent assay is positive. This 2-step test
(endorsed by the Centers for Disease Control and Prevention) Optimal regimens for Lyme arthritis (oral vs intravenous)
is both sensitive and specific for establishing the diagnosis of are not established. Intra-articular corticosteroids may cause
Lyme disease. Serologic tests should be ordered only in cases treatment failures. Joint rest and aspiration of reaccumulated
of a clinical syndrome compatible with Lyme disease. Serologic joint fluid are often needed. Response to antibiotics may be
testing is likely to be negative in the early stage (ie, with the delayed. If no neurologic disease is present, doxycycline is
erythema migrans rash). Treatment without testing should given (100 mg orally twice a day for 28 days). An alternative
be initiated in patients who reside in or visit endemic areas regimen is amoxicillin and probenecid (500 mg each, 4 times
and have the characteristic skin lesion of erythema migrans. a day for 28 days) or ceftriaxone (2 g per day intravenously for
False-positive results occur with infectious mononucleosis, 1428 days). Synovectomy may be necessary in the manage-
rheumatoid arthritis, systemic lupus erythematosus, echovirus ment of persistent monoarticular Lyme arthritis that has not
infection, and other spirochetal disease. responded to antimicrobial therapy.
Treatment
For stage 1 (early) Lyme disease in the absence of neuro- Prevention
logic involvement or complete heart block, doxycycline (100 Prophylactic antibiotic therapy after a tick bite is not
mg twice a day for 1021 days), amoxicillin (500 mg 3 times a recommended. Use of single-dose doxycycline is recom-
day for 1021 days), and cefuroxime axetil (500 mg twice a day mended only if 1) the adult or nymphal Ixodes scapu-
for 1021 days) are effective therapeutic agents. Azithromycin, laris tick has been attached for 36 hours (as evidenced by
clarithromycin, and erythromycin are less effective than doxy- engorgement of the tick or by certainty of time of exposure
cycline and should generally be avoided. Because of the risk to tick), 2) prophylaxis can be started within 72 hours of
of vertical transmission, all pregnant women with active Lyme tick removal, 3) the B burgdorferi prevalence rate is 20%
disease should be treated. Doxycycline is contraindicated in among ticks within the region of the tick bite, and 4) doxy-
pregnant women and children younger than 8 years. cycline is not contraindicated. In the vast majority of tick
In Lyme carditis, the outcome is usually favorable. If first- bites, disease is not transmitted. Appropriate use of DEET
or second-degree atrioventricular block is present, it should (N,N-diethyl-3-methylbenzamide)- or picaridin-containing
be treated with oral agents, whereas third-degree heart block insect repellents and protective clothing are strongly recom-
should be treated with intravenous ceftriaxone, 2 g a day for 14 mended during outdoor activities.
18. T H E I M MU N O C O M P R O M I S E D H O S T, B I OT E R R O R I S M I N F E C T I O N S , A N D I N F E C T I O U S SY N D R O M E S 259
Primary infection with C immitis causes pneumonitis that antifungals such as fluconazole should be avoided during the
is usually self-limited. first trimester of pregnancy.
Coccidioidomycosis is one of the many infectious causes Fluconazole, itraconazole, and amphotericin B are effective
of erythema nodosum. When present, it usually indicates for therapy of coccidioidomycosis.
an active immune response that will control the infection.
Therapy is indicated if a patient is pregnant, is
Erythema nodosum is more common in females and is often
immunocompromised, or has worsening infection without
associated with arthralgias, especially of the knees and ankles.
therapy.
Coccidioidomycosis is one of the many infectious causes of
erythema nodosum.
Histoplasmosis
The diagnosis of coccidioidomycosis is based on detect- Histoplasma capsulatum is also a dimorphic fungus that grows
ing the organism by culture or biopsy with silver stains. A C as a small (3 mm in diameter) yeast in tissue. Culture at room
immitis serologic (complement fixation) titer more than 1:4 is temperature produces the mycelial form. Although present
suggestive of infection. Skin testing is of epidemiologic value in many areas of the world, histoplasmosis is especially preva-
only. The diagnosis of coccidioidomycosis meningitis is usu- lent in the Ohio, Missouri, and Mississippi river valleys and
ally established by detecting cerebrospinal fluid anticoccidioi- parts of Mexico and Central America. Outbreaks have been
dal antibodies. A biopsy specimen may reveal a diagnostic C associated with large construction projects and exposure to
immitis spherule (Figure 18.2). Laboratory abnormalities may bird or bat droppings. Histoplasmosis is acquired by inhala-
include eosinophilia and hypercalcemia. tion of spores and also can be transmitted by organ transplant
Fluconazole, itraconazole, and amphotericin B are effec- from an infected donor. The risk of acquisition is increased
tive for therapy of coccidioidomycosis. The acute pulmonary with certain activities, including caving and bridge or other
form is usually self-limited, and observation may be ade- construction. Although healthy individuals may acquire his-
quate. However, therapy is indicated if a patient is pregnant, toplasmosis, patients with AIDS and those with cell-mediated
is immunocompromised (patients with AIDS or receiving immune deficiency are particularly susceptible to disseminated
immunosuppressive regimens for organ transplant or other disease. Histoplasma capsulatum infection is one of the causes
medical reasons), or has worsening infection without therapy. of caseating granulomata.
Amphotericin B is the drug of choice for severe manifesta-
tions and for pregnant women with coccidioidomycosis. Outbreaks of histoplasmosis have been associated with
An alternative to fluconazole is itraconazole (200 mg twice large construction projects and exposure to bird or bat
daily). For meningitis, therapy with high-dose fluconazole is droppings.
preferred and has largely replaced intrathecal amphotericin
B. Because of the high relapse rate of C immitis meningitis, Although healthy individuals may acquire histoplasmosis,
chronic suppressive therapy is necessary, usually with flucon- patients with AIDS and those with cell-mediated immune
azole. Coccidioides meningitis may be complicated by adhesive deficiency are particularly susceptible to disseminated
arachnoiditis. Newer antifungal medications such as voricon- disease.
azole are active in vitro but clinical studies are not available,
and caspofungin has limited in vitro activity against coccid- Primary (acute) histoplasmosis may be clinically indistin-
ioidomycosis. Because of their risk for teratogenicity, azole guishable from influenza or other upper respiratory tract infec-
tions. After resolution, multiple small, calcified granulomas
may be seen on subsequent chest radiography. The progressive
(disseminated) form of histoplasmosis is uncommon but seri-
ous. The disseminated form and reactivation of prior disease
are most likely to occur in infants, elderly men, and immuno-
suppressed persons, including those with HIV or AIDS and
those receiving therapy with tumor necrosis factor- inhibi-
tors such as etanercept and infliximab. Manifestations may
resemble those of lymphoma, with weight loss, fever, anemia,
increased erythrocyte sedimentation rate, and splenomegaly.
Mucosal ulcers, which can occur throughout the gastroin-
testinal tract and mouth, are not infrequent. Disseminated
histoplasmosis typically involves the reticuloendothelial
systembone marrow, spleen, lymph nodes, and liver. Bone
marrow involvement may be associated with pancytopenia.
As with tuberculosis, the adrenal glands may be infected, with
Figure 18.2 Coccidioides immitis Spherules in a Clinical Specimen resulting adrenal insufficiency. Chronic cavitary pulmonary
(Grocott Methenamine-Silver Stain). disease due to Histoplasma may resemble tuberculosis and
Blastomycosis Sporotrichosis
Yet another dimorphic fungal pathogen is Blastomyces der- Sporothrix schenckii, another dimorphic fungal pathogen, in
matitidis. In tissue, the yeast forms are thick-walled and tissue is a round, cigar-shaped yeast. In culture at room tem-
have broad-based buds (10 mm in diameter) (Figure 18.3). perature it is mycelial. Sporothrix schenckii is most often found
In culture at room temperature, a mycelial form is found. in soil, plants, plant products such as straw, wood, sphagnum
Blastomycosis is endemic in the southeastern and upper mid- moss, and thorny plants. Sporotrichosis is transmitted by
western United States. Primary pulmonary blastomycosis may cutaneous inoculation (rose-gardeners disease) and, rarely,
be asymptomatic and may disseminate hematogenously to through inhalation. It manifests as a suppurative and granu-
bone, skin, or prostate. Granulomas occur, but calcification is lomatous reaction.
less frequent than with histoplasmosis or tuberculosis. Cutaneous infection produces characteristic crusty lesions
ascending the lymphatics of the extremities from the initial
site of infection. Similar lesions may be produced by infection
with Mycobacterium marinum, Nocardia, or cutaneous leish-
maniasis. Septic arthritis can occasionally occur. Sporotrichosis
occasionally may cause chronic pneumonitis (with cavitation
and empyema) or meningitis.
18. T H E I M MU N O C O M P R O M I S E D H O S T, B I OT E R R O R I S M I N F E C T I O N S , A N D I N F E C T I O U S SY N D R O M E S 261
For the lymphocutaneous or cutaneous form, itraconazole Neutropenia predisposes to rapidly invasive
is the therapy of choice. An effective alternative is supersatu- bronchopulmonary disease with early dissemination to the
rated solution of potassium iodide. Amphotericin B is recom- brain and other tissues.
mended for disseminated disease (pulmonary, joint), although
it may respond poorly to therapy. Aspergillus also can cause localized disease in persons with
normal immunologic function. Chronic necrotizing pulmo-
Aspergillosis nary aspergillosis occurs in patients with pulmonary emphy-
sema. The chronic, progressive infiltrates of this condition
Aspergillus is an opportunistic pathogen that causes infection often require tissue sampling for diagnosis. Treatment with
in immunocompromised persons, particularly those with pro- surgical resection and systemic antifungal therapy is some-
longed neutropenia or steroid use. Although any species of times curative.
Aspergillus can cause disease, Aspergillus fumigatus is the most Aspergillus may produce a fungus ball in preexisting lung
common pathogenic species. The organisms have large, sep- bullae or cavities (such as from ankylosing spondylitis, pre-
tated hyphae (phycomycetes are nonseptated) branching at vious tuberculosis, or emphysema). Hemoptysis is the main
45 angles (Figure 18.4). Especially in neutropenic hosts, they symptom. Surgical excision may be necessary to prevent lethal
may invade blood vessels, producing a striking thrombotic hemorrhage.
angiitis similar to phycomycosis. Metastatic foci may cause Localized colonization with Aspergillus is common and
suppurative abscess formation. usually does not produce disease. However, otitis externa
(swimmers ear) and allergic bronchopulmonary asper-
Aspergillus organisms may invade blood vessels, producing gillosis are exceptions. The symptoms of allergic bron-
a striking thrombotic angiitis. chopulmonary aspergillosis resemble those of asthma. It
is characterized by migratory pulmonary infiltrates, thick,
The form of disease produced by aspergillosis primarily is brown, tenacious mucous plugs in the sputum, eosinophilia,
determined by the nature of the immunologic deficit in the and high titers of anti-Aspergillus antibodies; it typically
infected individual. Neutropenia predisposes to rapidly inva- occurs in the setting of chronic asthma. Endophthalmitis
sive bronchopulmonary disease with early dissemination to due to Aspergillus may develop after ocular operation or
the brain and other tissues. The longer the duration of neu- trauma.
tropenia, the higher the risk for invasive aspergillosis. Prompt Aspergillus frequently colonizes the respiratory tract.
therapy with high doses of amphotericin B and resolution of Isolating the organism from the sputum of an immunocom-
the neutropenia are necessary to control the disease. Diagnosis petent host usually does not indicate disease and does not
should be suspected when Aspergillus is isolated from any require treatment.
source in a susceptible individual.
T-cell deficiencies (primarily from corticosteroids) predis- Chronic necrotizing pulmonary aspergillosis occurs in
pose to somewhat more indolent, though no less serious, forms patients with pulmonary emphysema.
of aspergillosis. Progressive pulmonary infiltrates, necrotic
skin lesions, wound infections, and brain abscesses may result. Aspergillus may produce a fungus ball in preexisting lung
Sinus infections with Aspergillus may be localized or invasive bullae or cavities (such as from ankylosing spondylitis,
in patients with T-cell deficiencies. previous tuberculosis, or emphysema).
Serologic testing is not helpful for diagnosing invasive
Aspergillus in the compromised host. Aspergillus infections may respond poorly to currently
available antifungal medications. Amphotericin B prod-
ucts are very effective, but they must be given in high doses.
Lipid-based formulations of amphotericin B are advised
for patients in whom nephrotoxicity develops with deoxy-
cholate amphotericin B. Itraconazole was the first oral
agent with substantial activity against Aspergillus. However,
newer drugs such as voriconazole and caspofungin have
potent in vitro and in vivo activity against Aspergillus.
Intravenous voriconazole should be avoided in patients with
severe kidney disease (glomerular filtration rate, <50 mL/
min). Caspofungin is approved by the US Food and Drug
Administration for refractory invasive aspergillosis. This
has been used alone or in combination with amphotericin
B products. Surgical dbridement of infected tissues is often
necessary for cure. Allergic bronchopulmonary aspergillosis
responds to corticosteroid therapy, and itraconazole may be
an important adjunctive therapy in decreasing or sparing the
Figure 18.4 Aspergillus fumigatus in Bronchoalveolar Lavage (450). use of corticosteroids.
18. T H E I M MU N O C O M P R O M I S E D H O S T, B I OT E R R O R I S M I N F E C T I O N S , A N D I N F E C T I O U S SY N D R O M E S 263
vulvovaginal candidiasis. Oral thrush may result from the Candida esophagitis is a common cause of odynophagia
same conditions. in immunosuppressed patients, especially those with AIDS.
Candida species cause 5% to 10% of nosocomial blood- Endoscopy is necessary to prove the diagnosis. Candida
stream infections. Candidemia most often occurs in critically esophagitis is clinically indistinguishable from, and may coex-
ill patients receiving broad-spectrum antibiotics and paren- ist with, cytomegalovirus and herpes simplex virus esophagitis.
teral nutrition. Neutropenia is another predisposing factor. Fluconazole is effective therapy for oral or esophageal can-
Current blood culture techniques usually detect Candida, didiasis. Caspofungin is also active and is approved by the US
but culture results may be delayed. All intravenous catheters Food and Drug Administration for treatment of candidemia
should always be removed or replaced when bloodstream or candidiasis caused by Candida species, including those that
infection with Candida is discovered. Metastatic abscesses are resistant to azoles such as fluconazole. Caspofungin is
can occur in any site after an episode of candidemia. Candida available only as an intravenous drug.
osteomyelitis or joint infections can occur as complications
after an episode of line-related fungemia. Endophthalmitis Hepatosplenic candidiasis typically develops as
may occur as long as 1 month after initial fungemia. For cen- chemotherapy-induced neutropenia resolves.
tral venous catheter-related candidemias, catheter removal
followed by amphotericin B (250500 mg) or fluconazole is Candida esophagitis is clinically indistinguishable from,
indicated. and may coexist with, cytomegalovirus and herpes simplex
Candida tropicalis, Candida parapsilosis, Candida glabrata, virus esophagitis.
and multiple other species cause nosocomial illness, espe-
cially in immunocompromised patients. Note that these
non-albicans species of Candida are more often resistant to Mucormycosis (Rhizopus Species, Zygomycetes)
fluconazole therapy, especially C glabrata.
Injection drug use is a risk factor for Candida endocarditis Mucormycosis is a term used to describe infections caused
(and joint space infections, especially of the sternoclavicular by fungi of the order Mucorales. Older terms for this include
joint). It is often caused by species other than C albicans. phycomycosis and zygomycosis. There are many different
fungi or Zygomycetes within this order that are pathogenic to
humans. Of those, Rhizopus species are the most commonly
Fungemia develops from infected intravenous catheters, isolated, followed by Rhizomucor and Cunninghamella.
especially in the immunosuppressed host. Mucormycosis is a disease of immunocompromised hosts.
Risk factors for Candida bloodstream infection include Pulmonary, nasal, and sinus infections are the most common.
previous antibacterial therapy, cytotoxic or corticosteroid Facial pain, headache, and fever are common symptoms.
therapy, and parenteral nutrition. Rhinocerebral mucormycosis results from direct extension
into the brain. Diabetic ketoacidosis, neutropenia, renal
Candida endocarditis occurs most often in injection drug failure, and deferoxamine therapy are all risk factors for this
users. life-threatening infection. The diagnosis of mucormycosis
Diabetes, corticosteroids, oral contraceptives, obesity, depends on finding the typical black necrotic lesions (usu-
and HIV infection predispose to recurrent vulvovaginal ally in the nose or on the palate) and is confirmed by biopsy.
candidiasis. Treatment involves reversing the predisposing condition as
much as possible, surgical dbridement of necrotic tissue, and
Candida urinary tract infection is common in patients amphotericin B.
with urinary catheters and those receiving antibacterial drugs.
Removal of the catheter is the primary therapy. If necessary, The diagnosis of mucormycosis depends on finding the
treatment with fluconazole or bladder irrigation with dilute typical black necrotic lesions (usually in the nose or on the
amphotericin B may be curative, although recurrence is palate) and is confirmed by biopsy.
common. Diabetic ketoacidosis, neutropenia, renal failure, and
Hepatosplenic candidiasis, also called chronic disseminated deferoxamine therapy are all risk factors for mucormycosis.
candidiasis, occurs during the recovery phase after prolonged
neutropenia. Fever, abdominal pain, and increased alkaline
phosphatase level suggest the diagnosis. Typical bulls-eye V I RUS E S
lesions can be seen with ultrasonography, computed tomog-
Herpesviruses
raphy, or magnetic resonance imaging of the infected liver.
Current guidelines (2004) of the Infectious Diseases Society There are now 8 known herpesviruses: herpes simplex virus
of America recommend fluconazole (6 mg/kg per day) as the (HSV) types 1 and 2, Epstein-Barr virus (EBV), cytomega-
generally preferred antifungal in clinically stable patients. lovirus (CMV), varicella-zoster virus (VZV), human herpes-
However, amphotericin B deoxycholate (0.60.7 mg/kg per virus 6 (HHV-6), HHV-7 (not yet known to be associated
day) or a lipid formulation of amphotericin B (35 mg/kg per with clinical disease), and HHV-8. All herpesviruses are DNA
day) is an option in ill patients or patients with refractory dis- viruses that share the characteristic of establishing latency after
ease. Limited data suggest that caspofungin may be effective. primary infection, whether or not symptomatic.
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Table 18.4 INFECTIOUS MONONUCLEOSIS-LIKE SYNDROMES
ATYPICAL
DISEASE PHARYNGITIS ADENOPATHY SPLENOMEGALY LYMPHOCYTES HETEROPHILE OTHER TEST
Abbreviations and symbols: CMV, cytomegalovirus; EBV, Epstein-Barr virus; HIV, human immunodeficiency virus; IgM, immunoglobulin M; VCA, viral capsid anti-
gen; , absent; +, ++, +++, and ++++, present to varying degrees.
Uncomplicated cases require symptomatic care only. The or post partum and can cause congenital malformations.
patient should not participate in contact sports for several Primary infection of the mother during pregnancy results in
months because of the risk for splenic rupture. Corticosteroids a 15% chance of fetal cytomegalic inclusion disease. Young
are not indicated for uncomplicated infection. Acyclovir and children in day-care centers commonly shed CMV in their
other antiviral drug therapy are not effective. urine and saliva. Their parents are at risk of acquiring primary
Chronic fatigue syndrome is a syndrome characterized by infection from an asymptomatic child. CMV can cause fever
various nonspecific symptoms. EBV infection, however, does of unknown origin in healthy adults, especially in those with
not cause chronic fatigue syndrome. day-careaged children.
CMV can be transmitted by leukocytes in blood trans-
No therapy is indicated for uncomplicated cases of fusions. Use of leukocyte-poor packed red blood cells or
infectious mononucleosis. blood from CMV-seronegative donors decreases the risk of
transmission via this route. Symptomatic infection devel-
EBV does not cause chronic fatigue syndrome. ops about 4 weeks after transfusion and manifests as fever
with atypical lymphocytes in the peripheral blood smear.
EBV infection in males with X-linked lymphoproliferative Serologic testing confirms the diagnosis. Viral cultures are
syndrome is a rare disorder of young boys in whom fulminant rarely helpful in diagnosing CMV disease in the noncom-
EBV infections develop and is associated with a nearly 60% promised patient.
mortality rate. Complications include severe EBV hepatitis
with liver failure and hemophagocytic syndrome with bleed- CMV can cause heterophile-negative mononucleosis
ing. In survivors, hypogammaglobulinemia, malignant lym- syndrome.
phoma, aplastic anemia, and opportunistic infections develop.
Acyclovir and corticosteroids do not seem to be beneficial. CMV can be transmitted by blood transfusion.
In EBV-associated Burkitt lymphoma and nasopharyn-
Fever and infectious mononucleosis-like picture on
geal carcinoma, patients have high titers of immunoglobulin
peripheral smear are characteristics in postoperative
A antibodies to EBV. Polyclonal and monoclonal B-cell lym-
patients who have received blood transfusions.
phoproliferative syndromes have been associated with EBV in
patients who have had organ transplant and in patients with
In persons with impaired cellular immunity (such as those
AIDS. Oral hairy leukoplakia in patients with AIDS is asso-
with AIDS or organ and bone marrow transplant recipients),
ciated with EBV infection and responds to acyclovir therapy.
CMV causes serious infections (CMV syndrome, retinitis,
EBV recently has been associated with leiomyosarcomas in
pneumonia, gastrointestinal ulcerations, encephalitis, and
transplant recipients.
adrenalitis). The diagnosis most often is established by isola-
tion of CMV from blood or from culture, by histopathologic
Polyclonal and monoclonal B-cell lymphoproliferative
evidence of CMV infection in involved tissue (such as liver,
syndromes have been associated with EBV.
lung, gastrointestinal tract), or from clinical findings alone
(CMV retinitis).
Cytomegalovirus
Primary CMV infection is usually asymptomatic in immu- CMV causes serious infections (retinitis, pneumonia,
nocompetent patients, but it can cause a heterophile-negative gastrointestinal ulcerations, encephalitis, and adrenalitis)
mononucleosis syndrome. It is a significant cause of neonatal in patients who have AIDS or take immunosuppressive
disease. Perinatal infection can occur in utero, intra partum, medications.
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Corticosteroids do not prevent postherpetic neuralgia. For dis- Complications of measles include encephalitis.
seminated infections (encephalitis, cranial neuritis), a recent
Secondary bacterial infection is more common than
controlled trial showed that high-dose intravenous acyclovir
primary measles pneumonia.
decreases the duration of hospitalization. Acyclovir-resistant
VZV infection (which can occur in patients with AIDS) can
be treated with intravenous foscarnet or cidofovir. Atypical measles occurs in patients vaccinated before 1968.
Two effective live virus vaccines for VZV are available. After exposure to measles, atypical rash, fever, arthralgias, and
One VZV vaccine (Varivax) is for primary prevention of headache (aseptic meningitis) may develop. The presence of
varicella, and a new, different (higher attenuated varicella a high titer of measles antibody in serum helps confirm the
colony-forming units per milliliter) vaccine (Zostavax) is now diagnosis.
available and recommended for prevention of herpes zoster
(shingles) and postherpetic neuralgia in persons older than 60 Rubella
years. VZV vaccine for primary prevention is recommended
for children and VZV-seronegative adolescent and adult pop- The prodromal symptoms of rubella are mild (unlike those of
ulations. It is contraindicated in pregnancy. Both live vaccines rubeola). Posterior cervical lymphadenopathy, arthralgia (70%
are contraindicated in patients with impaired cellular immu- in adults), transient erythematous rash, and fever are charac-
nity such as AIDS, leukemias, lymphoma, chemotherapy, teristic. Infection is subclinical in many cases. Central nervous
transplant, chronic corticosteroid therapy, or other cellular system complications and thrombocytopenia are rare.
immunodeficiency states.
The characteristics of rubella are posterior cervical
Human Herpesvirus 6 lymphadenopathy, arthralgia (70% in adults), transient
HHV-6 is a recently discovered lymphotropic virus. It erythematous rash, and fever.
causes the mild childhood infectious exanthem known as
roseola infantum. Like CMV, reactivation of infection occurs The greatest danger from rubella is to the fetus. When a
after organ transplant. HHV-6 has been associated with pneu- pregnant female is exposed to rubella, rubella serologic test-
monitis after bone marrow transplant. ing should be done. If the titer indicates immunity, there is no
danger and no further testing is indicated. If the titer indicates
Human Herpesvirus 8 nonimmunity, the patient should be followed for evidence of
HHV-8 is also known as Kaposi sarcoma-associated virus. clinical rubella. The serum titer should be checked again in
As the name implies, it is thought to be the causative agent of 2 to 3 weeks to evaluate for evidence of asymptomatic infec-
Kaposi sarcoma. It is related to EBV. Most recently, HHV-8 tion. If the titer is not increased and there is no evidence of
has been linked to body cavity-based lymphomas in patients clinical rubella, then no intervention is indicated. If clinical
with AIDS and Castleman disease. rubella develops or seroconversion is demonstrated, there is a
high risk of congenital abnormalities or spontaneous abortion.
Measles (Rubeola) The risk varies from 40% to 60% if infection occurs during
the first 2 months of gestation to 10% by the fourth month.
There was a substantial increase in measles cases in the late Intravenous gamma globulin may mask symptoms of rubella,
1980s and early 1990s in unvaccinated preschool children but it does not protect the fetus.
and vaccinated high school and college students (1990:
27,786 cases). Prodromal upper respiratory tract symptoms Gamma globulin does not protect the fetus after exposure
are prominent. Oral lesions (Koplik spots) precede the rash. to rubella.
Both measles infection and measles vaccine cause temporary
cutaneous anergy (false-negative purified protein derivative From 6% to 11% of young adults remain susceptible to
test). Infection may cause more significant immunologic sup- rubella after receiving rubella vaccine. A pregnant female
pression, as exemplified by cases of reactivated tuberculosis in should not be given rubella vaccine because it can cause con-
persons with measles. genital abnormalities. Females of childbearing age should be
warned not to become pregnant within 2 to 3 months from
In measles, oral Koplik spots precede the rash. the time of immunization. Transient arthralgias develop in
Measles vaccine may cause temporary cutaneous anergy. 25% of immunized women. Fever, rash, and lymphadenopathy
also may develop. Symptoms may occur as long as 2 months
Complications of measles include encephalitis and after vaccination. They may be confused with other forms of
pneumonia. Encephalitis is often severe. It usually occurs arthritis.
after a period of apparent improvement of measles infec-
tion. In primary measles pneumonia, large, multinucleated
Mumps
cells (Warthin-Finkeldey cells) are found on lung biopsy.
Secondary bacterial infection is more common than primary Mumps virus commonly affects glandular tissue. Parotitis,
measles pneumonia. Staphylococcus aureus and Haemophilus pancreatitis, and orchitis are characteristic manifestations.
influenzae are the most common bacterial pathogens. Orchitis occurs in 20% of males with mumps. It is unilateral in
18. T H E I M MU N O C O M P R O M I S E D H O S T, B I OT E R R O R I S M I N F E C T I O N S , A N D I N F E C T I O U S SY N D R O M E S 269
lesions. Serum or cerebrospinal fluid serologic testing can aid Asymptomatic carriage of amebic cysts should be treated with
in the diagnosis. Treatment with praziquantel or albendazole one of the lumenocidal agents.
may be beneficial. Albendazole is considered superior for neu-
rocysticercosis because of better central nervous system pen- Metronidazole, followed by a lumenocidal agent such as
etration. The coadministration of corticosteroids often is used iodoquinol or paromomycin, is the preferred therapy for
to decrease cerebral inflammation associated with therapy. symptomatic amebiasis.
Neurocysticercosis is acquired by ingesting tapeworm eggs
Invasive amebiasis may lead to distant abscesses (primarily
from fecally contaminated food.
the liver, but other organs can be involved). An amebic liver
Seizures are the most common symptom of abscess usually is single and is commonly located in the poste-
neurocysticercosis. rior portion of the right lobe of the liver. The anatomical loca-
tion, the fact that it is usually a single abscess, and the absence
Strongyloides stercoralis is unique among the intestinal of other signs of bacterial infection help to distinguish amebic
nematode infections. Unlike the other helminths, the larvae of hepatic abscess from bacterial abscess. Serologic tests (comple-
this organism can mature in the human host (auto-infection). ment fixation) are positive in more than 90% of patients with
In immunocompromised hosts (neutropenia, steroids, AIDS, amebic abscess. Hepatic abscess may rupture through the dia-
HTLV-I), a superinfection can develop with larval migration phragm into the right pleural cavity.
throughout the body. Gram-negative bacteremia is a common
coinfection, resulting from disruption of the intestinal mucosa Amebic liver abscess may rupture through the diaphragm
by the invasive larvae. Treatment is with ivermectin. into the right pleural cavity.
Trichinosis is acquired from eating undercooked meat,
especially bear. Features include muscle pain (especially dia- Giardia lamblia is the parasite most frequently detected
phragm, chest, and tongue), eosinophilia, and periorbital in state parasitology laboratories. Infection characteristically
edema. Treatment is with mebendazole or albendazole. produces sudden onset of watery diarrhea with malabsorption,
Hookworm (Necator americanus) causes anemia. It is bloating, and flatulence. Prolonged disease that is refractory to
found mainly in tropical and subtropical regions. The larval standard therapy may occur in patients with immunoglobulin
form penetrates the skin. Walking barefoot is a risk factor. A deficiency. The organism may be detected in stool specimens.
Treatment is with mebendazole or albendazole. Stool Giardia antigen testing by enzyme-linked immunosor-
Ascariasis infection may cause intestinal obstruction bent assay is very sensitive and may obviate duodenal aspirates
or pancreatitis (worm migrates up the pancreatic duct). for diagnosis. Metronidazole, tinidazole, or nitazoxanide are
Treatment is with mebendazole or albendazole. effective for treating giardiasis.
Schistosomiasis is a tropical disease that causes hepatic cir-
rhosis, hematuria, and carcinoma of the bladder. Transverse Giardia lamblia is the parasite most frequently detected in
myelitis may develop as a result of schistosomiasis. It is state parasitology laboratories.
acquired by direct penetration of the Schistosoma cercariae
from contaminated water (lakes, rivers). Praziquantel is the Giardiasis causes sudden onset of watery diarrhea and
drug of choice for schistosomiasis. malabsorption, bloating, and flatulence.
Prolonged giardiasis is particularly common in patients
Trichinosis is acquired from eating undercooked meat, with immunoglobulin A deficiency.
especially bear.
Transverse myelitis may develop as a result of Toxoplasma gondii is acquired from eating undercooked
schistosomiasis. meat or exposure to cat feces. Primary toxoplasmosis is usu-
ally asymptomatic. In immunocompetent persons it may
cause a heterophile-negative mononucleosis-like syndrome.
Toxoplasmosis causes brain and eye lesions and pneumonia
Protozoan Parasites in patients with AIDS. Immunocompromised patients with
Acanthamoeba, a free-living ameba, causes amebic keratitis in toxoplasmosis can be treated effectively with pyrimethamine
persons swimming in fresh water while wearing soft contact in combination with either sulfadiazine or clindamycin.
lenses. The diagnosis is based on microscopic examination of Toxoplasma chorioretinitis can occur in immunocompetent
scrapings of the cornea. Treatment is with topical antifungal patients during primary infection. Patients may present with
agents. Patients often respond poorly to therapy and have pro- fever and blurry vision. On ophthalmologic examination, an
gressive corneal destruction. acute retinochoroiditis causes marked vitreous reaction over-
Symptomatic infection with Entamoeba histolytica (ame- lying the retinal infection, leading to the characteristic fundus
biasis) may cause diarrhea (often bloody), abdominal pain, picture of the optic nerve appearing as a headlight in the fog.
and fever. Metronidazole, followed by a lumenocidal agent
such as iodoquinol or paromomycin, is the preferred therapy Toxoplasmosis is acquired from eating undercooked meat
(metronidazole does not kill amebae in the intestinal lumen). or exposure to cat feces.
18. T H E I M MU N O C O M P R O M I S E D H O S T, B I OT E R R O R I S M I N F E C T I O N S , A N D I N F E C T I O U S SY N D R O M E S 271
19.
PULMONARY INFECTIONS AND MYCOBACTERIAL
INFECTIONS
Pritish K. Tosh, MD, Elie F. Berbari, MD, and M. Rizwan Sohail, MD
272
H A N TAV I RUS P U L MO NA RY S Y N D RO M E SARS is caused by a coronavirus.
Hantavirus pulmonary syndrome, first recognized in the No new cases have been documented since 2004.
southwestern United States in 1993, is caused by an RNA virus
(family, Bunyaviridae; genus, Hantavirus). The rodent reser-
voir for this virus is the deer mouse (Peromyscus maniculatus).
I N F LU E N Z A
Infection occurs by inhalation of rodent excreta. Epidemics
have been related to environmental conditions that result in Influenza causes annual, seasonal epidemics leading to tens of
explosive growth of deer mouse populations. No human-to- thousands of deaths each year in the United States. Two influ-
human transmission has been documented. The syndrome enza A strains (H3N2 and H1N1) and one influenza B strain
is more common in the southwestern United States. Among typically circulate during winter months and undergo minor
persons with the syndrome, the median age is 32 years (range, antigenic mutations (antigenic drift) resulting in annual sea-
1269 years), 52% are males, and 55% are Native Americans. sonal epidemics. Influenza pandemics occur more rarely (every
The illness is characterized by a short prodrome of fever, myal- 2030 years) and are the result of major antigenic changes
gia, headache, abdominal pain, nausea or vomiting, and cough, (antigenic shift) leading to large numbers of infections due to
followed by the abrupt onset of respiratory distress. Bilateral low levels of population immunity. During seasonal epidem-
pulmonary infiltrates (noncardiogenic pulmonary edema) ics, 80% to 90% of deaths due to influenza occur in persons
that occur within 48 hours after the onset of illness have been older than 65 years. Complications include 1) primary influ-
reported for all patients. Pleural effusions are common and enza pneumonia (interstitial desquamative pneumonia) and
can be transudative or exudative. Hemoconcentration, throm- 2) secondary bacterial infection, which usually is caused by
bocytopenia, and prolonged activated partial thromboplastin S pneumoniae, Haemophilus, or S aureus. Rare cases of toxic
time are common; disseminated intravascular coagulation shock syndrome have been reported when S aureus pneumo-
is rare. Early thrombocytopenia may provide a clue to the nia complicates influenza.
diagnosis of the infection. Myocardial suppression has been
documented. Autopsy can show pleural effusions and edema- About 80%-90% of deaths due to seasonal influenza occur
tous lungs, with interstitial mononuclear cells in the alveolar in persons older than 65 years.
septa, alveolar edema, focal hyaline membranes, and occa-
sional alveolar hemorrhage. Hantavirus antigens are detected Secondary infection usually is caused by S pneumoniae or
with immunohistochemistry. Serologic (Hantavirus-specific S aureus.
immunoglobulin M or increasing titers of immunoglobulin
G), polymerase chain reaction, and other studies are available. Amantadine and rimantadine are effective against only
Treatment is supportive; the mortality rate is as high as 50%. influenza A viruses, not influenza B. Therapy is most beneficial
if begun within 48 hours of onset of symptoms. Neuraminidase
The reservoir for Hantavirus is the deer mouse. inhibitors (oseltamivir and zanamivir) are effective against dis-
ease caused by both influenza A and B. Both reduce the dura-
tion of symptoms by 1 day when given within 48 hours after
onset of symptoms. Because of seasonal changes in antiviral
S EV E R E AC U T E R E S P I R ATO RY SY N D RO M E
resistance in circulating strains, recommendations for treat-
Severe acute respiratory syndrome (SARS) is a viral respira- ment from the Centers for Disease Control and Prevention
tory infection caused by a novel coronavirus that previously should be consulted each year. When oseltamivir resistance is
had infected only animals. SARS is transmitted through aero- suspected, treatment with zanamivir or a combination of osel-
sol and possibly fecal-oral routes. The majority of patients tamivir and rimantadine is recommended instead of oseltami-
with SARS have been adults 25 to 70 years old who were pre- vir alone.
viously healthy. Many of the cases have been reported in Asia, Inactivated injectable influenza and live attenuated intra-
particularly Hong Kong, Taiwan, and the Peoples Republic of nasal vaccines are used for the prevention of influenza. Target
China; however, cases have been reported in other countries in groups for vaccination with the inactivated vaccine are per-
Asia and in North America and Europe. Notably, no new cases sons older than 50 years, residents of chronic care facilities,
have been documented since 2004. SARS has an incubation persons with cardiopulmonary disorders, healthy children
period of 2 to 10 days. The illness begins with fever (>38.0C) between 6 and 23 months old, children 6 months to 18 years
and associated chills and rigors. Other frequent symptoms are old receiving long-term aspirin therapy (to prevent Reye syn-
headache, malaise, and myalgia. Within the first 7 days, a dry drome), health care personnel, employees of chronic care
nonproductive cough and dyspnea develop, with hypoxemia. facilities, providers of home health care, and persons sharing
This worsens in 20% of patients, who require mechanical ven- the same household as high-risk persons. The live attenuated
tilation and treatment in an intensive care unit. Currently, the vaccine is approved only for healthy immunocompetent per-
fatality rate is approximately 15%. Leukocyte counts generally sons between the ages of 2 and 49 years. Adverse reactions to
have been normal or decreased, with more than 50% of patients both vaccines include fever, myalgias, and hypersensitivity. For
having lymphopenia and thrombocytopenia. Increased levels persons who did not receive the vaccine, amantadine, rimanta-
of liver aminotransferases and creatine kinase have been noted. dine, or oseltamivir can be used for influenza prevention and
Treatment is primarily supportive, with no role for antivirals. are effective for prophylactic use after exposure to a patient
19. P U L M O N A RY I N F E C T I O N S A N D M YC O B AC T E R I A L I N F E C T I O N S 273
with influenza; amantadine and rimantadine are active against CAP for whom laboratory data are not available, a modified
only influenza A. Amantadine is given at a dose of 200 mg per index (CRB-65) can be used, in which the uremia risk factor
day; if the person is older than 65 years, only 100 mg per day is removed from the calculation. A patient with a CRB-65
is given to decrease the risk of adverse effects. The decreased score of 0 should be treated as an outpatient, a patient with a
dosage also is used for patients with impaired renal function score of 1 or 2 should be considered for hospitalization, and a
or seizure disorders. Toxicity manifests as dizziness, restless- patient with a score of 3 or 4 should be hospitalized.
ness, and insomnia. High-risk persons who have not received Chest imaging is a requirement for a diagnosis of CAP.
the vaccine during the influenza season should be considered Computed tomography is more sensitive, but chest radiog-
for chemoprophylaxis. raphy is usually sufficient. The usefulness of other diagnostic
tests is more controversial because they are generally of low
Target groups for influenza vaccine are persons older yield and infrequently affect clinical care. However, they can
than 50 years, residents of chronic care facilities, persons be helpful for individual patients and provide data for epide-
with cardiopulmonary disorders, healthy children miologic purposes. Other testing is optional for outpatients
between 6 and 23 months old, children 6 months to 18 with CAP. Pretreatment culturing of blood and sputum
years old receiving long-term aspirin therapy (to prevent should be performed on all patients hospitalized with CAP,
Reye syndrome), health care personnel, employees of and urinary antigen testing for Legionella pneumophila and S
chronic care facilities, providers of home health care, and pneumoniae should be performed on patients requiring care
household members of high-risk persons. in an intensive care unit. During influenza season, influenza
testing should be performed on all patients with CAP who
require hospitalization.
Empiric treatment of CAP should be directed toward the
B AC T E R I A L I N F E C T I O N S
suspected pathogens on the basis of a patients risk factors:
C O M MU N I T Y-AC Q U I R E D P N EUMO N I A For previously healthy patients who have not received
antimicrobials in the prior 3 months, reside in locations
There are more than 900,000 cases of community-acquired
with less than 25% macrolide resistance in S pneumoniae,
pneumonia (CAP) in persons older than 65 years in the
and will be treated as outpatients, macrolide monotherapy
United States each year. Despite the use of antimicrobi-
(eg, erythromycin, azithromycin, or clarithromycin) is
als, mortality remains high. CAP and influenza combine to
recommended, and doxycycline is recommended as an
be the seventh leading cause of death in the United States.
alternative.
Common microbiologic causes of CAP are Streptococcus pneu-
moniae, Mycoplasma pneumoniae, Haemophilus influenzae, For patients with significant medical comorbidities who
Chlamydophila (Chlamydia) pneumoniae, Legionella species, have received antimicrobials in the prior 3 months, have
Staphylococcus aureus, and respiratory viruses (most com- more than 25% macrolide resistance in S pneumoniae, and
monly influenza and respiratory syncytial virus). will be treated as outpatients, treatment options are as
Where patients are treated for CAP is important because follows:
unnecessary hospitalizations for CAP increase costs. In addi-
a. A respiratory fluoroquinolone as monotherapy (eg,
tion, patients transferred to an intensive care unit for CAP
levofloxacin or moxifloxacin) or
care have worse outcomes than those who are directly admit-
ted to an intensive care unit. Although not meant to supplant b. A -lactam antibiotic and a macrolide or doxycycline
good clinical judgment, CAP risk stratification indices help as a single-agent alternative
clinicians decide the site-of-care for patients with CAP. The
most validated index is the Pneumonia Severity Index, which For patients with significant medical comorbidities or who
calculates the risk of mortality using 20 demographic, comor- have received antimicrobials in the prior 3 months and will
bidity, physical examination, and laboratory risk factors. be treated as inpatients, treatment options are as follows:
CURB-65, an alternative index, is validated and easier to use. a. A respiratory fluoroquinolone as monotherapy (eg,
In a patient suspected of having CAP, 1 point is given for each levofloxacin or moxifloxacin) or
of the following: Confusion, Uremia (blood urea nitrogen
>19 mg/dL), Respiratory rate (>30 breaths/min), Blood pres- b. A -lactam antibiotic and a macrolide or doxycycline
sure (systolic <90 mm Hg or diastolic 60 mm Hg), and age as a single-agent alternative
65 years. Patients with a CURB-65 score of 0 or 1 are at low For patients who require management in an intensive care
risk and should be considered for outpatient therapy, a patient unit, recommended treatment is with a -lactam antibiotic
with a score of 2 should be considered for hospitalization or (eg, cefotaxime, ceftriaxone, or ampicillin-sulbactam)
closely supervised outpatient treatment, a patient with a score and azithromycin or a respiratory fluoroquinolone (eg,
of 3 should be hospitalized, and a patient with a score of 4 or 5 levofloxacin or moxifloxacin).
should be hospitalized and considered for care in an intensive
care unit. Of the CURB-65 criteria, uremia is the only one Empiric treatment of methicillin-resistant S aureus
that requires laboratory data. For patients suspected of having with the addition of vancomycin or linezolid should be
19. P U L M O N A RY I N F E C T I O N S A N D M YC O B AC T E R I A L I N F E C T I O N S 275
Table 19.1 RECOMMENDATIONS FOR ANTIMICROBIAL THERAPY IN ADULTS WITH COMMUNITY-ACQUIRED BACTERIAL MENINGITIS
EMPIRIC THERAPY
Age, y
1650 Neisseria meningitidis, Streptococcus pneumoniae Vancomycin plus a third-generation cephalosporina,b
>50 S pneumoniae, N meningitidis, Listeria monocytogenes, aerobic Vancomycin plus a third-generation cephalosporin plus ampicillinb,c
gram-negative bacilli
With risk factor presentd S pneumoniae, L monocytogenes, Haemophilus influenzae Vancomycin plus a third-generation cephalosporin plus ampicillinb,c
SPECIFIC ANTIMICROBIAL THERAPY
S pneumoniae
Penicillin MIC
<0.1 mg/L Penicillin G or ampicillin Third-generation cephalosporin,b chloramphenicol
0.11.0 mg/L Third-generation cephalosporinb Cefepime, meropenem
2.0 mg/L Vancomycin plus a third-generation cephalosporinb,e Fluoroquinolonef
N meningitidis
Penicillin MIC
<0.1 mg/L Penicillin G or ampicillin Third-generation cephalosporin,b chloramphenicol
0.11.0 mg/L Third-generation cephalosporinb Chloramphenicol, fluoroquinolone, meropenem
19. P U L M O N A RY I N F E C T I O N S A N D M YC O B AC T E R I A L I N F E C T I O N S 279
is not seen with Gram staining of the sputum. Serologic test- therapy with ceftazidime, meropenem, or imipenem should
ing (agglutinins) is considered diagnostic if it shows a fourfold be considered if B pseudomallei infection is likely or while sus-
increase in titer in paired samples 2 to 3 weeks apart or a single ceptibility tests are being performed.
titer greater than 1:160. Intravenous streptomycin or gentami-
cin is the recommended antimicrobial regimen for F tularensis Melioidosis may resemble chronic cavitary tuberculosis.
infection; ciprofloxacin or doxycycline given for 14 days is the
recommended treatment for postexposure prophylaxis.
N O C A R D I A P N EU M O N I A
Tularemia is transmitted to humans from wild animals and
bites of ticks or deer flies. Mowing grass and cutting brush Nocardia asteroides, Nocardia brasiliensis, and Nocardia otiti-
have also been identified as risk factors. discaviarum can cause pneumonia in susceptible persons. N
asteroides is a weakly acid-fast saprophytic bacteria present in
the soil, dust, plants, and water. Infection is more common in
immunosuppressed patients and in those with pulmonary alve-
Y E R S IN I A PESTI S olar proteinosis. Primary infection leads to necrotizing pneu-
Yersinia pestis is a gram-negative bacillus that causes plague. monia with abscess formation. No inflammatory response or
It is more prevalent in New Mexico, Arizona, Colorado, and granuloma formation occurs. Pulmonary nodules suggestive
California than in other states. It is spread from wild rodents of cancer metastases and dense alveolar infiltrates are com-
(occasionally cats), either directly or by fleas, usually in May mon chest radiographic findings. Infection may produce pleu-
to September. Because it is endemic to largely rural and unin- ral effusion. Lymphohematogenous spread occurs in 20% of
habited areas, the incidence of disease is low. The incubation patients; in nearly all those patients, a brain abscess develops.
period is 2 to 7 days. Clinical features include fever, headache, The diagnosis is made at autopsy in 40% of cases. Isolation of
bubo (groin or axilla), cough, and tachypnea. Pneumonia the organism from the sputum of immunocompetent patients
occurs in 10% to 20% of patients. Pneumonic plague is the might represent colonization because the saprophytic state is
most serious and fulminant form of this disease. Chest radi- well recognized; however, in an immunocompromised patient,
ography shows bilateral lower lobe alveolar infiltrates. Pleural this should be considered a true infection. Most Nocardia
effusion is common, and nodules and cavities can occur. The isolates are susceptible to trimethoprim-sulfamethoxazole,
leukocyte count is higher than 15 109/L. The organism is however initial combination therapy with the addition of
seen with Giemsa or direct fluorescent antibody staining and imipenem, ceftriaxone, or amikacin should be considered in
in cultures of blood, lymph node, or sputum. Serologic testing severe or complicated cases.
gives positive results. Intravenous streptomycin or gentamicin
is the recommended antimicrobial regimen for Y pestis infec- Brain abscess is common in patients with disseminated
tion; ciprofloxacin or doxycycline given for 7 days is the rec- Nocardia infection.
ommended treatment for postexposure prophylaxis.
19. P U L M O N A RY I N F E C T I O N S A N D M YC O B AC T E R I A L I N F E C T I O N S 281
The role of the serum interferon- release assay health care facilities, residential facilities for patients with
(QuantiFERON-TB Gold test, T-SPOT.TB test) continues AIDS, and homeless shelters; and patients with high-risk
to evolve and has the promise of increasing the specificity of clinical conditions (eg, diabetes mellitus, silicosis, chronic
testing to identify latent tuberculosis. The assay may help dis- renal failure, leukemias and lymphomas, carcinoma of the
tinguish latent tuberculous infection from nontuberculous head or neck and lung, weight loss 10% of ideal body
mycobacterial infection and bacille Calmette-Gurin vac- weight, gastrectomy, and jejunoileal bypass)
cination because it measures interferon- production from a
3. Reaction 15 mm or moreany person without a defined
patients blood sample incubated with M tuberculosisspecific
risk factor for tuberculosis
antigens. Current Centers for Disease Control and Prevention
guidelines suggest that the assay may be used in all circum-
stances in which the PPD skin test is used. Compared with Pleural tuberculosis used to be more common in younger
the PPD skin test, the assay is probably less subject to reader (<40 years) patients; now, it is more common among the
bias and error, requires only a single health care visit, and is elderly. In the United States, 4% of all tuberculous patients
less likely to be positive after bacille Calmette-Gurin vaccine. have pleural involvement, and pleural tuberculosis constitutes
Like the PPD skin test, the assay may be negative in patients 23% of the cases with extrapulmonary tuberculosis. Effusions
who have active tuberculosis. usually occur 3 to 6 months after the primary infection. Acute
presentation (cough, fever, and pleuritic chest pain) is more
common in younger patients. Bilateral exudative effusions
The PPD reaction is a delayed type of hypersensitivity
occur in up to 8% of patients, and the PPD skin test is positive
reaction.
in more than 66%. The effusions typically have high protein
The PPD skin test can become positive within 4 weeks levels (>5 g/dL), lymphocytosis (>50%), and low levels of
after exposure to M tuberculosis. glucose (<50 mg/dL). A low pleural fluid pH occurs in 20%
of patients. Measurement of levels of the enzyme adenosine
The PPD skin test and interferon- release assay may be
deaminase in the pleural fluid has a sensitivity of 70% to 90%
negative in a substantial proportion of patients with active
for pleural tuberculosis, with a specificity that varies from less
tuberculosis.
than 50% to 90%. The test is not diagnostic for pleural tuber-
Compared with the PPD skin test, the interferon- release culosis, and its main utility is to suggest tuberculosis infection
assay is probably less subject to reader bias and error, if the adenosine deaminase level is very high or to rule out the
requires only a single health care visit, and is less likely to diagnosis of pleural tuberculosis if the level is very low. Pleural
be positive after bacille Calmette-Gurin vaccine. biopsy specimens show caseous granulomas in up to 80%
of patients, and cultures of biopsy specimens are positive in
Targeted tuberculin testing for latent tuberculosis infection more than 75%. Cultures of pleural fluid are positive in only
identifies persons at high risk for tuberculosis who would benefit 20% to 40% of patients, and the sputum is positive in 40%.
from treatment of the infection. Indications for testing include Bronchopleural fistula is a complication.
persons with signs and symptoms suggestive of current tubercu-
losis infection, recent contacts with known or suspected cases of Pleural tuberculosis is more common among the elderly.
tuberculosis, abnormal chest radiographic findings compatible
Effusion occurs 36 months after primary infection.
with past tuberculosis, patients with diseases that increase the risk
of tuberculosis (silicosis, gastrectomy, diabetes mellitus, immune
suppression, and HIV infection), and groups at high risk of Miliary tuberculosis constitutes 10% of cases of extrapul-
recent infection with M tuberculosis (immigrants and long-time monary tuberculosis. It is characterized by the diffuse presence
residents and workers in hospitals, nursing homes, or prisons). of small (<2 mm) nodules throughout the body. The spleen,
The following criteria apply to a positive PPD skin test: liver, and lung are frequently involved. The disease can be
acute and fatal or insidious in onset and slowly progressive.
1. Reaction 5 mm or morepersons with HIV infection, Chest radiography shows typical miliary lesions in more than
close contact with infectious cases, patients with organ 65% of patients. Sputum findings are negative in up to 80% of
transplants and other immunosuppressed patients patients, and the PPD skin test is negative in approximately
(receiving the equivalent of 15 mg daily of prednisone 50% of patients with miliary tuberculosis. Mortality is high
for 1 month), and those with fibrotic lesions on chest (30%) even with therapy.
radiography consistent with prior tuberculosis Tuberculous lymphadenitis (ie, scrofula) is the most com-
mon form of extrapulmonary tuberculosis. It is more common
2. Reaction 10 mm or moreimmigrants within the past in children and young adults than in older persons. Cervical
5 years from high-prevalence countries; injection drug lymph nodes are affected most commonly; 1 or more nodes
users; mycobacteriology laboratory workers; children (painless, nontender, and rubbery) may be palpable. Abscess
younger than 4 years, or infants, children, and adolescents and sinus formation may occur.
exposed to adults at high risk of tuberculosis; and Skeletal tuberculosis is becoming less common; when iden-
employees and residents of high-risk congregate facilities tified, it is more common in the young than in older adults.
including prisons, nursing homes, hospitals and other Any bone can be involved, but the vertebrae are involved in
19. P U L M O N A RY I N F E C T I O N S A N D M YC O B AC T E R I A L I N F E C T I O N S 283
Table 19.2 DRUG REGIMENS FOR CULTURE-POSITIVE PULMONARY TUBERCULOSIS CAUSED BY
DRUG-SUSCEPTIBLE ORGANISMS
RANGE OF RATING a
INITIAL PHASE CONTINUATION PHASE TOTAL (EVIDENCE) b
DOSES
Interval & Doses c Interval & Doses c,d (MINIMAL HIV HIV
Regimen Drugs (Minimal Duration) Regimen Drugs (Minimal Duration) DURATION) Negative Positive
1 INH 7 d/wk for 56 doses (8 wk) or 1a INH/RIF 7 d/wk for 126 doses 182130 (26 wk) A (I) A (II)
RIF 5 d/wk for 40 doses (8 wk)e (18 wk) or 5 d/wk for
PZA 90 doses (18 wk)e
EMB 1b INH/RIF Twice weekly for 36 9276 (26 wk) A (I) A (II)f
doses (18 wk)
1cg INH/RPT Once weekly for 18 7458 (26 wk) B (I) E (I)
doses (18 wk)
2 INH 7 d/wk for 14 doses (2 wk), 2a INH/RIF Twice weekly for 36 6258 (26 wk) A (II) B (II)f
RIF then twice weekly for 12 doses (18 wk)
PZA doses (6 wk) or 5 d/wk for 2bg INH/RPT Once weekly for 18 4440 (26 wk) B (I) E (I)
EMB 10 doses (2 wk)e, then twice doses (18 wk)
weekly for 12 doses (6 wk)
3 INH 3 times weekly for 24 doses 3a INH/RIF 3 times weekly for 54 78 (26 wk) B (I) B (II)
RIF (8 wk) doses (18 wk)
PZA
EMB
4 INH 7 d/wk for 56 doses (8 wk) or 4a INH/RIF 7 d/wk for 217 doses 273195 (39 wk) C (I) C (II)
RIF 5 d/wk for 40 doses (8 wk)e (31 wk) or 5 d/wk for
EMB 155 doses (31 wk)e
4b INH/RIF Twice weekly for 62 118102 (39 wk) C (I) C (II)
doses (31 wk)
Abbreviations: EMB, ethambutol; INH, isoniazid; PZA, pyrazinamide; RIF, rifampin; RPT, rifapentine.
a
Definitions of ratings: A, preferred; B, acceptable alternative; C, offer when A and B cannot be given; E, should never be given.
b
Definitions of evidence: I, randomized clinical trial; II, data from clinical trials that were not randomized or were conducted in other populations; III, expert opinion.
c
When directly observed therapy is used, drugs may be given 5 days weekly & the necessary number of doses adjusted accordingly. Although there are no studies that
compare 5 with 7 daily doses, extensive experience indicates this would be an effective practice.
d
Patients with cavitation on initial chest radiograph & positive cultures at completion of 2 months of therapy should receive therapy for a 7-month (31 weeks; either 217
doses [daily] or 62 doses [twice weekly]) continuation phase.
e
Drugs given for 5 days weekly are always given by directly observed therapy. Rating for these regimens is A (III).
f
Not recommended for human immunodeficiency virus (HIV)-infected patients with CD4+ cell counts <100/mcL.
g
Options 1c and 2b should be used only in HIV-negative patients who have negative sputum smears at the time of completion of 2 months of therapy & who do not
have cavitation on the initial chest radiograph. For patients receiving this regimen & found to have a positive culture from the 2month specimen, treatment should be
extended an extra 3 months.
Adapted from Blumberg HM, Burman WJ, Chaisson RE, Daley CL, Etkind SC, Friedman LN, et al. American Thoracic Society/Centers for Disease Control and
Prevention/Infectious Diseases Society of America: treatment of tuberculosis. Am J Respir Crit Care Med. 2003 Feb 15;167(4):60362. Used with permission.
Disease Control and Prevention recommend an intensive provider monitors each patient as every dose of a 6-month
phase of therapy with 4 drugs if the local rate of resistance to regimen is taken. This approach makes a cure almost certain
isoniazid is more than 4%. Even though the mortality from with drug-sensitive tuberculosis. The DOT regimen is par-
MDR-TB is high in HIV-positive and HIV-negative patients, ticularly important for the homeless, chronic alcoholics, intra-
appropriate treatment produces a favorable outcome (>80%). venous drug abusers, AIDS patients, and prison inmates. A
MDR-TB is often treated for 18 to 24 months. fixed-dose combination should be considered in cases of newly
diagnosed disease. Even though fixed-dose combinations of
Drug-resistant tuberculosis may require multidrug (4 antituberculous drugs (isoniazid and rifampin; rifampin, iso-
drugs) therapy. niazid, and pyrazinamide) are available and have been strongly
recommended by the World Health Organization, Centers for
To prevent drug resistance and to effectively decrease the Disease Control and Prevention, American Thoracic Society,
number of cases of tuberculosis, many health care organiza- and the International Union Against Tuberculosis and Lung
tions recommend administration of antituberculous drugs Disease, less than 25% of rifampin-containing therapies
by directly observed therapy (DOT) in which a health care use the fixed-dose regimen. Treatment completion rates for
DOSE, MG/KG
DRUG Children d Adults Children d Adults Children d Adults ADVERSE REACTIONS MONITORING
INHe (maximal 1020 5 2040 15 2040 15 Liver enzyme elevation, hepatitis, Baseline measurements of liver enzymes for
dose, mg) (300) (300) (900) (900) (900) (900) peripheral neuropathy, mild effects on adults
central nervous system, drug Repeat measurements if baseline results are
interactions abnormal, if patient is at high risk of
adverse reactions, or if patient has
symptoms of adverse reactions
RIFf (maximal 1020 10 1020 10 1020 10 GI upset, drug interactions, hepatitis, Baseline measurements for adults: complete
dose, mg) (600) (600) (600) (600) (600) (600) bleeding problems, flulike symptoms, rash blood cell count, platelets, liver enzymes
Repeat measurements if baseline results are
abnormal or if patient has symptoms of
adverse reactions
PZAg (maximal 1530 1530 5070 5070 5070 5070 Hepatitis, rash, GI upset, joint aches, Baseline measurements for adults: uric acid,
dose, g) (2) (2) (4) (4) (3) (3) hyperuricemia, gout (rare) liver enzymes
Repeat measurements if baseline results are
abnormal or if patient has symptoms of
adverse reactions
EMBh 1525 1525 50 50 2530 2530 Optic neuritis Baseline & monthly tests: visual acuity, color
vision
SMi (maximal 2040 15 2530 2530 2530 2530 Ototoxicity (hearing loss or vestibular Baseline & repeat as needed: hearing, kidney
dose, g) (1) (1) (1.5) (1.5) (1.5) (1.5) dysfunction), renal toxicity function
Abbreviations: EMB, ethambutol; GI, gastrointestinal tract; INH, isoniazid; PZA, pyrazinamide; RIF, rifampin; SM, streptomycin.
a
Adjust weight-based dosages as weight changes.
b
INH, RIF, PZA, & EMB are administered orally; SM is administered intramuscularly.
c
Directly observed therapy should be used with all regimens administered 2 or 3 times weekly.
d
Younger than 12 years.
e
Hepatitis risk increases with age & alcohol consumption. Pyridoxine can prevent peripheral neuropathy.
f
Severe interactions with methadone, oral contraceptives, & many other drugs. Drug colors body fluids orange & may permanently discolor soft contact lenses.
g
Treat hyperuricemia only if patient has symptoms.
h
Not recommended for children too young to be monitored for changes in vision unless tuberculosis is drug resistant.
i
Avoid or decrease dose in adults older than 60 years.
Adapted from Centers for Disease Control and Prevention, Division of Tuberculosis. Elimination: core curriculum on tuberculosis. 3rd ed. c1994.
Table 19.4 TARGETED TUBERCULIN TESTING FOR LATENT TUBERCULOSIS INFECTION
Persons with chest radiographic findings suggestive of previous TB & inadequate or no treatmenta 5
Abbreviations: HIV, human immunodeficiency virus; PPD, purified protein derivative of tubercle bacillus; TB, tuberculosis.
a
Isolated calcified granulomas are excluded.
b
Increase of 10 mm if person is younger than 35 years or is a health care worker; increase of 15 mm if person is 35 years or older.
c
Appropriate cutoff for defining a positive reaction depends on the employees individual risk factors for TB & on the prevelence of TB in the facility.
Adapted from Van Scoy RE, Wilkowske CJ. Antimicrobial therapy. Mayo Clin Proc. 1999 Oct;74(10):103848. Used with permission of Mayo Foundation for Medical
Education and Research.
pulmonary tuberculosis are most likely to exceed 90% with Pyridoxine is usually added to prevent peripheral neuropa-
DOT. However, DOT may not increase the cure rate in areas thy, which is particularly common in patients with diabetes
where the rate of cure is high (without DOT). mellitus, alcohol abuse, or kidney disease. Rifampin (600 mg
daily) is an alternative option. Previous combination therapy
DOT for 6 months is effective for preventing relapses and with rifampin and pyrazinamide is no longer routinely recom-
emergence of drug-resistant tuberculosis. mended because of the increased frequency of fatal hepatitis.
Therapy with this combination should be supervised by a spe-
DOT is also useful for the treatment of drug-resistant cialist. The recommended duration for therapy of latent tuber-
tuberculosis and tuberculosis in immunocompromised culosis infection is outlined below:
patients.
A fixed-dose combination should be considered in cases of 1. Isoniazid for HIV-positive adults and children: 12 months
newly diagnosed disease. 2. Isoniazid for HIV-negative adults and children: 9 months
3. Rifampin, as an alternative to isoniazid: 4 months
Treatment of latent tuberculosis infection is indicated for
persons with a positive PPD skin test who do not have active 4. Silicosis or old fibrotic lesion on chest radiography
infection (Table 19.4). If an isoniazid-sensitive organism without active tuberculosis: 4-month therapy with
probably caused latent tuberculosis infection, the treatment isoniazid and rifampin, although 12 months of isoniazid
options include isoniazid 300 mg daily or 900 mg biweekly. alone is an acceptable alternative
Negative culture
at 2 mo
INH/RIF
Cavitation on CXR
or INH/RIF
Positive culture
Positive AFB smear at 2 mo
at 2 mo No cavitation
INH/RPTc,d
0 1 2 3 4 6 9
Time, months
Figure 19.1 Treatment Algorithm for Tuberculosis. Patients in whom tuberculosis is proved or strongly suspected should have treatment initiated with
isoniazid (INH), rifampin (RIF), pyrazinamide (PZA), and ethambutol (EMB) for the initial 2 months. Another acid-fast bacilli (AFB) smear and
culture should be performed after 2 months of treatment. If cavities were seen on the initial chest radiograph (CXR) or the AFB smear is positive at
completion of 2 months of treatment, the continuation phase of treatment should consist of INH and RIF daily or twice weekly for 4 months (total
of 6 months of treatment). If cavitation was present on the initial CXR and if the culture at the completion of 2 months of therapy is positive, the
continuation phase should be lengthened to 7 months (total of 9 months of treatment). If the patient has human immunodeficiency virus (HIV)
infection and the CD4+ cell count is <100/mcL, the continuation phase should consist of daily or 3-times-weekly doses of INH and RIF. In patients
without HIV infection who have no cavitation on CXR and negative AFB smears at completion of 2 months of treatment, the continuation phase
may consist of either once-weekly doses of INH and rifapentine (RPT), or daily or twice-weekly doses of INH and RIF (total of 6 months) (bottom
of figure). Patients receiving INH and RPT and whose 2-month cultures are positive should have treatment extended by an additional 3 months
(total of 9 months). a Use of EMB may be discontinued when results of drug susceptibility testing indicate no drug resistance. b Use of PZA may be
discontinued after it has been taken for 2 months (56 doses). c RPT should not be used in HIV-infected patients with tuberculosis or in patients with
extrapulmonary tuberculosis. d Therapy should be extended to 9 months if the 2-month culture is positive. (Adapted from Blumberg HM, Burman
WJ, Chiasson RE, Daley CL, Etkind SC, Friedman LN, et al. American Thoracic Society/Centers for Disease Control and Prevention/Infectious
Diseases Society of America: treatment of tuberculosis. Am J Respir Crit Care Med. 2003 Feb 15;167[4]:60362. Used with permission.)
In the United States, bacille Calmette-Gurin vaccine is NTM disease is not reportable in the United States.
recommended only for PPD-negative adults who are health
care workers and live where the likelihood of transmission Chronic pulmonary disease is caused most frequently by
and subsequent infection with M tuberculosis strains resistant M avium complex and Mycobacterium kansasii. Pulmonary
to isoniazid and rifampin is high, provided that comprehen- disease is more common in older adults, those with underly-
sive tuberculosis infection-control precautions have been ing chronic obstructive pulmonary disease, smokers, alcohol
implemented in the workplace and have not been successful. abusers, and some children with cystic fibrosis. Pulmonary
Bacille Calmette-Gurin vaccine is not recommended for infection from M avium complex also develops in white
HIV-positive children and adults. women in their 60s who are HIV-negative and who do not
have preexisting lung disease. Most of these patients (>90%)
have bronchiectasis or small nodules without predilection for
N O N T U B E RC U L O US MYC O BAC T E R I A
any lobe. High-resolution computed tomography may show
Mycobacteria other than M tuberculosis and Mycobacterium leprae associated multifocal bronchiectasis with small (<5 mm)
are commonly classified as nontuberculous mycobacteria (NTM) nodular infiltrates. Bilateral nodular or interstitial lung dis-
even though tubercle formation occurs. Most NTM have been ease (or both) or isolated disease in the right middle lobe or
isolated from natural water and soil. Human-to-human spread lingular disease is more predominant in elderly nonsmoking
has not been documented. Natural waters are the source for women. Hypersensitivity pneumonitis caused by exposure to
most human infections caused by Mycobacterium avium com- M avium complex growing in a hot tub has been reported.
plex; some cases are probably acquired from hospital tap water. Mycobacterium avium complex is responsible for 5% of the
Colonization or a saprophytic state of NTM is uncommon. cases of mycobacterial lymphadenitis in adults and more than
NTM disease is not reportable in the United States. 90% of the cases in children. Lymphadenopathy is usually uni-
lateral and nontender. Disseminated disease caused by NTM
Human-to-human spread of NTM has not been manifests as a fever of unknown origin in immunocompro-
documented. mised patients without AIDS.
19. P U L M O N A RY I N F E C T I O N S A N D M YC O B AC T E R I A L I N F E C T I O N S 287
Initial cultures negative
No change in CXR
RIF INH for 4 mo
INH for 9 mo
Low
suspicion
tm ent RIF/PZA for 2 mo
At-risk patient trea
Abnormal CXR No
Smears negative Initial cultures negative
No other diagnosis Improvement in CXR or Sx
Positive tuberculin IN
H/
test RIF INH/RIF for 2 mo
/EM
High B/P
ZA
suspicion
Treatment complete
Initial cultures negative
No change in CXR or Sx
Initial Repeat
evaluation evaluation
0 1 2 3 4 6 11
Time, months
Figure 19.2 Treatment Algorithm for Active, Culture-Negative Pulmonary Tuberculosis (TB) and Inactive TB. The decision to begin treatment of
a patient with sputum smears that are negative depends on the degree of suspicion that the patient has TB. If the clinical suspicion is high (bottom
of figure), multidrug therapy should be initiated before acid-fast smear and culture results are known. If the diagnosis is confirmed by a positive
culture, treatment can be continued to complete a standard course of therapy (see Figure 19.1). If initial cultures remain negative and treatment has
consisted of multiple drugs for 2 months, there are 2 options depending on reevaluation at 2 months (bottom of figure): 1) If the patient demonstrates
symptomatic or radiographic improvement without another apparent diagnosis, a diagnosis of culture-negative TB can be inferred. Treatment should
be continued with isoniazid (INH) and rifampin (RIF) alone for an additional 2 months. 2) If the patient demonstrates neither symptomatic nor
radiographic improvement, prior TB is unlikely and treatment is complete after treatment including at least 2 months of RIF and pyrazinamide
(PZA) has been administered. In low-suspicion patients not initially receiving treatment (top of figure), if cultures remain negative, the patient has
no symptoms, and the chest radiograph is unchanged at 23 months, the 3 treatment options are as follows: 1) INH for 9 months, 2) RIF with or
without INH for 4 months, or 3) RIF and PZA for 2 months. The RIF/PZA 2-month regimen should be used only for patients who are not likely
to complete a longer course of treatment and can be monitored closely. CXR indicates chest radiograph; EMB, ethambutol; Sx, signs and symptoms.
(Adapted from Blumberg HM, Burman WJ, Chaisson RE, Daley CL, Etkind SC, Friedman LN, et al. American Thoracic Society/Centers for Disease
Control and Prevention/Infectious Diseases Society of America: treatment of tuberculosis. Am J Respir Crit Care Med. 2003 Feb 15;167[4]:60362.
Used with permission.)
Mycobacterium avium complex infection occurs in kansasii infection can be clinically indistinguishable from
bronchiectasis. tuberculosis; however, symptoms may be less severe and more
chronic than with tuberculosis. In HIV-negative patients,
HIV-infected persons are at high risk of NTM infections. common symptoms are cough (90%), purulent sputum
More than 95% of NTM disease in HIV-infected persons is (85%), weight loss (55%), and dyspnea (50%). In immuno-
caused by M avium complex. In those with AIDS, dissemi- compromised patients, including those with AIDS, the lung
nated infection occurs in up to 40% and localized infection is most commonly involved and symptoms include fever,
in 5%; dissemination is more likely in those with a CD4 cell chills, night sweats, cough, weight loss, dyspnea, and chest
count less than 50/mcL. The risk of disseminated infection pain. Disseminated M kansasii infection occurs in 20%
is 20% per year when the CD4 cell count is less than 100/ of HIV-positive patients who have M kansasii pulmonary
mcL. High fever and sweats are common, as are anemia and disease.
increased alkaline phosphatase levels. Dissemination is usually
documented with positive blood cultures (sensitivity, 90%). Cavitation occurs in 90% of patients with M kansasii
infection.
Disseminated M avium complex in AIDS is more likely
when the CD4 count is <50/mcL.
Specific skin tests are not available for the diagnosis of
A single blood culture in disseminated M avium complex NTM. Routine cultures of sputum, blood, or stool are not rec-
infection has a sensitivity of 90%. ommended for asymptomatic patients. All specimens positive
for acid-fast bacilli must be considered to indicate M tuber-
Mycobacterium kansasii is the second most common cause culosis until final culture results are available. Bronchoscopy
of NTM pulmonary disease in the United States. It primarily or open lung biopsy is required for diagnosis in nearly half
affects adult white men. Approximately 90% of patients with the cases. Therapy fails in half the patients. More than 80%
M kansasii disease have cavitary infiltrates. Mycobacterium of patients remain symptomatic, and 60% do not tolerate the
19. P U L M O N A RY I N F E C T I O N S A N D M YC O B AC T E R I A L I N F E C T I O N S 289
treatment. Renal failure prolongs the half-life of the drug and and gradual onset of dyspnea, fever, tachypnea, hypoxia,
increases the frequency of ocular toxicity. cyanosis, cough; relatively normal findings on lung
examination; and a patchy or diffuse interstitial or alveolar
Retrobulbar neuritis is a serious adverse effect of process on chest radiography.
ethambutol.
Renal failure prolongs the half-life of the drug and PA R A S I T I C D I S E A S E S
increases the frequency of ocular toxicity.
Parasitic infections of the lung are less common in the United
States than in other parts of the world. Travelers to regions
Streptomycin where parasitic infestations are endemic may become infected
Because streptomycin is excreted by the kidneys, the dosage and, when they return to the United States, present with diffi-
should be decreased in renal insufficiency. The most com- cult diagnostic problems. However, dirofilariasis is indigenous
mon adverse effect is vestibular toxicity, which causes vertigo. to the eastern and southeastern United States. Other parasitic
Hearing loss may also occur. These effects are more likely in infections, including helminthic infestations, also occur in the
the elderly (>60 years). Ototoxicity and nephrotoxicity are United States. The parasites most likely to cause pulmonary
related to both the cumulative dose and the peak serum con- infections include Paragonimus westermani (paragonimiasis),
centration. Streptomycin should be avoided in pregnancy. Echinococcus granulosus (echinococcosis or hydatid disease),
Dirofilaria immitis (dirofilariasis), Schistosoma japonicum
Streptomycin-associated nephrotoxicity and vestibular and Schistosoma mansoni (schistosomiasis), and Entamoeba
toxicity are more common in persons >60 years. histolytica (amebiasis). Protozoal infections are more likely in
patients whose cellular immunity is suppressed.
Streptomycin should be avoided in pregnancy. Dirofilariasis, caused by the heartworm that infects dogs, is
transmitted to humans by mosquitoes. The disease is endemic
to the Mississippi River Valley, the southeastern United States,
P N EU M O C YST I S J I R O V EC I IN F E C T I O N and the Gulf Coast. Characteristically, the infection manifests
as a well-defined solitary lung nodule or multiple lung nodules
Pneumocystis jiroveci (formerly Pneumocystis carinii) is a fun- 1.5 to 2.5 cm in diameter. Eosinophilia occurs in less than 15%
gus with trophic and cyst forms. Pneumocystis jiroveci infec- of patients. Serologic tests may aid in the diagnosis.
tions occur in immunosuppressed patients, especially those Echinococcosis has occurred in Alaska and the south-
with AIDS (CD4 cell count 200/mcL) or malignancy, and western United States. When persons have lung disease, chest
after organ transplant. Infection causes alveolar and interstitial radiography shows well-defined round or oval cystic or solid
inflammation and edema with plasma cell infiltrates. Clinical lesions up to 15 cm in diameter. Rupture of the cysts can cause
features in patients with AIDS include the gradual onset of anaphylactic shock, hypersensitivity reactions, and seeding of
dyspnea, fever, tachypnea, and hypoxia. In patients without adjacent anatomical areas. Liver involvement (in 40% with
AIDS, the onset is more abrupt and progression to respiratory lung disease) and positive serologic findings are common.
failure occurs quickly. Patients typically have relatively normal Paragonimiasis is more likely in immigrants from Southeast
findings on lung examination and a patchy or diffuse intersti- Asia, but sporadic cases occur in the United States. It is trans-
tial or alveolar process on chest radiography. An upper lobe mitted typically through consumption of raw or undercooked
process is seen on the chest radiographs of patients receiving crabs or crayfish. Respiratory features resemble those of
pentamidine aerosolized prophylaxis. The typical computed chronic bronchitis, bronchiectasis, or tuberculosis. Profuse
tomographic finding is ground-glass attenuation. However, brown-colored sputum and hemoptysis can be seen. Pleural
this classic radiographic presentation is less frequent now and effusion is relatively common, and peripheral eosinophilia is
is being replaced by cystic lung disease, spontaneous pneu- common. Ova can be found in pleural fluid, bronchial wash,
mothorax, and an upper lobe distribution of parenchymal or sputum.
opacities. Routine laboratory data are unhelpful. The diagno- Schistosomiasis is not acquired in the United States. The
sis can be made with induced sputum, bronchoalveolar lavage, infection leads to gradual development of secondary pul-
or lung biopsy. Induced sputum or bronchoalveolar lavage monary hypertension caused by occlusion of the pulmonary
is an excellent method for diagnosis, and the cyst stains best arterial tree by the parasite. Cor pulmonale develops in 5% of
with methenamine silver nitrate. The number of organisms patients.
present in immunocompromised patients without AIDS is Amebiasis may manifest as lobar pneumonia or lung
smaller and overall mortality is greater. abscess (pleuropulmonary complications are almost always
right-sided). Rupture into the bronchial tree (hepatobron-
An upper lobe process is seen on chest radiographs of chial fistula) may be followed by expectoration of sputum
patients receiving pentamidine aerosolized prophylaxis. that resembles anchovy paste or chocolate. Rupture of the
liver abscess into the pleural space causes empyema along with
A typical clinical scenario of P jiroveci infection is a respiratory distress in many patients. Pericardial involvement
patient with AIDS who has a CD4 cell count <200/mcL can also occur.
19. P U L M O N A RY I N F E C T I O N S A N D M YC O B AC T E R I A L I N F E C T I O N S 291
discrete, raised, violaceous, or bright-red tracheobronchial The lymphoma in these patients is usually extranodal
lesions can be seen on bronchoscopy. Bronchoscopic biopsy non-Hodgkin B-cell lymphoma. Lung involvement is a late
is associated with a high incidence of considerable bleeding. occurrence. Nodules, masses, and infiltrates can be seen on
Chest radiography may show typical nodular infiltrates in less chest radiography. A 6.5-fold increased incidence of primary
than 10% of patients. Pleural effusion is present in more than lung cancer has been noted among patients with HIV infec-
two-thirds of patients with lung involvement with Kaposi sar- tion and AIDS.
coma. Clinically, pulmonary Kaposi sarcoma is indistinguish-
able from P jiroveci pneumonia or opportunistic pneumonia.
S U M M A RY
Pulmonary Kaposi sarcoma is usually preceded by
cutaneous lesions. About 80%-90% of deaths due to seasonal influenza occur
in persons 65 years.
Lung involvement due to Kaposi sarcoma occurs in up to
35% of patients with this neoplasm. Streptococcus pneumoniae (pneumococcus) is a leading
cause of community-acquired infections such as
Clinically, pulmonary Kaposi sarcoma is indistinguishable
pneumonia, meningitis, otitis media, and sinusitis.
from P jiroveci pneumonia or opportunistic pneumonia.
Immunocompromised patients, especially those receiving
Multiple, discrete, raised, violaceous, or bright-red
long-term corticosteroid therapy, are susceptible to
tracheobronchial lesions can be seen on bronchoscopy.
Legionella infections.
Non-Hodgkin lymphoma involving the lungs occurs in The PPD skin test indicates infection with mycobacteria
less than 10% of patients with AIDS who have lymphoma. and not active disease.
G OA L S Nonsuppurative Complications
Understand the epidemiology and management of sexually The nonsuppurative complications of group A streptococcal
transmitted infections in patients with and without human infection are acute rheumatic fever and acute glomerulone-
immunodeficiency virus (HIV) infection. phritis. Treatment of group A streptococcal infection does not
prevent poststreptococcal glomerulonephritis.
Distinguish differences in pathogenesis and Rheumatic fever occurs only after streptococcal pharyngi-
management of urinary tract infections in men and tis, never after skin infection. The diagnostic criteria for rheu-
women. matic fever are described in Box 20.1. Decreasing inflammation
Differentiate infectious diarrhea syndromes. with aspirin (or corticosteroids) is the main therapy for acute
rheumatic fever, although it will not prevent the development
of chronic rheumatic heart disease.
293
Box 20.1 UPDATED JONES CRITERIA FOR DIAGNOSIS The combination of a painful genital ulcer and tender suppu-
OF INITIAL ATTACK OF RHEUMATIC FEVER a (1992) rative inguinal adenopathy is highly suggestive of chancroid,
which is caused by Haemophilus ducreyi. Nevertheless, clini-
Major manifestations cal inspection may not distinguish these 3 conditions, and all
Carditis patients with genital ulcers should have syphilis serologic test-
Polyarthritis ing and herpes simplex virus (HSV) cell culture or polymerase
Chorea chain reaction. In settings where chancroid is prevalent, such
Erythema marginatum as in Africa and other tropical or subtropical regions, special-
Subcutaneous nodules ized culture for H ducreyi can be performed.
Minor manifestations Chancroid is treated with azithromycin (1 g orally once),
Clinical findings ceftriaxone (250 mg intramuscularly in a single dose), cipro-
Arthralgia floxacin (500 mg orally twice a day for 3 days), or erythromy-
Fever cin base (500 mg orally 3 times a day for 7 days). Persons who
Laboratory findings have had sexual contact with an index patient during the 10
Elevated acute-phase reactants (erythrocyte sedimentation days preceding the patients onset of symptoms should receive
rate, C-reactive protein) treatment.
Prolonged PR interval
Supporting evidence of antecedent group A streptococcal infection Herpes Simplex Virus
Positive throat culture or rapid diagnostic test
Elevated or rising streptococcal antibody titer At least 50 million persons in the United States are infected
with HSV1 or HSV2. Most of them have not been diagnosed
a
If supported by evidence of recent Streptococcus pyogenes infection, then the with genital herpes. Infected persons intermittently shed virus
presence of 2 major, or 1 major and 2 minor, criteria is enough for diagnosis. from the genital tract despite a lack of symptoms, leading to
Exceptions in which the Jones criteria do not need to be fulfilled: 1) recurrent
rheumatic fever (a single major or several minor criteria are sufficient if there is transmission. Isolation of HSV in cell culture or a type-specific
supporting evidence of a recent S pyogenes infection), 2) isolated chorea, and 3) polymerase chain reaction from genital lesions is the preferred
indolent carditis. virologic test. Herpes simplex may also be associated with ery-
Adapted from Special Writing Group of the Committee on Rheumatic Fever,
thema multiforme.
Endocarditis, and Kawasaki Disease of the Council on Cardiovascular Disease in Antivirals can partially control the signs and symptoms of
the Young of the American Heart Association. Guidelines for the diagnosis of rheu- herpes episodes when they are used to treat first and recurrent
matic fever: Jones Criteria, 1992 update. JAMA. 1992 Oct 21:268(15):206973.
Erratum in: JAMA. 1993 Jan 27;269(4):476. Used with permission.
episodes or when they are used as daily suppressive therapy.
Recommended regimens for a first episode of genital HSV
include acyclovir 400 mg orally 3 times a day for 7 to 10 days,
Acute glomerulonephritis may occur after either acyclovir 200 mg orally 5 times a day for 7 to 10 days, famci-
streptococcal skin infections or pharyngitis. clovir 250 mg orally 3 times a day for 7 to 10 days, or valacyclo-
vir 1 g orally twice a day for 7 to 10 days.
Because recurrences are common, especially with HSV
S E XUA L LY T R A N S M I T T E D I N F E C T I O N S
type 2, episodic or continuous suppressive antiviral therapy
with acyclovir (400 mg orally twice a day), famciclovir (250
Sexually transmitted infections remain a major public health
mg orally twice a day), valacyclovir (500 mg orally once a
burden. About 19 million infections occur annually in the
day), or valacyclovir (1 g orally once a day) are all effective in
United States. Rates of sexually transmitted infections are
reducing the frequency of recurrences. Daily treatment with
higher in young African-American women and in men who
valacyclovir (500 mg daily) decreases the rate of HSV type 2
have sex with men. The most common sexually transmitted
transmission in discordant, heterosexual couples in whom the
infections are human papillomavirus, chlamydiosis, herpes
source partner has a history of genital HSV type 2 infection.
simplex, and trichomoniasis. Although selected types of
human papillomavirus are preventable with vaccination, other
sexually transmitted infections require effective barriers to HSV in Pregnancy
prevent transmission. These infections are characterized by
In the first trimester of pregnancy, the development of primary
their clinical presentations: 1) genital ulcers and lesions, 2)
HSV infection may be associated with chorioretinitis, micro-
urethritis, 3) vulvovaginitis and cervicitis, 4) pelvic inflamma-
cephaly, and skin lesions. The risk for transmission to the baby
tory disease, and 5) vaginal discharge.
from an infected mother is 30% to 50% among women who
acquire genital herpes near the time of delivery, 3% for women
G E N I TA L U L C E R S A N D L E S I O N S with a recurrence at delivery, and less than 1% among women
with histories of recurrent herpes with no lesions at the time
Chancroid
of delivery. Prevention of neonatal herpes relies on prevent-
In the United States, patients who present with genital ulcers ing acquisition of genital HSV late in pregnancy and avoid-
usually have genital herpes, syphilis, or chancroid. These con- ing exposure of the infant to herpetic lesions during delivery.
ditions are associated with an increased risk for HIV infection. Women without known genital herpes should be counseled
2 0. P H A RY N G I T I S , S E XUA L LY T R A N S M I T T E D I N F E C T I O N S , U R I N A RY T R AC T I N F E C T I O N S 295
The diagnosis is made from cerebrospinal fluid examination. per oil immersion field, or a positive result of leukocyte esterase
test on first-void urine. The presence of gram-negative intracel-
VDRL testing of cerebrospinal fluid is only 30%-70%
lular diplococci on a urethral smear is indicative of gonorrhea
sensitive.
infection and is often accompanied by chlamydial infection.
Nongonococcal urethritis is diagnosed when microscopy indi-
Treatment of syphilis is based on whether the disease is early cates inflammation without gram-negative intracellular diplo-
or late. For early syphilis (primary, secondary, or early latent [<1 cocci. Urine or urethral exudates should be sent for testing for
year]), benzathine penicillin G 2.4 million units intramuscularly gonorrhea and Chlamydia trachomatis. Chlamydia trachomatis
is used; follow-up serologic testing with RPR is done to ascer- is a frequent cause of nongonococcal urethritis (15%-55% of
tain response to therapy. Alternatives are doxycycline (100 mg cases); however, the prevalence varies by age group, with lower
twice daily for 14 days) or tetracycline (500 mg orally 4 times prevalence among older men. The etiologic agent of most cases
daily for 14 days). Erythromycin (500 mg orally 4 times daily) is of nonchlamydial nongonococcal urethritis is unknown; how-
the least effective. After treatment (especially in early syphilis), ever, Mycoplasma genitalium is emerging as an increasingly
10% to 25% of patients may experience a Jarisch-Herxheimer recognized cause. Complications of nongonococcal urethritis
reaction, manifested by varying degrees of fever, chills, myalgias, among men infected with C trachomatis include epididymitis,
headache, tachycardia, and hypotension. This reaction lasts for prostatitis, and Reiter syndrome.
12 to 24 hours and can be managed symptomatically.
Treatment for late disease (>1 year in duration, cardiovas-
cular disease, gumma, late latent syphilis) is with benzathine GONORRHEA
penicillin 2.4 million units intramuscularly weekly for 3 weeks.
Alternatives are doxycycline (100 mg orally twice daily) or tet- Neisseria gonorrhoeae is a gram-negative intracellular diplococ-
racycline (500 mg orally 4 times daily) for 4 weeks. cus. Rates of gonorrhea have remained stable, but resistance to
Treatment of neurosyphilis is with aqueous penicillin G therapy has increased. The disease often causes symptomatic
(1224 million units intravenously per day) for 10 to 14 days urethritis and discharge in men, but it has few symptoms in
or procaine penicillin (2.4 million units intramuscularly per women and may lead to cervicitis, infertility, ectopic preg-
day) plus probenecid (500 mg 4 times daily) for 10 to 14 days. nancy, and chronic pelvic pain. In women, concomitant proc-
Pregnant patients should receive a penicillin-based regimen titis is common (rectal cultures should be done in all women).
for treatment of all stages of syphilis. If a pregnant patient has Gonococcal pharyngitis is often asymptomatic. The diagnosis
a penicillin allergy, she should be desensitized to penicillin. of gonorrhea may be made with a Gram stain of urethral exu-
For early and secondary syphilis, follow-up clinical and date in men showing intracellular gram-negative diplococci or
serologic testing should be performed at 6 and 12 months. by using urine or urethral-cervicalbased nucleic acid amplifi-
Re-treatment with 3 weekly injections of 2.4 million units of cation tests.
benzathine penicillin G should be given to patients with signs
or symptoms that persist or whose VDRL result has a sustained Neisseria gonorrhoeae commonly causes urethritis,
4-fold increase in titer. HIV testing should be performed if not cervicitis, pharyngitis, and proctitis.
done previously. If the VDRL titer does not decrease 4-fold by
Asymptomatic carrier state occurs in both males and
6 months, consideration also should be given to re-treatment.
females, but it is more common in females.
Patients with latent syphilis should have a follow-up exam-
ination at 6, 12, and 24 months. If the VDRL result increases
4-fold, if a high titer (>1:32) fails to decrease 4-fold within 12 Resistance to penicillin, tetracycline, and, most recently,
to 24 months, or if signs or symptoms attributable to syphi- fluoroquinolones has limited the treatment options to cepha-
lis occur, a cerebrospinal fluid examination should be done losporins. Because concomitant chlamydial infection is often
to rule out the possibility of neurosyphilis and re-treatment present, a second agent is often included in the treatment regi-
should be done accordingly. men. Primary treatment is ceftriaxone (125 mg intramuscu-
Follow-up in patients who receive treatment for neuro- larly) plus doxycycline (100 mg orally twice daily for 7 days) or
syphilis should include testing of cerebrospinal fluid every 6 azithromycin (a single 1-g dose) to also treat chlamydial infec-
months if cerebrospinal fluid pleocytosis was present initially; tion. Cefixime (400 mg once daily) is available as a first-line
this testing is done until the results are normal. If the cell count oral option. Alternative therapies are limited for patients who
is not decreased at 6 months or if the cerebrospinal fluid is not are allergic to -lactam. Spectinomycin is not available in the
entirely normal at 2 years, re-treatment should be considered. United States. Limited data suggest that high-dose azithromy-
cin (2 g in 1 dose) might be an option. Pharyngeal infection is
best treated with ceftriaxone. Therapy recommended for preg-
U R ET H R IT I S S Y N D RO M E S
nant women includes ceftriaxone (125 mg intramuscularly)
or cefixime (400 mg orally) plus azithromycin (1 g orally).
The clinical syndrome of urethral pain and discharge is often Follow-up nucleic acid amplification tests 3 weeks after treat-
associated with chlamydial infection, gonorrhea, and nongono- ment are recommended for all pregnant women. All patients
coccal urethritis. A diagnosis is made on the basis of the following with sexually transmitted diseases should be tested for HIV.
findings: the presence of mucopurulent or purulent discharge, Sexual partners should be offered evaluation and treatment.
a Gram stain of urethral secretions with 5 or more leukocytes Table 20.2 outlines the treatment of gonococcal infections.
(continued)
2 0. P H A RY N G I T I S , S E XUA L LY T R A N S M I T T E D I N F E C T I O N S , U R I N A RY T R AC T I N F E C T I O N S 297
Table 20.2 TREATMENT REGIMENS FOR GONOCOCCAL INFECTIONS AND ASSOCIATED
CONDITIONS (CONTINUED)
Primary treatment of N gonorrhoeae includes ceftriaxone results of joint culture are positive in about 50%. Culture
(125 mg intramuscularly) or cefixime (400 mg orally) specimens should be obtained from the urethra, cervix, rec-
plus doxycycline (100 mg orally twice daily for 7 days) or tum, and pharynx.
azithromycin (single 1-g dose).
Disseminated gonococcemia is most likely to occur during
Fluoroquinolones are no longer recommended for empiric menstruation.
treatment of gonorrhea.
A bacteremic phase may manifest as tenosynovitis,
In 1% to 3% of patients, this infection may lead to skin lesions, and arthralgias; joint cultures are usually
disseminated gonococcal infection. Risk factors include negative.
complement deficiency, female sex, pharyngeal infec-
Rarely, a destructive form of infective endocarditis may
tion, pregnancy, and menstruation. It occurs most often
develop, primarily affecting the aortic valve.
in women during menstruation (when sloughing of endo-
metrium allows access to blood supply, enhanced growth A nonbacteremic phase may present as monoarticular
of gonococci due to necrotic tissue, and change in pH). arthritis of the knee, wrist, and ankle; results of joint
There are 2 distinct phases. The bacteremic phase may man- cultures are positive in about 50%.
ifest as tenosynovitis (around the wrists or ankles [lovers
heels]); painful, distally distributed skin lesions (usually Treatment is with ceftriaxone (1 g intravenously daily for
less than 30 in number, peripheral macular or pustular with 710 days); alternatives include ceftriaxone for 3 or 4 days or
a hemorrhagic component); and polyarthralgias involving until clinical improvement followed by oral cefixime (400 mg
the knees and elbows (the classic dermatitis arthritis syn- daily) to complete a course of 7 to 10 days. If the strain is tested
drome). Rarely, a destructive form of infective endocarditis and found to be penicillin-susceptible, treatment includes
may develop, primarily affecting the aortic valve. Results of penicillin G (10 million units intravenously daily) for 7 to 10
synovial fluid testing are usually negative. The nonbacter- days, or it is given for 3 or 4 days and then oral amoxicillin is
emic phase follows 1 week later and may present as mono- used to finish a 7- to 10-day course. For meningitis, treatment
articular infectious arthritis of the knee, wrist, and ankle; includes ceftriaxone (12 g intravenously every 12 hours for at
2 0. P H A RY N G I T I S , S E XUA L LY T R A N S M I T T E D I N F E C T I O N S , U R I N A RY T R AC T I N F E C T I O N S 299
outpatient therapy is precluded by severe nausea and vomit- Treatment of recurrent disease should include re-treatment
ing, the diagnosis is uncertain, pelvic abscess or peritonitis is followed by a prolonged course of twice-weekly metronida-
present, the patient is pregnant, the patient is an adolescent, zole gel. Bacterial vaginosis has been associated with adverse
or noncompliance is suspected. Table 20.2 outlines the treat- pregnancy outcomes. All symptomatic pregnant women
ment of pelvic inflammatory diseases. should be treated. In pregnant patients, systemic therapy with
Tubo-ovarian abscess may be characterized by an adnexal metronidazole (500 mg twice daily for 7 days) or clindamycin
mass on physical examination or radiographic examination or (300 mg orally twice daily for 7 days) is recommended rather
by failure of antimicrobial therapy. Most abscesses 4 to 6 cm in than topical therapy. Treatment of asymptomatic nonpreg-
diameter respond to medical therapy alone with the preferred nant carriers is not recommended. Some experts recommend
regimen of ampicillin, gentamicin, and clindamycin. Large treatment of asymptomatic pregnant women at high risk for
abscesses (>10 cm) often necessitate operation. preterm delivery. Routine treatment of sex partners is not
recommended.
Tubo-ovarian abscess is characterized by an adnexal mass
on physical examination or radiographic examination or by Bacterial vaginosis diagnosis is based on the presence
failure of antimicrobial therapy. of grayish white discharge that is homogeneous, the
presence of clue cells on wet-mount examination,
a vaginal fluid pH more than 4.5, and a fishy smell
when secretion is mixed with 10% potassium hydroxide
VAG I N IT I S
(positive whiff test).
Vaginitis is characterized by a vaginal discharge or vulvar
Therapy options are metronidazole (500 mg orally twice
itching, odor, or irritation. The 3 entities most frequently
daily for 7 days) or clindamycin (300 mg orally twice daily
associated with vaginal discharge are bacterial vaginosis (a
for 7 days).
replacement of the normal vaginal flora by an overgrowth of
anaerobic microorganisms, mycoplasmas, and Gardnerella
vaginalis), trichomoniasis (T vaginalis), and candidiasis. Trichomoniasis
Women with trichomoniasis may have a malodorous
Bacterial Vaginosis yellow-green vaginal discharge with vulvar irritation, dys-
uria, or dyspareunia. Petechial lesions may be noted on the
Bacterial vaginosis is the most common vaginal infection cervix with colposcopy (strawberry cervix). Although sex-
affecting women of childbearing age. Risk factors for bacterial ual transmission is most common, trichomoniasis has been
vaginosis include multiple sex partners (increased incidence transmitted to health care workers via urine soaked sheets.
has also been reported among women who have sex with The diagnosis is established from wet mount of vaginal
women), new partners, douching, and a lack of vaginal lacto- secretions showing the motile organisms. The vaginal pH
bacilli. Women with bacterial vaginosis are at increased risk for is usually more than 4.5. New rapid tests for trichomonia-
sexually transmitted infections, low-birth-weight infants, and sis in women include the 10-minute dipstick assay (OSOM
a substantial reduction in their quality of life. Bacterial vagi- Trichomonas Rapid Test) and the 45-minute nucleic acid
nosis is due to a change in local vaginal ecology from a flora of probe test (Affirm VPIII) that evaluates for T vaginalis, G
predominant lactobacilli to one of various anaerobic bacteria. vaginalis, and Candida albicans. Both of these tests are per-
Organisms associated with the syndrome include Atopobium formed on vaginal secretions and have a sensitivity of more
vaginae, Gardnerella, Prevotella, Mobiluncus species, M homi- than 83% and a specificity of more than 97%; the rapid test
nis, Megasphaera species, and the Clostridiales bacteria (bacte- for trichomoniasis is much more sensitive than the direct
rial vaginosisassociated bacterium 1, 2, and 3). wet-mount examination.
Bacterial vaginosis can be diagnosed with clinical (Amsel) Treatment is with metronidazole (2 g as a single dose) or
or microbiologic (Nugent) criteria. The Amsel clinical crite- tinidazole (2 g: 4 500-mg tablets as a single dose). A 7-day
ria require 3 of the following: a grayish white discharge that course of metronidazole (500 mg twice daily) is an alternative.
is homogeneous and coats the vaginal walls, clue cells on Gastrointestinal tolerance may be better with tinidazole. All
wet-mount examination, a vaginal fluid pH more than 4.5, partners should be examined and treated. Although treatment
and a fishy smell when secretion is mixed with 10% potas- in asymptomatic pregnant women is controversial, treatment
sium hydroxide (positive whiff test). Rapid nucleic acid in symptomatic pregnant women should be a one-time dose of
tests (eg, Affirm VPIII) can also be used. 2 g of metronidazole.
Recommended treatment regimens include metro-
nidazole (500 mg orally twice daily for 7 days), clindamycin Infection with T vaginalis often is characterized by
(300 mg orally twice daily for 7 days) as an alternative, topi- yellow-green, purulent discharge.
cal clindamycin cream (2% for 7 days), or metronidazole gel
Diagnosis is established with wet mount or a rapid test of
(0.75% intravaginal applicator nightly for 5 days) (the clin-
vaginal secretions (the latter has increased sensitivity).
damycin cream appears less efficacious than the metronida-
zole regimens). Single-dose metronidazole therapy should Treatment of T vaginalis is with metronidazole or
not be used. Recurrence of bacterial vaginosis is common. tinidazole orally.
2 0. P H A RY N G I T I S , S E XUA L LY T R A N S M I T T E D I N F E C T I O N S , U R I N A RY T R AC T I N F E C T I O N S 301
as the patient improves. A urine culture is recommended 1 to Causes of UTI in males include E coli in 50%, other
2 weeks after completion of therapy only in pregnant women, gram-negative organisms in 25%, enterococci in 20%, and
children, and patients with recurrent pyelonephritis in whom others in 5%.
suppressive therapy is being considered.
Men with UTI should not receive short-course therapy.
Recurrent UTIs are common in women. Prophylaxis may
be offered to women who have 2 or more symptomatic UTIs
within 6 months or 3 or more over 12 months. For these
women, 3 options have all been shown to be effective: con-
tinuous prophylaxis, postcoital prophylaxis, or intermittent GASTROINTESTINAL INFECTIONS
self-treatment. For postmenopausal women, vaginal estrogen
supplementation is beneficial. BAC T E R I A L A N D TOX I G E N I C D I A R R H E A
Asymptomatic bacteriuria (>105 colony-forming units/ The principal causes of toxigenic diarrhea are listed in
mL) in a midstream urine specimen should be treated only Table 20.3, and those of invasive diarrhea are listed in
in pregnant women and in patients undergoing urinary Table 20.4. Fecal leukocytes usually are absent in toxigenic
tract instrumentation. diarrhea. In invasive diarrhea, fecal leukocytes may be present.
The travel history is often important.
For acute uncomplicated pyelonephritis, 5 days of oral
levofloxacin therapy is as effective as 10 days of twice-daily
ciprofloxacin therapy.
Campylobacter jejuni
Campylobacter jejuni is the most common cause of sporadic
A follow-up urine culture is not usually recommended.
acute bacterial diarrhea. Outbreaks, although less common,
Cephalosporins and trimethoprim-sulfamethoxazole are associated with consumption of unpasteurized dairy
should not be used to treat enterococcal UTI. products and undercooked poultry. The incidence of dis-
ease peaks in summer and early fall. Diarrhea may be bloody.
Fever usually is present. The diagnosis is established by iso-
IN MALES lation of the organism from stool culture. Treatment is usu-
In men, UTI is less common, but it increases in frequency with ally symptomatic because the disease tends to be self-limited.
age. Urologic abnormalities (such as benign prostatic hyper- Erythromycin (500 mg twice daily for 5 days) or azithromy-
plasia) are common. Men with symptomatic dysuria should be cin can be used when symptoms are prolonged or the host is
investigated for sexually transmitted diseases and prostatism. immunocompromised.
When a UTI is suspected, urine culture and sensitivity testing
should be done. Causative organisms include E coli in 50% of Outbreaks of bacterial diarrhea caused by C jejuni are
cases, other gram-negative organisms in 25%, enterococci in associated with consumption of unpasteurized milk and
20%, and others in 5%. If signs and symptoms of epididymitis, undercooked poultry.
acute prostatitis, and pyelonephritis are present, treat accord- Macrolide therapy is the therapy of choice for
ingly. If uncomplicated lower UTI is present, treatment dura- Campylobacter-associated diarrhea.
tion is 10 to 14 days. If symptoms persist or relapse, the urine
culture should be repeated. If results are positive, treat for a
Staphylococcal Enterotoxin
minimum of 6 weeks. If culture results are negative, consider
further evaluation for one of the chronic prostatitis-chronic Preformed enterotoxins produced by Staphylococcus aureus
pelvic pain syndromes. are a common cause of food poisoning in the United States.
Escherichia coli 12 No No No
The toxin is heat stable and, therefore, is not destroyed by diarrhea develops and usually is associated with eating meat
cooking contaminated foods. Preformed toxin by S aureus or vegetables. The diagnosis is confirmed by isolation of the
is ingested in contaminated food. It has a short incubation organism from contaminated food. The illness is self-limited
period of 4 to 6 hours. Onset is abrupt, with severe vomit- and treatment is supportive.
ing (often predominates), diarrhea, and abdominal cramps.
The duration of infection is 8 to 24 hours. Diagnosis is based Escherichia coli
on rapid onset, absence of fever, and history. Treatment is
supportive. Diarrhea caused by E coli can be either enterotoxigenic or
enterohemorrhagic. Enterotoxigenic E coli is the most com-
Bacterial diarrhea due to S aureus is caused by ingestion mon etiologic agent of travelers diarrhea. Treatment consists
of preformed toxin in contaminated food; it has a short of fluid and electrolyte replacement along with loperamide
incubation period (46 hours). plus a fluoroquinolone or rifaximin. Medical evaluation
should be sought if fever and bloody diarrhea occur. For pro-
Preformed enterotoxins produced by S aureus are not phylaxis, travelers should use food and water precautions.
destroyed by cooking food. Routine prophylactic use of trimethoprim-sulfamethoxazole,
Diagnosis is based on rapid onset, absence of fever, and ciprofloxacin, and doxycycline is not recommended. The use
history. of bismuth subsalicylate as primary prophylaxis in travelers
reduces the incidence of enterotoxigenic E coli-associated
diarrhea by up to 60%.
Clostridium perfringens
Bacterial diarrhea caused by C perfringens is associated with Enterotoxigenic E coli is the most common etiologic agent
ingestion of bacteria that produce toxin in vivo, often in improp- in travelers diarrhea.
erly prepared or stored precooked foods (meat and poultry Treatment consists of fluid and electrolyte replacement
products). Food is precooked and toxin is destroyed but spores along with loperamide plus a fluoroquinolone or
survive; when food is rewarmed, spores germinate. When food rifaximin.
is ingested, toxin is produced. Diarrhea is more severe than
vomiting, and abdominal cramping is prominent. Onset of
symptoms is later than with S aureus infection. Duration of ill- Escherichia coli O157:H7 causes an uncommon form of
ness is 24 hours. The diagnosis is based on the later onset of bloody diarrhea. This agent has been identified as the cause
symptoms, a typical history. Treatment is supportive. of waterborne illness, outbreaks in nursing homes and child
care centers, and sporadic cases. It also has been transmitted
In diarrhea caused by C perfringens, ingested bacteria by eating undercooked beef and other contaminated food
produce toxin in vivo in precooked food. products. Bloody diarrhea, severe abdominal cramps, fever,
and profound toxicity characterize this enterohemorrhagic ill-
Diarrhea is more severe than vomiting; abdominal ness. It may mimic ischemic colitis. At extremes of age (old
cramping is prominent. and young), the infection may produce hemolytic uremic
syndrome and death. This organism should be considered in
all patients with hemolytic uremic syndrome. Antibiotics are
Bacillus cereus Toxin not known to be effective and may increase the likelihood of
Two types of food poisoning are associated with B cereus hemolytic uremic syndrome.
infection. Profuse vomiting follows a short incubation period
(16 hours); this is associated with the ingestion of a pre- Escherichia coli O157:H7 has been identified as the cause
formed toxin (usually in fried rice). A disease with a longer of waterborne illness, outbreaks in nursing homes and
incubation occurs 8 to 16 hours after consumption; profound child care centers, and sporadic cases.
2 0. P H A RY N G I T I S , S E XUA L LY T R A N S M I T T E D I N F E C T I O N S , U R I N A RY T R AC T I N F E C T I O N S 303
Eating undercooked beef also transmits E coli O157:H7. sources that were not previously associated with this
infection.
Bloody diarrhea, severe abdominal cramps, and profound
toxicity characterize E coli O157:H7 infection; it may Salmonella infection may cause septicemia in patients with
resemble ischemic colitis. sickle cell anemia or AIDS.
Infection should be considered in all patients with Bloody diarrhea is often absent (a feature distinguishing it
hemolytic uremic syndrome. from Shigella infection).
Antibiotic therapy is not recommended. Salmonella bacteremia can lead to hematogenous
seeding of abdominal aortic plaques resulting in mycotic
aneurysms.
Shigella
In nonbacteremic patients with Salmonella-associated
Diarrhea caused by Shigella species is often acquired out- diarrhea, antibiotics may prolong the carrier state and do
side the United States. It often is spread from person to per- not affect the course of the disease.
son or consumption of contaminated food or water. Bloody
diarrhea is characteristic, bacteremia may occur, and fever Salmonella serotype typhi is rare in the United States;
is present. The diagnosis is confirmed by stool culture and often, it is found in travelers returning from endemic regions
blood culture (occasionally positive). Treatment is with who present with fever. Patients with typhoid fever have rela-
ampicillin, trimethoprim-sulfamethoxazole, norfloxacin, tive bradycardia and rose spots (50%). The leukocyte count
ciprofloxacin, or azithromycin. Resistance to ampicillin, may be decreased. Blood cultures usually are positive within
trimethoprim-sulfamethoxazole, fluoroquinolone, or azithro- approximately 10 days of symptom onset, whereas stool cul-
mycin has been reported. The illness may precede the onset tures become positive later.
of spondyloarthropathy (reactive arthritis) in persons with There are many nontyphoidal Salmonella species.
HLA-B2 and group B Shigella flexneri. Salmonella typhimurium and S enteritidis produce gastroen-
teritis and occasionally bacteremia. Nontyphoidal Salmonella
Diarrhea caused by Shigella species is associated with species can cause chronic bacteremia and infections of athero-
person-to-person transmission and the consumption of sclerotic aortic aneurysms. Urinary tract infections caused by
contaminated food or water. Salmonella particularly occur in patients who are coinfected
Bloody diarrhea is characteristic, bacteremia may occur, with Schistosoma haematobium. Antimicrobial resistance is
and fever is present. increasingly common with Salmonella serotype typhi. Most
cases of Salmonella gastroenteritis resolve without ther-
The illness may precede the onset of spondyloarthropathy apy. Serious or invasive infections should be treated with a
(reactive arthritis) in persons with HLA-B2 and group B S third-generation cephalosporin or fluoroquinolone pending
flexneri. susceptibility data.
2 0. P H A RY N G I T I S , S E XUA L LY T R A N S M I T T E D I N F E C T I O N S , U R I N A RY T R AC T I N F E C T I O N S 305
Vomiting is a more common early manifestation than watery There is no effective therapy for Cryptosporidium.
diarrhea. Hospitalization for dehydration is common in young Paromomycin and nitazoxanide, a new drug, show some effi-
children. Diagnosis is made by detection of antigen in stool. cacy. Nitazoxanide has efficacy of 56% to 88% in immuno-
Treatment is symptomatic. competent patients.
Noroviruses are a common cause of epidemic diarrhea and
winter vomiting disease in older children and adults and have Cryptosporidiosis is an important cause of diarrhea in
high secondary attack rates. Outbreaks have been reported patients with AIDS.
from day-care facilities, nursing homes, hospitals, family gath-
erings, and cruise ships. Various contaminated foods such as Waterborne outbreaks have been reported.
shellfish, undercooked fish, cake frosting, salads, and water The diagnosis may be missed on standard stool
have been implicated. The illness is an explosive, self-limited examination for ova and parasites.
(36 hours) condition with severe nausea, vomiting, watery
diarrhea, and dehydration. Treatment is symptomatic. Cyclospora cayetanensis is a protozoan that can cause per-
sistent diarrhea, fever, and profound fatigue. First described
Outbreaks of norovirus are associated with eating shellfish, in travelers to tropical areas of the world, disease due to
undercooked fish, cake frosting, and salads and with Cyclospora also has been linked to consumption of contami-
drinking contaminated water. nated food shipped to the United States (eg, raspberries from
Numerous outbreaks of noroviruses have occurred on Guatemala). Like Cryptosporidium, the organism may not
cruise ships. be detected on routine stool examinations; therefore, testing
specific to the organism should be ordered. The illness can be
Illness, although potentially severe and dominated by effectively treated with trimethoprim-sulfamethoxazole.
vomiting, is self-limited.
Infection with C cayetanensis causes persistent diarrhea,
fever, and profound fatigue.
PA R A S IT I C D I A R R H E A Disease due to Cyclospora has been linked to consumption
The travel and exposure histories are critical to determining which of contaminated food shipped to the United States
agents should be sought. The parasitic conditions that are most (raspberries from Guatemala).
common in the United States are giardiasis, amebiasis, and cryp-
tosporidiosis. Giardiasis may present with abdominal bloating,
I N T R A-A B D O M I NA L A B S C E S S E S
weight loss, and flatulence. Hosts at risk are homosexual men,
hikers with exposures to streams, day-care contacts, and persons Intra-abdominal abscesses may arise from a hematogenous,
with immunoglobulin A deficiency or HIV. A wet preparation contiguous, traumatic, or operative route. Hepatic abscesses
examination of stool or a Giardia antigen test may establish the are among the most common and may be bacterial or non-
diagnosis. Treatment is with metronidazole or tinidazole. bacterial in origin. Nonbacterial organisms are Candida and E
Entamoeba histolytica infection is acquired through inges- histolytica (amebic abscess). However, most hepatic abscesses
tion of contaminated water or food containing cysts from an are bacterial in origin as a result of portal vein bacteremia from
infected carrier. The disease may be more common in immi- an intestinal source such as appendicitis or diverticulitis; bac-
grants from regions with high endemic rates of amebiasis such teremia from a primary focus elsewhere; biliary tract origin,
as Central and South America. Infected persons most com- as in obstruction or ascending cholangitis; direct extension
monly present with a subacute onset of colitis or liver abscess. (subphrenic abscess); or trauma. Most often, patients present
The diagnosis can be made by stool testing or serum antibody with the insidious onset of symptoms of malaise and anorexia
tests. Treatment is with metronidazole (750 mg 3 times daily followed by right upper abdominal pain and fever. Computed
for 710 days). After treatment, the intestinal carrier state is tomography is the best test for diagnosis of intra-abdominal
eradicated with paromomycin or iodoquinol. and hepatic abscesses. The microbiologic nature is variable,
Cryptosporidium parvum is an important cause of diarrhea, depending on the origin. Biliary-source infections are usu-
especially in persons with AIDS, who may have a chronic, debil- ally due to enteric gram-negative bacteria such as E coli or
itating illness. Cryptosporidiosis is also a cause of self-limited Enterobacter species, whereas intestinal sources are often poly-
diarrhea in otherwise healthy persons. Waterborne outbreaks microbial (Enterobacteriacae, Streptococcus anginosus group,
have been reported in Georgia and Wisconsin. They occur and Bacteroides). The initial evaluation of a hepatic abscess
most often in late summer or fall. The organism is resistant to should include blood cultures and amebic serologic tests. If
chlorination and can best be eliminated from water sources by the amebic serologic results are negative, aspiration should
microfiltration. Thirty-five percent of patients have a coinfec- be performed and antibiotics directed according to culture
tion, most commonly with Giardia. results. Pyogenic abscesses are best managed by percutaneous
The stool Cryptosporidium enzyme-linked immunosorbent drainage and antimicrobial therapy. Empiric options include
assaybased antigen test has sensitivity of 87%, specificity ampicillin plus gentamicin, a fluoroquinolone plus metron-
99%, and positive predictive value 98%. It has to be ordered idazole, or a third-generation cephalosporin plus metron-
specifically if cryptosporidiosis is in the differential diagnosis. idazole, a -lactam/-lactamase inhibitor combination, or a
2 0. P H A RY N G I T I S , S E XUA L LY T R A N S M I T T E D I N F E C T I O N S , U R I N A RY T R AC T I N F E C T I O N S 307
21.
HIV INFECTIONa
Mary J. Kasten, MD, and Zelalem Temesgen, MD
G OA L S E P I D E M I O L O GY
Identify how human immunodeficiency virus (HIV) is An estimated 33.3 million people in the world are living with
transmitted and what behaviors and conditions affect the HIV. Approximately 2.6 million people were infected with the
risk of transmission. virus in 2009. More than 25 million people have died of AIDS,
Review the natural history of HIV infection and AIDS, 1.8 million in 2009 alone. More than 90% of the people liv-
including AIDS-defining conditions. ing with HIV reside in developing countries where resources
for diagnosis, prevention, and management of HIV are scarce.
Recognize when treatment for HIV is indicated and In the United States, an estimated 1.2 million persons are liv-
understand the basic principles of antiretroviral treatment. ing with HIV; about one-fifth of these do not know they are
infected. Persons with undiagnosed infection are thought to
Recognize when prophylaxis is indicated for opportunistic
be responsible for a substantial proportion of new infections
infection in HIV-infected patients and for which
in the United States.
infections it should be given.
Nearly half of all persons with newly diagnosed HIV in the
United States are African Americans even though they make
AIDS was first reported in 1981, when gay men presented
up only 13% of the general population. One-fourth of newly
with Pneumocystis pneumonia or Kaposi sarcoma. HIV was
diagnosed cases in the United States are in women. Globally,
identified as the cause of AIDS in 1984. Testing for HIV
half of HIV-infected persons are women.
became available in the United States in 1985. Considerable
gains in the understanding and treatment of HIV have been
Persons with undiagnosed HIV infection are responsible
made during the past 30 years.
for a substantial proportion of HIV transmission.
There are 2 types of HIV: HIV-1 and HIV-2. Most reported
cases of HIV disease around the world are caused by HIV-1. Globally, half of HIV-infected persons are women.
HIV-2 occurs predominantly in western Africa. Although
HIV-1 and HIV-2 are clinically indistinguishable and have
identical modes of transmission, HIV-2 is less easily transmit- TR ANSMISSION
ted than HIV-1 and slower to progress to AIDS.
HIV is transmitted sexually, perinatally, by parenteral
There are 2 types of HIV: HIV-1 and HIV-2. inoculation (eg, intravenous drug injection, occupational
exposure), through blood products, and, less commonly,
Most reported cases of HIV disease are caused by
through donated organs or semen. Sexual transmission
HIV-1.
is the most common means of infection. Conditions that
may increase the risk of sexually acquiring HIV infection
include traumatic intercourse (ie, receptive anal), ulcerative
genital infections (including syphilis, herpes simplex, and
a
Portions previously published in Warnke D, Barreto J, Temesgen Z. chancroid), and lack of circumcision. The proper use of
Antiretroviral drugs. J Clin Pharmacol. 2007 Dec;47(12):15709. Used with per- latex condoms substantially reduces the risk of HIV trans-
mission; treatment guidelines for opportunistic infections based on Benson CA,
Kaplan JE, Masur H, Pau A, Holmes KK; CDC; National Institutes of Health; mission. Nonoxynol spermicide increases the risk of HIV
Infectious Diseases Society of America. Treating opportunistic infections among transmission; therefore, condoms that do not contain sper-
HIV-infected adults and adolescents: recommendations from CDC, the National micide are preferred for HIV prevention. Perinatal trans-
Institutes of Health, and the HIV Medicine Association/Infectious Diseases
Society of America. MMWR Recomm Rep. 2004 Dec 17;53(RR-15):1112. mission can occur in utero, at the time of birth, and through
Erratum in: MMWR Morb Mortal Wkly Rep. 2005 Apr 1;54(12):311. breast milk.
308
Table 21.1 RISK OF ACQUIRING HIV, BY TYPE OF multiple transfusions) and participation in HIV vaccine stud-
EXPOSURE ies. Causes of false-negative results include testing during the
pre-seroconversion (window) period, bone marrow transplant,
TYPE OF EXPOSURE RISK, %
agammaglobulinemia, seroreversion in late-stage disease, and
infection with HIV-2 or unusual HIV subtypes (eg, subtypes
Transfusion of HIV-positive blood >90
O and N). Technical or laboratory error can be a cause of both
Percutaneous needlestick 0.3 false-positive and false-negative results. Rapid tests for HIV
with high sensitivity and specificity similar to conventional
Receptive anal intercourse 0.5
HIV screening tests have been approved by the US Food and
Receptive penile-vaginal intercourse 0.1 Drug Administration (FDA); positive results of these tests
also require confirmatory testing.
Insertive intercourse 0.050.07
Individuals with positive results of ELISA, EIA, or a
Oral intercourse 0.0050.01 rapid test should undergo confirmatory testing, usually
Western blot (WB) antibody testing. The guidelines of
Blood to mucous membranes 0.09
the Centers for Disease Control and Prevention (CDC)
Blood to nonintact skin <0.1 for interpretation of the WB test are as follows: the pres-
ence of antibody against any 2 of the 3 major viral gene
Abbreviation: HIV, human immunodeficiency virus. products (p24, gp41, or gp120/gp160) is classified as posi-
tive; an HIV WB result is classified as negative if no major
or minor bands are present; results that cannot be classi-
The mode of transmission of HIV infection varies from fied as positive or negative on the basis of these criteria are
region to region. In North America, men who have sex with categorized as indeterminate. If results are indeterminate,
men make up the largest population of those living with HIV the clinician should assess the risk of HIV infection in the
and those with a new diagnosis. In sub-Saharan Africa, het- patient and retest in 1 to 3 months. HIV RNA assays may
erosexual intercourse is the primary mode of transmission of be of additional help in these cases, particularly if a patient
HIV. In eastern Europe and central Asia, more than half of is at high risk for HIV infection. The risk of HIV infection
new HIV infections are due to the use of nonsterile equip- is extremely low in patients with repeatedly indeterminate
ment used for injecting drugs. WB results.
In the United States, all blood donations have been rou-
tinely tested for HIV-1 antibody since early 1985. This prac-
An HIV ELISA, EIA, or an FDA-approved rapid
tice has virtually eliminated the transmission of HIV through
test should be used to screen people for chronic HIV
blood products in the United States.
infection.
The risk of acquiring HIV varies greatly depending on the HIV WB testing is used to confirm positive results of
exposure (Table 21.1). screening tests for HIV.
The risk of sexually acquiring HIV varies greatly: receptive
anal intercourse > receptive vaginal intercourse > insertive The CDC recommends that screening for HIV infection
intercourse >>> oral intercourse. be performed routinely for all patients 13 to 64 years old.
An opt-out approach, similar to what has been used success-
Circumcision decreases the risk of acquiring HIV fully for many years with pregnant women, is recommended.
infection. With the opt-out approach, testing is performed after the
Proper use of latex condoms decreases HIV transmission patient is notified, unless the patient declines. Neither sepa-
during sex. rate written consent nor prevention counseling is required;
general consent for medical care is considered sufficient to
encompass consent for HIV testing. It is hoped that rou-
tine screening will lead to earlier diagnosis and earlier treat-
L A B O R ATO RY D I AG N O S I S ment of HIV and thus improved health, extended lifespan,
decrease in HIV transmission, and decrease in the stigma of
The enzyme-linked immunosorbent assays (ELISAs) and testing. Studies have shown that most people, once HIV is
enzyme immunoassays (EIAs) are the most common assays diagnosed, change their behavior to decrease risk of trans-
used as a screening test for HIV-1 infection. They detect mission to others.
HIV-specific antibodies. They have high (>99%) sensitivity Patients who engage in behaviors that place them at risk
and specificity but low positive predictive values in of being infected with HIV should be screened on a regular
low-prevalence populations. For this reason, positive results basis. All pregnant women should be screened for HIV infec-
require confirmation with an additional test. False-positive tion even if the results of previous screening have been nega-
results can occur for several reasons. These include the tive. Chronic HIV infection should be considered in patients
presence of cross-reacting antibodies in certain patients with many different presentations; some of the more common
(eg, multiparous women and persons who have received clues are listed in Box 21.1.
21. H I V I N F E C T I O N 309
Box 21.1 COMMON CLINICAL CLUES TO CHRONIC HIV Table 21.2 FREQUENCY OF SYMPTOMS AND FINDINGS
INFECTION ASSOCIATED WITH ACUTE HIV-1 INFECTION
AC U T E H I V I N FEC T I O N Adapted from Kahn JO, Walker BD. Acute human immunodeficiency virus type 1
infection. N Engl J Med. 1998 Jul 2;339(1):339. Used with permission.
Days to weeks after exposure to HIV, most infected persons
present with a brief illness that may last from a few days to a few
weeks. This period of illness is associated with an enormous The viral load is usually very high during acute HIV.
amount of circulating virus, a rapid decline in the CD4 cell
count, and a vigorous immune response. Occasionally, CD4
counts decrease to levels at which patients can present with oppor-
C H RO N I C H I V I N FEC T I O N
tunistic illness. Patients often present with a mononucleosis-like
illness, but the clinical manifestations of acute HIV infection After acute HIV infection, CD4 counts rebound, although
are extremely varied (Table 21.2). Severe acute infections have not always to baseline, and the viral load decreases to a set
been associated with more rapid progression of HIV disease. point that often stays stable for years. Over time, most patients
One should consider acute HIV infection in patients with any have a gradual loss of CD4 cells. Some patients remain asymp-
unusual febrile illness or viral-like syndrome. Results of ELISA tomatic with relatively preserved CD4 counts for more than
are usually negative (window period), and the results of WB a decade; other patients progress to AIDS in 2 to 3 years. The
testing should be negative or indeterminate. However, p24 anti- loss of CD4 cells eventually places the individual at risk for
gen, HIV culture, and polymerase chain reaction results may opportunistic infections and other complications of HIV. The
be positive. During acute symptomatic infection, the viral load CDC defines AIDS as known HIV infection with a CD4
(HIV RNA level) is high, generally more than 100,000 copies/ count less than 200 cells/mcL or HIV infection associated
mL, and patients are highly infectious. with an AIDS-defining illness (Box 21.2).
Acute HIV infection occurs within days to weeks after Gradual loss of CD4 cells is the hallmark of HIV infection.
exposure to HIV.
The rate of progression to AIDS is variable.
Acute HIV often presents with a mononucleosis-type
illness. The illnesses and conditions associated with HIV infec-
Acute HIV can imitate many other illnesses and syndromes. tion vary greatly depending on an individuals CD4 count
and other behaviors. Figure 21.1 illustrates the natural history
Results of WB testing should be negative or indeterminate of HIV infection and the stages at which conditions that are
for HIV with acute infection. commonly associated with HIV infection occur.
I M MU N I Z AT I O NS S U B S TA N C E A BUS E
Patients with HIV infection should have routine immuniza- Many patients with HIV have healthy lifestyles, but oth-
tions, but live virus vaccines should be given cautiously and ers use illicit drugs, drink alcohol to excess, or smoke. It is
generally avoided in patients with CD4 counts less than 200 imperative to address these issues with HIV-infected patients,
cells/mcL. One should consider deferring vaccination for and this should be done in a nonjudgmental way that helps
patients with low CD4 cell counts and immunizing them patients move toward healthier behaviors. Illicit drug use is
once their immune system has improved. Alternatively, immu- not a contraindication to antiretroviral medication, and many
nizations can be given and potentially repeated after immune drug users are compliant with use of HIV medications. The
recovery. provider needs to be aware of what substances are being used
All patients with HIV infection who are not immune to or to ensure there are no worrisome drug interactions between
infected with hepatitis B should receive the hepatitis B series. prescribed and nonprescribed substances. Many patients with
Antibody response to the vaccination should be verified after HIV smoke; as HIV-infected patients live longer and do well
the series is completed. with HIV, illness related to tobacco use is increasing, includ-
Hepatitis A vaccine is recommended for all patients who ing an increased risk of lung cancer and heart disease.
are at risk, including men who have sex with men, travelers
to developing countries, and patients with hepatitis B or C or Lifestyles and habits of patients with HIV need to be
other liver disease. addressed because they may affect treatment and outcome.
21. H I V I N F E C T I O N 311
Candida esophagitis
Herpes simplex
Cryptococcosis
1,000 Persistent generalized PCP 107
lymphadenopathy Toxoplasmosis
Wasting 106
800
copies/mL
600
104
Pneumococcal pneumonia
400 Candida vaginitis 103
ITP
TB 102
Kaposi
200 Oral thrush
Hairy leukoplakia 101
Lymphoma MAC
CMV
0 0
Time
Figure 21.1 Natural History of Human Immunodeficiency Virus (HIV) Infection: CD4 Counts, Viral Load, and Clinical Manifestations. CMV indicates
cytomegalovirus; ITP, idiopathic thrombocytopenic purpura; MAC, Mycobacterium avium complex; PCP, Pneumocystis pneumonia; TB, tuberculosis.
CANCER SCREENING
are generally well whether or not they are receiving antiretro-
Three malignancies (Kaposi sarcoma, non-Hodgkin lym- viral treatment should have routine cancer screening as recom-
phoma, and invasive cervical cancer) have been designated as mended for uninfected persons, with the exception of the need
AIDS-defining cancers. Several other malignancies, although for more frequent Papanicolaou (Pap) smears. HIV-infected
not classified as AIDS-defining, seem to be more common women should have a Pap smear at the time of diagnosis. If the
among people infected with HIV. HIV-infected patients who result is normal, the Pap smear should be repeated in 6 months
Pneumocystis jiroveci CD4 <200 TMP-SMX DS or TMP-SMX SS TMP-SMX DS PO 3 times weekly or dapsone 100
pneumonia (PCP) cells/mcL 1 tablet PO daily mg or 50 mg PO bid or dapsone 50 mg PO daily +
or pyrimethamine 50 mg PO weekly + leucovorin 25
oropharyngeal mg PO weekly or aerosolized pentamidine 300 mg
candidiasis monthly or atovaquone 1,500 mg PO daily
Toxoplasma gondii Toxoplasma TMP-SMX DS 1 tablet PO daily TMP-SMX DS 1 tablet PO 3 times weekly or TMP-SMX
encephalitis IgG-positive with SS 1 tablet PO daily or dapsone 50 mg 1 tablet PO
CD4 <100 cells/ daily + pyrimethamine 50 mg & leucovorin 25 mg PO
mcL weekly or dapsone 200 mg + pyrimethamine 75 mg +
leucovorin 25 mg weekly or atovaquone 1,500 mg +
pyrimethamine 25 mg + leucovorin 10 mg PO daily
MAC disease CD4 <50 cells/ Azithromycin 1,200 mg PO once Rifabutin 300 mg PO daily (adjust based on interactions
mcL after ruling weekly or clarithromycin 500 with antiretroviral therapy)
out active MAC mg PO twice weekly or azithro-
infection mycin 600 mg PO twice weekly
Abbreviations: bid, twice daily; DS, double strength; Ig, immunoglobulin; MAC, Mycobacterium avium complex; PCP, Pneumocystis pneumonia; PO, orally; SS, single
strength; TMP-SMX, trimethoprim-sulfamethoxazole.
Adapted from Kaplan JE, Benson C, Holmes KK, Brooks JT, Pau A, Masur H. Guidelines for prevention and treatment of opportunistic infections in HIV-infected
adults and adolescents: recommendations from CDC, the National Institutes of Health, and the HIV Medicine Association of the Infectious Diseases Society of America.
MMWR Morb Mortal Wkly Rep. 2009 Apr 10;58(RR04):1198.
Abbreviations: bid, twice daily; DS, double strength; IV, intravenously; PCP, Pneumocystis pneumonia; PO, orally; tid, 3 times daily; TMP-SMX, trimethoprim-
sulfamethoxazole.
Adapted from Kaplan JE, Benson C, Holmes KK, Brooks JT, Pau A, Masur H. Guidelines for prevention and treatment of opportunistic infections in HIV-infected
adults and adolescents: recommendations from CDC, the National Institutes of Health, and the HIV Medicine Association of the Infectious Diseases Society of America.
MMWR Morb Mortal Wkly Rep. 2009 Apr 10;58(RR04):1198.
21. H I V I N F E C T I O N 313
200 cells/mcL for at least 3 months as a result of antiretroviral function, the yield of sputum smear and culture is similar to
therapy. Rarely, PCP occurs at higher CD4 counts, and sec- that in HIV-negative patients.
ondary prophylaxis should then be continued longer. The management of HIV-infected patients taking antiret-
roviral agents and undergoing treatment for active TB is com-
plex. Protease inhibitors and nonnucleoside analogue reverse
T U B E RC U L O S I S
transcriptase inhibitors (NNRTIs) have significant interac-
Tuberculosis (TB) is the most common HIV-associated tions with the rifamycins (rifampin, rifabutin, and rifapen-
opportunistic infection globally. TB is a preventable disease; tine) used to treat mycobacterial infections. Compared with
all patients with HIV infection should be screened with either rifampin, rifabutin has substantially less activity as an inducer
a tuberculin skin test or an interferon- release assay. All of cytochrome P450. Substitution of rifabutin for rifampin in
HIV-infected patients with a positive test result (5 mm for treatment regimens for TB is a practical choice for patients
the skin test), a past history of a positive test result, or recent who are also undergoing therapy with protease inhibitors or
exposure to a person with active TB should be treated for with NNRTIs. TB in HIV-infected persons that is susceptible
latent TB provided they have no symptoms or signs to sug- to all first-line antituberculosis drugs may be treated with the
gest active infection and have not been previously treated. standard 6-month drug program. Clinicians should consider
Box 21.3 reviews effective treatment programs for latent TB. factors that increase a persons risk for a poor clinical outcome
TB occurs among HIV-infected persons at all CD4 counts. (eg, lack of adherence to TB therapy, delayed conversion of
However, clinical manifestations generally differ depending Mycobacterium tuberculosis sputum cultures from positive to
on the degree of immunosuppression. When TB occurs late negative, and delayed clinical response) when deciding the
in the course of HIV infection, it tends to have atypical fea- total duration of TB therapy. Directly observed therapy is
tures, such as extrapulmonary disease, disseminated disease, recommended. Patients who have successfully completed a
and unusual chest radiographic appearance (lower lung zone regimen of treatment for TB do not require secondary pro-
lesions, intrathoracic adenopathy, diffuse infiltrations, and phylaxis or chronic maintenance therapy. Patients with multi-
lower frequency of cavitation). Patients with low CD4 counts ple drug-resistant TB are at high risk for relapse and treatment
and TB have a high mortality rate (70%) and often have a ful- failure. Treatment regimens for these patients are complex
minant course leading to death in 2 to 3 months. When TB and require expertise in management of both TB and HIV
occurs early in the course of HIV infection (CD4 count >350 infection.
cells/mcL), it tends to manifest with the classic presentation
of upper lobe fibronodular infiltrates with cavitation. Antituberculosis drugs, particularly the rifamycins, interact
with many anti-HIV drugs.
TB can occur at all CD4 counts in HIV infection.
A 6-month course of treatment may be used for pulmonary
TB that occurs late in HIV infection tends to have atypical TB that is susceptible to all first-line antituberculosis
features and a more aggressive course. drugs.
A tuberculin skin test result of 5 mm is interpreted as
Paradoxical reactions have been reported with the con-
positive in HIV-infected patients.
current administration of antiretroviral and antituberculo-
All HIV-infected patients with latent TB should be sis therapy. These reactions, termed immune reconstitution
treated. inflammatory syndrome, are attributed to the recovery of the
patients delayed hypersensitivity response and include hectic
The diagnosis of TB requires evaluation with a chest radio- fevers, lymphadenopathy, worsening of chest radiographic
graph, sputum samples for acid-fast bacillus smear and culture, manifestations of TB (eg, miliary infiltrates, pleural effusions),
and aspiration or tissue biopsy if extrapulmonary disease is and worsening of original tuberculous lesions (eg, expanding
suspected. Mycobacterial blood cultures are useful in cases of central nervous system lesions). Changes in antituberculosis
disseminated disease. In patients with relatively intact immune or antiretroviral therapy are rarely needed. If the symptoms
are severe, a short course of steroids to suppress the enhanced
immune response can be attempted while continuing with
antituberculosis and antiretroviral therapy. Patients with both
Box 21.3 PREFERRED REGIMENS FOR THE TREATMENT
active TB and HIV benefit from prompt antiretroviral treat-
OF LATENT TUBERCULOSIS INFECTION
ment of HIV in addition to treatment of TB despite the risk
of immune reconstitution inflammatory syndrome.
Isoniazid 300 mg PO daily + pyridoxine 50 mg PO daily for
9 mo
MYCOB ACTE RIUM AVIUM C OM PLE X
Isoniazid 900 mg twice weekly + pyridoxine 50 mg PO twice
IN F E C T I O N
weekly for 9 mo
Rifampin 600 mg PO daily for 4 mo Organisms of the Mycobacterium avium complex (MAC)
are ubiquitous in the environment and include M avium
Abbreviation: PO, orally.
and Mycobacterium intracellulare. They cause disseminated
For patients with AIDS whose CD4 count is less than Initial therapy should include amphotericin B with flu-
50 cells/mcL, prophylaxis with azithromycin 1,200 mg cytosine for 2 weeks; this is followed by fluconazole 400 mg
weekly or clarithromycin 500 mg twice daily is recommended. daily for a total of 10 weeks. This initial therapy is followed
Rifabutin 300 mg daily is an alternative if these drugs are not by fluconazole (200 mg daily) for chronic maintenance ther-
tolerated. The detection of MAC organisms in the respiratory apy. Chronic maintenance therapy can be discontinued if the
or gastrointestinal tract when a blood culture is negative is not, patient remains asymptomatic and has a sustained increase
in itself, an indication for prophylaxis or treatment. Primary in CD4 count to more than 200 cells/mcL for 6 months.
prophylaxis may be discontinued in patients with CD4 counts However, chronic suppression or maintenance therapy needs
of more than 100 cells/mcL and a sustained suppression of to be reinitiated if the CD4 count decreases to less than
HIV plasma RNA for more than 3 to 6 months. 200 cells/mcL. Although fluconazole and itraconazole can
reduce the frequency of cryptococcal disease, routine primary
Prophylaxis for MAC is indicated for patients with AIDS prophylaxis is not recommended for several reasons. These
whose CD4 count is <50 cells/mcL. include cost, the relative infrequency of cryptococcosis, the
21. H I V I N F E C T I O N 315
possibility of drug interactions, and the potential for develop- 900 mg orally twice daily for 14 to 21 days followed by valgan-
ment of drug resistance. ciclovir once daily until immune recovery. For gastrointestinal
disease, maintenance therapy can be deferred until relapse is
Initial therapy for C neoformans infection in HIV includes actually demonstrated. Immune recovery uveitis, character-
amphotericin B with flucytosine followed by fluconazole. ized by inflammation in the anterior chamber or vitreous, can
occur in patients who experience a substantial increase in the
Routine primary prophylaxis for C neoformans disease is CD4 count 4 to 12 weeks after antiretroviral therapy is started.
not recommended. Chronic maintenance therapy can be discontinued if patients
remain asymptomatic and have a sustained increase in the
Immune reconstitution disease related to Cryptococcus may CD4 count to more than 100 cells/mcL for 3 to 6 months. All
occur in patients with excellent virologic and immunologic patients whose maintenance therapy is discontinued should
response to HIV treatment. Generally, this occurs within 1 undergo regular ophthalmologic monitoring for detection of
to 6 weeks of initiating antiretroviral treatment. Presentation relapse and immune recovery uveitis. Chronic maintenance
is often with headache and more severe meningismus and therapy will need to be reinitiated if there is ophthalmologic
inflammation in the cerebrospinal fluid than were seen at the evidence of relapse or the CD4 counts decrease to less than
time of the original diagnosis of meningitis. Cultures are usu- 100 cells/mcL.
ally sterile. Increased opening pressure should be managed All patients with AIDS should undergo annual fundu-
with drainage. scopic examination to screen for CMV retinitis and other
HIV-related eye disease and should have prompt evaluation of
C Y TO M E G A L O V I RUS
visual complaints. Routine prophylaxis against CMV is not rec-
ommended because of concerns regarding treatment-induced
Cytomegalovirus (CMV) disease usually affects persons toxicities (such as neutropenia and anemia), conflicting reports
with advanced HIV disease (CD4 count <50 cells/mcL). of efficacy, lack of proven survival benefit, and cost.
Other risk factors include previous opportunistic infections
and high plasma HIV-1 RNA level (>100,000 copies/mL). CMV disease usually affects persons with advanced HIV.
Chorioretinitis is the most common clinical manifestation of
CMV in patients with HIV infection. The usual symptoms CMV can cause chorioretinitis, gastrointestinal disease,
are floaters, visual field deficits, and painless loss of vision. hepatitis, and other organ involvement.
Funduscopic examination reveals yellowish or white retinal CMV retinitis is painless and can lead to blindness.
infiltrates with or without intraretinal hemorrhage. In CMV
gastrointestinal disease, the esophagus and colon are most
commonly involved, and the disease manifests with dysphagia, SYPHILIS
abdominal pain, and bloody diarrhea. Hepatitis, pneumonitis,
sclerosing cholangitis, encephalitis, adrenalitis, polyradiculop- Sexually transmitted diseases, including syphilis, that cause
athy, and myelopathy can also be caused by CMV. genital ulceration may be cofactors for acquiring HIV
Agents used for the treatment of CMV disease and their infection. In general, the clinical manifestations of syphi-
general characteristics are listed in Table 21.5. The preferred lis are similar to those among nonHIV-infected persons.
therapy for sight-threatening lesions is immediate place- However, atypical presentations may occur. For example,
ment of a ganciclovir intraocular implant plus valganciclovir in primary syphilis, multiple or atypical chancres can
Systemic
Ganciclovir IV 5 mg/kg twice daily Bone marrow suppression
Valganciclovir 900 mg PO twice daily Bone marrow suppression
Foscarnet IV 60 mg/kg 3 times daily or 90 mg/kg twice daily Renal toxicity
Cidofovir IV a 5 mg/kg weekly for 2 wk, followed by 5 mg/kg every 2 wk Renal toxicity
Local anti-CMV therapy
for retinitis
Ganciclovir intraocular-release device (Vitrasert)b Every 6 mo Retinal detachment
Ganciclovir intravitreal injectionb 2,000 mcg in 0.050.1 mL Bone marrow suppression
Foscarnet intravitreal injectionb 1.22.4 mg in 0.1 mL Renal toxicity
TOXO P L A S MO S I S
14 days, the diagnosis of Toxoplasma encephalitis should be
Toxoplasma gondii, a protozoan, is the most common cause questioned and a diagnostic brain biopsy considered.
of focal central nervous system lesions in patients with AIDS. Drugs used for the treatment of HIV-associated toxoplas-
The most common symptoms of Toxoplasma encephalitis mosis are listed in Box 21.4. The initial regimen of choice is
include headache and confusion; fever may be absent. Focal the combination of pyrimethamine plus sulfadiazine plus
neurologic deficits occur in 69% of cases. The median CD4 leucovorin. The preferred alternative regimen for patients
count at diagnosis is 50 cells/mcL. Multiple ring-enhancing unable to tolerate or who fail to respond to first-line therapy is
lesions with associated edema are usually noted on brain pyrimethamine plus clindamycin plus leucovorin. Acute ther-
imaging studies. Magnetic resonance imaging is more sensi- apy should be continued for at least 6 weeks if there is clinical
tive than computed tomography for identifying lesions. The and radiologic improvement. Suppressive therapy (secondary
differential diagnosis of central nervous system mass lesions in prophylaxis), with the same agents used for acute therapy but
patients with AIDS includes not only toxoplasmosis but also at a reduced dose, is necessary to prevent relapse. Secondary
lymphoma and other infections, such as TB, cryptococcosis, prophylaxis can be discontinued in patients who successfully
histoplasmosis, bacterial abscess, and progressive multifocal complete initial therapy, remain asymptomatic with respect
leukoencephalitis. to signs and symptoms of toxoplasmosis, and have a sustained
(ie, >6 months) increase in their CD4 counts to more than
The organism T gondii is the most common cause of focal 200 cells/mcL with antiretroviral therapy. Secondary pro-
central nervous system lesions in patients with AIDS. phylaxis should be started again if the CD4 count decreases
to less than 200 cells/mcL. All HIV-infected persons with a
Multiple ring-enhancing lesions usually are noted on brain CD4 count of less than 100 cells/mcL who are seropositive
imaging studies. for Toxoplasma should receive primary prophylaxis against
Toxoplasma encephalitis, as reviewed in Table 21.3.
Empiric antitoxoplasmosis therapy is indicated in patients
with AIDS and positive Toxoplasma serologic testing who Pyrimethamine plus sulfadiazine plus leucovorin is the
present with multiple intracranial lesions. The absence of anti- preferred treatment regimen for toxoplasmosis in patients
toxoplasma immunoglobulin (Ig) G antibody makes a diagno- with AIDS.
sis of toxoplasmosis unlikely. Effective treatment should result
not only in amelioration of symptoms but also in a reduction The agent of choice for primary prophylaxis against
of the number, size, and contrast enhancement of the brain Toxoplasma encephalitis is TMP-SMX.
lesions. If the patient is seronegative for Toxoplasma, has a sin-
gle mass lesion on both computed tomography and magnetic HIV-infected patients should be tested for IgG antibody
resonance imaging, or did not achieve the desired response to Toxoplasma as part of their initial work-up; if the result is
after an empiric course of antitoxoplasmosis therapy for 10 to negative, they should be counseled about the various potential
21. H I V I N F E C T I O N 317
sources of Toxoplasma infection, such as raw or undercooked The diagnosis of esophageal candidiasis is usually made
meat and handling of cat litter. presumptively on clinical grounds (retrosternal burning pain
or odynophagia in a patient with a low CD4 count or oral
candidiasis). A diagnostic trial of antifungal therapy is recom-
P RO G R E S S I VE MU LT I F O C A L
mended before endoscopy is used for identifying the cause of
L EU KO E N C E P H A L O PAT H Y
the disease. Fluconazole 100 to 400 mg daily by mouth is usu-
Progressive multifocal leukoencephalopathy is a demyelinat- ally used for 14 to 21 days to treat esophageal candidiasis.
ing disease caused by the JC virus, a polyomavirus. Symptoms Chronic maintenance therapy for recurrent oropharyngeal
and signs are progressive, variable, and usually chronic or sub- or vulvovaginal candidiasis is not recommended unless recur-
acute. Symptoms include cognitive dysfunction, dementia, rences are frequent or severe. Fluconazole 100 to 200 mg daily
seizures, ataxia, aphasia, cranial nerve deficits, and focal defi- can be used to prevent esophageal candidiasis or other prob-
cits such as hemiparesis and visual field cuts. Fever is usually lematic candidiasis.
absent. Occasionally, symptoms present rapidly and progress
in a few weeks to dementia or coma.
ENTERIC DISEASE
Diagnosis is based on clinical findings and magnetic
resonance imaging, which shows characteristic white mat- A wide variety of organisms (protozoa, bacteria, fungal and
ter changes (bright areas on T2-weighted images) without viral organisms, including HIV itself ) can cause diarrhea in
contrast enhancement or mass effect. Routine cerebrospinal patients with HIV. The CD4 count as a surrogate for the level
fluid studies are generally nondiagnostic, but identification of immunosuppression is an important guide when consid-
of JC virus DNA in the cerebrospinal fluid by polymerase ering the differential diagnosis. For example, diarrhea due to
chain reaction may confirm the diagnosis. Absence of MAC or CMV does not usually occur with CD4 counts of
JC virus DNA does not rule out progressive multifocal more than 100/mcL. Initial evaluation of patients with HIV
leukoencephalopathy. infection who have considerable diarrhea, with or without
There is no established specific therapy for progressive abdominal pain or weight loss, after exclusion of dietary and
multifocal leukoencephalopathy. The prognosis has consid- medication causes, should include stool cultures for bacteria,
erably improved with antiretroviral treatment, and approxi- 3 separate stool specimens for ova and parasites and acid-fast
mately half of patients with a good response to antiretroviral bacilli, testing for Clostridium difficile, and specific examina-
treatment have long-term remission. Thus, all patients with tion for cryptosporidiosis, isosporiasis, microsporidiosis, and
progressive multifocal leukoencephalopathy should be receiv- cyclosporiasis. If no cause is found, sigmoidoscopy with biop-
ing effective antiretroviral therapy. sies should be done to look for CMV in patients with low
CD4 counts. If this result is also negative, upper endoscopy or
Progressive multifocal leukoencephalopathy is caused by colonoscopy with biopsy of the terminal ileum can sometimes
the JC virus. recover treatable pathogens in the small bowel.
The diagnosis is based on clinical findings and on white
matter changes on magnetic resonance imaging. S A L M O NE L L A IN F E C T I O N
All patients with HIV and progressive multifocal In contrast to immunocompetent persons, HIV-infected per-
leukoencephalopathy should be receiving effective sons are more likely to have Salmonella infection that is severe,
antiretroviral therapy. invasive, and widespread. Bacteremia is common and consti-
tutes an AIDS-defining diagnosis. The source for Salmonella
infection is usually ingestion of contaminated food, particu-
larly undercooked poultry and eggs. Salmonellosis can pres-
MU C O CU TA N EO US C A N D I D I A S I S
ent in 3 ways in HIV infection: a self-limited gastroenteritis;
Mucocutaneous disease, such as oral thrush, recurrent vagini- a more severe and prolonged diarrheal disease associated with
tis, and candidal esophagitis, is common. Candidal esophagitis fever, bloody diarrhea, and weight loss; and septicemia, with
is an AIDS-defining condition. Systemic candidal infection, or without gastrointestinal symptoms. In the United States,
including candidemia, is rare unless additional risk factors for the majority of cases of Salmonella septicemia are caused by
disseminated fungal infection such as severe neutropenia or nontyphoidal strains, in particular Salmonella enteritidis and
indwelling catheters are present. Salmonella typhimurium. Bacteremia can occur with each of
Mucocutaneous disease can often be successfully treated these syndromes and has a propensity for relapse.
with clotrimazole troches or nystatin suspension or pastilles. Ciprofloxacin is the preferred agent for treatment. The
Fluconazole is used for the treatment of candidal esophagitis treatment duration for mild gastroenteritis without bacte-
and topical treatment failures. Amphotericin B or caspofungin remia is 10 to 14 days. However, for patients with advanced
can be used for azole failures. HIV-1 disease (CD4 count <200 cells/mcL) or for those who
Diagnosis of oropharyngeal candidiasis is usually clinical have Salmonella bacteremia, treatment for 4 to 6 weeks is rec-
and is based on the appearance of lesions. Visualization of the ommended. Alternatives to the fluoroquinolone antibiotics
organisms by microscopic examination of scrapings provides include TMP-SMX or third-generation cephalosporins (eg,
supportive diagnostic information. ceftriaxone or cefotaxime).
Bacillary angiomatosis caused by Bartonella quintana and Kaposi sarcoma is related to HHV-8 infection.
Bartonella henselae is characterized by vascular prolifera- Antiretroviral treatment and immune recovery are
tive lesions that can involve any organ in the body. The most important aspects of treatment of Kaposi sarcoma.
commonly involved site is the skin, where it may present as
nodules or plaques that are sometimes difficult to differenti-
ate from those of Kaposi sarcoma. Other sites include bone,
N O N-H O D G K I N LY M P H O M A
lymph nodes, brain, respiratory tract, and gastrointestinal
tract. Characteristic fluid-filled spaces occasionally are noted Non-Hodgkin lymphoma is much more common (as high
in the liver and spleen and are called peliosis hepatis or pelio- as 200-fold increased risk) among HIV-infected patients
sis splenis. Patients with bacillary angiomatosis usually have than in the general population. It is a heterogeneous group
21. H I V I N F E C T I O N 319
of malignancies with varying biologic behavior and occurs in Lesions of PCNSL found on imaging studies may be
patients with widely ranging levels of immune function. The difficult to distinguish from those of toxoplasmosis.
vast majority of non-Hodgkin lymphomas in patients with
HIV are of B-cell origin. Intermediate- or high-grade B-cell
non-Hodgkin lymphoma is a CDC-defined AIDS diagnosis. A N T I R ET R O VI R A L AG E N T S
As patients with AIDS live longer, this complication is likely
to become more frequent. It commonly presents with constitu- T H E R E P L I C AT I O N C YC L E O F H I V
tional symptoms (fever, night sweats, and weight loss), lymph-
adenopathy, and involvement of extranodal sites such as the A working knowledge of the HIV replication cycle is essen-
central nervous system, bone marrow, gastrointestinal tract, tial for understanding the mechanism of action of antiretro-
and liver. Involvement of the brain can manifest as an isolated viral agents. Figure 21.2 reviews the interaction between the
disease (primary central nervous system lymphoma) or as virus and the host cell that leads to production of infectious
leptomeningeal involvement in the context of spread of lym- virions.
phoma elsewhere. The optimal treatment of HIV-associated Currently, 25 individual antiretroviral drugs and 6 cofor-
non-Hodgkin lymphoma has not been well defined. Current mulated products categorized in 6 classes have been approved
recommendations suggest that most patients should receive by the FDA for the treatment of HIV. The 6 classes of antiret-
standard-dose chemotherapy, PCP prophylaxis (regardless of roviral drugs are nucleoside and nucleotide analogue reverse
CD4 count), and growth factor support. Additionally, highly transcriptase inhibitors (NRTI), nonnucleoside analogue
active antiretroviral therapy should be a component of the reverse transcriptase inhibitors (NNRTI), protease inhibi-
strategy. tors, fusion inhibitors, integrase inhibitors, and chemokine
coreceptor antagonists.
The vast majority of non-Hodgkin lymphomas in patients
with HIV are of B-cell origin. NU C L EO S I D E A N D NU C L EOT I D E A NA L O GU E
Non-Hodgkin lymphoma in HIV commonly presents R EVE R S E T R A NS C R I P TA S E I N H I B ITO R S
with constitutional symptoms (eg, fever, night sweats, The NRTIs were the first agents to be developed as antiretro-
and weight loss), lymphadenopathy, and involvement of virals. These agents are structurally similar to nucleic acids (the
extranodal sites. building blocks of RNA and DNA). They block HIV reverse
P R I M A RY C E N T R A L N E RVO US S YS T E M
A
LY M P H O M A
The incidence of primary central nervous system lymphoma
(PCNSL) in HIV-infected individuals is 1,000-fold higher
than that in the general population. It occurs most often
B
in the advanced stages of AIDS at a median CD4 count of
less than 50 cells/mcL and is almost always associated with
Epstein-Barr virus. The result of polymerase chain reaction F
C
testing of cerebrospinal fluid for Epstein-Barr virus is usually
positive in patients with HIV and PCNSL but rarely positive
in patients with toxoplasmosis or other causes of central ner- E
vous system brain lesions. The clinical presentation includes D
headache, confusion, lethargy, personality changes, memory
loss, focal neurologic deficits, and seizure. Brain imaging stud-
ies show single or multiple contrast-enhancing lesions, which
may be difficult to distinguish from those of toxoplasmosis.
Biopsy is required for definitive diagnosis. Whole-brain radia- Figure 21.2 Life Cycle of Human Immunodeficiency Virus. A, The virus
is an enveloped virus that contains viral genomic RNA and various
tion has been the primary treatment of PCNSL. Despite good Gag and Pol protein products. B, The interaction between the envelope
initial radiographic response rates, the survival rate is poor proteins of the virus and CD4 receptor and other receptors of the host
with median survival times of 2 to 5 months. Since the advent cell leads to the binding of the viral envelope and the host cytoplasmic
of potent combination antiretroviral therapy, the incidence membrane. C, The viral reverse transcriptase enzyme catalyzes the
of PCNSL has declined, and antiretroviral therapy in combi- conversion of viral RNA into DNA. D, The viral DNA enters the
nucleus and becomes inserted into the chromosomal DNA of the host
nation with radiation has been associated with an improved cell. E, Expression of the viral genes leads to production of viral RNA
prognosis compared with brain radiation alone. and proteins. F, These viral proteins, as well as viral RNA, are assembled
at the cell surface into new viral particles and leave the host cell by a
PCNSL is associated with Epstein-Barr virus infection. process called budding. During the process of budding, they acquire the
outer layer and envelope. At this stage, the protease enzyme cleaves the
PCNSL usually occurs in patients with advanced AIDS. precursor Gag and Gag-Pol proteins into their mature products.
Abacavir (ABC) 300 mg twice daily or 600 mg once daily Hepatic by alcohol dehy- Diarrhea, anorexia, nausea, vomit-
No food effect drogenase & glucuronyl ing, headache, fatigue, hypersensi-
No adjustment needed for renal insufficiency transferase tivity reaction
Dose adjustment for hepatic impairment required
Didanosine (ddI) Body weight 60 kg: 400 mg once daily Unknown Rash, abdominal pain, diarrhea, nau-
Body weight <60 kg: 250 mg once daily sea, vomiting, asthenia, headache,
Take 1/2 h before or 2 h after a meal fever, pancreatitis, peripheral
Dose adjustment for renal insufficiency required neuropathy
Emtricitabine (FTC) 200-mg capsule once daily or 240 mg (24 mL) oral Limited, oxidation & Hyperpigmentation of skin, rash,
solution once daily conjugation diarrhea, nausea, vomiting,
Take without regard to meals headache
Dose adjustment for renal insufficiency required
Lamivudine (3TC) 150 mg twice daily or 300 mg once daily 5.6% to transsulfoxide Decrease in appetite, nausea, vomit-
Take without regard to meals metabolite ing, headache, fatigue, pancreatitis
Dose adjustment for renal insufficiency required in children
Stavudine (d4T) Body weight 60 kg: 40 mg twice daily Intracellular phosphoryla- Rash, diarrhea, nausea, vomiting,
Body weight <60 kg: 30 mg twice daily tion to active metabolite headache, lipoatrophy, hyper-
Take without regard to meals lipidemia, peripheral neuropathy,
Dose adjustment for renal insufficiency required muscle weakness
Tenofovir (TDF) 300 mg once daily Intracellular hydrolysis Diarrhea, flatulence, nausea, vomit-
Take without regard to meals ing, osteopenia, renal impairment
Dose adjustment for renal insufficiency required
Zidovudine (ZDV) 300 mg twice daily or 200 mg 3 times daily Hepatic glucuronidation Headache, nausea, anorexia, vomit-
Take without regard to meals ing, anemia, leukopenia, myopa-
Dose adjustment for renal insufficiency required thy, lipoatrophy, hyperlipidemia
Adapted from Panel on Antiretroviral Guidelines for Adults and Adolescents: Guidelines for the use of antiretroviral agents in HIV-1-infected adults and adoles-
cents. Department of Health and Human Services. December 1, 2009; 1161. [cited 2011 Nov 23]. Available from: http://www.aidsinfo.nih.gov/ContentFiles/
AdultandAdolescentGL.pdf.
21. H I V I N F E C T I O N 321
to normal, antiretroviral drug therapy can be reintroduced with in whites. HLA-B*5701 testing is now recommended before
NRTIs that have low potential for mitochondria toxicity ([cited starting therapy with abacavir; other drugs should be chosen if
2011 Nov 23]. Available from: http://www.aidsinfo.nih.gov/ a patient is positive for HLA-B*5701.
ContentFiles/AdultandAdolescentGL.pdf ).
Patients in whom abacavir therapy is being considered
A rare and potentially fatal syndrome of lactic acidosis in should be tested for HLA-B*5701.
the absence of hypoxemia can occur with NRTIs.
Abacavir should not be reintroduced once its use has been
Symptomatic lactic acidosis is most common with discontinued because of adverse effects.
stavudine, didanosine, and zalcitabine.
Use of stavudine and didanosine together is N O N N U C L E O S I D E A NA L O GU E R EV E R S E
contraindicated. T R A NS C R I P TA S E I N H I B ITO R S
The NNRTIs bind directly and noncompetitively to the
Hypersensitivity reactions have been reported in approxi- enzyme reverse transcriptase. They block DNA polymerase
mately 5% of patients receiving abacavir. Symptoms consist activity by causing conformational change and disrupting
of rash accompanied by systemic signs and symptoms such as the catalytic site of the enzyme. Unlike nucleoside analogues,
fever, fatigue, nausea, vomiting, diarrhea, or abdominal pain. NNRTIs are not incorporated into viral DNA. They have no
These symptoms usually appear within the first 6 weeks of treat- activity against HIV-2.
ment. The rash is usually maculopapular but can be variable in
appearance. Hypersensitivity reactions also may occur without NNRTIs bind directly and noncompetitively to the
a rash. Symptoms usually resolve rapidly when use of the drug enzyme reverse transcriptase.
is discontinued. Once use of abacavir has been discontinued
because of adverse effects, it should not be reintroduced. More NNRTIs are not active against HIV-2.
severe symptoms, including death, have been reported when
use of abacavir is reinstituted. A genetic marker, HLA-B*5701, Five NNRTIs have been approved for the treatment of
has been associated with an increased risk for development of HIV: delavirdine, efavirenz, etravirine, nevirapine, and
a hypersensitivity reaction to abacavir and is more common rilpivirine (Table 21.7). When first-generation NNRTIs
Delavirdine (DLV) 400 mg 3 times daily CYP substrate, CYP3A4 inhibitor Rash, hepatotoxicity, headache
Take without regard to meals
No adjustment for renal insufficiency
Efavirenz (EFV) 600 mg once daily at or before bedtime CYP3A4 & 2B6 substrate, mixed Rash, central nervous system symp-
Take on an empty stomach to reduce CYP3A4 inducer or inhibitor toms (dizziness, light-headedness,
adverse effects abnormal dreams, difficulty with
No adjustment for renal insufficiency concentration), hepatotoxicity
Etravirine (ETR) 200 mg twice daily CYP3A4, 2C9, & 2C19 substrate Rash, hypersensitivity reaction
Take after a meal 3A4 inducer; 2C9 & 2C19 inhibitor
No adjustment for renal insufficiency
Nevirapine (NVP) 200 mg once daily for 14 days (lead-in CYP3A4 substrate, CYP3A4 inducer Rash, hepatotoxicity, including
period); thereafter, 200 mg twice symptomatic hepatitis & fatal
daily hepatic necrosis
Take without regard to meals
No adjustment for renal insufficiency
Rilpivirine (RPV) 25 mg once daily CYP3A substrate, CYP3A4 inhibitors Headache, insomnia, depres-
Take with a meal (protease inhibitors, macrolides, azole sion, transient rash, increased
No adjustment for renal insufficiency antifungals) can increase levels of transaminase levels, increased
RPV, highly protein-bound, requires total and LDL cholesterol levels.
stomach acid for absorption (PPIs May prolong QT intervaluse
contraindicated, avoid H2RAs, take caution or avoid QT-interval
RPV 2 h before or 4 h after antacids) prolonging drugs
Abbreviations: CYP, cytochrome P450; H2RA, histamine2-receptor antagonist; LDL, low-density lipoprotein; PPI, proton pump inhibitor.
Adapted from Panel on Antiretroviral Guidelines for Adults and Adolescents: Guidelines for the use of antiretroviral agents in HIV-1-infected adults and adoles-
cents. Department of Health and Human Services. December 1, 2009; 1161. [cited 2011 Nov 23]. Available from: http://www.aidsinfo.nih.gov/ContentFiles/
AdultandAdolescentGL.pdf.
21. H I V I N F E C T I O N 323
Table 21.8 GENERAL CHARACTERISTICS OF PROTEASE INHIBITORS
DRUG NAME
(ALIAS) DOSING & ADJUSTMENTS METABOLISM TOXIC/ADVERSE EFFECTS
Atazanavir ATZ 300 mg + RTV 100 mg once daily CYP3A4 substrate & Indirect hyperbilirubinemia; prolonged PR
(ATZ) Take with food inhibitor interval, including symptomatic first-degree
No adjustment for renal insufficiency AV block; nephrolithiasis; hyperglycemia; fat
Dose adjustment for hepatic impairment required maldistribution; possible increased bleeding
episodes in patients with hemophilia
Darunavir DRV 800 mg + RTV 100 mg once daily (for CYP3A4 substrate & Rash, hepatotoxicity, diarrhea, nausea, head-
(DRV) treatment-nave) inhibitor ache, hyperlipidemia, transaminase increased,
Antiretroviral-experienced: DRV 600 mg + RTV hyperglycemia, fat maldistribution, possible
100 mg twice daily increased bleeding episodes in patients with
Take with food hemophilia
No dose adjustment for renal insufficiency required
Fosamprenavir FPV 1,400 mg twice daily or FPV 1,400 mg + RTV CYP3A4 substrate, Rash, diarrhea, nausea, vomiting, headache,
(FPV) 100200 mg once daily (not recommended for inhibitor, & hyperlipidemia, transaminase increased,
treatment-experienced) inducer nephrolithiasis, hyperglycemia, fat maldistri-
FPV 700 mg + RTV 100 mg twice daily bution, possible increased bleeding episodes in
Take without regard to meals patients with hemophilia
No dose adjustment for renal insufficiency required
Dose adjustment for hepatic impairment required
Indinavir IDV 800 mg + RTV 100200 mg twice daily CYP3A4 substrate & Nephrolithiasis, GI intolerance, nausea, indirect
(IDV) Take without regard to meals inhibitor hyperbilirubinemia, hyperlipidemia, head-
No dose adjustment for renal insufficiency required ache, asthenia, blurred vision, dizziness, rash,
Dose adjustment for hepatic impairment required metallic taste, thrombocytopenia, alopecia,
hemolytic anemia, hyperglycemia, fat maldis-
tribution, possible increased bleeding episodes
in patients with hemophilia
Lopinavir/ LPV/r 400 mg/100 mg twice daily or LPV/r CYP3A4 substrate & GI intolerance, nausea, vomiting, diarrhea,
ritonavir 800 mg/200 mg once daily (once daily not inhibitor asthenia, hyperlipidemia (especially hypertrig-
(LPV/r) recommended for treatment-experienced or lyceridemia), increased serum transaminases,
pregnant women) hyperglycemia, fat maldistribution, possible
Take without regard to meals increased bleeding episodes in patients with
No dose adjustment for renal insufficiency required hemophilia
Nelfinavir 1,250 mg twice daily or 750 mg 3 times daily CYP 2C19 & 3A4 Diarrhea, hyperlipidemia, hyperglycemia, fat
(NFV) Take with food substrate & maldistribution, possible increased bleeding
No dose adjustment for renal insufficiency required inhibitor episodes in patients with hemophilia, increased
Has an active serum transaminase
metabolite
Ritonavir Current use only as a pharmacokinetic enhancer CYP3A4 & 2D6 sub- GI intolerance, nausea, vomiting, diarrhea,
(RTV) for other PIs: 100400 mg per day in 1 dose or 2 strate & inhibitor paresthesias (circumoral & extremities), hyper-
divided doses lipidemia (especially hypertriglyceridemia),
Take with food hepatitis, asthenia, taste perversion, hypergly-
No dose adjustment for renal insufficiency required cemia, fat maldistribution, possible increased
bleeding episodes in patients with hemophilia
Saquinavir SQV 1,000 mg + RTV 100 mg twice daily CYP3A4 substrate & GI intolerance, nausea, diarrhea, headache,
(SQV) Take within 2 h after a meal inhibitor increased transaminase enzymes, hyperlipi-
No dose adjustment for renal insufficiency required demia, hyperglycemia, fat maldistribution,
possible increased bleeding episodes in
patients with hemophilia
Tipranavir TPV 500 mg + RTV 200 mg twice daily CYP3A4 substrate & Hepatotoxicity (including clinical hepatitis),
(TPV) Take without regard to meals inducer (but when rash, intracranial hemorrhages, hyperlipidemia
No dose adjustment for renal insufficiency required combined with (especially hypertriglyceridemia), hypergly-
RTV, the net effect cemia, fat maldistribution, possible increased
is inhibition) bleeding episodes in patients with hemophilia
Abbreviations: AV, atrioventricular; CYP, cytochrome P450; GI, gastrointestinal; PI, protease inhibitor.
Adapted from Panel on Antiretroviral Guidelines for Adults and Adolescents: Guidelines for the use of antiretroviral agents in HIV-1-infected adults and adoles-
cents. Department of Health and Human Services. December 1, 2009; 1161. [cited 2011 Nov 23]. Available from: http://www.aidsinfo.nih.gov/ContentFiles/
AdultandAdolescentGL.pdf.
Enfuvirtide (T-20) 90 mg (1 mL) subcutaneously twice daily Catabolism to its constituent Local injection site reactions, increased bacte-
No adjustment for renal insufficiency amino acids rial pneumonia, hypersensitivity reaction
Adapted from Panel on Antiretroviral Guidelines for Adults and Adolescents: Guidelines for the use of antiretroviral agents in HIV-1-infected adults and adoles-
cents. Department of Health and Human Services. December 1, 2009; 1161. [cited 2011 Nov 23]. Available from: http://www.aidsinfo.nih.gov/ContentFiles/
AdultandAdolescentGL.pdf.
therefore a tropism assay to ensure that R5 virus is present is associated nephropathy, and 3) hepatitis B virus coinfection in
recommended before starting treatment with maraviroc. which treatment for hepatitis B virus is indicated.
Perinatal transmission of HIV has dramatically decreased
Maraviroc is a pure CCR5 antagonist. in the United States since the 1990s. This decrease is a result of
recommendations from the US Public Health Service for uni-
A tropism assay should be done before initiating treatment versal prenatal HIV counseling and HIV testing of all pregnant
with maraviroc. women, in addition to antiretroviral therapy for reduction of
perinatal HIV transmission. Zidovudine administered to the
mother during the antepartum and intrapartum periods and
GU I D E L I N E S F O R US E O F A N T I R ET ROVI R A L
to the newborn for the first 6 weeks of life reduces the perina-
T H E R A P Y F O R H I V I N FEC T I O N
tal transmission of HIV by two-thirds. Antiretroviral therapy
Guidelines addressing the issue of antiretroviral therapy in should be offered to all HIV-1 infected women during preg-
different populations and situations have been developed nancy. Treatment is recommended to prevent transmission of
and are updated regularly electronically as new information HIV to the child and for the long-term health of the mother.
becomes available (http://www.aidsinfo.nih.gov/). There is The regimen should be a potent 3-drug program; efavirenz
broad agreement that antiretroviral therapy should be ini- should be avoided because of the risk of fetal malformation.
tiated in adults with symptoms ascribed to HIV infection Ideally, zidovudine is incorporated into the antiretroviral
regardless of the CD4 cell count. The optimal time to start regimen. Zidovudine should also be given to the newborn for
antiretroviral therapy in asymptomatic patients is less clear. the first 6 weeks of life. The currently preferred antiretroviral
Current guidelines recommend initiating antiretroviral treatment regimen for pregnant women is lopinavir/ritonavir
therapy in asymptomatic patients with less than 350 CD4 (coformulated as Kaletra) twice daily with zidovudine and
cells/mcL. Treatment has been proved to decrease morbid- lamivudine (coformulated as Combivir). Cesarean section
ity and mortality related to HIV and to improve quality of has also been shown to substantially decrease the risk of trans-
life. Treatment is also recommended for patients with a CD4 mission of HIV to the infant at the time of delivery. Elective
cell count between 350 and 500 cells/mcL, but the strength cesarean section is recommended for women with viral loads
of this recommendation is less than that for patients with of more than 1,000 copies/mL. Women in developed coun-
lower CD4 cell counts. Initiating antiretroviral therapy for tries with access to clean water and formula should avoid
asymptomatic HIV-infected persons who have CD4 cell breast-feeding, which can transmit HIV to the infant.
counts of more than 500 cells/mcL remains controversial. Patients coinfected with hepatitis B who need treatment
Benefits of early treatment include prevention of poten- for hepatitis B should also be treated for HIV with a program
tially irreversible damage to the immune system, decreased that includes drugs active against both HIV and hepatitis B.
risk of HIV-associated complications, and decreased risk Thus, the combination of tenofovir and emtricitabine or teno-
of transmission of HIV to others. Table 21.12 reviews the fovir and lamivudine should be used as the nucleoside back-
current recommendations for antiretroviral treatment in bone of the regimen.
treatment-nave patients.
Antiretroviral therapy is recommended for 3 condi- All patients with symptomatic HIV infection should be
tions, regardless of CD4 cell counts: 1) pregnancy, 2) HIV- offered antiretroviral treatment.
Raltegravir (RAL) 400 mg twice daily Uridine diphosphoglucuronosyl-transferase Nausea, headache, diarrhea, fever,
Take without regard to food 1A1-mediated glucuronidation increased creatine kinase
No adjustment for renal insufficiency
Adapted from Panel on Antiretroviral Guidelines for Adults and Adolescents: Guidelines for the use of antiretroviral agents in HIV-1-infected adults and adoles-
cents. Department of Health and Human Services. December 1, 2009; 1161. [cited 2011 Nov 23]. Available from: http://www.aidsinfo.nih.gov/ContentFiles/
AdultandAdolescentGL.pdf.
21. H I V I N F E C T I O N 325
Table 21.11 GENERAL CHARACTERISTICS OF CHEMOKINE CORECEPTOR (CCR5) ANTAGONISTS
Maraviroc (MVC) 300 mg twice daily with drugs that are not strong CYP3A CYP3A4 substrate Abdominal pain, cough,
inhibitors dizziness, musculoskeletal
150 mg twice daily with drugs that are strong CYP3A inhibitors symptoms, pyrexia, rash,
600 mg twice daily with drugs that are CYP3A inducers upper respiratory tract
Take without regard to food infections, hepatotoxicity,
No adjustment for renal insufficiency orthostatic hypotension
Antiretroviral treatment should be considered for all care workers after occupational exposure to HIV. Systems of
asymptomatic HIV-infected individuals with CD4 cell care, including written protocols, should be in place to prompt
count of less than 500 cells/mcL. reporting and to facilitate management of exposed health care
workers.
All pregnant women should receive antiretroviral
treatment.
In health care workers, the use of zidovudine is associated
with a 79% decrease in the risk for HIV transmission.
NRTI combination Coformulated tenofovir + Coformulated zidovudine + lamivudine (Epzicom) or coformulated zidovudine +
emtricitabine (Truvada) lamivudine (Combivir)
Emcitrabine & lamivudine can be interchanged when not used in a coformulation
PI Atazanavir + ritonavir once daily or Fosamprenavir + ritonavir or coformulated lopinavir + ritonavir (Kaletra) or
Darunavir + ritonavir once daily saquinavir + ritonavir twice daily
Abbreviations: NNRTI, nonnucleoside reverse transcriptase inhibitor; NRTI, nucleoside reverse transcriptase inhibitor; PI, protease inhibitor.
a
Raltegravir is the preferred and only currently available integrase inhibitor.
b
Unless pregnancy likely.
Adapted from Panel on Antiretroviral Guidelines for Adults and Adolescents: Guidelines for the use of antiretroviral agents in HIV-1-infected adults and adoles-
cents. Department of Health and Human Services. December 1, 2009; 1161. [cited 2011 Nov 23]. Available from: http://www.aidsinfo.nih.gov/ContentFiles/
AdultandAdolescentGL.pdf.
21. H I V I N F E C T I O N 327
22.
HEALTH CAREASSOCIATED INFECTIONS, INFECTIONS
OF THE CENTRAL NERVOUS SYSTEM, INFECTIVE
ENDOCARDITIS, SKIN AND SOFT TISSUE INFECTIONS,
AND B ONE AND JOINT INFECTIONS
Pritish K. Tosh, MD, M. Rizwan Sohail, MD, and Elie F. Berbari, MD
328
should be used for empiric therapy. Antimicrobial therapy can from the peripheral site) or a catheter tip with growth >15
be narrowed once the cause and antimicrobial susceptibili- colony-forming units per milliliter suggests the catheter as
ties are known. If started early, antimicrobial therapy can be the source of bloodstream infection.
stopped after 7 days, with the exception of infections caused
by Pseudomonas, for which 14 or more days are often needed. Removal of the infected catheter is always the preferred
The following are recommended strategies for the preven- method of treating CR-BSI. Antibiotic lock therapy, in com-
tion of HAP, VAP, and HCAP: bination with systemic antimicrobial agents, is a key ingredient
of catheter salvage attempts. A clinically unstable patient, pres-
General ence of local or systemic complications, and infection with vir-
Staff education and hand hygiene ulent organisms (such as S aureus, Candida, or gram-negative
Surveillance of infections in the intensive care unit, bacteria) warrant removal of an infected catheter.
including susceptibility
Aspiration precautions
Semirecumbent position (30-45) rather than supine C O M M O N N O S O C O M I A L PAT H O G E N S
Preference of enteral feeding over parenteral nutrition
S aureus
Intubation and mechanical ventilation
Avoid reintubation Staphylococcus aureus is a common cause of nosocomial infec-
Noninvasive ventilation should be used when possible tions, including surgical site infections, CR-BSI, and VAP. In
in select patients cases in which nosocomial S aureus bacteremia is caused by a
Orotracheal and orogastric tubes are preferred over removable focus of infection (such as an intravenous catheter),
nasotracheal and nasogastric tubes a 2-week course of therapy may be sufficient if the infected
Continuous aspiration of subglottic secretions should catheter is quickly removed; such an approach leads to rapid
be used resolution of fever and bacteremia. However, most cases of
Endotracheal tube cuff pressure should be maintained community-acquired S aureus bacteremia should be treated for
>20 cm H2O 4 to 6 weeks with parenteral antibiotics because of the poten-
Contaminated condensate should be carefully removed tial for metastatic abscesses and infective endocarditis. Some
from ventilator circuits experts recommend using transesophageal echocardiography
Protocols to reduce sedation and accelerate weaning in all cases of S aureus bacteremia to screen for endocarditis.
should be enacted Urine cultures positive for S aureus should raise concern for S
aureus bacteremia with secondary seeding of the urinary tract.
C AT H ET E R-R E L AT E D B L O O D S T R E A M
Cases of community-acquired S aureus bacteremia should
I N FEC T I O N
be treated for 46 weeks with parenteral antibiotics.
Approximately 5 million central venous catheters are placed in
the United States annually. About 1 in 20 of these catheters Most S aureus strains produce -lactamase (a penicilli-
get infected. Indeed, catheter-related bloodstream infection nase) and thus are resistant to penicillin G or amoxicillin but
(CR-BSI) is the most common cause of health careassociated are susceptible to -lactam-lactamase inhibitor combina-
bacteremia in the United States. CR-BSI is associated with sub- tion drugs such as amoxicillin-clavulanic acid. The semisyn-
stantial cost (about $28,000 per survivor), increased length of thetic penicillins (nafcillin, oxacillin) and first-generation
stay (average 6.5 days), and substantial mortality (10%-25%). cephalosporins remain active and are drugs of choice against
Catheter infection may present with local manifestations methicillin-sensitive S aureus (MSSA) strains. Strains of S
(port, tunnel, or exit site infection) or CR-BSI. Local infec- aureus with resistance to the -lactam antibiotics have spread
tions are easy to recognize and always necessitate removal of worldwide. This resistance is caused by an alteration of the
the infected catheter. However, CR-BSI may present without penicillin-binding proteins in the cell wall. These strains,
any inflammatory signs or drainage from the exit site or tunnel. referred to as MRSA, are resistant to all -lactam antibiotics,
In these situations, blood should be simultaneously drawn from and often to other classes of antibiotics, but remain susceptible
the catheter and a peripheral site. If cultures of blood drawn to drugs such as vancomycin, linezolid, or daptomycin. Strains
from the catheter have positive results 2 hours before the cul- of MRSA with decreased susceptibility to vancomycin have
tures from the peripheral site (differential time to positivity), also emerged. Vancomycin intermediately resistant S aureus
this finding has high correlation (>80%) with catheter infec- (VISA) has a minimum inhibitory concentration (MIC) of 4
tion. If the catheter is urgently removed (eg, because of absence to 8 mcg/mL, whereas vancomycin-resistant S aureus (VRSA)
of an alternative source of infection), the catheter tip should be has an MIC of 16 or more mcg/mL.
submitted for culture. Growth of more than 15 colony-forming If S aureus is penicillin susceptible (<5% of clinical isolates),
units (per milliliter) of bacteria is highly suggestive of the cath- penicillin G is the most active agent. For penicillin-allergic
eter being the source of bloodstream infection. patients, effective alternatives include cefazolin and vanco-
mycin. If the isolate is methicillin-susceptible, then nafcillin,
Differential time to culture positivity (cultures of blood oxacillin, or cephalosporins (first-generation) have better effi-
drawn from the catheter are positive 2 hours before those cacy than vancomycin. Vancomycin is the most reliable and
22 . H E A LT H C A R E A S S O C I AT E D I N F E C T I O N S 329
well-studied drug for treating serious infections caused by Unless in vitro susceptibility testing shows alternative
MRSA. Linezolid, dalfopristin/quinupristin, daptomycin, active agents, serious infections due to coagulase-negative
and tigecycline are newer drugs that are also active against staphylococci should be treated with vancomycin.
MRSA. Some strains of MRSA may retain susceptibility to
Removal of infected hardware usually is necessary to cure
trimethoprim-sulfamethoxazole, minocycline, or the mac-
infections due to coagulase-negative staphylococci.
rolides. However, these antibiotics are mostly used for treat-
ment of nonlife-threatening infections such as skin and soft
tissue infections or chronic suppression of hardware-associated Pseudomonas aeruginosa
S aureus infections after completion of a parenteral antibiotic Pseudomonas aeruginosa is typically associated with nosoco-
course for acute infection. mial infection and is frequently resistant to common anti-
Staphylococcus aureus organisms frequently colonize the biotics. Pseudomonas aeruginosa and S aureus are the most
nares, which may predispose to invasive infections. Subclinical frequent causes of infections complicating severe burn inju-
nasal colonization can result in nosocomial transmission of ries. Other infections caused by P aeruginosa include follic-
MRSA. Topical mupirocin ointment or other therapies (such as ulitis associated with hot tub use, osteomyelitis (particularly
trimethoprim-sulfamethoxazole with or without rifampin) may in injection drug users), malignant otitis externa in patients
temporarily eradicate the nasal colonization and have been suc- with diabetes mellitus, complicated urinary tract infections,
cessful for reducing the rate of postoperative wound infection. ventilator-associated pneumonias, and pulmonary infections
However, recolonization after a short interval is frequent. in patients with cystic fibrosis. Patients with neutropenia are
also at high risk for Pseudomonas infection, especially bacter-
Vancomycin is the most reliably active drug for treating emia. Hence, the febrile neutropenic patient should be treated
serious infections caused by MRSA. empirically with antipseudomonal antibiotics while culture
results are pending. Ecthyma gangrenosum, a necrotizing skin
lesion, may develop in neutropenic patients with bacteremia
Coagulase-Negative Staphylococci due to P aeruginosa.
Staphylococcus epidermidis is the most common of the Pseudomonas aeruginosa and S aureus are the most frequent
coagulase-negative staphylococci, although many other staph- causes of infections complicating massive burns.
ylococcal species are included in this group. For clinical pur-
poses, they are mostly interchangeable, except Staphylococcus Patients with neutropenic fever should receive empiric
lugdunensis, which is more aggressive and clinically behaves antipseudomonal coverage while culture results are
like S aureus. Coagulase-negative staphylococci are normal pending.
skin flora. They are opportunistic pathogens that commonly
cause infections associated with medical devices. They rarely Agents active against most P aeruginosa organisms include
cause disease in otherwise healthy persons. the extended-spectrum penicillins (piperacillin, ticarcil-
Coagulase-negative staphylococci are frequently associ- lin), aminoglycosides, ceftazidime and cefepime (the only
ated with intravascular devicerelated bacteremias, infections cephalosporins reliably active against this organism), aztre-
associated with cardiac devices (ie, pacemakers, defibrillators), onam, meropenem, imipenem, doripenem, and ciprofloxacin.
prosthetic valve endocarditis, osteomyelitis (usually after joint Ertapenem, unlike the other carbapenems, does not have activ-
arthroplasty or other prosthetic implantations), meningitis ity against P aeruginosa. Administering 2 active drugs, usually
after neurosurgical procedures, and infections of ventriculo- a -lactam and an aminoglycoside, is recommended when
peritoneal shunts and atrioventricular shunts. Treatment usu- treating serious infections caused by P aeruginosa, especially
ally requires removal of the foreign body and administration endocarditis. Antibiotic resistance frequently emerges during
of appropriate antibiotics. Coagulase-negative staphylococci and after treatment.
have also been associated with peritonitis in patients undergo-
ing chronic ambulatory peritoneal dialysis. Use 2 active agents against P aeruginosa for all serious
Determining the significance of blood cultures growing infections until susceptibility data are available.
coagulase-negative staphylococci can be difficult. True infec-
tions generally result in systemic symptoms with multiple pos- Stenotrophomonas (Xanthomonas) maltophilia
itive blood cultures, whereas a single positive blood culture is
generally a contaminant. Stenotrophomonas maltophilia infection usually occurs in
Treatment duration for bacteremia due to coagulase- nosocomial settings. Its most notable trait is its resistance to
negative staphylococci is variable. Although a catheter-related imipenem and meropenem and also the aminoglycosides, quin-
bacteremia can be adequately treated with antibiotics admin- olones, except occasionally levofloxacin, and most -lactam
istered for 1 to 2 weeks, prosthetic valve endocarditis due to drugs. Stenotrophomonas maltophilia is usually susceptible to
coagulase-negative staphylococci warrants a 6-week regimen trimethoprim-sulfamethoxazole and ticarcillin-clavulanate.
of vancomycin plus rifampin, with gentamicin added for the
first 2 weeks. Moreover, valve replacement surgery may be nec- Stenotrophomonas maltophilia is resistant to imipenem and
essary in recalcitrant cases. meropenem.
22 . H E A LT H C A R E A S S O C I AT E D I N F E C T I O N S 331
A
Suspicion for bacterial meningitis Indications for imaging before B
Typical signs may be absent, prior antibiotics may mask severity of illness lumbar puncture:
Signs of brain shift
Papilledema
Focal neurologic signs, not including
Start investigations cranial nerve palsy
Assess severity Blood cultures Glasgow Coma Scale score <10
Ventilation Blood gases Severe immunocompromised state
Circulation Serum laboratory investigations New-onset seizures
Neurologic examination Chest x-ray
Rash: skin biopsy
Yes Yes No
Figure 22.1 Algorithm for Management of Suspected Community-Acquired Bacterial Meningitis. A, Algorithm for initial management of adults with
bacterial meningitis. B, Indications for performing imaging before lumbar puncture. C, Recommendations for adjunctive dexamethasone therapy in
adults with bacterial meningitis. D, Criteria for admission of patients with bacterial meningitis to the intensive care unit. CSF indicates cerebrospinal
fluid; CT, computed tomography; DXM, dexamethasone; MRI, magnetic resonance imaging. (Adapted from van de Beek D, de Gans J, Tunkel
AR, Wijdicks EFM. Community-acquired bacterial meningitis in adults. N Engl J Med. 2006 Jan 5;[Suppl Appendix]354[1]:4453. Used with
permission.)
EMPIRIC THERAPY
Age, y
1650 Neisseria meningitidis, Streptococcus pneumoniae Vancomycin plus a third-generation cephalosporina,b
>50 S pneumoniae, N meningitidis, Listeria monocytogenes, aerobic gram-negative Vancomycin plus a third-generation cephalosporin plus ampicillinb,c
bacilli
With risk factor presentd S pneumoniae, L monocytogenes, Haemophilus influenzae Vancomycin plus a third-generation cephalosporin plus ampicillinb,c
SPECIFIC ANTIMICROBIAL THERAPY
S pneumoniae
Penicillin MIC
<0.1 mg/L Penicillin G or ampicillin Third-generation cephalosporin,b chloramphenicol
0.11.0 mg/L Third-generation cephalosporinb Cefepime, meropenem
2.0 mg/L Vancomycin plus a third-generation cephalosporinb,e Fluoroquinolonef
Cefotaxime or ceftriaxone MIC
1.0 mg/L Vancomycin plus a third-generation cephalosporinb,g Fluoroquinolonef
N meningitidis
Penicillin MIC
<0.1 mg/L Penicillin G or ampicillin Third-generation cephalosporin,b chloramphenicol
0.11.0 mg/L Third-generation cephalosporinb Chloramphenicol, fluoroquinolone, meropenem
Escherichia coli & other Enterobacteriaceae Third-generation cephalosporinb Aztreonam, fluoroquinolone, meropenem,
trimethoprim-sulfamethoxazole, ampicillin
(continued)
Table 22.1 RECOMMENDATIONS FOR ANTIMICROBIAL THERAPY IN ADULTS WITH COMMUNITY-ACQUIRED BACTERIAL MENINGITIS (CONTINUED)
EMPIRIC THERAPY
H influenzae
-Lactamase negative Ampicillin Third-generation cephalosporin,b cefepime, chloramphenicol,
fluoroquinolone
-Lactamase positive Third-generation cephalosporinb Cefepime, chloramphenicol, fluoroquinolone
Chemoprophylaxisi
N meningitidis Rifampicin (rifampin), ceftriaxone, ciprofloxacin, azithromycin
Streptococcus pneumoniae Any age, but often elderly Most common cause of recurrent Cerebrospinal fluid leak, alcoholism,
meningitis in adults splenectomy, functional asplenia,
multiple myeloma, hypogammaglobuline-
mia, Hodgkin disease, HIV
Neisseria meningitidis Infants to 40 y Petechial rash is common Terminal component complement deficiency
Epidemics occur in closed populations
Haemophilus influenzae, >Neonate to 6 y Significant decrease in incidence since Hypogammaglobulinemia in adults, HIV,
type B licensure of H influenzae B vaccine splenectomy, functional asplenia
Gram-negative bacilli Any age Staphylococcus aureus & coagulase-negative Neurosurgical procedures, bacteremia due
staphylococci also common to urinary tract infection, pneumonia, etc,
after neurosurgical procedure Strongyloides hyperinfection syndrome
Listeria monocytogenes Neonates;
immunosuppressed
sporadic cases (95%-97%) are caused by serogroups B, C, Saudi Arabia is a risk factor for meningococcal meningitis,
and Y, whereas A and C strains are usually observed in epi- and vaccination is required.
demics. Risk factors for meningococcal infection include Neisseria meningitidis infection often begins with a mild
host and environmental factors. Host defects include termi- upper respiratory tract illness that may then disseminate into
nal complement component (C5-C9) deficiencies, which the bloodstream, leading to the development of a petechial
increase attack rates but are associated with low mortality, rash that often occurs around the same time as the develop-
and properdin defects, which increase the risk of invasive ment of fever and meningeal signs. The diagnosis can be made
disease. The organism is spread via airborne droplets from by visualizing the small Gram-negative diplococci on a cere-
asymptomatic pharyngeal carriers. Environmental factors brospinal fluid Gram stain. Treatment is with penicillin G if
include a preceding viral respiratory infection; household, the MIC concentration is less than 0.1 mcg/mL, otherwise
barracks, or dormitory crowding; chronic medical illnesses; high-dose ceftriaxone or cefotaxime is preferred.
corticosteroid use; and active or passive smoking. Travel to Close contacts of the index case (hospital workers with
the meningitis belt of north central Africa or to the Haj in direct exposure to respiratory secretions during intubation or
AGE GROUP/PATIENT
GROUP COMMON PATHOGENS ANTIMICROBIAL THERAPY
Age
04 wk Group B streptococci, Escherichia coli, Listeria monocytogenes, Ampicillin plus cefotaxime or ampicillin plus an
Klebsiella pneumoniae, Enterococcus spp, Salmonella spp aminoglycoside
123 mo Group B streptococci, E coli, L monocytogenes, Haemophilus Vancomycin plus cefotaxime or ceftriaxone
influenzae, Streptococcus pneumoniae, Neisseria meningitidis
250 y N meningitidis, S pneumoniae Vancomycin plus cefotaxime or ceftriaxone
>50 y S pneumoniae, L monocytogenes, aerobic gram-negative bacilli Vancomycin plus either cefotaxime or ceftriaxone
plus ampicillin (cephalosporins have NO activity
vs Listeria)
Basilar skull fracture S pneumoniae, H influenzae, group A -hemolytic streptococci Vancomycin plus cefotaxime or ceftriaxone
Post-neurosurgery Coagulase-negative staphylococci, Staphylococcus aureus, aero- Vancomycin plus cefepime or ceftazidime or
bic gram-negative bacilli (including P aeruginosa) meropenem
Adapted from Tunkel AR, Hartman BJ, Kaplan SL, Kaufman BA, Roos KL, Scheld WM, et al. Practice guidelines for the management of bacterial meningitis. Clin Infect
Dis. 2004 Nov 1;39(9):126784. Epub 2004 Oct 6. Used with permission.
22 . H E A LT H C A R E A S S O C I AT E D I N F E C T I O N S 335
mouth-to-mouth resuscitation, roommates, household con- The most common cause of bacterial meningitis in adults is
tacts, day-care center members, persons exposed to patients S pneumoniae.
oral secretions) should be offered chemoprophylaxis within
Consider the possibility of a cerebrospinal fluid leak in
24 hours of exposure. For adults, ceftriaxone (250 mg intra-
patients with recurrent S pneumoniae meningitis.
muscularly), rifampin (600 mg twice daily for 2 days), or cip-
rofloxacin (use only in patients 18 years or older, 500 mg for 1
dose) has been used. Cases of ciprofloxacin-resistant N men-
ingitidis have been reported recently in Minnesota and North Haemophilus influenzae
Dakota (in these cases, ceftriaxone, rifampin, or azithromycin
is an alternative). Because the carrier state is not eliminated Widespread use of the vaccine against H influenzae B has dra-
by penicillin, the index patient may require one of these pro- matically reduced the incidence of invasive disease in children.
phylaxis regimens for eradication of carriage. Immunization Non-typeable strains of H influenzae more frequently cause
of certain populations (eg, military recruits, college students disease in adults (primarily respiratory infection). Infections
living in dormitories, Haj pilgrims, patients with terminal caused by H influenzae include pneumonia, meningitis, epi-
complement component deficiencies or asplenia) is also glottitis, and primary bacteremia. The organism is associated
recommended. Two meningococcal vaccines are currently with infectious exacerbations of chronic obstructive pulmo-
available for serogroups A, C, Y, and W-135: the older polysac- nary disease and with sinusitis and otitis media. Chronic lung
charide vaccine (Menomune) and a newer conjugate vaccine disease, pregnancy, human immunodeficiency virus infection,
(Menactra, MCV4) that offers longer protection. The MCV4 hypogammaglobulinemia, splenectomy, and malignancy are
vaccine is now recommended at entry to high school. risk factors for invasive disease.
Terminal component complement deficiencies can Chronic lung disease, pregnancy, human
predispose patients to repeated episodes of meningococcal immunodeficiency virus infection, splenectomy, and
meningitis. malignancy are risk factors for invasive disease due to H
influenzae.
If the risk for the carrier state is high (household contacts),
rifampin, ceftriaxone, or ciprofloxacin should be given for Up to 40% of H influenzae organisms recovered from
prophylaxis within 24 hours of index case. adults with invasive disease are resistant to ampicillin by vir-
tue of -lactamase production. Nonmeningeal infections
P N EU M O C O C C A L M E N I N G I T I S with H influenzae can be treated with trimethoprim-sulfa-
methoazole, third-generation cephalosporins, fluoroquinolones,
Streptococcus pneumoniae is the most common cause of bac- or a -lactam-lactamase inhibitor combination such as
terial meningitis in adults (Figure 22.2), including those ampicillin-sulbactam.
with recurrent meningitis due to cerebrospinal fluid leaks.
Meningitis due to susceptible strain of S pneumoniae can still Approximately 40% of H influenzae clinical isolates are
be treated successfully with high-dose penicillin G. However, resistant to ampicillin.
given the spread of penicillin-resistant strains, bacterial men-
ingitis should be empirically treated with high-dose cefo- Infection with H influenzae is now an uncommon cause
taxime or ceftriaxone, in combination with vancomycin, while of meningitis in adults, although it can occur with hypo-
awaiting the susceptibility results. Adjunctive treatment with gammaglobulinemia, asplenia, or cerebrospinal fluid leak.
dexamethasone has been shown to be beneficial if started at Third-generation cephalosporins (cefotaxime or ceftriaxone)
the same time or before the first dose of antibiotic. are the drugs of choice for H influenzae meningitis.
LISTERIOSIS
Listeria monocytogenes is a small, motile, gram-positive,
rod-shaped organism. Meningitis and bacteremia are the most
common clinical manifestations of infection. Listeria organ-
isms may be difficult to visualize on Gram stain of spinal fluid.
The elderly, neonates, pregnant women, and persons taking
corticosteroids are at highest risk for invasive disease due to
Listeria. Epidemics have been associated with consumption
of contaminated dairy products and some ready-to-eat foods
such as hot dogs and luncheon meats. Diarrhea is usually a fea-
ture of epidemic listeriosis.
Penicillin and ampicillin are the most effective agents
against Listeria. Antimicrobial coverage for Listeria (with
Figure 22.2 Streptococcus pneumoniae in Sputum (Gram Stain). ampicillin or trimethoprim-sulfamethoxazole) should always
Table 22.4 EPIDEMIOLOGIC CLUES TO INFECTIOUS CAUSES OF ACUTE ASEPTIC MENINGITIS AND
MENINGOENCEPHALITIS
Winter Mumps
Mosquito bites Eastern and Western Equine viruses, West Nile virus, St. Louis virus, La Crosse virus
Ticks Lyme disease, Ehrlichia or Anaplasma infection, Rocky Mountain spotted fever
Risk factors for sexually transmitted infections Herpes simplex virus or human immunodeficiency virus
22 . H E A LT H C A R E A S S O C I AT E D I N F E C T I O N S 337
Empiric therapy for encephalitis should always include and bats. Spread by other animals is very rare. Rodents rarely,
intravenous high-dose acyclovir and antibiotics (to cover the if ever, transmit rabies.
possibility of bacterial meningitis), including doxycycline if Rabies acquisition in the United States is predominantly
risk factors for Rickettsia or Ehrlichia infections are present. related to bat bites, which may not be apparent, especially
Once an etiologic agent is identified, therapy should be tar- if they occur during sleep. Aerosol spread is possible, and it
geted to that pathogen and use of other antimicrobial agents is most often due to exposure to bats during spelunking or
should be discontinued. in medical laboratories. Annually, 1 or 2 cases of rabies are
reported in the United States. From 1995 to 2006, 7 of 37
Characteristic features of aseptic meningitis are fever, cases in the United States were due to exposure to rabid ani-
neck stiffness, cerebrospinal fluid pleocytosis (usually mals outside the country, whereas the majority of the rest (28,
lymphocytic), and negative results of bacterial cultures. including 4 transplant recipients from a donor with rabies)
were from exposure to bats in the United States. Rabies also
Empiric therapy for meningoencephalitis should include has been reported to occur in patients after corneal transplant.
acyclovir until herpes simplex virus-1 infection is excluded The risk for nosocomial transmission is low.
by polymerase chain reaction test of cerebrospinal fluid. Definitive diagnosis of rabies encephalitis is established by
finding Negri bodies on biopsy of the hippocampus. Serum
C H RO N I C M E N I N G IT I S SY N D RO M E and cerebrospinal fluid can be tested for rabies antibodies
when trying to diagnose the disease. Direct fluorescent anti-
Signs and symptoms of meningeal inflammation are more body testing of a skin biopsy specimen from the nape of the
subtle in chronic meningitis and evolve over weeks to months. neck can be used to detect rabies antigen.
Chronic meningitis may be due to either infectious or nonin-
fectious causes. Delayed presentation with apathy or altered
Rabies should be considered in any case of encephalitis or
mentation can occur. The cerebrospinal fluid profile shows
myelitis of unknown cause.
inflammatory changes. The infection is most often due to
organisms such as Brucella, Nocardia, spirochetes (syphilis, Most common sources of exposure are dogs, cats, skunks,
Lyme disease), fungi (Cryptococcus, Coccidioides, Histoplasma, foxes, raccoons, wolves, and bats, but rarely rodents.
Blastomyces), mycobacteria, and parasites.
Any bite by bats or other animals suspected of carry-
OT H E R C AUS E S O F C E N T R A L N E RVO US ing rabies should be taken very seriously. Post-bite manage-
SYST E M I N FEC T I O NS ment includes observing the animal, if possible, immediate
soap and water washing of the wound, administering rabies
Poliovirus immunoglobulin (injected into the bite site), and starting the
Although wild-type polio has been eliminated from the Western postexposure rabies vaccine schedule. Human diploid vaccine
Hemisphere, it remains endemic in parts of Asia and Africa. is more effective and less toxic than the older duck embryo
Disease still can be imported from these areas. Notably, a recent vaccine. Human rabies immunoglobulin is now widely avail-
outbreak in the Netherlands occurred among members of reli- able, mitigating the need to use horse serum immunoglobu-
gious groups that were not vaccinated. Polio is most often an lin. However, rabies immunoglobulin and vaccine are not of
asymptomatic infection. The virus affects the nuclei of cranial benefit after the onset of clinical disease. Pre-exposure rabies
nerves and anterior motor neurons of the spinal cord, causing vaccination is advised for patients likely to be in situations that
a flaccid paralysis. When paralysis develops, it is usually asym- put them at high risk for rabies, such as occupational expo-
metric. Vaccine-related polio, although rare, can occur with the sure in veterinary medicine, spelunking, and prolonged stay in
live oral polio vaccine (OPV). In July 2000, a vaccine-strain rabies-endemic countries. Pre-exposure vaccination mitigates
polio outbreak occurred in the Dominican Republic and Haiti. the need for rabies immunoglobulin and decreases the postex-
Patients traveling to these countries are advised to receive an posure doses to only 2 (days 0 and 3 after the bite).
injectable inactivated polio vaccine booster. A polio-like illness
in the United States, without travel or exposure, should also S L OW V I RUS E S A N D P R I O N-A S S O C I AT E D
raise suspicion for West Nile virus. C E N T R A L N E RVO US S YS T E M D I S E A S E S
Progressive Multifocal Leukoencephalopathy
Rabies
Progressive multifocal leukoencephalopathy is caused by a
A high index of suspicion is a requisite for antemortem diag- papovavirus ( JC virus) and usually occurs in immunocom-
nosis of rabies. Cardinal clinical manifestations are hydropho- promised patients, such as those with AIDS, leukemia, lym-
bia and copious salivation. Rabies should be considered in any phoma, and immunosuppression for organ transplant. It can
case of encephalitis or myelitis of unknown cause, especially in cause either diffuse or focal central nervous system abnor-
persons who have recently traveled outside the United States. malities. Despite its name, progressive multifocal leukoen-
The virus spreads along peripheral nerves to the central ner- cephalopathy usually causes solitary brain lesions, as seen
vous system. The most common sources of exposure are dogs, on computed tomography or magnetic resonance imaging.
cats, skunks, foxes, raccoons (Florida, Connecticut), wolves, Results of spinal fluid analysis are normal in most cases, and
NAT I V E VA LVE E N D O C A R D IT I S Adapted from Li JS, Sexton DJ, Mick N, Nettles R, Fowler VG Jr, Ryan T, et
al. Proposed modifications to the Duke criteria for the diagnosis of infective
Native valve infective endocarditis is more common in men endocarditis. Clin Infect Dis. 2000 Apr;30(4):6338. Epub 2000 Apr 3. Used
with permission.
and patients older than 65 years. The age- and sex-adjusted
22 . H E A LT H C A R E A S S O C I AT E D I N F E C T I O N S 339
Box 22.2 DEFINITIONS OF TERMINOLOGY USED valve endocarditis are due to viridans group streptococci (ie,
IN THE MODIFIED DUKE CRITERIA FOR THE Streptococcus sanguis, Streptococcus mutans, and Streptococcus
DIAGNOSIS OF INFECTIVE ENDOCARDITIS mitis), S aureus, and enterococci. Less common causes include
Streptococcus bovis (associated with gastrointestinal malig-
Major criteria nancy), S pneumoniae, coagulase-negative staphylococci
Blood culture positive for infective endocarditis (Staphylococcus lugdunensis has a behavior similar to that of
Typical microorganisms consistent with infective endocardi- S aureus), gram-negative bacilli, and fungi. In injection drug
tis from 2 separate blood cultures users, S aureus (60%), streptococci (16%), gram-negative
Viridans streptococci, Streptococcus bovis, HACEK group, bacilli (13.5%), polymicrobial infection (8.1%), group JK
Staphylococcus aureus, or Corynebacterium (1.4%), and Candida species may be culprits.
Community-acquired enterococci, in the absence of a pri- Tricuspid valve involvement is common in injection drug users
mary focus, or and patients with health careassociated endocarditis due to
Microorganisms consistent with infective endocarditis from central venous catheters or cardiac devices.
persistently positive blood cultures, defined as follows: Empiric antibiotic therapy before obtaining blood for cul-
At least 2 positive cultures of blood samples drawn more ture is the most common cause of culture-negative endocardi-
than 12 hours apart, or tis. Other reasons for culture-negative endocarditis include
All of 3 or a majority of 4 or more separate blood cultures, infection with fastidious organisms that are difficult to culti-
with first & last samples drawn at least 1 hour apart vate in blood cultures, such as Bartonella species, Chlamydia
Single blood culture positive for Coxiella burnetii or anti- species, Tropheryma whippelii, fungi, and Coxiella burnetii.
phase I immunoglobulin G antibody titer 1:800 The most frequent causes of culture-negative endocardi-
Evidence of endocardial involvement tis are listed in Box 22.3. Several of these can be diagnosed
Echocardiogram positive for infective endocarditis (TEE with serologic tests or molecular assays. The HACEK group
recommended in patients with prosthetic valves, rated at (Haemophilus species, Actinobacillus actinomycetemcomitans,
least possible infective endocarditis by clinical criteria, or Cardiobacterium hominis, Eikenella species, and Kingella kin-
complicated infective endocarditis [paravalvular abscess]; gae) has become a less frequent cause of culture-negative endo-
TTE as first test in other patients), defined as follows: carditis because the organisms are more easily detected with
Oscillating intracardiac mass on valve or supporting struc- contemporary blood culturing systems.
tures, in the path of regurgitant jets, or on implanted Treatment guidelines for native valve infective endocardi-
material in the absence of an alternative anatomical tis are listed in Table 22.5.
explanation, or Native valve endocarditis may be complicated by invasion
Abscess, or and destruction of the valve or endocardium or by distant
New partial dehiscence of prosthetic valve embolization. Large vegetations, more than 15 mm, increase
New valvular regurgitation (worsening or changing of preex- the risk for embolization. The risk for embolization is greatest
isting murmur not sufficient) before the receipt of appropriate antimicrobials and decreases
Minor criteria after the first week of therapy. Large vegetations may be asso-
Predisposition: predisposing heart condition or intravenous ciated with prolonged, yet unrecognized infection or specific
drug use microorganisms such as group B streptococci, HACEK, and
Fever: >38.0C (100.4F) fungi. Embolization may lead to strokes, mycotic aneurysms,
Vascular phenomena: major arterial emboli, septic pulmonary and splenic, hepatic, and renal abscesses. Abscesses due to
infarcts, mycotic aneurysm, intracranial hemorrhage, con- native valve infective endocarditis need to be drained before
junctival hemorrhages, Janeway lesions valve replacement.
Immunologic phenomena: glomerulonephritis, Osler nodes, The indications for surgical treatment of native valve infec-
Roth spots, rheumatoid factor tive endocarditis are listed in Box 22.4.
Microbiologic evidence: positive blood culture but not meet-
ing major criteria as noted previouslya or serologic evidence Congestive heart failure, refractory to medical
of active infection with organisms consistent with infective management, is the most common indication for valve
endocarditis replacement surgery in native valve endocarditis.
Echocardiographic minor criteria eliminated
Abbreviations: HACEK, Haemophilus spp, Actinobacillus actinomycetem- P RO S T H ET I C VA LVE E N D O C A R D IT I S
comitans, Cardiobacterium hominis, Eikenella spp, and Kingella kingae; TEE,
transesophageal echocardiography; TTE, transthoracic echocardiography. Prosthetic valve endocarditis accounts for 1% to 5% of all
a
Excluding single positive cultures for coagulase-negative staphylococci & endocarditis cases. However, the increasing number of patients
organisms that do not cause endocarditis. with prosthetic valves and pacemakers is increasing the popu-
lation at risk. Prosthetic valve endocarditis can be broadly cat-
Adapted from Li JS, Sexton DJ, Mick N, Nettles R, Fowler VG Jr, Ryan T, et
al. Proposed modifications to the Duke criteria for the diagnosis of infective
egorized into early and late onset. Early-onset prosthetic valve
endocarditis. Clin Infect Dis. 2000 Apr;30(4):6338. Epub 2000 Apr 3. Used endocarditis is an infection occurring within 2 months after
with permission. valve replacement surgery, whereas late-onset prosthetic valve
endocarditis occurs more than 2 months postoperatively.
+ +
Rx Look for
other
source
Look for Rx
other
source Follow-up TEE or TTE
to reassess vegetations,
complications, or Rx
response as clinically
indicated
Figure 22.3 An Approach to the Use of Echocardiography (Echo) for the Diagnosis of Infective Endocarditis (IE). aFor example, a patient with fever
and a previously known heart murmur and no other stigmata of IE. bHigh initial patient risks include prosthetic heart valves, many congenital heart
diseases, previous endocarditis, new murmur, heart failure, or other stigmata of endocarditis. cHigh-risk echocardiographic features include large or
mobile vegetations, valvular insufficiency, suggestion of perivalvular extension, or secondary ventricular dysfunction. Rx indicates antibiotic treatment
for endocarditis; TEE, transesophageal echocardiography; TTE, transthoracic echocardiography. (Adapted from Bayer AS, Bolger AF, Taubert KA,
Wilson W, Steckelberg J, Karchmer AW, et al. Diagnosis and management of infective endocarditis and its complications. Circulation. 1998 Dec
2229;98[25]:293648. Used with permission.)
22 . H E A LT H C A R E A S S O C I AT E D I N F E C T I O N S 341
Table 22.5 TREATMENT OF NATIVE VALVE INFECTIVE ENDOCARDITIS
Penicillin-sensitive viridans group streptococci Aqueous crystalline penicillin G, 1218 10 6 U/24 h IV either Vancomycin,b 30 mg/kg IV in 2 equally divided doses, not to exceed
and Streptococcus bovis (MIC, 0.1 mcg/mL) continuously or in 6 equally divided doses for 4 wk 2 g/24 h unless serum levels are monitored for 4 wk
Or Vancomycin therapy is recommended for patients allergic to -lactams
Ceftriaxone sodium 2 g IV or IM for 4 wkc (immediate-type hypersensitivity); serum concentration of vancomy-
Or cin should be obtained 1 h after completion of the infusion & should
Aqueous penicillin G, 1218 10 6 U/24 h IV either continuously or be in the range of 3045 mcg/mL for twice-daily dosing
in 6 equally divided doses for 2 wk
Plus
Gentamicin sulfate,d 1 mg/kg IV or IM every 8 h for 2 wk
Relatively penicillin-resistant viridans group Aqueous crystalline penicillin G, 24 10 6 U/24 h IV either continu- Vancomycin,b 30 mg/kg IV in 2 equally divided doses, not to exceed
streptococci (MIC, >0.1 mcg/mL & <0.5 mcg/ ously or in 46 equally divided doses for 4 wk 2 g/24 h unless serum levels are monitored for 4 wk
mL) Plus Vancomycin therapy is recommended for patients allergic to -lactams
Gentamicin sulfate,d 1 mg/kg IV or IM every 8 h for 2 wk (immediate-type hypersensitivity); serum concentration of vancomy-
cin should be obtained 1 h after completion of the infusion & should
be in the range of 3045 mcg/mL for twice-daily dosing
Enterococci (gentamicin- or Aqueous crystalline penicillin G, 1830 10 6 U/24 h IV either Vancomycin,b 30 mg/kg IV in 2 equally divided doses, not to exceed
vancomycin-susceptible) or viridans group continuously or in 6 equally divided doses for 46 wk 2 g/24 h unless serum levels are monitored for 46 wk
streptococci with MIC 0.5 mcg/mL or Or Plus
nutritionally variant streptococci (All entero- Ampicillin sodium 12 g/24 h IV either continuously or in 6 equally Gentamicin,d 1 mg/kg IV or IM every 8 h for 46 wk
cocci causing endocarditis must be tested for divided doses
antimicrobial susceptibility in order to select
optimal therapy) Plus
Gentamicin sulfate,d 1 mg/kg IV or IM every 8 h for 46 wk (4-wk Vancomycin therapy is recommended for patients allergic to -lactams
therapy recommended for patients with symptoms 3 mo in dura- (immediate-type hypersensitivity); serum concentration of vancomy-
tion; 6-wk therapy recommended for patients with symptoms >3 cin should be obtained 1 h after completion of the infusion & should
mo in duration) be in the range of 3045 mcg/mL for twice-daily dosing
Cephalosporins are not acceptable alternatives for patients allergic to
penicillin
High-level aminoglycoside-resistant Enterococcus Linezolid, 1,200 mg/24 h IV or PO in 2 divided doses for 8 wk Patients with endocarditis caused by these strains should be treated in
faecalis: ceftriaxone 2 g IV every 12 h plus consultation with an infectious diseases specialist
ampicillin 2 g IV every 4 h for 46 wk Cardiac valve replacement may be necessary for bacteriologic cure
Or Cure with antimicrobial therapy alone may be <50%
Severe, usually reversible thrombocytopenia may occur with use of
linezolid, especially after 2 wk of therapy
Dalfopristin/quinupristin, 22.5 mg/kg per 24 h IV in 3 divided doses Dalfopristin/quinupristin only effective against E faecium & can cause
for 8 wk severe myalgias, which may require discontinuation of therapy
Only small number of patients have reportedly been treated with imi-
penem/cilastatin-ampicillin or ceftriaxone + ampicillin
Enterococcus faecalis Imipenem/cilastatin, 2 g/24 h IV in 4 equally divided doses
for 8 wk
Plus
Ampicillin sodium, 12 g/24 h IV in 6 divided doses for 8 wk
Or
Ceftriaxone sodium, 2 g/24 h IV or IM in 1 dose for 8 wk
Plus
Ampicillin sodium, 12 g/24 h IV in 6 divided doses for 8 wk
Pediatric dose (should not exceed that of a normal adult): linezolid
30 mg/kg per 24 h IV or PO in 3 divided doses; dalfopristin/qui-
nupristin 22.5 mg/kg per 24 h IV in 3 divided doses; imipenem/
cilastatin 60100 mg/kg per 24 h IV in 4 divided doses; ampicillin
300 mg/kg per 24 h IV in 46 divided doses; ceftriaxone 100 mg/
kg per 24 h IV or IM once daily
Staphylococcus aureuse
Methicillin-sensitive Nafcillin sodium or oxacillin sodium, 2.0 g IV every 4 h for 46 wk Cefazolin (or other first-generation cephalosporins in equivalent dos-
Plus ages), 2 g IV every 8 h for 46 wk
Gentamicin sulfate (optional),d 1 mg/kg every 8 h IV or IM for first Plus
35 d Gentamicin (optional),d 1 mg/kg every 8 h IV or IM for first 35 d
Benefit of additional aminoglycoside has not been established Cephalosporins should be avoided in patients with immediate-type
hypersensitivity to penicillin
Vancomycin,b 30 mg/kg IV in 2 equally divided doses, not to exceed
2 g/24 h unless serum levels are monitored for 46 wk
Vancomycin therapy is recommended for patients allergic to -lactams
(immediate-type hypersensitivity); serum concentration of vancomy-
cin should be obtained 1 h after completion of the infusion & should
be in the range of 3045 mcg/mL for twice-daily dosing
Daptomycin 6 mg/kg once daily may be used as an alternative in
right-sided endocarditis due to MSSA or MRSA
Methicillin-resistant Vancomycin,b 30 mg/kg IV in 2 equally divided doses, not to exceed Consult infectious diseases specialist
2 g/24 h unless serum levels are monitored for 46 wk Daptomycin 6 mg/kg once daily may be used as an alternative in
right-sided endocarditis due to MSSA or MRSA
HACEK group Ceftriaxone sodium, 2 g IV or IM for 4 wkc Consult infectious diseases specialist
Or
Ampicillinf-sulbactam 12 g/24 h IV in 4 divided doses for 4 wk
Or
Ciprofloxacin 1,000 mg/24 h PO or 800 mg/24 h IV in 2 divided
doses if unable to tolerate alternatives
Cefotaxime sodium or other third-generation cephalosporins may be
substituted
Neisseria gonorrhoeae Ceftriaxone, 12 g every 24 h for 4 wk Aqueous crystalline penicillin G, 20 10 6 U/24 h IV either continu-
ously or in 6 equally divided doses for 4 wk, for penicillin-susceptible
isolates
(continued)
Table 22.5 TREATMENT OF NATIVE VALVE INFECTIVE ENDOCARDITIS (CONTINUED)
Urgent empiric treatment for culture-negative Vancomycin,b 30 mg/kg IV in 2 equally divided doses, not to exceed
endocarditis 2 g/24 h unless serum levels are monitored for 6 wk
Plus
Gentamicin sulfate,d 1.0 mg/kg IV every 8 h for 6 wk
Suspected Bartonella, culture negative Ceftriaxone sodium, 2 g/24 h IV or IM in 1 dose for 6 wk Consult infectious diseases specialist
Plus
Gentamicin sulfate, 3 mg/kg per 24 h IV or IM in 3 divided doses for
2 wk
With or without
Doxycycline 200 mg/kg per 24 h IV or PO in 2 divided doses for
6 wk
Abbreviations: HACEK, Haemophilus spp, Actinobacillus actinomycetemcomitans, Cardiobacterium hominis, Eikenella spp, and Kingella kingae; IM, intramuscularly; IV, intravenously; MIC, minimal inhibitory concentration; MRSA,
methicillin-resistant Staphylococcus aureus; MSSA, methicillin-sensitive Staphylococcus aureus; PO, orally.
a
Dosages recommended are for patients with normal renal function.
b
Vancomycin dosage should be reduced in patients with impaired renal function. Vancomycin given on an mg/kg basis produces higher serum concentrations in obese patients than in lean patients. Therefore, in obese patients, dosing
should be based on ideal body weight. Each dose of vancomycin should be infused over at least 1 hour to reduce the risk of the histamine-release red man syndrome.
c
Patients should be notified that IM injection of ceftriaxone is painful.
d
Dosing of gentamicin on an mg/kg basis produces higher serum concentrations in obese patients than in lean patients. Therefore, in obese patients, dosing should be based on ideal body weight. (Ideal body weight for men is 50 kg +
2.3 kg per inch over 5 feet, and ideal body weight for women is 45.5 kg + 2.3 kg per inch over 5 feet.) Relative contraindications to the use of gentamicin are age older than 65 years, renal impairment, or impairment of the eighth nerve.
Other potentially nephrotoxic agents (such as nonsteroidal anti-inflammatory drugs) should be used cautiously in patients receiving gentamicin.
e
For treatment of endocarditis due to penicillin-susceptible staphylococci (MIC, <0.1 mcg/mL), aqueous crystalline penicillin G, 1218 106 U/24 h IV either continuously or in 6 equally divided doses for 4 to 6 weeks, can be used
instead of nafcillin or oxacillin. Shorter antibiotic courses have been effective in some injection drug users with right-sided endocarditis due to Staphylococcus aureus. The routine use of rifampin is not recommended for the treatment
of native valve staphylococcal endocarditis.
f
Ampicillin should not be used if laboratory tests show -lactamase production.
Data from Wilson WR, Karchmer AW, Dajani AS, Taubert KA, Bayer A, Kaye D, et al; American Heart Association. Antibiotic treatment of adults with infective endocarditis due to streptococci, enterococci, staphylococci, and
HACEK microorganisms. JAMA. 1995 Dec 6;274(21):170613; adapted from Steckelberg JM, Guiliani ER, Wilson WR. Infective endocarditis. In: Giuliani ER, Fuster V, Gersh BJ, McGoon MD, McGoon DC, editors. Cardiology:
fundamentals and practice. 2nd ed. Vol 2. St. Louis (MO): Mosby Year Book; c1991. p. 173972. Used with permission of Mayo Foundation for Medical Education and Research; and adapted from Baddour LM, Wilson WR, Bayer AS,
Fowler VG Jr, Bolger AF, Levison ME, et al. Infective endocarditis: diagnosis, antimicrobial therapy, and management of complications: a statement for healthcare professionals from the Committee on Rheumatic Fever, Endocarditis,
and Kawasaki Disease, Council on Cardiovascular Disease in the Young, and the Councils on Clinical Cardiology, Stroke, and Cardiovascular Surgery and Anesthesia, American Heart Association: executive summary. Circulation.
2005 Jun 14;111(23):316784. Used with permission.
Box 22.4 INDICATIONS FOR SURGICAL with the 4-week regimen. Therefore, 6 weeks of therapy is
REPLACEMENT OF CARDIAC VALVES IN INFECTIVE recommended. Vancomycin is considered less effective than
ENDOCARDITIS penicillin and therefore should be used only in cases of peni-
cillin resistance or if a patient is allergic to penicillin. Optimal
Congestive heart failure refractory to medical management >1 regimens for isolates resistant to both gentamicin and strep-
serious systemic embolic episode tomycin are unknown. A valve replacement procedure may
Uncontrolled bacteremia despite antimicrobial therapy increase the chance for successfully treating subacute bacterial
Invasive perivalvular infection endocarditis due to drug-resistant enterococci.
New ECG changes
Persistent unexplained fever Enterococcal endocarditis is best treated with a
Fungal endocarditis combination of penicillin (or ampicillin) plus gentamicin
Relapse of treated prosthetic valve encocarditis due to penicillin- (or streptomycin).
sensitive streptococci
Abbreviation: ECG, electrocardiographic.
Haemophilus Species Other Than influenzae
Viridans Group Streptococci Haemophilus parainfluenzae, H aphrophilus, and H paraphro-
philus are part of normal oral flora. When these or other mem-
Several species of non-Lancefield typeable streptococci are bers of the HACEK (Haemophilus species; Actinobacillus
referred to as the viridans group of streptococci. These are actinomycetemcomitans; Cardiobacterium hominis; Eikenella
part of normal oral and enteric flora. This group of organisms corrodens; and Kingella species) group of organisms are recov-
is a common cause of subacute bacterial endocarditis, which ered from blood cultures, infective endocarditis should be
should be suspected when viridans group of streptococci are suspected. Large valvular vegetations with systemic emboli are
found in blood cultures. Like the pneumococci, these organ- frequent with HACEK endocarditis. Usual treatment is with
isms are increasingly likely to display variable resistance to ceftriaxone or ampicillin-sulbactam (if the organism is suscep-
penicillin. tible) for 4 weeks.
22 . H E A LT H C A R E A S S O C I AT E D I N F E C T I O N S 345
Table 22.6 CAUSATIVE ORGANISMS FOR PROSTHETIC VALVE ENDOCARDITIS (PVE) IN 556
PATIENTS
CAUSATIVE ORGANISM TOTAL, NO. (%) (N=556) EARLY PVE, NO. (%) (n=53) LATE PVE, NO. (%) (n=331)
Abbreviations: HACEK, Haemophilus spp, Actinobacillus actinomycetemcomitans, Cardiobacterium hominis, Eikenella spp, and Kingella kingae; NOS,
not otherwise speciated.
Adapted from Wang A, Athan E, Pappas PA, Fowler VG Jr, Olaison L, Par C, et al. Contemporary clinical profile and outcome of prosthetic valve endo-
carditis. JAMA. 2007 Mar 28;297(12):135461. Used with permission.
I N F EC T I O N S O F C A R D I O VA S C U L A R
staphylococcus) account for two-thirds of the cases. Regardless
I M P L A N TA B L E E L EC T RO N I C D EVI C E S
of the infecting pathogen and clinical presentation, complete
Permanent pacemakers, implantable cardioverter-defibrillators, removal of the infected device (including generator and trans-
and other cardiac devices are being increasingly used and are asso- venous leads) is a requisite for curing these infections.
ciated with infectious complications. Infections associated with Box 22.5 and Figure 22.4 summarize Mayo Clinic guide-
these devices may present as localized generator pocket infec- lines for the diagnosis and management of cardiac devices.
tion or systemic infection associated with bacteremia or lead American Heart Association endorsed these guidelines in the
endocarditis. Staphylococci (S aureus and coagulase-negative updated Scientific Statement published in 2010.
Staphylococcus aureus or coagulase-negative staphylo- Vancomycin,b 30 mg/kg IV in 2 equally divided doses, not Rifampin increases the amount of warfarin sodium required for antithrom-
cocci: methicillin-resistant to exceed 2 g/24 h unless serum levels are monitored for botic therapy
6 wk
Plus
Rifampin,c 300 mg PO every 8 h for 6 wk
Plus
Gentamicin sulfate,d 1 mg/kg IV or IM every 8 h for first
2 wk of therapy. (If organism is not susceptible to gen-
tamicin, ciprofloxacin may be substituted if the organism
is susceptible in vitro)
Staphylococcus aureus or coagulase-negative staphy- Nafcillin sodium or oxacillin sodium, 2 g IV every 4 h Rifampin increases the amount of warfarin sodium required for antithrom-
locci: methicillin-susceptible for 6 wk botic therapy
Plus First-generation cephalosporins or vancomycin should be used in patients
Rifampin,c 300 mg orally every 8 h for 6 wk allergic to -lactams
Plus Cephalosporins should be avoided in patients with immediate-type hypersen-
Gentamicin sulfate,d 1 mg/kg IV or IM every 8 h for first sitivity to penicillin or to methicillin-resistant staphylococci
2 wk of therapy. (If organism is not susceptible to gen-
tamicin, ciprofloxacin may be substituted if the organism
is susceptible in vitro)
Enterococci (gentamicin- or vancomycin-susceptible) Aqueous crystalline penicillin G, 1830 10 6 U/24 h IV Vancomycin,b 30 mg/kg IV in 2 equally divided doses, not to exceed 2 g/24 h
or viridans group streptococci or nutritionally either continuously or in 6 equally divided doses for 6 wk unless serum levels are monitored for 46 wk
variant streptococci or Streptococcus bovis (All Or Plus
streptococci causing endocarditis must be tested Ampicillin sodium, 12 g/24 h IV either continuously or in Gentamicin sulfate,d 1 mg/kg IV or IM every 8 h for 46 wk
for antimicrobial susceptibility in order to select 6 equally divided doses Vancomycin therapy is recommended for patients allergic to -lactams
optimal therapy) Plus (immediate-type hypersensitivity); serum concentration of vancomycin
Gentamicin sulfate,d 1 mg/kg IV or IM every 8 h for 6 wk should be obtained 1 h after completion of the infusion & should be in the
range of 3045 mcg/mL for twice-daily dosing
Cephalosporins are not acceptable alternatives for patients allergic to
penicillin
Enterococcus faecium Linezolid, 1,200 mg/24 h IV or PO in 2 divided doses for Patients with endocarditis caused by these strains should be treated in
8 wk consultation with an infectious diseases specialist
Cardiac valve replacement may be necessary for bacteriologic cure
Or Cure with antimicrobial therapy alone may be <50%
Severe, usually reversible thrombocytopenia may occur with use of linezolid,
especially after 2 wk of therapy
Dalfopristin/quinupristin, 22.5 mg/kg per 24 h IV in Dalfopristin/quinupristin only effective against E faecium & can cause severe
3 divided doses for 8 wk myalgias, which may require discontinuation of therapy
Only small number of patients have reportedly been treated with imipenem/
cilastatin-ampicillin or ceftriaxone + ampicillin
(continued)
Table 22.7 TREATMENT OF PROSTHETIC VALVE INFECTIVE ENDOCARDITIS (CONTINUED)
22 . H E A LT H C A R E A S S O C I AT E D I N F E C T I O N S 349
A
Suspected PPM/ICD infection
TEE
Treat with Treat with Treat with Treat with Treat with
antibiotics for antibiotics for antibiotics for antibiotics for antibiotics for
4-6 wka 2 wka 4 wka 10-14 da 7-10 da
B
Reimplantation of new PPM/ICD
Repeat blood cultures after Repeat blood cultures after Negative blood cultures for
device removal device explantation 72 h after device removal
Figure 22.4 Algorithm for Management of Cardiac Device Infection. A, Approach to management of adults (also see Box 22.6). This algorithm
applies only to patients with complete device explantation. B, Guidelines for reimplantation of new device (also see Box 22.5). aDuration of
antibiotic treatment should be counted from the day of device explantation. AHA indicates American Heart Association; ICD, implantable
cardioverter-defibrillator; PPM, permanent pacemaker; S aureus, Staphylococcus aureus; TEE, transesophageal echocardiography; +, positive; ,
negative. (Adapted from Sohail MR, Uslan DZ, Khan AH, Friedman PA, Hayes DL, Wilson WR, et al. Management and outcome of permanent
pacemaker and implantable cardioverter-defibrillator infections. J Am Coll Cardiol. 2007 May 8;49[18]:18519. Epub 2007 Apr 23. Used with
permission.)
be drained and sent for Gram stain and bacterial culture to vulnificus after saltwater exposure, Erysipelothrix rhusiopathiae
exclude community-acquired MRSA. and Streptococcus iniae after fish exposure, and P aeruginosa
Unusual causes of soft tissue infection are Eikenella cor- after hot tub exposure.
rodens and oral anaerobes after human bites (knuckles celluli- Several severe complications can occur with soft tissue
tis after fist fight), Pasteurella multocida after cat or dog bites, infections. These include necrotizing fasciitis (usually due
Capnocytophaga canimorsus after dog bites, Aeromonas hydro- to a polymicrobial infection or a toxin-producing group A
phila after freshwater exposure or exposure to leeches, Vibrio Streptococcus) and pyomyositis (usually due to S aureus).
22 . H E A LT H C A R E A S S O C I AT E D I N F E C T I O N S 351
Staphylococcal toxic shock syndrome is caused by the
establishment or growth of a toxin-producing strain of S
aureus in a nonimmune person. Clinical scenarios associ-
ated with this syndrome include prolonged, continuous use
of tampons in young menstruating women, postoperative
and nonoperative wound infections, localized abscesses, and
S aureus pneumonia developing after influenza. It is a mul-
tisystem disease. Clinical criteria include fever, hypotension,
erythroderma (often leads to desquamation, particularly on
palms and soles), and involvement in 3 or more organ sys-
tems. Onset is acute; blood culture results are usually nega-
tive. The condition is caused by production of staphylococcal
toxin (toxic shock syndrome toxin 1, TSST-1). Treatment is
supportive; subsequent episodes are treated with a -lactam
Figure 22.5 Chaining of -Hemolytic Streptococcus in a Blood Culture
antibiotic, which decreases the frequency and severity of sub-
(Gram Stain). sequent attacks. The relapse rate may be as high as 30% to
40% (menstruation-related disease). The mortality rate is 5%
to 10%.
TOX I C S H O C K S Y N D RO M E
Toxic shock syndrome is caused by a toxin-producing strain
Group A streptococci produce many disease-causing exotox- of S aureus in a nonimmune person.
ins. Scarlet fever may develop in persons with no previous
immunity to erythrogenic toxin. Production of hyaluronidase Toxic shock syndrome is a multisystem disease:
causes the rapidly advancing margins characteristic of cellulitis fever, hypotension, and erythroderma (often leads to
due to -hemolytic streptococci. Streptococcal exotoxin A is desquamation, particularly on palms and soles).
similar to the toxin produced by S aureus, which causes toxic The onset of toxic shock syndrome is acute; results of
shock syndrome. blood culture are usually negative.
Streptococcal toxic shock syndrome is similar to staphy-
lococcal toxic shock syndrome (see below). Patients have Toxic shock syndrome is caused by production of
invasive group A streptococcal infections with associated staphylococcal toxin (TSST-1).
hypotension and 2 of the following: renal impairment,
coagulopathy, liver impairment, adult respiratory distress
syndrome, rash (may desquamate), or soft tissue necrosis. S K I N A N D S O F T T I S S U E I N FEC T I O N D U E TO
Symptoms are caused by production of streptococcal toxin U N US UA L O RG A N I S M S
(pyrogenic exotoxin A). Most patients have skin or soft tis-
sue infection, are younger than 50 years, and are otherwise
Community-Acquired Methicillin-Resistant S aureus
healthy compared with patients with invasive group A strep-
(CA-MRSA)
tococcal infections without the streptococcal toxic shock CA-MRSA should be suspected 1) in patients with recurrent
syndrome. They may present only with severe limb pain furunculosis, 2) in patients with cellulitis who have a prior
without skin lesions. Most patients are bacteremic (in con- personal history or a family member or close contact with
trast to toxic shock syndrome due to S aureus). Treatment a case of CA-MRSA, and 3) in patients who fail to respond
includes early administration of antibiotics, supportive care, to antimicrobial coverage for methicillin-sensitive S aureus
and surgical dbridement if needed. The case-fatality rate (MSSA) and streptococci. Options for treatment in these
is 30%. Although there is no reported resistance to peni- cases include trimethoprim-sulfamethoxazole, clindamycin,
cillin, clindamycin plus high-dose penicillin G is the pre- or doxycycline with or without rifampin. The use of vancomy-
ferred regimen because clindamycin may suppress exotoxin cin, daptomycin, or linezolid should be strongly considered in
and M-protein production in addition to its activity against patients who fail to respond to initial therapy, who are quite
group A streptococci. In severe cases, consideration should ill at initial presentation, and in whom multidrug-resistant S
be given to the use of early intravenous immunoglobulin aureus is suspected.
therapy.
Vibrio vulnificus can cause a severe bullous soft tissue infec- Fever, pain, and swelling are frequent.
tion in patients with underlying cirrhosis or hemochromato- Synovial fluid is turbid; the leukocyte count generally
sis. Disease is usually acquired by the ingestion of raw oysters exceeds 40 109/L.
or through injury sustained in warm salt water. Chronic liver
disease predisposes to infection. After the abrupt onset of Blood culture results are often positive.
fever and hypotension, multiple hemorrhagic bullae develop. Drainage is essential.
Clinical syndromes associated with V vulnificus include bacter-
emia, gastroenteritis, and cellulitis. Even with prompt therapy,
mortality exceeds 30%. Bacteremia or cellulitis is treated with
tetracycline, cefotaxime, or ciprofloxacin. Vibrio vulnificus is VI R A L A RT H R IT I S
not uniformly susceptible to the aminoglycosides. Viral arthritis often presents as transient, self-limited polyar-
thritis. It may be caused by rubella (also may occur after vac-
Vibrio vulnificus infection is usually acquired by the cination), hepatitis B, mumps, coxsackievirus, adenovirus,
ingestion of raw oysters or through injury sustained in parvovirus B19, human immunodeficiency virus, Ross River
warm salt water. virus, and chikungunya virus infections in travelers. Parvovirus
Vibrio vulnificus may cause a severe bullous soft tissue can cause a chronic symmetric, small joint arthritis that mim-
infection, especially in persons with underlying cirrhosis or ics rheumatoid arthritis, especially in women.
hemochromatosis.
C H RO N I C MO N OA RT I CU L A R A RT H R IT I S
Tuberculosis and nontuberculous mycobacteria and fungi
B ONE AND JOINT INFECTIONS should be considered in patients presenting with insidious-on-
set arthritis and chronic arthritis. Exposure to fish tank or
brackish water should raise the possibility of Mycobacterium
AC U T E BAC T E R I A L A RT H R IT I S
marinum septic arthritis typically involving the small hand
( N O N G O N O C O C C A L)
joints. A history of travel to the southwestern United States
Acute bacterial arthritis is most commonly due to hematog- or being a gardener should raise the possibility of Coccidioides
enous seeding (usually in the setting of trauma, injection drug immitis and Sporothrix schenckii, respectively. In patients with
use, and hemodialysis) in a patient with underlying crystalline chronic monoarticular arthritis of the knee and a history of
or rheumatoid arthritis. The hip and knee joints are the 2 most tick exposure, positive serologic results, or erythema migrans,
commonly involved joints. These infections are commonly chronic Lyme arthritis should be considered.
due to S aureus (most common) and -hemolytic streptococci.
Salmonella infection may occur in patients with sickle cell dis-
O S T E O MY E L I T I S
ease. Gram-negative aerobic bacilli cause 20% of septic arthritis
cases; P aeruginosa infection is associated with injection drug Osteomyelitis can occur as a result of hematogenous seeding,
use. Clinical features include fever, joint pain, and swelling. contiguous spread of infection to bone from adjacent soft
22 . H E A LT H C A R E A S S O C I AT E D I N F E C T I O N S 353
tissues and joints, or direct inoculation of infection into the tissues, genitourinary tract, infective endocarditis, infected
bone as a result of trauma or surgery. intravenous sites, injection drug use, or respiratory tract infec-
Hematogenous osteomyelitis is usually monomicrobial, tion. The incidence is greatest among males, peaks in the fifth
whereas osteomyelitis due to contiguous spread or direct decade of life, and is increasing, particularly among the elderly.
inoculation is usually polymicrobial. Acute hematogenous Risk factors for spine infections include advanced age, immu-
osteomyelitis is more common in children, but it can occur nocompromise, diabetes, intravenous drug use, renal failure,
in adults in the setting of prolonged bacteremias, intravenous bacteremia, cancer, chronic corticosteroid use, intravascular
drug use, dialysis, and sickle cell disease. Staphylococcus aureus, devices, and recent instrumentation or spine surgery.
coagulase-negative staphylococci, and aerobic gram-negative The clinical presentation of vertebral osteomyelitis
bacilli are the most common organisms. In long bone involve- includes localized insidious pain and tenderness in the spine
ment, the acute onset of pain and fever is typical. In vertebral area in 90% of patients. Most commonly affected is the
infection, pain may be the sole feature. Compatible radio- lumbar or lumbosacral region; cervical disease may occur in
graphic changes and bone biopsy for culture and pathologic patients with head and neck infections or in injection drug
examination are used to establish the diagnosis. Results of users. Fever is present in less than half of cases. Because of the
blood culture may be positive. Specific parenteral antibiotic clinical uncertainty, a delay in diagnosis by weeks to months
therapy is used for 3 to 6 weeks on the basis of culture and occurs, which can lead to motor and sensory deficits in 15%
sensitivity test results. Dbridement is usually not necessary of patients. The erythrocyte sedimentation rate is increased in
unless a sequestrum is present. more than 90% of cases, and the leukocyte count is increased
in less than 50%.
Staphylococcus aureus is a common organism in acute Plain radiography may show vertebral end-plate irregular-
hematogenous osteomyelitis. ity 2 to 8 weeks after the onset of symptoms, but it is neither
sensitive nor specific. Gadolinium-enhanced magnetic reso-
Acute onset of pain and fever is typical. nance imaging is the most useful test for diagnosis because of
its high sensitivity (96%) and specificity (94%). In patients
Chronic, contiguous osteomyelitis more commonly occurs who cannot undergo magnetic resonance imaging, computed
in adults, particularly in the setting of traumatic wounds, vas- tomography or nuclear scanning may help establish the diag-
cular insufficiency, and diabetic foot ulcers. The infections nosis. The best nuclear study for imaging disk space infec-
are usually mixed, but S aureus is the single most commonly tions is technetium combined with gallium citrate scanning.
isolated organism. In the presence of foreign bodies (such as Computed tomography-guided percutaneous aspiration or
plate or screws), coagulase-negative staphylococci is often the biopsy is often used to identify the causative organism. If the
culprit. Local pain, tenderness, erythema, and draining sinuses initial result is negative, the test should be repeated before
are common. Fever is atypical unless there is concurrent cel- proceeding to an open biopsy procedure.
lulitis. Compatible radiographic changes (often vague) and Staphylococcus aureus and coagulase-negative staphylo-
bone biopsy for culture and pathologic examination are used cocci are the most common microorganisms cultured in ver-
to establish the diagnosis. Blood culture results are rarely posi- tebral osteomyelitis. Mycobacterium tuberculosis and Brucella
tive. Adequate dbridement, removal of dead space, soft tis- are common in regions endemic for these organisms. Most
sue coverage, and fixation of infected fractures are essential. patients can be managed conservatively with antimicrobials.
Specific parenteral antibiotic therapy is given for 4 to 6 weeks. Antibiotics should be given parenterally for a minimum of
If a foreign body is retained in patients with staphylococcal 4 to 6 weeks or longer if there is extensive vertebral destruc-
osteomyelitis, a rifampin-based therapy such as the combina- tion or undrained collections. Surgical interventions are lim-
tion of fluoroquinolones and rifampin is warranted. ited to patients with progressive neurologic deterioration,
spinal instability, progressive epidural abscess, or failed medi-
Staphylococcus aureus is the most common causative cal therapy.
organism in chronic osteomyelitis.
Coagulase-negative staphylococci are common pathogens
if a foreign body is present. S U M M A RY
Local pain, tenderness, erythema, and draining sinuses are Differential time to culture positivity (cultures of blood
common. drawn from the catheter are positive 2 hours before those
Antibiotic therapy is given for 46 weeks. from the peripheral site) or a catheter tip with growth >15
colony-forming units per milliliter suggests the catheter as
the source of bloodstream infection.
D I S K I T I S A N D VE RT E B R A L I N FEC T I O NS Vancomycin is the most reliably active drug for treating
serious infections caused by MRSA.
Infection of the intervertebral disk and the adjacent verte-
brae may occur with or without associated epidural or psoas Organisms most commonly causing community-acquired
abscesses. These infections most often arise from hematog- infection in adults are S pneumoniae, N meningitidis, L
enous dissemination of infection from the skin and soft monocytogenes, and H influenzae.
22 . H E A LT H C A R E A S S O C I AT E D I N F E C T I O N S 355
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PA RT V
R H E U M ATO L O GY
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23.
NONARTICULAR RHEUMATISM
Kevin G. Moder, MD
359
Box 23.1 1990 CLASSIFICATION CRITERIA FOR fibromyalgia treatment programs may benefit some patients.
FIBROMYALGIA Chronic pain management techniques may also be helpful for
patients with impaired life skills.
Widespread pain Several controlled trials have shown that the antidepressant
Above & below the waist agent duloxetine is efficacious for patients with fibromyalgia
Right & left sides of the body with or without depression. This agent seems to be effica-
Axial pain cious in female patients but less so in males with fibromyalgia.
Pain in at least 11 of 18 tender points (bilateral) Pregabalin, which is used for treatment of peripheral neuropa-
Occiput thy, has also been shown to be beneficial in some patients with
Low cervical area fibromyalgia. Pramipexole has been shown to be beneficial in
Trapezius a subset of patients with fibromyalgia.
Supraspinatus
Second rib In fibromyalgia, symptoms wax and wane.
Lateral epicondyle Several thereapeutic approaches, including medications,
Gluteus may provide symptomatic relief.
Greater trochanter
Knee
Symptoms present for at least 3 months
L OW B AC K PA I N
points at muscle attachment sites supports the diagnosis of One-third of all people older than 50 years have episodes of
fibromyalgia. No laboratory test confirms the diagnosis of acute low back pain. Chronic low back pain is the most com-
fibromyalgia. Laboratory tests are used to rule out other con- mon compensable work-related injury. The vast majority of
ditions and usually are unrevealing. Vitamin D levels have episodes of acute low back pain cannot be explained on a
been reported to be low in some patients with chronic pain structural basis. Only 3% of patients presenting with acute low
syndromes, including fibromyalgia. Response to vitamin D back pain have an identifiable cause that is not apparent after
replacement, however, is variable. Radiographs of specific, the initial interview and physical examination. More than 90%
particularly problematic, joints may be helpful for identifying of patients have resolution with or without the help of a medi-
coexisting conditions. For example, patients with fibromyalgia cal practitioner within the first 6 weeks after symptoms occur.
may also have degenerative joint disease of a particular joint
that contributes to their pain. If sleep disturbance is promi- Only 3% of patients presenting with acute low back pain
nent, a sleep study may be helpful. have an identifiable cause that is not apparent after the
initial interview and physical examination.
Chronic widespread musculoskeletal pain not explained
by physical findings of a rheumatic disease supports the More than 90% of episodes of acute low back pain resolve
diagnosis of fibromyalgia. with or without the help of a medical practitioner within
the first 6 weeks after symptoms occur.
No laboratory test confirms the diagnosis of fibromyalgia.
D I AG N O S I S
NAT U R A L H I S TO RY
During the initial evaluation of acute low back pain, it is
Fibromyalgia is a chronic waxing and waning condition. important to look for signs, symptoms, and findings sugges-
Patients have periods of pain and dysfunction alternating with tive of radiculopathy, myelopathy, or cauda equina. In the
periods of feeling reasonably well. Over a period of years, a absence of evidence for acute spinal cord compromise, spinal
patients symptoms and concerns can shift considerably from infection, or neoplastic involvement, immediate pursuit of a
musculoskeletal concerns to fatigue or other associated symp- cause for the acute back pain is usually unrevealing. Objective
toms. There is no increased physical disability in patients who leg weakness or bladder or bowel dysfunction is an indica-
have had fibromyalgia for longer periods in comparison with tion for more extensive examination and possible surgical
those for whom the diagnosis is recent. decompression. Involuntary weight loss and pain that increase
with recumbency suggest a neoplastic or infectious process.
T R E AT M E N T
Pain that worsens with coughing, straining, or sneezing sug-
gests irritation of the dura mater. Radiating pain, weakness,
Treatment includes reassurance and education, address- or numbness in an extremity implicates irritation of a spinal
ing sleep problems, and establishing an exercise program. nerve root.
Nonsteroidal anti-inflammatory drugs, simple analgesics, Exertional calf or thigh cramping but normal periph-
and medications to help with sleep (such as tricyclic anti- eral pulses suggest the pseudoclaudication of spinal stenosis.
depressants) have a role in some patients. Comprehensive Pseudoclaudication symptoms improve with leaning forward
360 R H E U M ATO L O GY
on a shopping cart while walking or with sitting (not standing of acetaminophen, nonsteroidal anti-inflammatory drugs, and
still). Typically, pseudoclaudication also begins in the back or muscle relaxants such as cyclobenzaprine. Physical therapy
buttock and gradually radiates down the thigh into the leg. measures include local heat and ice massage. Pelvic traction
This is in contrast to claudication, which usually begins dis- and transcutaneous electrical nerve stimulation add little to
tally and then gradually spreads proximally. the management of acute nonspecific low back pain. Epidural
Referred pain from the hips, abdomen, and pelvis can glucocorticosteroid injections are best suited to acute disk
sometimes be interpreted as low back pain. An insidious onset herniation, although their role is controversial. Injections into
with prominent morning stiffness suggests an inflammatory the facets are helpful occasionally, particularly if the patient
axial arthropathy. describes a locking or catching as part of the pain syndrome.
Objective leg weakness or bladder or bowel dysfunction In 90% of patients, acute low back pain (local or sciatic
in patients with low back pain is an indication for more presentations) remits within 6 weeks.
extensive examination.
Pelvic traction and transcutaneous electrical nerve
Involuntary weight loss and pain that interferes with sleep stimulation add little to the management of acute
suggest a neoplastic or infectious process. nonspecific low back pain.
Exertional calf or thigh cramping but normal peripheral
pulses suggest pseudoclaudication.
BUR SITIS
An insidious onset with prominent morning stiffness
suggests an inflammatory axial arthropathy. A bursa is a fluid-filled sac lined with a membrane. Bursae are
present in the areas where tendons and muscles move over
In the absence of specific historical or physical examina- bony prominences. Additional bursae can form in response
tion findings, laboratory or plain radiographic findings often to irritative stimuli. Trauma or overuse, crystalline disease,
are unrevealing. The radiographic findings of spondylosis, disk chronic inflammatory arthritis, and infection cause bursitis.
degeneration, facet osteoarthritis, transitional lumbosacral Common locations of bursitis include the olecranon and the
segments, Schmorl nodes, spina bifida occulta, or mild sco- greater trochanter.
liosis are often incidental findings not relevant to a patients Treatment of aseptic bursitis may involve immobilization,
complaints of acute back pain. Bone scanning, electromyog- ice compresses, nonsteroidal anti-inflammatory drugs, bursal
raphy, computed tomography, or magnetic resonance imaging aspiration, corticosteroid injections, and, occasionally, physi-
are usually not necessary to evaluate acute low back pain. The cal therapy.
indications for spinal radiography in patients with acute low
back pain are listed in Box 23.2. Always consider infection or crystalline disease in the
differential diagnosis of acute bursitis.
T R E AT M E N T
Septic bursitis may result from puncture wounds or cel-
The treatment of acute nonspecific low back pain begins with lulitis, or it can occur after a local injection. In many cases
reassuring the patient, because 90% of all patients with acute of septic bursitis, no clear portal of entry for infection is
low back pain have considerable improvement in 6 weeks. apparent. The organisms frequently responsible for infec-
Temporary modification of activities may lessen symptoms. tion are staphylococci and streptococci. Patients with septic
Bed rest should never be prescribed for more than 3 days to treat superficial bursitis present with localized pain and swelling.
acute nonspecific low back pain. Longer bed rest has not been Warmth about the area of the superficial bursa should raise
shown to be beneficial and may prolong disability. Short-term the possibility of a septic bursa. If there is doubt, the bursa
use of narcotic analgesics or tramadol can supplement the use should be aspirated with strict aseptic technique. The needle
should enter from the side through uninvolved skinnot at
the point of maximal fluctuanceto avoid creating a chronic
Box 23.2 INDICATIONS FOR SPINAL RADIOGRAPHY IN
draining fistula.
PATIENTS WITH ACUTE LOW BACK PAIN
When infection is suspected, empiric treatment with
antistaphylococcal and antistreptococcal antibiotics should
First episode of acute back pain is after age 50 y
be given pending the microbiologic results. Gram stains are
History of back disease
positive in only 40% to 60% of patients. The number of leu-
History of back surgery
kocytes in infected bursal fluid can be low compared with that
History of neoplasm
in infected joint fluid. This difference may be due to the mod-
Acute history of direct trauma to the back
est blood supply of the bursae compared with that of joints.
Fever
Patients with more severe infections or with associated cel-
Weight loss
lulitis frequently do not respond to outpatient management.
Severe pain unrelieved in any position
Repeated aspirations or even surgical dbridement is neces-
Neurologic symptoms or signs
sary in some cases.
23. N O N A RT I C U L A R R H E U M AT I S M 361
Septic bursitis frequently occurs without evidence of a Box 23.3 SYSTEMIC ILLNESSES PRESENTING WITH A
portal of entry. POLYMYALGIA-LIKE SYNDROME
Bursal warmth is the best predictor of infection. RHEUMATIC SYNDROMES OTHER SYSTEMIC ILLNESSES
Gram stains are positive in only 40%-60% of patients. Systemic vasculitis Paraneoplastic syndromes
Myositis Systemic amyloidosis
The number of leukocytes in infected bursal fluid can be Systemic lupus erythematosus Infectious endocarditis
low. Seronegative rheumatoid Hyperthyroidism
arthritis Hypothyroidism
Patients with more severe infections should be Polyarticular osteoarthritis Hyperparathyroidism
hospitalized. Fibromyalgia Osteomalacia
Remitting seronegative, Depression
symmetric synovitis &
peripheral edema
P O LY M YA L G I A R H E U M AT I C A
362 R H E U M ATO L O GY
prednisone (10-20 mg/day). Sometimes, split-dose prednisone Box 23.4 COMMON CLINICAL FEATURES IN PATIENTS
(5 mg 3 times per day) is more effective than the same single WITH VASCULITIS
daily dose (15 mg once per day). Patients should be followed
clinically, and usually the erythrocyte sedimentation rate Constitutional features
should be measured monthly to monitor for disease activity. Fever
Polymyalgia rheumatica is thought to be a self-limited disease, Weight loss
but relapses can occur. Prednisone is discontinued in more Fatigue
than half of patients within 2 years. A minority of patients may Anorexia
be at risk of later appearance of giant cell arteritis. Patients with Cutaneous manifestations
polymyalgia rheumatica that does not respond promptly to Palpable purpura
corticosteroids or those who have severe symptoms suggestive Necrotic ulcers
of giant cell arteritis (head, jaw, and arm claudication; visual Livedo reticularis
loss; significantly different blood pressures for the right and Urticarial lesions
left arms) should have a temporal artery biopsy. Occasionally, Digital infarcts
a patient presents with polymyalgia rheumatica and over time Musculoskeletal features
the condition evolves into true rheumatoid arthritis. Arthralgia
Arthritis
All patients with polymyalgia rheumatica should have a Myalgia
considerable response within 4 days of treatment with Claudication
prednisone. Neurologic features
Polymyalgia rheumatica is usually a self-limited disease, Peripheral neuropathy
although relapses occur, and a minority of patients may be Mononeuritis multiplex
at risk of late appearance of giant cell arteritis. Cerebrovascular accidents
Headache
Other
VA S C U L I T I C SY N D R O M E S Cough
Hemoptysis
Vasculitis, or angiitis, is an inflammatory disease of blood ves- Edema
sels. Damage to the vessel wall and stenosis or occlusion of the Hypertension
vessel lumen by thrombosis and progressive intimal prolifera- Abdominal pain
tion of the vessel result in the clinical manifestations of the
illness. The distribution of the vascular lesions and the size older than 50 years. Three-quarters of patients are women.
of the blood vessels involved vary considerably in different The prevalence exceeds 223 cases per 100,000 persons older
vasculitic syndromes and in different patients with the same than 50 years. Polymyalgia rheumatica symptoms may develop
syndrome. Vasculitis can be transient, chronic, self-limited, in 40% to 50% of all patients with giant cell arteritis. Up to
or progressive. It can be the primary abnormality or due to 15% of patients with polymyalgia rheumatica have temporal
another systemic process. Histopathologic classification does artery biopsy findings positive for giant cell arteritis. There
not distinguish local from systemic illness or secondary from is considerable morbidity with this disease; however, the
primary insult. The key clinical features suggestive of vasculitis
are listed in Box 23.4. Vasculitis look-alikes, or simulators,
are listed in Box 23.5. These diseases and conditions should be Box 23.5 SYNDROMES THAT MIMIC VASCULITIS
considered whenever a patients condition suggests vasculitis.
Common test abnormalities found in patients with vasculitis
Cardiac myxoma with embolization
are listed in Box 23.6. The ability to recognize characteristic
Infective endocarditis
clinical patterns of involvement is very helpful for making the
Thrombotic thrombocytopenic purpura
diagnosis of systemic necrotizing vasculitis.
Atheroembolism: cholesterol or calcium emboli
Ergotism
Vasculitic symptoms reflect the nonspecific systemic Pseudoxanthoma elasticum
features of inflammation (constitutional features) and the Ehlers-Danlos type 4
ischemic consequences of vascular occlusion. Neurovasculopathy secondary to antiphospholipid syndrome
Arterial coarctation or dysplasia
Infectious angiitis
S P EC I F I C VA S C U L IT I C S Y N D RO M E S Lyme disease
Rickettsial infection
Giant Cell Arteritis
HIV infection
Giant cell arteritis, also known as temporal arteritis, pre-
Abbreviation: HIV, human immunodeficiency virus.
dominantly affects persons of northern European ancestry
23. N O N A RT I C U L A R R H E U M AT I S M 363
Box 23.6 LABORATORY AND RADIOGRAPHIC Box 23.7 CLASSIC CLINICAL FEATURES OF GIANT
ABNORMALITIES IN VASCULITIS CELL ARTERITIS
rate of blindness is declining. Affected patients are at higher peripheral artery involvement. Patients with large peripheral
subsequent risk of aortic aneurysms. The mortality rate for artery involvement do not differ from those with more classic
patients with giant cell arteritis is similar to that for the gen- giant cell arteritis, either histologically or with regard to labo-
eral population. ratory findings. Patients who have had giant cell arteritis are at
increased risk for the development of aneurysms.
Giant cell arteritis is most common in persons of northern
European ancestry. A patient with giant cell arteritis typically is 60 years
old and presents with temporal headache, polymyalgia
Polymyalgia rheumatica may develop in 40%-50% of
rheumatica-like symptoms, fatigue, and fever. The
patients with giant cell arteritis.
sedimentation rate is markedly increased. Physical
Up to 15% of patients with polymyalgia rheumatica have examination shows scalp tenderness.
temporal artery biopsy findings positive for giant cell arteritis.
Blindness occurs in <15% of untreated patients.
Pathology Diagnosis
Giant cell arteritis involves the primary and secondary The necessary length of an adequate temporal artery
branches of the aorta in a segmental or patchy fashion. However, biopsy specimen is controversial. However, because of patchy
any artery, and occasionally veins, can be affected. It is unusual involvement and skin lesions, a length of at least 1 cm is rec-
for intracranial arteries to be involved. Histopathologically, ommended. In 15% of patients, the biopsy is positive on the
all layers of the vessel wall are extensively disrupted, with inti- opposite side if that on the initial side is negative. Typical labo-
mal thickening and a prominent mononuclear and histiocytic ratory abnormalities in acute active giant cell arteritis include a
infiltrate. Multinucleated giant cells infiltrate the vessel wall in markedly increased erythrocyte sedimentation rate, moderate
50% of cases. Fragmentation and disintegration of the internal normochromic anemia, and thrombocytosis. A mild increase
elastic membrane, the other characteristic features, are closely in liver enzyme values, most typically alkaline phosphatase,
associated with the accumulation of giant cells and vascular occurs in one-third of patients because of granulomatous hep-
occlusive symptoms. atitis. The erythrocyte sedimentation rate is rarely normal in
patients with active giant cell arteritis.
Giant cell arteritis affects primary and secondary branches
of the aorta in a segmental or patchy fashion. The temporal artery biopsy specimen needed to test
for giant cell arteritis should be at least 1 cm long to
compensate for patchy involvement.
Clinical Features In 15% of patients with giant cell arteritis, the biopsy is
Early clinical features of giant cell arteritis include temporal positive on the opposite side if that on the initial side is
headache, polymyalgia rheumatica symptoms, fatigue, and fever. negative.
The classic features of this disease are listed in Box 23.7. Arteritis
of the branches of the ophthalmic or posterior ciliary arteries Typical laboratory abnormalities in giant cell arteritis
causes ischemia of the optic nerve (ischemic optic neuritis) and are markedly increased erythrocyte sedimentation rate,
blindness. Less often, retinal arterioles are occluded. Blindness moderate normochromic anemia, and thrombocytosis.
occurs in fewer than 15% of untreated patients. Large peripheral
artery involvement in giant cell arteritis occurs in about 10% of Treatment
patients. Extremity claudication, Raynaud phenomenon, aortic Treatment is initiated with corticosteroids when the
dissection, decreased pulses, and vascular bruits suggest large diagnosis of giant cell arteritis is considered and the biopsy
364 R H E U M ATO L O GY
High-risk patients Low- and intermediate-risk patients
Aortic insufficiency murmur No aortic insufficiency murmur
PMR in combination with No PMR in combination with
ESR >100 mm in 1 h ESR >100 mm in 1 h
At least 2 of the following: Not more than 1 of the following:
Hypertension Hypertension
Hyperlipidemia Hyperlipidemia
PMR PMR
Coronary artery disease Coronary artery disease
is requested. A temporal artery biopsy specimen remains been identified, but methotrexate or azathioprine has been
positive for disease even after several weeks of corticoster- used in some patients. The diagnosis of giant cell arteritis does
oid treatment. Initial treatment includes prednisone, typi- not influence mortality rates. Relapse may occur in a third of
cally 40 to 60 mg/day. A higher dose of corticosteroids can patients, and a thoracic or abdominal aneurysm develops in a
be given parenterally in cases of visual or life-threatening third. Screening guidelines for aortic aneurysms are shown in
symptoms. A recent study suggested parenteral corticoster- Figure 23.1.
oids initially may lessen the total duration and cumulative
dose needed. Most symptoms of giant cell arteritis begin to Giant cell arteritis typically has a self-limited course over
respond within 24 hours after corticosteroid therapy is ini- about 2 years, although relapses and late consequences,
tiated. Visual changes that are present for more than a few including aortic aneurysms, occur.
hours are often irreversible. Alternate-day administration of
corticosteroids does not control symptoms in at least half of Patients with a history of giant cell arteritis are at increased
patients. risk for the development of aneurysms.
23. N O N A RT I C U L A R R H E U M AT I S M 365
Box 23.8 CLASSIFICATION CRITERIA FOR TAKAYASU treatment is indicated in resistant cases. On average, patients
ARTERITIS a receive corticosteroids for about 2 years. Late stenotic compli-
cations are amenable to vascular operation and bypass grafting.
Age at disease onset 40 y Survival is more than 90% at 10 years. Congestive heart failure
Claudication of upper extremities from previous coronary artery involvement and cerebrovascu-
Decreased brachial artery pulse lar accidents are major causes of mortality.
Blood pressure difference between arms 10 mm Hg
Aortic or subclavian bruit Survival in patients with Takayasu arteritis is >90% at 10
Arteriographic abnormality of aorta, primary branches, or large years.
arteries in the upper or lower extremities
a
If at least 3 of the 6 criteria are present, the sensitivity for diagnosis is 90% and Classic Polyarteritis Nodosa and Microscopic
the specificity is 98%.
Polyangiitis
Systemic necrotizing vasculitis occurs alone or in association
Classification criteria for Takyasu arteritis are listed in with several diseases (secondary). When it occurs as a primary
Box 23.8. vasculitis, it is most commonly a small vessel antineutrophil
cytoplasmic antibody (ANCA)associated disease of Wegener
Among patients with Takayasu arteritis, most are female granulomatosis or microscopic polyangiitis. Medium-vessel
and between the ages of 15 and 40 years. polyarteritis nodosa, frequently associated with hepatitis B,
The aorta and its primary branches are most commonly is far less common. A secondary necrotizing vasculitis can
affected. occur in association with rheumatoid arthritis, systemic lupus
erythematosus, other connective tissue diseases, cryoglobu-
linemia, hepatitis C infection, hairy cell leukemia, and other
Clinical and Laboratory Features malignant conditions.
The constitutional features of fever, weight loss, fatigue, and
arthralgia can precede symptoms of ischemia to the brain or claudi- Systemic necrotizing vasculitis occurs alone or in
cation of the extremities. Renovascular hypertension, pulmonary association with several diseases.
hypertension, and coronary artery insufficiency can complicate
Takayasu arteritis. Cutaneous vasculitis, erythema nodosum, and ANCA-associated vasculitis disorders of Wegener
synovitis occasionally occur in cases of active Takayasu arteritis. granulomatosis and microscopic polyangiitis are more
Compromise of the cerebral vasculature can lead to dizziness, common than classic polyarteritis nodosa.
blurry or fading vision, syncope, and, occasionally, stroke. Physical
examination findings confirm vascular bruits, absence of periph-
eral pulses, and, occasionally, fever. When the disease is active, Pathology
results of laboratory studies usually show increased erythrocyte These diseases are characterized by transmural inflamma-
sedimentation rate, normochromic anemia, and thrombocytosis. tion and necrosis of blood vessels. Classic polyarteritis nodosa
However, in some cases of active disease, the erythrocyte sedi- affects medium-sized muscular arteries. ANCA-associated
mentation rate is normal. The diagnosis can be confirmed with vasculitis affects arterioles, venules, and capillaries. The size of
conventional angiography, although magnetic resonance angiog- the affected vessels plays a large part in determining the clini-
raphy may become the imaging method of choice. cal manifestations of the syndromes.
Renovascular hypertension, pulmonary hypertension, and Systemic vasculitis may affect a spectrum of vessel sizes.
coronary artery insufficiency can complicate Takayasu
arteritis.
Clinical Features
Patients with active Takayasu arteritis can have a normal Systemic vasculitis usually is associated with prominent
erythrocyte sedimentation rate, although this finding is rare. constitutional features, including fever, fatigue, weight loss,
A patient with Takayasu arteritis typically is young and and, occasionally, myalgia or arthralgia, along with manifesta-
presents with fever, weight loss, fatigue, and arthralgia. tions of multisystem organ involvement. Virtually any organ
Physical examination shows carotid bruits and absence of can be affected eventually. Rarely, vasculitis is limited to a sin-
peripheral pulses. On laboratory testing, there is a mild gle organ or found incidentally associated with cancer at the
normochromic anemia, and the erythrocyte sedimentation time of operation and cured by surgical removal. Other cases
rate is increased. are limited to isolated involvement of the skin (cutaneous vas-
culitis) or peripheral nerves.
Classic polyarteritis nodosa is a necrotizing vasculitis of
Treatment and Outcome small and medium-sized arteries and is associated with vascu-
Corticosteroid therapy alone is usually adequate for con- lar nephropathy (usually without glomerulonephritis), caus-
trolling the inflammation. Methotrexate or cyclophosphamide ing multiple renal infarctions, hypertension, and renal failure.
366 R H E U M ATO L O GY
Hypertension develops as a result of angiographically demon-
strable renal artery compromise or, less commonly, glomerular
involvement. Lung involvement is very uncommon. Patients
with classic polyarteritis nodosa are usually ANCA-negative.
Microscopic polyangiitis is distinguished from polyar-
teritis nodosa as a necrotizing vasculitis that affects capillar-
ies, venules, and arterioles and most frequently presents with
pauci-immune and sometimes rapidly progressive necrotiz-
ing glomerulonephritis. Proteinuria is common, and, rarely,
a nephritic syndrome may develop. There is an active urinary
sediment, with red blood cells and red cell casts characteristic
of glomerular involvement. Renal insufficiency is frequently
noted at presentation, and glomerulonephritis causes oliguric
renal failure in one-third of all patients. Renal angiography in
microscopic polyangiitis is usually normal. Hypertension is
uncommon. Lung involvement, including pulmonary capil-
laritis and hemorrhage, eventually may affect up to a third of
patients with microscopic polyangiitis.
Systemic vasculitis may be a manifestation or complica-
tion of other diseases. This secondary vasculitis complicates
hepatitis C infection, rheumatoid arthritis, Sjgren syndrome, Figure 23.2 Visceral Polyarteritis Nodosa. Angiography shows the
mixed cryoglobulinemia, hairy cell leukemia, myelodysplastic classic features of smooth tapers followed by normal or dilated vessels.
Note the large saccular aneurysm in the hepatic artery. (Adapted from
syndrome, and other hematologic malignancies. Some forms Audiovisual Aids Subcommittee of the Education Committee of the
of secondary vasculitis have more favorable clinical presenta- American College of Rheumatology. Syllabus: revised clinical slide
tions. For example, systemic rheumatoid vasculitis most com- collection on the rheumatic diseases and 1985, 1988, and 1989 slide
monly manifests with constitutional symptoms, skin lesions, supplements. Atlanta [GA]: American College of Rheumatology. Used
and neuropathy. It rarely causes a necrotizing glomerulone- with permission.)
phritis or pulmonary hemorrhage.
should be of accessible symptomatic tissue. If medium-sized
Systemic vasculitis is associated with prominent
vessel polyarteritis nodosa is suspected, visceral angiography,
constitutional features, including fever, fatigue, weight
including views of the renal and mesenteric arteries, shows sac-
loss, and, occasionally, myalgia or arthralgia, along with
cular or fusiform aneurysm formation coupled with smooth,
manifestations of multisystem organ involvement.
tapered stenosis alternating with normal or dilated blood ves-
Secondary vasculitis may be a complication of other sels (Figure 23.2). In some cases, other imaging methods such
diseases. as ultrasonography and magnetic resonance angiography may
be helpful and less invasive than conventional angiography.
Classic polyarteritis nodosa usually does not affect the
lungs.
Microscopic polyangiitis often presents with positive
myeloperoxidase-specific p-ANCA.
Diagnosis Hepatitis B infection occurs in a small proportion of
Abnormal laboratory findings include normocytic patients with ANCA-negative (classic) polyarteritis
anemia, increased erythrocyte sedimentation rate, and nodosa.
thrombocytosis. Microscopic polyangiitis presents with a
Confirmatory diagnostic tests include angiography or
myeloperoxidase-specific perinuclear (p-) ANCA in 90% of
biopsy of involved tissue showing vasculitis.
cases. Hypocomplementemia is not common in patients with
active vasculitis. However, low complement may be evident if Visceral angiography often shows saccular or fusiform
immune complexes such as cryoglobulins are part of the patho- aneurysm formation coupled with smooth, tapered stenosis
genesis of secondary vasculitis or if vasculitis occurs in associa- in patients with classic polyarteritis nodosa.
tion with systemic lupus erythematosus. Hepatitis B infection
occurs in a small proportion of patients with ANCA-negative
(classic) polyarteritis nodosa and should always be sought, Treatment
because treatment is directed against the infection. Hepatitis The cornerstone of treatment is early diagnosis and corti-
C is associated with mixed cryoglobulinemia, and vasculitis costeroid therapy. Cytotoxic or antimetabolite drugs such as
may occur in patients with cryoglobulinemia. cyclophosphamide, methotrexate, mycophenolate mofetil,
Evaluation should document the extent and severity of and azathioprine are often used in combination with cortico-
the condition. The confirmatory test typically is angiography steroids. The choice of the second agent is usually determined
or biopsy of involved tissue showing vasculitis. The biopsy by the severity and type of organ involvement and patient
23. N O N A RT I C U L A R R H E U M AT I S M 367
Box 23.9 FIVE FACTORS ASSOCIATED WITH 70% for microscopic polyangiitis and about 80% for classic
INCREASED MORTALITY IN POLYARTERITIS NODOSA polyarteritis nodosa.
1. Proteinuria >1 g/d In the first year after diagnosis, deaths are related to the
2. Azotemia extent of disease activity, particularly gastrointestinal tract
3. Cardiomyopathy ischemia and renal insufficiency.
4. Gastrointestinal involvement Complications from treatment affect long-term mortality.
5. Central nervous system involvement
A patient with systemic vasculitis typically presents
with fever, fatigue, weight loss, arthralgia, mononeuritis
comorbid conditions. Five factors have been identified that multiplex, and renal failure. Laboratory testing shows
are associated with increased mortality in patients with poly- increased sedimentation rate and anemia.
arteritis nodosa (Box 23.9). In patients with 1 or more of
these factors, strong consideration should be given to using
cyclophosphamide. Churg-Strauss Vasculitis
A new treatment that has shown promise in some patients
with systemic vasculitis, especially those with Wegener gran- Churg-Strauss vasculitis, or Churg-Strauss syndrome, is simi-
ulomatosis, is rituximab. When a patients condition dete- lar to microscopic angiitis and Wegener granulomatosis in that
riorates in the face of potent treatment, consider possible it involves small vessels and may be associated with ANCA
progression of disease, superimposed infection, or noninflam- antibodies. The median age at onset is about 38 years (range,
matory, proliferative, occlusive vasculopathy. 1569 years). Churg-Strauss vasculitis is defined by 1) a his-
tory of, or current symptoms of, asthma, 2) peripheral eosino-
Cyclophosphamide, mycophenolate mofetil, methotrexate, philia (>1.5109 eosinophils/L), and 3) systemic vasculitis of
and azathioprine are often used in conjuction with at least 2 extrapulmonary organs. There is a slight male pre-
corticosteroids for the treatment of systemic vasculitis. dominance. The histopathologic features of the disease include
eosinophilic extravascular granulomas and granulomatous or
Rituximab is a new therapy that has shown promise in nongranulomatous small vessel necrotizing vasculitis. It typi-
some cases of ANCA-associated vasculitis. cally involves the small arteries, veins, arterioles, and venules.
Abbreviations: ANCA, antineutrophil cytoplasmic antibody; MPO, myeloperox- Churg-Strauss syndrome involves a prodrome of allergic
ide; p-ANCA, perinuclear ANCA. rhinitis, nasal polyposis, or asthma.
368 R H E U M ATO L O GY
Peripheral blood and tissue eosinophilia develops. only the upper respiratory tract or kidneys. The clinical fea-
tures of this disease are summarized by the mnemonic ELKS:
Transient, patchy pulmonary infiltrates, extravascular
involvement of ear/nose/throat, lung, kidney, and skin. Lung
necrotizing granulomata of the skin, and mononeuritis
involvement most commonly includes thick-walled, centrally
multiplex can complicate Churg-Strauss syndrome.
cavitating pulmonary nodules. Alveolitis and pulmonary
hemorrhage occur in up to 20% of patients. Biopsy in patients
with renal involvement usually does not show changes that
Treatment and Outcome
are specific for Wegener granulomatosis. Renal biopsy often
The 1-year survival with treated Churg-Strauss syndrome
shows focal segmental necrotizing glomerulonephritis and,
is similar to that with microscopic polyangiitis. There is more
occasionally, granulomatous vasculitis. Skin involvement
cardiac involvement but fewer renal deaths than in polyarteri-
may include urticaria, petechiae, papules, vesicles, ulcers, pyo-
tis nodosa. Treatment includes corticosteroids with or with-
derma, and livedo reticularis. Inflammatory arthritis is usually
out the addition of cytotoxic agents. The eosinophilia resolves
oligoarticular and transient, occurring early in the clinical
with treatment.
presentation. Central nervous system involvement includes
distal sensory neuropathy, mononeuritis multiplex, and cra-
In Churg-Strauss syndrome, there is more cardiac
nial nerve palsies. Conjunctivitis, uveitis, and proptosis are
involvement but fewer renal deaths than in polyarteritis
not unusual. Neurosensory hearing loss has been described
nodosa.
together with serous otitis and inner ear vasculitis. Wegener
A patient with Churg-Strauss syndrome typically presents granulomatosisassociated subglottic tracheal stenosis due to
with a history of bronchial asthma with recent worsening chondritis should be distinguished from primary polychon-
of pulmonary symptoms and development of mononeuritis dritis. On laboratory testing, cytoplasmic (c-) ANCA test
multiplex. There is a history of nasal polyposis. Palpable with antibodies directed against PR3 is positive.
purpura is noted on physical evaluation. On laboratory
testing, the eosinophil count is markedly increased. In a typical case of Wegener granulomatosis, a 50-year-old
patient presents with the triad of upper and lower
respiratory tract necrotizing granulomatous inflammation
Buerger Disease and focal segmental necrotizing glomerulonephritis. On
Buerger disease, or thromboangiitis obliterans, occurs almost laboratory testing, the c-ANCA test is positive.
exclusively in young adult smokers. There is a male predomi- The clinical features of Wegener granulomatosis are
nance. Patients usually present with ischemic injury to fingers summarized by the mnemonic ELKS: involvement of ear/
or, less commonly, toes. Buerger disease affects the small and nose/throat, lung, kidney, and skin.
medium-sized arteries and veins of the extremities. Acute
vasculitis in Buerger disease is accompanied by characteristic Alveolitis and pulmonary hemorrhage occur in up to 20%
intraluminal thrombus that contains microabscesses. Usually, of patients.
the disease is arrested when smoking is stopped. In contrast to Central nervous system involvement includes distal
other forms of vasculitis, Buerger disease is best thought of as sensory neuropathy, mononeuritis multiplex, and cranial
a vasculopathy in that it does not require immunosuppressive nerve palsies.
therapy.
23. N O N A RT I C U L A R R H E U M AT I S M 369
The diagnosis of Wegener granulomatosis is established Cyclophosphamide has revolutionized the treatment of
with a positive result of c-ANCA directed against Wegener granulomatosis and dramatically altered the
proteinase 3 and granulomatous inflammation on natural history.
biopsy.
Corticosteroids are useful initially, and the dose can be
tapered quickly after the disease is controlled.
ANCA Rituximab is a potential new therapy for Wegener
c-ANCA is directed against proteinase 3, a serine protease granulomatosis and other ANCA-associated vasculitides.
from azurophilic granules. c-ANCA occurs in more than
90% of active cases of generalized Wegener granulomatosis. In recent years there has been an initiative to change the
Occasionally, it is found in idiopathic crescentic glomerulone- nomenclature and no longer use the term Wegener granuloma-
phritis, microscopic polyarteritis nodosa, and Churg-Strauss tosis. There is a proposal to instead use the term granulomatosis
syndrome. The antibody titer tends to correlate with disease with polyangitis. This would be one type of vasculitis under the
activity in an individual patient. more general heading of ANCA-associated vasculitis.
p-ANCA is directed against myeloperoxidase and
other neutrophil cytoplasmic constituents. p-ANCA
(anti-myeloperoxidasespecific) is found in idiopathic cres- Small Vessel Vasculitis and Cutaneous Vasculitis
centic glomerulonephritis, microscopic polyarteritis nodosa,
Churg-Strauss syndrome, in occasional cases of Wegener gran- Clinical Features
ulomatosis, and other connective tissue diseases. Therefore, a Small vessel vasculitis occurs by itself or complicates many
positive p-ANCA result with antibodies directed against infectious, neoplastic, and connective tissue diseases. The
myeloperoxidase can be suggestive of vasculitis. However, most common cause of isolated cutaneous vasculitis is drugs.
p-ANCA directed against other antigens is much less spe- It manifests with urticaria, palpable purpura, livedo reticularis,
cific. It can occur in patients with inflammatory bowel disease, or skin ulceration. Small vessel vasculitis occurs with many ill-
autoimmune liver disease, other connective tissue diseases, nesses; a partial listing is given in Box 23.10.
malignancies, and even drug-induced syndromes.
The most common cause of isolated cutaneous vasculitis is
Proteinase 3, c-ANCA occurs in >90% of active cases of a medication reaction.
Wegener granulomatosis. Isolated cutaneous vasculitis manifests with urticaria,
Nonmyeloperoxidase p-ANCA is found in many palpable purpura, livedo reticularis, or skin ulceration.
different conditions.
370 R H E U M ATO L O GY
It can complicate most types of primary and secondary Cryoglobulinemia
systemic vasculitis.
Cryoglobulins are immunoglobulins that reversibly precipi-
Histopathology tate at reduced temperatures. They are grouped into 2 major
A neutrophilic- or (uncommonly) lymphocytic-predom- categories. Type I cryoglobulins are aggregates of a single
inant infiltrate surrounds small arteries, veins, arterioles, or monoclonal immunoglobulin and generally are associated
venules. The histopathologic picture called leukocytoclastic with multiple myeloma, Waldenstrm macroglobulinemia,
vasculitis includes immune complexes deposited in vessel and lymphomas. They usually are found in high concentra-
walls, along with fibrin deposition, endothelial cell swelling tions (15 g/dL). Patients with type I cryoglobulins are often
and necrosis, and a polymorphonuclear leukocytoclasis with asymptomatic. Symptoms of type I cryoglobulinemia are
scattering of nuclear fragment or nuclear dust. A classic clinical usually related to increased viscosity and include headaches,
correlate of leukocytoclastic vasculitis is palpable purpura. This visual disturbances, nosebleeds, Raynaud phenomenon, and
is a pathologic diagnosis and not a specific clinical condition. ischemic ulceration from occlusion of arterioles and venules
by precipitated immune complexes. Vasculitis is rare.
A classic clinical correlate of leukocytoclastic vasculitis is
Type I cryoglobulins are aggregates of a single monoclonal
palpable purpura.
immunoglobulin.
Diagnosis Patients with type I cryoglobulins are often asymptomatic.
The clinician must interpret small vessel or cutaneous vas-
culitis as a clinical finding and not a diagnosis. These various Symptoms of type I cryoglobulinemia are usually related to
conditions are distinguished clinically and pathologically. increased viscosity.
For instance, Schnlein-Henoch vasculitis is suggested by the Vasculitis is rare in type I cryoglobulinemia.
clinical features of abdominal pain or gastrointestinal hemor-
rhage in addition to the classic picture of lower extremity pur- Type II and type III cryoglobulins consist of more than 1
pura, arthritis, and hematuria. Schnlein-Henoch vasculitis class of immunoglobulin (mixed cryoglobulinemia) and can
has immunoglobulin A deposition in vessel walls and normal occur alone (essential, primary) or be due to another disease.
complement levels. Mixed cryoglobulinemia has circulating Type II cryoglobulinemia involves a monoclonal immunoglob-
cryoglobulins and evidence of complement consumption. ulin (usually immunoglobulin M) with anti-immunoglobulin
Complement levels, especially C4, may be low transiently in specificity. Affected patients often have a positive rheumatoid
hypersensitivity vasculitis. Hypersensitivity vasculitis is almost factor. Type III cryoglobulinemia involves polyclonal immu-
always a nonsystemic small vessel vasculitis temporally related noglobulins (usually immunoglobulin M) directed against
to infection, ingestion of drugs, or, less commonly, malig- other polyclonal immunoglobulins (usually immunoglobulin
nancy. The results of other laboratory studies are nonspecific. G). Other components of the immune complexes formed in
The leukocyte count and platelet count may be increased. mixed cryoglobulinemia include hepatitis C antigen, other
Eosinophilia may be present. The erythrocyte sedimentation infectious agents, cellular/nuclear antigens, and comple-
rate usually is increased. ment. These immune complexes precipitate slowly and are
present in smaller quantities (50500 mg/dL) than type I
Complement levels may be low in mixed cryoglobulinemia cryoglobulins.
and hypersensitivity vasculitis. Type II cryoglobulins frequently are associated with
chronic infections (most commonly hepatitis C), autoim-
Schnlein-Henoch vasculitis has 4 classic clinical features:
mune disorders, and, occasionally, lymphoma. The immune
lower extremity purpura, arthritis, gastrointestinal
complexes that form precipitate on endothelial cells in periph-
hemorrhage, and nephritis. Immunoglobulin A is noted on
eral blood vessels and fix complement, promoting vasculitic
biopsy.
inflammation. The size of immune complexes, ability to fix
complement, persistent immunoglobulin M production, and
Treatment and Outcome many other factors may influence the clinical presentation
The outcome of nonsystemic small vessel vasculitis of mixed cryoglobulinemia. The typical presentation is that
depends on the underlying condition. Control of the infec- of nonsystemic small vessel vasculitis with palpable purpura,
tion or discontinuing use of the offending drug may be all urticaria, and cutaneous ulceration. Peripheral neuropathy,
that is required. In other cases, corticosteroids or nonsteroidal arthralgia, and arthritis are common. Less commonly, mixed
anti-inflammatory drugs are beneficial. Hypersensitivity vas- cryoglobulinemia is complicated by hepatosplenomegaly,
culitis is usually self-limited, but it may recur with repeated pneumonitis or pulmonary hemorrhage, focal segmental
exposure to the antigen or drug. necrotizing glomerulonephritis, serositis (pleurisy, pericardi-
tis), and thyroiditis.
The outcome is good in nonsystemic small vessel vasculitis.
Type II cryoglobulins frequently are associated with
Hypersensitivity vasculitis may recur with repeated chronic infections (most often hepatitis C) and immune
exposure to the antigen or drug. disorders.
23. N O N A RT I C U L A R R H E U M AT I S M 371
The typical presentation of type II cryoglobulinemia is Box 23.11 PALPABLE PURPURA: DIFFERENTIAL
nonsystemic small vessel vasculitis with palpable purpura, DIAGNOSIS
urticaria, and cutaneous ulceration.
Peripheral neuropathy, arthralgia, and arthritis are Polyarteritis
common in type II cryoglobulinemia. Churg-Strauss syndrome
Wegener granulomatosis
Schnlein-Henoch purpura/vasculitis
Laboratory Studies Cryoglobulinemic vasculitis
Patients with type II cryoglobulinemia and small vessel Connective tissue disease-associated vasculitis (rheumatoid arthri-
vasculitis usually have an increased erythrocyte sedimentation tis, Sjgren syndrome, systemic lupus erythematosus)
rate, increased immunoglobulin levels, positive rheumatoid Hypersensitivity vasculitis
factor, and low levels of complement. Evidence of chronic hep- Drugs, infection, malignancy
atitis infection (particularly hepatitis C) frequently is identi-
fied. For cryoglobulin testing, it is important to draw blood
into a warmed syringe and to keep it warm until transferred Skin Lesions Associated With Vasculitis
to a cryocrit tube. Cooled specimens must be kept for up to 3
Palpable purpura suggests leukocytoclastic vasculitis, but
days to identify type II cryoglobulins. Serum protein electro-
this pathologic diagnosis does not define the clinical syn-
phoresis, immunoelectrophoresis, and quantitative immuno-
drome. Box 23.11 outlines the differential diagnosis of pal-
globulin determinations can be helpful in some cases.
pable purpura. Nodules or papules diagnosed as necrotizing
granuloma on biopsy occur in Churg-Strauss syndrome,
In type II cryoglobulinemia, immunoglobulin levels and the
Wegener granulomatosis, rheumatoid arthritis, and, occa-
erythrocyte sedimentation rate are increased, rheumatoid
sionally, systemic lupus erythematosus. Other nodules or
factor is positive, and complement levels are low.
papules without necrotizing granulomata can be the sign of
Evidence of chronic hepatitis infection (particularly angiocentric lymphoproliferative disorders or sarcoidosis or
hepatitis C) frequently is identified in type II they may be related to inflammatory bowel disease. Urticarial
cryoglobulinemia. or pustular lesions complicate hypocomplementemic vas-
culitis, inflammatory bowel arthritis syndrome, and Behet
syndrome. Livedo reticularis, which is associated with pro-
Outcome liferative endarteropathy, occurs in connective tissue diseases
The clinical course depends on the underlying associated and antiphospholipid antibody syndrome and in associa-
conditions and on the organs involved. Progressive renal dis- tion with cholesterol emboli and many systemic necrotizing
ease is the most common systemic complication. Pulmonary vasculitides.
hemorrhage can be life-threatening.
Urticarial or pustular lesions complicate
Outcome depends on associated conditions and organs hypocomplementemic vasculitis, inflammatory bowel
involved. arthritis syndrome, and Behet syndrome.
Progressive renal disease is the most common systemic Livedo reticularis occurs in connective tissue diseases and
complication. antiphospholipid antibody syndrome.
372 R H E U M ATO L O GY
24.
INFLAMMATORY AND NONINFLAMMATORY ARTHRITIS
Clement J. Michet, MD
R H E U M ATO I D A RT H R I T I S
NAT U R A L H I S TO RY O F R H EU M ATO I D
A RT H R IT I S
Rheumatoid arthritis is a chronic systemic inflammatory dis-
ease characterized by joint destruction. It affects 0.03% to 1.5% In the majority of patients, the onset of the joint disease is insid-
of the population worldwide. Women are affected 3 times ious, occurring over weeks to months. However, in a third of
more frequently than men. Its incidence peaks between the patients, the onset is rapid, occurring over days or weeks. Early
ages of 35 and 45 years; however, the age-related prevalence of in the course of the disease, most patients have oligoarthritis.
the disease increases even after age 65. The presentation of an Their disease becomes polyarticular with time. Ten percent to
unknown antigen to genetically susceptible persons is believed 20% of patients have relentlessly progressive arthritis, and 70%
to trigger rheumatoid arthritis. Recently, cigarette smoking to 90% have persistent, chronic, and progressive arthritis. The
has been identified as a risk factor for seropositive rheumatoid course may be slow, fluctuating, or rapid, but the end point is
arthritis. the same: disabling and destructive arthritis. Seventy percent
There is an immunogenetic predisposition to the develop- of patients experience polycyclic disease, with repeated flares
ment of rheumatoid arthritis. Class II major histocompatibil- interrupted by partial or complete remissions. Spontaneous
ity complex molecules on the surface of antigen-presenting remissions in the polycyclic or progressive group almost never
cells are responsible for initiating cellular immune responses occur after 2 years of disease. Patients who experience a per-
and for stimulating the differentiation of B lymphocytes into sisting polyarthritis with increased acute-phase reactants and
plasma cells that produce antibody. Most white patients with a positive rheumatoid factor or anticyclic citrullinated pep-
rheumatoid arthritis have class II major histocompatibility tide (CCP) antibody are at high risk for early erosive disease
complex type HLA-DR4 or HLA-DR1 or both. HLA-DR4 within 1 to 2 years of symptom onset and early disability. The
can be divided into 5 subtypes, 2 of which independently relationship between disease duration and inability to work
promote susceptibility to rheumatoid arthritis (shared is nearly linear. After 15 years of rheumatoid arthritis, 15% of
epitope). The relative risk of rheumatoid arthritis is increased patients are completely disabled. Life expectancy in seroposi-
3 to 5 times in white Americans with HLA-DR4. The con- tive rheumatoid arthritis is shortened, but it may be improving
cordance of rheumatoid factorpositive rheumatoid arthritis with more aggressive early intervention in the illness. Age, dis-
is increased 6 times among dizygotic twins. The risk of rheu- ease severity, comorbid cardiovascular disease, and functional
matoid arthritis in a monozygotic twin is increased 30 times status predict mortality. Educational level and socioeconomic
when a sibling has the disease. factors also influence mortality.
Rheumatoid arthritis affects 0.03%-1.5% of the In a third of patients, the onset of rheumatoid arthritis is
population. rapid (days or weeks).
373
Among patients with rheumatoid arthritis, 70%-90% have specific for rheumatoid arthritis. They are present at the onset
persistent, chronic, progressive arthritis. of disease, and in a high titer they are associated with progres-
sive erosive disease.
Joint damage occurs early in patients with seropositive
disease.
Swelling, pain, and joint stiffness occur with the onset of
The relationship between disease duration and inability to immune-mediated vascular injury of the synovial lining,
work is nearly linear. angiogenesis, and cellular proliferation.
Anti-CCP antibodies are equally sensitive and more
specific than rheumatoid factor for the diagnosis of early,
PAT H O G E N E S I S O F R H EU M ATO I D A RT H R I T I S erosive rheumatoid arthritis.
The immune reaction begins in the synovial lining of the joints Cytokines, in particular tumor necrosis factor-, and
in a genetically predisposed person. The earliest pathologic immune complexes, including rheumatoid factor, are
changes in the disease are microvascular injury that increases important components of the joint inflammatory reaction
vascular permeability and the accumulation of inflammatory in rheumatoid arthritis.
cells (CD4+ lymphocytes, polymorphonuclear leukocytes,
and plasma cells) in the perivascular space. Proinflammatory
C L I N I C A L F E AT U R E S O F R H EU M ATO I D
cytokines are released. Mediators of inflammation promote
A RT H R IT I S
synovial angiogenesis and synovial cell proliferation, the accu-
mulation of neutrophils in synovial fluid, and the maturation The joints most commonly involved in early rheumatoid
of B cells into plasma cells. Plasma cells in the joint locally syn- arthritis are the metacarpophalangeal, proximal interphalan-
thesize rheumatoid factor and other antibodies that promote geal, wrist, and metatarsophalangeal joints (more than 85% of
inflammation. Immune complexes activate the complement patients) (Figure 24.1). The distal interphalangeal joints are typ-
system, releasing chemotactic factors and promoting vascular ically spared. The distribution of involvement is symmetric and
permeability and opsonization. Phagocytosis releases lyso- polyarticular (5 or more joints); predominantly, small joints
somal enzymes and fosters the digestion of collagen, cartilage are involved. Ultimately, multiple other joints may be involved,
matrix, and elastic tissues. The release of oxygen-free radicals including the knees, ankles, elbows, shoulders, and the cri-
injures cells. Damaged cell membranes set free phospholipids coarytenoid and C12 articulations. Joints affected with rheu-
that fuel the arachidonic acid cascade. matoid arthritis are warm and swollen. The joint enlargement
The local inflammatory response becomes self-perpetuating. feels spongy and occurs with the thickening of the synovium.
Cytokines continue to play an important role, including An associated joint effusion may make the joint feel fluctuant.
tumor necrosis factor-, interleukin-1, and interleukin-6. Patients describe deep aching and soreness in the involved joints,
Proliferating synovium of activated macrophages and fibro- which are aggravated by use and can be present at rest.
blasts polarizes into a centripetally invasive pannus, destroying
the weakened cartilage and subchondral bone. Chondrocytes, The joints most commonly involved in early rheumatoid
stimulated in the inflammatory milieu, release their own pro- arthritis are the metacarpophalangeal, proximal
teases and collagenases. interphalangeal, wrist, and metatarsophalangeal joints.
Patients have swelling, pain, and joint stiffness with the
onset of vascular injury of the synovial lining, angiogenesis,
and cellular proliferation. Joint warmth, swelling, pain, and
limitation of motion worsen as the synovial membrane prolif-
erates and the inflammatory reaction builds. In studies of early
arthritis, histologic and radiographic evidence of rheumatoid
synovitis is found in clinically unaffected joints, an indica-
tion that the disease is present before clinical manifestations
appear.
Rheumatoid factor is an immunoglobulin (Ig) directed
against the Fc portion of IgG. It is not specific for rheumatoid
arthritis, and the prevalence of rheumatoid factor increases
with aging in healthy persons. Rheumatoid factor may be
detected in other inflammatory diseases such as primary
Sjgren syndrome, systemic lupus erythematosus, mixed cryo-
globulinemia, hepatitis C, and systemic vasculitis.
Anti-CCP antibodies are detected in the majority of
patients with seropositive rheumatoid arthritis. These target Figure 24.1 Moderately Active Seropositive Rheumatoid Arthritis.
The patient has soft tissue swelling across the entire row of
antigens are found in peptides containing citrulline, an amino metatarsophalangeal joints and proximal interphalangeal joints bilaterally
acid resulting from posttranslational enzyme modification and soft tissue swelling mounding up over the wrists. Note the nearly
of arginine. Unlike rheumatoid factor, these antibodies are complete lack of change at the distal interphalangeal joints.
374 R H E U M ATO L O GY
The distribution of involvement in rheumatoid arthritis is stiffness in the neck and occipital region. Patients may present
symmetric and polyarticular; predominantly, small joints dramatically with drop attacks or tetraplegia, but more com-
are involved. monly progression can be slow and subtle with symptoms of
hand weakness or paresthesias or signs of cervical myelopathy.
Hallmarks of joint inflammation in rheumatoid arthritis
Interference with blood flow by ischemic compression of the
are stiffness, heat, redness, soft tissue swelling, pain, and
anterior spinal artery or vertebral arteries (vertebrobasilar
dysfunction.
insufficiency) causes the neurologic symptoms. All patients
with destructive rheumatoid arthritis should be managed with
intubation precautions and the assumption that cervical insta-
C O N S T I T U T I O NA L FE AT U R E S O F bility is present. New neurologic symptoms mandate urgent
R H EU M ATO I D A RT H R IT I S neurologic evaluation, including magnetic resonance imaging
of the cervical spine and consideration of surgical interven-
Morning stiffness of more than 1 hour, gelling throughout tion. Indications for surgical treatment include neurologic or
the body, and recurrence of the stiffness after resting are some vascular compromise and intractable pain. In active patients,
of the many constitutional features that complicate rheu- prophylactic cervical spine stabilization is recommended
matoid arthritis. Fatigue, weight loss, muscle pain, excessive when there is evidence of extreme (>8 mm) subluxation of C1
sweating, or low-grade fever may be reported by patients pre- over C2. The probability of cervical involvement is predicted
senting with rheumatoid arthritis. Adult seropositive rheuma- by the severity and chronicity of peripheral arthritis.
toid arthritis is not a cause of fever of unknown origin because
temperatures greater than 38.3C cannot be attributed to the
Half of all patients with chronic rheumatoid arthritis have
disease.
radiographic involvement of the atlantoaxial joint.
Patients with cervical spine involvement by rheumatoid
MUS C U L O S K E L ETA L C O M P L I C AT I O NS O F
arthritis may present with occipital pain, signs of
R H EU M ATO I D A RT H R IT I S
myelopathy, weakness and paresthesias of the hands, or
The musculoskeletal complications of rheumatoid arthritis are drop attacks.
listed in Box 24.1.
Indications for surgical treatment in rheumatoid arthritis
are neurologic or vascular compromise or intractable pain.
Cervical Spine
The probability of cervical involvement is predicted by the
Half of all patients with chronic rheumatoid arthritis have severity and chronicity of peripheral arthritis.
radiographic involvement of the atlantoaxial joint. It is diag-
nosed from cervical flexion and extension radiographs showing
subluxation. Alternatively, some patients have subaxial sub- Popliteal Cyst
luxations, typically at 2 or more levels. The cervical instability Flexion of the knee markedly increases the intra-articular pres-
is usually asymptomatic; however, patients may have pain and sure of a swollen joint. This pressure produces an out-pouching
of the posterior components of the joint space, termed a
popliteal or a Baker cyst. Ultrasonographic examination of the
Box 24.1 MUSCULOSKELETAL COMPLICATIONS OF
popliteal space confirms the diagnosis. A popliteal cyst should
RHEUMATOID ARTHRITIS
be distinguished from a popliteal artery aneurysm, lymphade-
nopathy, phlebitis, and (more rarely) a benign or malignant
Characteristic deformities
tumor. The cyst can rupture down into the calf or, rarely, supe-
Boutonnire deformity of the finger, with hyperextension of the
riorly into the posterior aspect of the thigh. Rupture of the
distal interphalangeal joint & flexion of the proximal inter-
popliteal cyst with dissection into the calf may resemble acute
phalangeal joint
thrombophlebitis and is called pseudothrombophlebitis.
Swan-neck deformity of the finger, with hyperextension at the
Fever, leukocytosis, and ecchymosis around the ankle (cres-
proximal interphalangeal joint & flexion of the distal inter-
cent sign) can occur with the rupture. Treatment of an acute
phalangeal joint
cyst rupture includes bed rest, elevation of the leg, ice massage
Ulnar deviation of the metacarpophalangeal joints; it can pro-
or cryocompression, and an intra-articular injection of corti-
gress to complete volar subluxation of the proximal phalanx
costeroid. Treatment of the popliteal cyst requires improve-
from the metacarpophalangeal head
ment in the knee arthritis.
Compression of the carpal bones & radial deviation at the
carpus
Popliteal cyst is also called Baker cyst.
Subluxation at the wrist
Valgus of the ankle & hindfoot Rupture of a popliteal cyst may resemble acute
Pes planus thrombophlebitis (pseudothrombophlebitis).
Forefoot varus & hallux valgus
Ultrasonography can distinguish a cyst from a popliteal
Cock-up toes from subluxation at the metatarsophalangeal joints
artery aneurysm, lymphadenopathy, phlebitis, and tumor.
Rheumatoid Vasculitis
Carpal Tunnel Syndrome Rheumatoid vasculitis usually occurs in persons with severe,
deforming arthritis and a high titer of rheumatoid factor. The
Rheumatoid arthritis is a common cause of carpal tunnel vasculitis is mediated by the deposition of circulating immune
syndrome. The sudden appearance of bilateral carpal tunnel complexes on the blood vessel wall. At its most benign, it
syndrome should raise the question of an early inflammatory occurs as rheumatoid nodules, with small infarcts over the
arthritis. This syndrome is associated with paresthesias of the nodules and at the cuticles. Proliferation of the vascular intima
hand in a typical median nerve distribution. Discomfort may and media causes this obliterative endarteropathy, which has
radiate up the forearm or into the upper arm. The symptoms little associated inflammation. It is best managed by control-
worsen with prolonged flexion of the wrist and at night. Late ling the underlying arthritis. Leukocytoclastic or small vessel
complications include thenar muscle weakness and atro- vasculitis produces palpable purpura or cutaneous ulceration,
phy and permanent sensory loss. Treatment includes resting particularly over the malleoli of the lower extremities.
splints, control of inflammation, and local injection of gluco- This vasculitis can cause pyoderma gangrenosum or
corticosteroid. Surgical release is recommended for persistent peripheral sensory neuropathy. Secondary polyarteritis, which
symptoms. is clinically and histopathologically identical to polyarteritis
nodosa, results in mononeuritis multiplex. Occasionally, the
Rheumatoid arthritis is a common cause of carpal tunnel vasculitis occurs after the joint disease appears burned out.
syndrome.
Carpal tunnel syndrome is associated with paresthesias of Rheumatoid vasculitis usually occurs in the setting of
the hand in a typical median nerve distribution. severe, deforming arthritis and a high titer of rheumatoid
factor.
Rheumatoid vasculitis is mediated by the deposition of
E X T R A-A RT I C U L A R C O M P L I C AT I O N S O F circulating immune complexes on the blood vessel wall.
R H EU M ATO I D A RT H R IT I S
Rheumatoid vasculitis comprises a spectrum of vascular
Extra-articular complications of rheumatoid arthritis occur disease, including rheumatoid nodules and obliterative
almost exclusively in patients who have high titers of rheu- endarteropathy, leukocytoclastic or small vessel vasculitis,
matoid factor. In general, the number and severity of the and secondary polyarteritis (systemic necrotizing
extra-articular features vary with the duration and severity of vasculitis).
disease. Many of the classical extra-articular manifestations
of rheumatoid arthritis have become less common with the
advent of more aggressive treatment of early disease.
Neurologic Manifestations
Neurologic manifestations of rheumatoid arthritis include
Rheumatoid Nodules
mild peripheral sensory neuropathy. Painful sensory-motor
Rheumatoid nodules are the most common extra-articular neuropathy (mononeuropathy) suggests vasculitis or nerve
manifestation of seropositive rheumatoid arthritis. More than entrapment (eg, carpal tunnel syndrome). Cervical vertebral
20% of patients have rheumatoid nodules, which occur over subluxation can cause myelopathy. Erosive changes may pro-
extensor surfaces and at pressure points. They are rare in the mote basilar invagination of the odontoid process of C2 into
lungs, heart, sclera, and dura mater. The nodules have charac- the underside of the brain, causing spinal cord compression
teristic histopathologic features. A collagenous capsule and a and death.
376 R H E U M ATO L O GY
Pulmonary Manifestations not respond to medical therapies. Surgical pericardiectomy is
necessary.
Pleural disease has been noted in more than 40% of autop-
sies in cases of rheumatoid arthritis, but clinically significant
Patients rarely present with acute pericardial symptoms
pleural disease is less frequent. Characteristically, rheumatoid
despite frequent serous pericarditis.
pleural effusions are asymptomatic until they become large
enough to interfere mechanically with respiration. The pleu- Rheumatoid pericardial disease frequently presents with
ral fluid is an exudate with a concentration of glucose that is edema or ascites due to occult constrictive disease.
low (1050 mg/dL) because of impaired transport of glucose
Chronic constrictive pericarditis necessitates surgical
into the pleural space. Pulmonary nodules appear singly or in
treatment.
clusters. Single nodules have the appearance of a coin lesion.
Nodules typically are pleural-based and may cavitate and cre-
ate a bronchopleural fistula. Pneumoconiosis complicating Liver Abnormalities
rheumatoid lung disease, or Caplan syndrome, results in a vio-
lent fibroblastic reaction and large nodules. Patients with rheumatoid arthritis can have increased levels
Acute interstitial pneumonitis is a rare complication that of liver enzymes, particularly alkaline phosphatase. Increased
may begin as alveolitis and progress to respiratory insuffi- levels of aspartate aminotransferase, -glutamyltransferase,
ciency and death. Interstitial fibrosis is a chronic, slowly pro- and acute-phase proteins and hypoalbuminemia also occur
gressive process. It has physical findings of diffuse dry crackles in active rheumatoid arthritis. Liver biopsy shows nonspecific
on lung auscultation and a reticular nodular radiographic changes of inflammation. Nodular regenerative hyperplasia is
pattern affecting both lung fields, initially in the lung bases. rare and causes portal hypertension and hypersplenism. Many
A decrease in the diffusing capacity for carbon dioxide and a medications used to treat rheumatoid arthritis may cause
restrictive pattern are characteristic pulmonary function test increased levels of the transaminases.
findings. Interstitial disease is highly associated with smok-
ing. Bronchiolitis obliterans with or without cryptogenic Increased levels of liver enzymes, particularly alkaline
organizing pneumonia may occur with rheumatoid arthritis phosphatase, may occur in rheumatoid arthritis.
or its treatment. It produces an obstructive picture on pulmo- Nodular hyperplasia of the liver can rarely complicate
nary function testing and typically responds to corticosteroid rheumatoid arthritis and lead to portal hypertension and
treatment. High-resolution computed tomography is useful hypersplenism.
for distinguishing these different interstitial rheumatoid lung
syndromes and predicting treatment response. Methotrexate Many medications used to treat rheumatoid arthritis
treatment causes a hypersensitivity lung reaction in 1% to 3% increase the levels of transaminases.
of patients. It can present insidiously with a dry cough or with
life-threatening pneumonitis. Ophthalmic Abnormalities
Rheumatoid pleural disease is common but asymptomatic Keratoconjunctivitis sicca, or secondary Sjgren syndrome, is
until pleural effusions interfere with respiration. the most common ophthalmic complication in rheumatoid
arthritis. Episcleritis and scleritis also occur independently of
The exudative pleural fluid is remarkable for low levels of the joint inflammation and are usually treated topically. Severe
glucose. scleritis progressing to scleromalacia perforans causes blind-
High-resolution computed tomography helps to ness. Infrequent ocular complications of rheumatoid arthri-
distinguish among rheumatoid-associated interstitial lung tis include episcleral nodules, palsy of the superior oblique
diseases, including interstitial pneumonitis, interstitial muscle caused by tenosynovitis of its tendon sheath (Brown
fibrosis, and bronchiolitis obliterans with or without syndrome), and uveitis. Retinopathy is an infrequent compli-
cryptogenic organizing pneumonia. cation of antimalarial drug treatment.
Methotrexate hypersensitivity pneumonitis may be a Keratoconjunctivitis sicca, or secondary Sjgren syndrome,
life-threatening complication of therapy. is the most common ophthalmic complication in
rheumatoid arthritis.
Severe scleritis progressing to scleromalacia perforans
Cardiac Complications causes blindness.
Pericarditis has been noted in 50% of autopsies in cases of
rheumatoid arthritis. However, patients rarely present with
acute pericardial symptoms or cardiac tamponade. Recurrent
L A B O R ATO RY FI N D I N G S I N R H EUM ATO I D
effusive pericarditis without symptoms may evolve to chronic
A RT H R IT I S
constrictive pericarditis. Signs of unexplained edema or ascites
may be the presenting manifestations. Untreated constrictive Nonspecific alterations in many laboratory values are com-
pericarditis has a very high 1-year mortality of 70%. It will mon. In very active disease, normocytic anemia (hemoglobin
378 R H E U M ATO L O GY
detection of CCP antibody has allowed rheumatologists to Low-dose or tapered prednisone may be necessary to
identify rheumatoid arthritis very early in the clinical evolu- preserve function and diminish joint damage during the
tion of the disease before patients would meet these classifi- initiation of DMARD therapy.
cation criteria.
With disease-modifying agents, uninterrupted treatment
for 36 months is needed to assess efficacy. Combination
T R E AT M E N T O F R H EU M ATO I D A RT H R IT I S DMARD therapy has become more common.
The management of patients with rheumatoid arthritis requires An orthopedic surgical procedure for resistant rheumatoid
making the correct diagnosis, determining the functional sta- arthritis remains the most important therapeutic option for
tus of the patient, and selecting the goals of management with preserving or enhancing function. Synovectomy of the wrist
the patient. Goals of management include relieving inflamma- and nearby tendon sheaths is beneficial when medication
tion and pain and maintaining function. alone fails to control the synovitis. The operation preserves
The principles emphasized by physical medicine include joint function and prevents the lysis of extensor tendons that
bed rest or rest periods, improving nonrestorative sleep, and can result in a loss of function. Synovectomy of the knee,
joint protection (including modification of activities of daily either open or through an arthroscope, can delay the pro-
life, range-of-motion exercises, orthotics, and splints, if they gression of rheumatoid arthritis from 6 months to 3 years.
help the pain). Exercise should begin with range of motion Removal of nodules and treatment for local nerve entrapment
and stretching to overcome contracture. Strengthening and syndromes are also important surgical treatments for rheuma-
conditioning exercises should be prescribed carefully, depend- toid arthritis. Arthroplasty is reserved for patients in whom
ing on the activity of the patients disease. medical management has failed and in whom intractable pain
The primary goal of rheumatoid arthritis therapy is to begin or compromise in function developed because of a destroyed
treatment as soon as the diagnosis is made. Using nonsteroidal joint. Arthroplasty, arthrodesis (wrist), and synovectomy are
anti-inflammatory drugs alone for rheumatoid arthritis is not important components of well-balanced rheumatology treat-
recommended. Treatment should be managed and advanced ment programs. Total joint arthroplasty has a slightly poorer
with the goal of achieving low disease activity based on a tar- long-term outcome in rheumatoid arthritis than in osteoar-
geted disease activity score. thritis. Nevertheless, joint replacement has had a major impact
The choice of first disease-modifying antirheumatic drug on reducing patient disability.
(DMARD) is determined by the potential for early joint
damage. Therefore, in seropositive patients, methotrexate is Orthopedic surgery is the most important advance in the
the drug of choice. In seronegative polyarthritis, sulfasala- treatment of medically resistant rheumatoid arthritis.
zine, hydroxychloroquine, or minocycline may be options.
Uninterrupted treatment with a disease-modifying agent for 3 Total joint arthroplasty has a slightly poorer long-term
to 6 months is usually necessary to assess its effect. Traditionally, outcome in rheumatoid arthritis than in osteoarthritis.
DMARDs have been used sequentially, although recent stud-
ies have shown an enhanced benefit with early combination
C O N D I T I O N S R E L AT E D TO R H EU M ATO I D
DMARD treatments that include methotrexate. Tapered oral
A RT H R IT I S
corticosteroid therapy is another option in some protocols for
early rheumatoid arthritis. Evidence supporting the pivotal Seronegative Rheumatoid Arthritis
pro-inflammatory role of tumor necrosis factor in rheuma-
toid arthritis has been exploited clinically with the develop- Rheumatoid factornegative (seronegative) rheumatoid
ment of several effective tumor necrosis factor antagonists. arthritis is not associated with extra-articular manifestations.
These generally are reserved for patients not responding to tri- However, the arthritis usually is destructive, deforming, and
als of more traditional and less expensive DMARDs, although otherwise indistinguishable from seropositive rheumatoid
evidence is accumulating that early use of these agents may arthritis.
result in better disease control. Abatacept (a T-cell costimula-
tory inhibitor), tocilizumab (an interleukin-6 inhibitor), and Seronegative rheumatoid arthritis is not associated with
rituximab (an anti-CD20 B-celldepleting agent) are options extra-articular manifestations.
in treatment failures.
Goals of management of rheumatoid arthritis include Seronegative Rheumatoid Arthritis of the Elderly
relieving inflammation and pain and maintaining
A subgroup of patients older than 60 years with seronegative
function.
rheumatoid arthritis may have milder arthritis. In this subgroup,
A disease-modifying regimen is started when rheumatoid polyarticular inflammation suddenly develops and is controlled
arthritis is diagnosed, and treatment should be guided best with low doses of prednisone. The presence of anti-CCP
by targeting improvement to a low level of disease antibodies may help to distinguish this condition from polymy-
activity. Methotrexate is the DMARD of choice in early algia rheumatica. Minimal destructive changes and deformity
seropositive rheumatoid arthritis. occur. Some elderly patients with seronegative arthritis, such as
Fever, rash, and arthritis are the classic triad of Still disease.
Rheumatoid factor and antinuclear antibodies are absent in Sjgren Syndrome
Still disease. Sjgren syndrome has a triad of clinical features: keratocon-
There is a predilection for the wrists, shoulders, hips, and junctivitis sicca (with or without lacrimal gland enlargement),
knees. xerostomia (with or without salivary gland enlargement),
and connective tissue disease (usually rheumatoid arthritis).
Sore throat occurs at onset in 60% of patients. Histologically, CD4 lymphocytic infiltration and destruction
of lacrimal salivary glands characterize it. Clinically, it mani-
fests with dry eyes and dry mouth. Primary Sjgren syndrome is
Felty Syndrome
diagnosed predominantly in middle-aged women. Additional
Felty syndrome has the classic triad of rheumatoid arthritis, features of primary Sjgren syndrome are listed in Box 24.5.
leukopenia, and splenomegaly. Classic Felty syndrome usually Most patients have a polyclonal hypergammaglobulinemia.
380 R H E U M ATO L O GY
Box 24.5 FEATURES OF SJ GREN SYNDROME A Sjgren-like syndrome has been described in patients
with HIV infection and hepatitis C.
Classic triad
Arthritis: typically episodic polyarthritis
O S T E OA RT H R I T I S
Dry eyes
Dry mouth (& other dry mucous membranes)
Osteoarthritis is the failure of articular cartilage and subse-
Other features
quent degenerative changes in subchondral bone, bony joint
Constitutional features: fatigue, malaise, myalgia
margins, synovium, and para-articular fibrous and muscular
Raynaud phenomenon
structures. Osteoarthritis is the most common rheumatic dis-
Cutaneous vasculitis
ease; 80% of patients have some limitation of their activities,
CNS abnormalities
and 25% are unable to perform major activities of daily living.
Cerebritis, CNS vasculitis
The prevalence of osteoarthritis is strongly associated with
Stroke
aging. Joints most commonly affected include the knee, hand,
Multiple sclerosis-like illness
spine, metatarsophalangeal, and hip. Radiologic evidence of
Peripheral neuropathy
the disease greatly exceeds the prevalence of symptomatic
Sensory
cases.
Autonomic
Interstitial lung disease
Osteoarthritis is the most common chronic rheumatic
Pleurisy
disease.
Abbreviation: CNS, central nervous system.
PAT H O G E N E S I S O F O S T EOA RT H R IT I S
Autoantibodies typically are present, including rheumatoid
factor, antinuclear antibodies, and antibodies to extractable Two principal changes associated with osteoarthritis are the
nuclear antigens (SSA and SSB). progressive focal degeneration of articular cartilage and the
Patients can present with primary Sjgren syndrome with- formation of new bone in the floor of the cartilage lesion at the
out any additional connective tissue disease. The primary joint margins (osteophytes). Not all the mechanisms causing
syndrome typically has episodic and nondeforming arthritis. osteoarthritis have been identified. Current theories include 1)
More commonly, rheumatoid arthritis, systemic lupus erythe- mechanical process: cartilage injury, particularly after impact
matosus, scleroderma, polyarteritis nodosa, or polymyositis loading, and 2) biochemical process: failure of cartilage repair
accompanies Sjgren syndrome. There is no perfect defini- processes to adequately compensate for injury. A combination
tion for Sjgren syndrome, and no test is completely diagnos- of mechanical and biochemical processes likely contributes
tic. Simple dry eyes of the elderly, benign sicca syndrome, in most cases of osteoarthritis. It must be emphasized that
is distinguished from Sjgren syndrome by the absence of osteoarthritis is not just the consequence of wear and tear.
SSA antibodies. Patients with Sjgren syndrome, but not
the rheumatoid factornegative, SSA antibodynegative Osteoarthritis is associated with progressive focal
sicca syndrome, have an increased risk for development of degeneration of articular cartilage and subsequent
non-Hodgkin lymphoma. degeneration of surrounding soft tissues and proliferation
Treatment of primary Sjgren syndrome is mainly symp- (osteophytosis) of bone.
tomatic. Pilocarpine, 5 mg orally 4 times daily, improves sali- Osteoarthritis is not the consequence of normal use (wear
vary and lacrimal gland function in the majority of the patients. and tear).
Adverse effects, including flushing and sweating, limit its use-
fulness. In addition to hydration, systemic therapy is indicated
C L I N I C A L F E AT U R E S O F O S T E OA RT H R I T I S
if there is evidence of systemic inflammation.
A Sjgren-like syndrome has been described in patients The pain of an osteoarthritic joint is usually described as a
with human immunodeficiency virus (HIV) infection and deep ache. Subchondral bone edema contributes to the pain.
hepatitis C. Other infiltrative diseases of the parotid glands The pain occurs with use of the joint and is relieved with rest
should also be considered, including sarcoidosis, lymphoma, and cessation of weight bearing. As the disease progresses,
or an Ig-G4related inflammatory syndrome. the involved joint may be symptomatic with minimal activity
or even at rest. The pain originates in the structures around
Sjgren syndrome presents with dry eyes, dry mouth, and a the disintegrating cartilage (there are no nerves in cartilage).
connective tissue disorder (usually rheumatoid arthritis). There may be stiffness in the joint with initial use, but this ini-
tial stiffness is not prolonged as it is in inflammatory arthri-
Sjgren syndrome can exist by itself or with another formal
tis, such as rheumatoid arthritis. Although the symptoms
connective tissue disease such as rheumatoid arthritis,
are related predominantly to mechanical failure and motion
systemic lupus erythematosus, scleroderma, or myositis.
limits, joint debris and the associated repair process promote
Treatment focuses on control of inflammation and mild inflammation, accumulation of synovial fluid, and mild
symptoms of dryness. hypertrophy of the synovial membrane. Acute inflammation
382 R H E U M ATO L O GY
Table 24.1 INHERITED DISORDERS OF CONNECTIVE TISSUE
Marfan syndrome (autosomal dominant) Fibrillin gene Hypermobile joints: osteoarthritis, arachnodactyly,
kyphoscoliosis
Lax skin, striae, ectopic ocular lens
Aortic root dilatation (aortic insufficiency), mitral valve
prolapse, aneurysms, & aortic dissection
Ehlers-Danlos syndrome (10 subtypes) Type I & type III col- Joint hypermobility, friable skin, osteoarthritis
lagen gene defects Type III collagen defects associated with vascular aneurysms
Osteogenesis imperfecta (autosomal dominant & Type I collagen gene Brittle bones, blue sclerae, otosclerosis & deafness, joint
recessive variations; the most common heritable defects hypermobility, & tooth malformation
disorder of connective tissue: 1:20,000; 4 subtypes)
Type II collagenopathies: Type II collagen gene Spectrum from lethal (achondrogenesis) to premature
Achondrogenesis type II defects osteoarthritis (Stickler syndrome)
Hypochondrogenesis
Spondyloepiphyseal dysplasia
Spondyloepimetaphyseal dysplasia
Kniest dysplasia
Stickler syndrome
Familial precocious osteoarthropathy
osteoarthritis. Secondary osteoarthritis frequently compli- disease (idiopathic avascular necrosis of the femoral head),
cates trauma and the damage caused by inflammatory arthritis. first present as premature osteoarthritis years after they occur.
Inherited disorders of connective tissue and several meta- Inherited disorders of connective tissue frequently predispose
bolic abnormalities, including ochronosis, hemochromatosis, the affected person to premature osteoarthritis. Table 24.1
Wilson disease, and acromegaly, are complicated by secondary describes several inherited disorders, including their gene
osteoarthritis. Paget disease of bone, involving the femur or defects and characteristics.
pelvis about the hip joint, can predispose to osteoarthritis.
Injury to joint or supporting periarticular tissues can
Osteoarthritis involving the shoulder, metacarpophalangeal predispose to osteoarthritis.
joints, or isolated large joints or with chondrocalcinosis
Posttraumatic osteoarthritis is the most common form of
should prompt physicians to consider secondary causes of
secondary osteoarthritis.
osteoarthritis.
Isolated large joint involvement is a clue to posttraumatic
Trauma or injury to joint and supporting periarticular osteoarthritis.
tissues predisposes persons to the most common type of sec-
ondary osteoarthritis. Stress from repeated impact loading
Hemochromatosis
could weaken subchondral bone. Internal joint derangement
with ligamentous laxity or meniscal damage alters the normal Hemochromatosis was formerly considered an unusual auto-
mechanical alignment of the joint. Isolated large joint involve- somal recessive disorder of white males. It is now considered
ment is a clue to posttraumatic osteoarthritis. Chronic rota- the commonest inherited disease. The full clinical spectrum
tor cuff tear with subsequent loss of shoulder joint cartilage of hemochromatosis includes hepatomegaly, bronze skin
(cuff arthropathy) and knee osteoarthritis that develops years pigmentation, diabetes mellitus, the consequences of pitu-
after meniscal cartilage damage are examples of secondary itary insufficiency, and degenerative arthritis. The arthropa-
osteoarthritis. thy affects up to 50% of patients with hemochromatosis and
Congenital malformations of joints, such as congenital generally resembles osteoarthritis; however, it involves the
hip dysplasia and epiphyseal dysplasia, lead to premature metacarpophalangeal joints and shoulders, joints not typically
osteoarthritis. Other developmental abnormalities, includ- affected by generalized primary osteoarthritis. Attacks of acute
ing slipped capital femoral epiphysis and Legg-Calv-Perthes pseudogout arthritis may occur in relation to deposition of
384 R H E U M ATO L O GY
Avascular necrosis of bone usually affects the hips, shoul-
ders, knees, or ankles. Treatment is conservative, including
reduced weight bearing and analgesics. Some investigators
have treated patients successfully with vascularized bone
grafts in the bed of necrotic trabecular bone, although con-
trolled studies are not available. Core decompression may help
with pain but does not influence progression to osteoarthritis.
When there is evidence of cortical bone collapse, progression
to advanced osteoarthritis is inevitable. The most sensitive test
for avascular necrosis is magnetic resonance imaging. Plain
radiography is insensitive to early aseptic necrosis.
Hypertrophic Osteoarthropathy
Hypertrophic osteoarthropathy is characterized by clubbing
of the fingernails and painful distal long bone periostitis. The
patient may have a noninflammatory arthritis at the ankles,
knees, or wrists. This condition complicates primary and meta-
static pulmonary malignancies, chronic pulmonary infections,
cystic fibrosis, and hypoxic congenital heart disease. Treatment Figure 24.3 Severe Osteoarthritis. Hypertrophic changes, asymmetric
is usually symptomatic. joint-space narrowing, and subchondral sclerosis are prominent at the
interphalangeal joints and at the first carpometacarpal joint. Note that
Hemophilic arthropathy, a type of progressive degenera-
the metacarpophalangeal joints are completely spared, distinguishing this
tive arthropathy, is more destructive than primary osteoarthri- arthritis from rheumatoid arthritis. Also, there is joint-space narrowing
tis. Patients with hemophilia and recurrent hemarthroses are and sclerosis at the base of the thumb at the first carpometacarpal joint
at risk for hemophilic arthropathy. Widening of the intercon- and between the trapezium and the scaphoid. Osteoarthritis does not
dylar notch of the knees is an early radiographic feature sug- affect the entire wrist compartment equally. The involvement seen here is
the most common. An additional interesting feature seen here is central
gesting the diagnosis of this condition.
erosions at the second and third proximal interphalangeal joints. This
variant occasionally has been called erosive osteoarthritis.
R A D I O G R A P H I C FE AT U R E S O F
O S T E OA RT H R I T I S No laboratory studies of blood are useful in the diagnosis
of osteoarthritis.
The radiographic features of osteoarthritis do not always
predict the extent of symptoms. With aging, radiographic
osteoarthritis is far more prevalent than the clinical illness.
T H E R A P Y F O R O S T E OA RT H R I T I S
Common radiographic features include osteophyte forma-
tion, asymmetric joint-space narrowing, subchondral bony Therapeutic goals include relieving pain, preserving joint
sclerosis, and subchondral cysts. Later bony changes include motion and function, and preventing further injury and wear
malalignment and deformity (Figure 24.3). In the spine, the of cartilage. Weight loss (especially in knee osteoarthritis),
radiographic finding called spondylosis includes anterolateral use of canes or crutches, correction of postural abnormalities,
spinous osteophytes, degenerative disk disease with disk-space and proper shoe support are helpful measures. Isometric or
narrowing, and facet sclerosis. A defect in the bony structure isotonic range-of-motion exercises and muscle strengthening
of the posterior neural arch produces spondylolysis. With provide para-articular structures with extra support and help
bilateral spondylolysis, subluxation of one vertebra on another reduce symptoms. Relief of muscle spasm with local applica-
may occur, a condition called spondylolisthesis. The causes of tion of heat or cold to decrease pain can help. Addressing the
spondylolisthesis are trauma, osteoarthritis, and congenital. patients ability to cope with the illness may be more helpful
No laboratory studies of blood are useful in the diagnosis of than medication therapy alone.
osteoarthritis. Initial drug therapy should be analgesics, such as ace-
taminophen (1 g 4 times daily as needed). Nonsteroidal
Common radiographic features of osteoarthritis include anti-inflammatory drugs are beneficial for inflammatory
osteophyte formation, asymmetric joint-space narrowing, flares of osteoarthritis and usually do not need to be taken
subchondral bony sclerosis, subchondral cysts, and in anti-inflammatory doses every day. Selective use of opioid
buttressing of angle joints. analgesics can be considered for disabling pain, especially in
386 R H E U M ATO L O GY
25.
GOUT AND SPONDYLOARTHROPATHIES
William W. Ginsburg , MD
387
PRPP + Glutamine
PRPP syn
Guanosine Inosine Adenosine
HGPRT-ase
Adenosine
deaminase
Guanine Hypoxanthine
Figure 25.1 Purine Metabolism. HGPRT-ase
indicates hypoxanthine-guanine
Xanthine Xanthine oxidase phosphoribosyltransferase; PRPP,
phosphoribosylpyrophosphate; PRPP
syn, phosphoribosylpyrophosphate
Uric acid synthetase; , feedback inhibition.
388 R H E U M ATO L O GY
patients are already receiving these medications, their use 2. Correction of hyperuricemia has no apparent effect on
should be continued. renal function.
Because of severe gastrointestinal adverse effects, high-dose 3. Most rheumatologists do not treat asymptomatic
oral colchicine is rarely used for an acute attack. hyperuricemia.
4. 30% of patients with chronic tophaceous gout are
Treatment During Intercritical Period positive for rheumatoid factor (usually weakly positive).
Oral colchicine, 0.6 mg twice daily, should be given prophy- 5. 10% of patients with acute gout are positive for
lactically with probenecid, allopurinol, and febuxostat for 6 to rheumatoid factor (usually weakly positive).
12 months to prevent exacerbation of acute gout. Long-term 6. 5%10% of patients will have a gout and a pseudogout
use of low-dose colchicine can be associated with a myopathy attack simultaneously.
and neuropathy, especially in patients with renal insufficiency. A
myoneuropathy may appear in patients taking medications that 7. 50% of synovial fluids aspirated from first
affect colchicine metabolism via the cytochrome P450 system. metatarsophalangeal joints of asymptomatic patients
These include cyclosporine, simvastatin, lovastatin, atorvastatin, with gout have crystals of monosodium urate.
diltiazem, cimetidine, verapamil, and amiodarone. If a statin is 8. Up to 33% of patients with acute gout have a
needed in conjunction with colchicine in a patient with renal normal level of serum uric acid at the time of the
insufficiency, fluvastatin and pravastatin are preferred because acute attack.
they are not handled by the cytochrome P450 system.
Probenecid inhibits tubular reabsorption of filtered and 9. Gout in a premenopausal female is very unusual.
secreted urate. Probenecid should not be used if the patient 10. There are reports of superimposed gout occurring in
has a creatinine clearance less than 50 mL/minute or a his- Heberden and Bouchard nodes in older women taking
tory of kidney stones or if 24-hour uric acid value is more than thiazide diuretics.
1,000 mg. Notably, probenecid delays renal excretion of indo-
methacin and may increase the risk of methotrexate toxicity. 11. A septic joint can trigger a gout or pseudogout attack in
a predisposed person. Synovial fluid should always be
Colchine should be used with caution in patients with analyzed for crystals, Gram stain, and culture.
renal impairment. 12. The frequency of gout in patients who have had cardiac
transplant is high (25%). (Both cyclosporine and
Allopurinol is a xanthine oxidase inhibitor and can precip- diuretics cause hyperuricemia.)
itate gout. Its use should not be started during an acute attack.
Allopurinol can cause a severe toxicity syndrome: eosinophilia,
fever, hepatitis, decreased renal function, and erythematous
C A L C I U M P Y RO P H O S P H AT E D E P O S I T I O N
desquamative rash. It should be given in the lowest dose pos-
DISEASE
sible to keep the uric acid value less than 6 mg/dL. In patients
with chronic renal disease, the starting dose should always be Etiologic Classification
low (50100 mg) and increased slowly. If allopurinol is used
Diseases associated with calcium pyrophosphate depo-
in conjunction with 6-mercaptopurine or azathioprine, the
sition disease (CPPD) include hyperparathyroidism,
dose of 6-mercaptopurine or azathioprine needs to be reduced
hemochromatosis-hemosiderosis, hypothyroidism, and
at least 25% or bone marrow toxicity can occur.
hypomagnesemia.
Allopurinol use should not be initiated during an acute
attack. Pseudogout
When CPPD causes an acute inflammatory arthritis, the
Febuxostat is a recently approved nonpurine xanthine oxi-
term pseudogout is applied. CPPD pseudogout is an acute
dase inhibitor. It can be used in patients who are intolerant of
inflammatory arthritis caused by CPPD. CPPD crys-
allopurinol or who have mild to moderate renal insufficiency.
tals are weakly positively birefringent under polarized
Pegloticase (uricase) converts uric acid to allantoin. It was
light microscopy. Pseudogout most commonly affects the
recently approved for chronic gout refractory to conventional
knees, but the wrists, elbows, ankles, and intervertebral
therapy. In patients with tophaceous deposits it promotes
disks can be affected. It usually occurs in older individuals.
resolution.
Chondrocalcinosis is found on radiographs in most patients
with pseudogout.
For treatment of acute attacks of pseudogout, NSAIDs or an Calcium oxalate arthropathy occurs in patients with primary
injection of steroid preparation can be used. Prophylactic oral oxalosis and in patients undergoing chronic hemodialysis.
colchicine can lead to a decrease in the frequency and severity It can cause acute inflammatory arthritis. Crystals are large,
of attacks. bipyramidal, and birefringent. Calcium oxalate can cause
chondrocalcinosis.
BA S I C C A L C I U M P H O S P H AT E D I S E A S E
Calcium oxalate arthropathy occurs in patients with
( H Y D ROX YA PAT I T E D E P O S I T I O N D I S E A S E)
primary oxalosis and patients undergoing chronic
Presentation hemodialysis.
Clinical presentations of basic calcium phosphate disease
include 1) acute inflammation, including calcific tendini-
tis, osteoarthritis with inflammatory episodes, periarthri- OT H E R C RYS TA L S I M P L I C AT E D I N J O I N T
tis or arthritis dialysis syndrome, and calcinotic deposits DISEASE
in scleroderma and 2) chronic inflammation, including
Cholesterol crystals are a nonspecific finding and have been
severe osteoarthritis and Milwaukee shoulder or knee
found in the synovial fluid of patients with various types of
(advanced glenohumeral and knee osteoarthritis, rotator
chronic inflammatory arthritis. Cryoglobulin crystals are
cuff tear, noninflammatory paste-like joint fluid containing
found in essential cryoglobulinemia and paraproteinemia.
hydroxyapatite).
Corticosteroid crystals are found in an arthritis flare after a
corticosteroid injection, and Charcot-Leyden crystals have
Basic calcium phosphate disease can present as acute or
been found in hypereosinophilic syndromes. In patients
chronic inflammation.
undergoing hemodialysis, aluminum phosphate crystals can
develop.
390 R H E U M ATO L O GY
6th chromosome 6th chromosome
chromosome 6, 1 inherited from each parent. On each of early disease, magnetic resonance imaging can detect inflam-
these there is an HLA-A and HLA-B allele. Therefore, every- mation in the sacroiliac joints even when radiographs of the
one has 2 HLA-A types and 2 HLA-B types. With regard to sacroiliac joints are normal.
inheritance, an offspring has a 50% chance of acquiring a spe-
cific HLA-A or HLA-B antigen from a parent (Figure 25.2). Laboratory Findings
Siblings have a 25% chance of being identical for all 4 HLA-A
and HLA-B alleles. The erythrocyte sedimentation rate may be increased, there
The frequency of HLA-B27 in control populations is as may be an anemia of chronic disease, rheumatoid factor is
follows: whites (United States), 8%; African Americans, absent, and 95% of white patients are positive for HLA-B27.
2% to 4%; Asians, 1%; Haida (North American Indian), 50%.
In randomly selected persons with HLA-B27, the chance Extraspinal Involvement
of the disease developing is 2%. In B27-positive relatives of
Enthesopathic involvement is characteristic of ankylosing
B27-positive patients with ankylosing spondylitis, the risk of
spondylitis and the other spondyloarthropathies and includes
the disease developing is 20%.
plantar fasciitis, Achilles tendinitis, and costochondritis. Hip
The rheumatic diseases associated with HLA-B27 are
and shoulder involvement are common (up to 50%), but
peripheral joints can be affected, usually with asymmetric
1. Ankylosing spondylitis (HLA-B27 in !90%)
involvement of the lower extremities.
2. Reactive arthritis (!80%)
3. Enteropathic spondylitis (approximately 75%) Extraskeletal Involvement
4. Psoriatic spondylitis (approximately 50%) Other findings in active disease include 1) fatigue, 2) weight
loss, 3) low-grade fever, and 4) uveitis. Uveitis is an impor-
tant clue to the diagnosis of spondyloarthropathies and is not
A N KY L O S I N G S P O N DY L IT I S found in adults with rheumatoid arthritis. Uveitis typically
flares at a time the arthritis is inactive. Osteoporosis is a com-
Ankylosing spondylitis is a chronic systemic inflammatory mon complication of ankylosing spondylitis and can occur
disease that affects the sacroiliac joints, the spine, and the in early stages of the disease. Late complications can include
peripheral joints. Sacroiliitis and low back pain define this traumatic spinal fracture leading to cord compression, cauda
disease.
Table 25.2 FINDINGS IN ANKYLOSING SPONDYLITIS
Features CHARACTERISTIC FINDING
Schober Make a mark on the spine at level of L5 & 1 at 10 cm directly above An increase of <5 cm indicates early lumbar
with the patient standing erect. Patient then bends forward involvement
maximally & the distance between the 2 marks is measured
Chest expansion Measure maximal chest expansion at nipple line Chest expansion of <5 cm is clue to early
costovertebral involvement
Sacroiliac compression Exert direct compression over sacroiliac joints Tenderness or pain suggests sacroiliac
involvement
equina syndrome (symptoms include neurogenic bladder, difficile, and Chlamydia trachomatis. Inflammatory eye disease
fecal incontinence, and radicular leg pain), fibrotic changes in (conjunctivitis or uveitis) and mucocutaneous disease (balani-
upper lung fields, aortic insufficiency, complete heart block, or tis, oral ulcerations, or keratoderma) can occur. Keratoderma
secondary amyloidosis. blennorrhagicum is a characteristic skin disease on the palms
and soles that is indistinguishable histologically from pso-
Differential Diagnosis riasis. Joint predilection is for the toes and asymmetric large
joints in the lower extremities. It can cause sausage toe, as
The differential diagnosis includes diffuse idiopathic skel- can psoriatic arthritis. Cardiac conduction disturbances and
etal hyperostosis, osteitis condensans ilii, fusion of sacro- aortitis can develop. Long-term studies indicate that the dis-
iliac joint seen in paraplegia, osteitis pubis, infection, and ease remains episodically active in 75% of patients and that
degenerative joint disease. The clinical symptoms of diffuse disability is a frequent outcome.
idiopathic skeletal hyperostosis are stiffness of spine and Treatment is with NSAIDs. Sulfasalazine and metho-
relatively good preservation of spine motion. It generally trexate are used in patients with chronic disease. Treatment
affects middle-aged and elderly men. Patients with diffuse with tetracycline or erythromycin-type antibiotics may
idiopathic skeletal hyperostosis can have dysphagia related to decrease the duration and severity of illness in some cases of
cervical osteophytes. Criteria for the condition are flowing Chlamydia-triggered reactive arthritis.
ossification along the anterolateral aspect of at least 4 con-
tiguous vertebral bodies, preservation of disk height, absence
A RT H R I T I S A S S O C I AT E D WI T H
of apophyseal joint involvement, absence of sacroiliac joint
I N FL A M M ATO RY B OWE L D I S E A S E
involvement, and extraspinal ossifications, including liga-
mentous calcifications. Two distinct types of arthritis are associated with chronic
Osteitis condensans ilii usually affects young to middle- inflammatory bowel disease:
aged females with normal sacroiliac joints. Radiography shows
sclerosis on the iliac side of the sacroiliac joint only. The sacro- 1. Oligoarthritis of the peripheral joints tending to correlate
iliac joint also can be involved with 1) tuberculosis, 2) meta- with the activity of the bowel disease
static disease, 3) gout, 4) Paget disease, or 5) other infections
(eg, Brucella, Serratia, Staphylococcus). 2. Enteropathic spondylitis that is not a complication
of the bowel disease. It may be diagnosed many years
before the onset of bowel symptoms, and its subsequent
Treatment progress bears little relationship to the bowel disease.
Treatment involves physical therapy (upright posture is very Approximately 75% of patients with enteropathic
important), exercise (swimming), cessation of smoking, spondylitis and inflammatory bowel disease are
genetic counseling, and drug therapy with NSAIDs. Tumor HLA-B27positive.
necrosis factor inhibitors can provide benefit for spinal and
peripheral joint symptoms. Adalimumab is more effective In patients with arthritis, NSAIDs must be used with cau-
than etanercept for preventing recurrent uveitis. tion because they may flare the bowel disease. Infliximab or
adalimumab are the drugs of choice to treat both spondyli-
tis and Crohn disease. Etanercept is not beneficial for Crohn
R E AC T I VE A RT H R IT I S
disease.
Reactive arthritis is an aseptic arthritis induced by a host
response to an infectious agent rather than direct infection.
P S O R I AT I C A RT H R IT I S
HLA-B27 is associated in 80% of cases. Reactive arthritis
develops after infections with Salmonella, Shigella flexneri, Psoriatic arthritis develops in approximately 25% of patients
Yersinia enterocolitica, Campylobacter jejuni, Clostridium with psoriasis. Pitting of nails is strongly associated with joint
392 R H E U M ATO L O GY
disease. Sausage finger or toe is characteristic of psoriatic OSTEOID OSTEOM A
arthritis. Pencil-in-cup deformity of the distal and proximal
interphalangeal joints is found on radiography. Osteoid osteoma is a benign bone tumor. Bone pain at night is
There are 5 clinical groups of psoriatic arthritis: 1) predom- relieved by aspirin or another NSAID.
inantly distal interphalangeal joint involvement, 2) asymmet-
ric oligoarthritis, 3) symmetric polyarthritis-like rheumatoid
arthritis but negative for rheumatoid factor, 4) arthritis muti- BY PA S S A RT H R I T I S
lans, and 5) psoriatic spondylitis. Treatment is with NSAIDs,
methotrexate, and tumor necrosis factor inhibitors. Bypass arthritis occurs in patients who have had intestinal
bypass operations. The most commonly affected joints are
metacarpophalangeal, proximal interphalangeal, wrists, knees,
U VE I T I S A N D R H E U M ATO L O G I C and ankles. Bypass arthritis is commonly associated with der-
DISEASES matitis. Circulating immune complexes composed of bacterial
antigens are thought to be the cause of this disorder. Treatment
Various rheumatologic diseases are associated with uveitis, consists of NSAIDs and antibiotics such as tetracycline, but
particularly the spondyloarthropathies. Uveitis is uncom- reanastomosis may be necessary for complete resolution of
mon in rheumatoid arthritis and systemic lupus erythemato- symptoms.
sus. Nongranulomatous uveitis without any other associated
symptoms may be associated with HLA-B27 in almost 50%
of patients. Other causes of uveitis include sarcoid, Behet S U M M A RY
syndrome, polychondritis, and juvenile idiopathic arthri-
tis, especially in young females who are antinuclear Spondyloarthropathies are characterized by sacroiliitis,
antibodypositive. uveitis, peripheral arthritis, enthesopathic involvement,
and an association with HLA-B27.
Dactylitis (sausage finger or toe) is characteristic of
B E H ET SY N D R O M E psoriatic arthritis and reactive arthritis.
The common manifestations of Behet syndrome include Gout and pseudogout are diagnosed from synovial fluid
oral and genital ulcers and uveitis. Behet syndrome is most analysis demonstrating characteristic crystals.
common in Middle Eastern countries and Japan. HLA-B51
The treatment of acute gout and pseudogout is with
is associated with the syndrome. Uveitis, synovitis, cutaneous
NSAIDs unless contraindicated.
vasculitis, and meningoencephalitis may be present. Treatment
is with corticosteroids, although more aggressive immunosup- A uric acid value 6 mg/dL is the goal of therapy with
pression often is required. probenecid, allopurinol, or febuxostat.
D I AG N O S I S
Among relatives of patients with SLE, 25% have antinuclear
antibodies, circulating immune complexes, antilymphocyte
Findings in patients with SLE are listed in Box 26.1. At least 4 antibodies, or a false-positive result on the VDRL test without
of the findings are needed for the diagnosis of SLE. clinical disease. Concordance for SLE among monozygotic
twins is much greater than among dizygotic twins. Multiple
genetic and environmental factors are important in the devel-
E P I D E M I O L O GY
opment of SLE.
The female to male ratio is 8:1 during the reproductive years.
The first symptoms usually occur between the second and In SLE, the frequency of HLA-B8, HLA-DR2, and
fourth decades of life. The disease seems to be less severe in the HLA-DR3 is increased.
elderly. In SLE with onset at an older age, the female to male
ratio is equal. The frequency of SLE is increased in African Multiple genetic and environmental factors are important
Americans, Native Americans, and Asians. in the development of SLE.
PAT H O G E N E S I S
a
Portions previously published in Ginsburg WW. Drug-induced systemic lupus There is a change in the activity of the cellular immune sys-
erythematosus. Semin Respir Med. 1980;2:518. Used with permission. tem with an absolute decrease in T-suppressor cells. There is
394
Box 26.1 CRITERIA FOR THE DIAGNOSIS OF SYSTEMIC The arthritis of SLE is inflammatory but nondeforming
LUPUS ERYTHEMATOSUS and nonerosive.
Renal biopsies are helpful for directing therapy in renal Nucleolar RNA Scleroderma
disease associated with SLE.
Abbreviations: DNP, deoxyribonucleoprotein; ENA, extractable nuclear antigen;
Patients with mesangial changes alone do not require MCTD, mixed connective tissue disease; nDNA, native DNA; SLE, systemic lupus
aggressive therapy. erythematosus.
396 R H E U M ATO L O GY
Table 26.2 AUTOANTIBODIES IN RHEUMATIC Table 26.3 TREATMENT OF MANIFESTATIONS OF
DISEASES SYSTEMIC LUPUS ERYTHEMATOSUS
AntinDNA SLE, 50%-60% Arthritis, fever, mild systemic symptoms ASA, NSAID
AntiSS-B (Sjgren syndrome B) Sjgren, 60% Rapidly deteriorating renal function Cyclophosphamide,
SLE, 15% mycophenolate mofetil
Hemolytic anemia (Coombs positive) can occur in SLE. The 10-year survival rate is 90% in newly diagnosed SLE.
Idiopathic thrombocytopenic purpura can be the initial Among patients with SLE, the prognosis is worse in
manifestation of SLE. African Americans and Hispanics.
Hypocomplementemia (CH50, C3, C4) usually correlates
with active disease.
Hypocomplementemia with increased antinative DNA Table 26.4 COMPLICATIONS OF TREATMENT FOR
antibodies usually implies renal disease (or skin disease).
SYSTEMIC LUPUS ERYTHEMATOSUS
Antinative DNA levels fluctuate with disease activity, but
TREATMENT COMPLICATION
other associated antibodies do not.
A positive result of an antinuclear antibody test is not Ibuprofen Aseptic meningitis (headache, fever, stiff neck,
specific for lupus. CSF pleocytosis)
C L I N I C A L FE AT U R E S
T R E AT M E N T
The clinical manifestations of drug-induced lupus include
arthralgias and polyarthritis, which occur in approximately When possible, patients with drug-induced lupus should stop
80% of cases. Malaise is common, and fever has been reported using the offending drug. Symptoms usually subside within
in up to 40% of cases. Approximately 30% of patients have several weeks, although the duration for complete resolu-
pleural-pulmonary manifestations as their presenting symp- tion varies depending on the drug. Serologic abnormalities
toms. Pericarditis has been reported in approximately 20% can remain for years after resolution of clinical symptoms.
of cases. Diffuse interstitial pneumonitis has been noted. Treatment depends on the clinical manifestations and could
Asymptomatic pleural effusions may be found on routine chest include nonsteroidal anti-inflammatory drugs or possibly
radiography. In contrast to SLE, the incidence of renal and low-dose prednisone, if needed.
398 R H E U M ATO L O GY
Patients with drug-induced lupus should stop using the Box 26.3 COAGULATION TEST RESULTS
offending drug. CHARACTERIZING THE LUPUS ANTICOAGULANT
Screening tests
M I X E D C O N N E C T I VE T I S S U E D I S E A S E
Prothrombin time normal
aPTT prolonged
This is a distinct disease with variable features of SLE, poly-
Plasma clot time prolonged
myositis, systemic sclerosis, and rheumatoid arthritis. The
Test identifying the lupus anticoagulant
incidence of renal disease is low. It is serologically character-
Prolonged aPTT not corrected by adding normal plasma
ized by a positive antinuclear antibody and by a high titer of
anti-RNP. Antinative DNA usually is not present. Raynaud Abbreviation: aPTT, activated partial thromboplastin time.
phenomenon is common.
Patients with mixed connective tissue disease have a high Many, but not all, patients with the lupus anticoagulant
titer of anti-RNP. also have increased IgG or IgM antiphospholipid antibody
levels.
The lupus anticoagulant and antiphospholipid antibod-
U N D I F F E R E N T I AT E D C O N N E C T I VE ies are associated with SLE, but they also have been reported
TISSUE DISE ASE in various other autoimmune, malignant, infectious, and
drug-induced diseases. The antibodies are also found in per-
In this category, patients have symptoms that do not fulfill the sons with no apparent disease but in whom recurrent throm-
diagnostic criteria for a definite or specific connective tissue bosis develops; these patients have primary antiphospholipid
disease. Common symptoms include Raynaud phenomenon, antibody syndrome, which represents approximately 50% of
arthralgias, fatigue, and variable joint or soft tissue swelling. The cases in which the antibodies are present.
antinuclear antibody may be positive, but other autoantibodies are
not present. Patients need to be observed to determine whether Lupus anticoagulant and antiphospholipid antibodies also
progression to a distinct connective tissue disease occurs. have been reported in various autoimmune, malignant,
infectious, and drug-induced diseases.
The primary antiphospholipid antibody syndrome
A N T I P H O S P H O L I P I D A N T I B O DY
represents 50% of cases in which the antibodies are present.
SY N D R O M E
R AY N AU D P H E N O M E N O N
SYS T E M I C S C L E R O S I S ( S C L E R O D E R M A )
This is biphasic or triphasic color changes (pallor, cyanosis,
erythema) accompanied by pain and numbness in the hands Systemic sclerosis (scleroderma) can be subdivided into several
or feet. Cold is a common precipitating agent. Associated fac- categories: 1) diffuse systemic sclerosis (diffuse scleroderma);
tors are listed in Box 26.4. 2) limited cutaneous scleroderma, which includes the CREST
(calcinosis cutis, Raynaud phenomenon, esophageal dysmotil-
ity, sclerodactyly, telangiectasias) syndrome; 3) localized sclero-
derma, which includes morphea and linear scleroderma; and 4)
Box 26.4 CAUSES OF SECONDARY RAYNAUD
overlap and undifferentiated connective tissue diseases, which
PHENOMENON
include some component of scleroderma in conjunction with
a manifestation of another connective tissue disease. For the
Chemotherapeutic agents
diagnosis of systemic sclerosis, 1 major criterion or 2 or more
Bleomycin
minor criteria need to be present. The major criterion is sym-
Vinblastine
metric induration of the skin of the fingers and the skin proxi-
Toxins
mal to metacarpophalangeal or metatarsophalangeal joints.
Vinyl chloride
The minor criteria are sclerodactyly, digital pitting scars or
Vibration-induced injuries
loss of substance from the finger pad, and bibasilar pulmonary
Jackhammer use
fibrosis. The pathologic hallmark of the disease is an oblitera-
Vascular occlusive disorders
tive noninflammatory vasculopathy and the accumulation of
Thoracic outlet obstruction
collagen in the skin and other organs that leads to fibrosis.
Atherosclerosis
Vasculitis Systemic sclerosis is characterized by symmetric induration
Connective tissue diseases of the skin of the fingers and the skin proximal to
Scleroderma, 90%-100% metacarpophalangeal or metatarsophalangeal joints,
Mixed connective tissue disease, 90%-100% sclerodactyly, fingertip pitting or scarring, and bibasilar
Systemic lupus erythematosus, 15% pulmonary fibrosis.
Rheumatoid arthritis, <10%
Polymyositis
C L I N I C A L M A N I FE S TAT I O NS
Miscellaneous
Cryoglobulinemia Skin
Cold agglutinins
Patients with rapidly progressive acral and trunk skin thicken-
Increased blood viscosity
ing are at risk for early visceral abnormalities.
400 R H E U M ATO L O GY
Raynaud Phenomenon Pulmonary hypertension with cor pulmonale is a serious
potential problem.
Raynaud phenomenon occurs in almost all patients with
scleroderma. It usually occurs more than 2 years before skin
changes. If Raynaud phenomenon is not present but skin find- Gastrointestinal
ings are suggestive of scleroderma, another disease such as
Esophageal dysfunction is the most frequent gastrointestinal
eosinophilic fasciitis should be considered.
abnormality. It occurs in 90% of patients and often is asymp-
tomatic. Lower esophageal sphincter incompetence with acid
Almost all patients with scleroderma have Raynaud reflux may produce esophageal strictures or ulcers. Medications
phenomenon. to reduce acid production are important. Reduced esopha-
geal motility may respond to therapy with metoclopramide,
Articular cisapride, or erythromycin. Small bowel hypomotility may be
associated with pseudo-obstruction, bowel dilatation, bacte-
Nondeforming symmetric polyarthritis similar to rheumatoid rial overgrowth, and malabsorption. Treatment with tetracy-
arthritis may precede cutaneous manifestations by 12 months. cline may be helpful, but promotility agents are less effective.
Patients can have both articular erosions and nonarticular Colonic dysmotility also occurs, and wide-mouthed diver-
bony resorptive changes of ribs, mandible, radius, ulna, and ticuli may be found.
distal phalangeal tufts, which are unique to systemic sclerosis.
Up to 60% of patients have leathery crepitation of the ten- Esophageal dysmotility occurs in more than 90% of
dons of the wrist. patients with scleroderma.
Pulmonary Renal
A considerable decrease in diffusing capacity can be present Renal involvement may result in fulminant hypertension,
with a normal chest radiograph. Diffuse interstitial fibro- renal failure, and death if not treated aggressively. Proteinuria,
sis occurs in approximately 70% of patients and is the most newly diagnosed mild hypertension, microangiopathic hemo-
common pulmonary abnormality. Patients who have active lytic anemia, vascular changes on renal biopsy, and rapid
alveolitis demonstrated by 1) bronchopulmonary lavage, 2) progression of skin thickening may precede overt clinical find-
high-resolution computed tomography showing ground-glass ings of renal crisis. Renal involvement with hyperreninemia
appearance without honeycombing, or 3) lung biopsy are necessitates the use of angiotensin-converting enzyme inhibi-
most likely to respond to prednisone and cyclophosphamide tors. Aggressive early antihypertensive therapy can extend life
therapy with improvement of pulmonary function. Pleuritis expectancy.
(with effusion) is very rare. Pulmonary hypertension is more
common in patients with CREST variant. Patients with pul- Renal involvement in scleroderma may be life-threatening.
monary hypertension can have an isolated decrease in the
diffusing capacity of the lung for carbon monoxide (Dlco).
Although echocardiography is helpful for making a diagno- L A B O R ATO RY F I N D I N G S
sis, right heart catheterization should always be performed to Antinuclear antibodies are found in 95% or more of patients.
confirm the diagnosis and to obtain accurate measurements of Antitopoisomerase I antibody (anti-Scl-70) is found in
pulmonary artery and capillary wedge pressures. approximately 25% of patients with scleroderma and is usually
associated with more severe disease. Anticentromere antibody
Patients with pulmonary hypertension can have an isolated occurs in 10% to 20%.
decrease in Dlco.
Diffuse interstitial fibrosis occurs in approximately 70% of T R E AT M E N T
patients and is the most common pulmonary abnormality.
No remissive or curative therapy is available. Aggressive nutri-
Pulmonary hypertension is more common in patients with tional support, including hyperalimentation, may be required
CREST variant. for extensive gastrointestinal disease.
CUTANEOUS DISEASE
Raynaud phenomenon Precedes other symptoms by years Onset associated with other symptoms within 1 y
Telangiectasia, digital ulcers, calcinosis Frequent Rare early, but frequent later in the course
Visceral disease Pulmonary hypertension Renal, intestinal, & cardiac disease; pulmonary interstitial fibrosis
the extremities. Development of internal organ involvement Laboratory findings are peripheral eosinophilia, increased
occurs but is delayed. Lung involvement occurs in 70% of sedimentation rate, and hypergammaglobulinemia. The diag-
patients. Diffusing capacity may be low, and pulmonary hyper- nosis is based on the findings of inflammation and thickening
tension can develop. The latter is more common in CREST of the fascia on deep fascial biopsy. Treatment is with predni-
than in diffuse scleroderma. Bosentan and sildenafil were sone (40 mg daily). The response is usually good. Associated
recently approved for pulmonary hypertension in scleroderma conditions are aplastic anemia and thrombocytopenia (both
and CREST syndrome. Anticentromere antibody is found in antibody-mediated) and leukemia and myeloproliferative
70% to 90% of patients and anti-Scl-70 antibody in 10%. The diseases.
incidence of primary biliary cirrhosis is increased.
Eosinophilic fasciitis is characterized by tight bound-down
In CREST syndrome, 70% of patients have lung skin of the extremities, usually sparing the hands and feet.
involvement.
Raynaud phenomenon does not occur.
The diffusing capacity may be low, and pulmonary
There is no visceral involvement.
hypertension can develop.
Laboratory findings include peripheral eosinophilia.
Anticentromere antibody is present in 70%-90% of
patients. Treatment with prednisone provides good response.
There is an increased incidence of primary biliary cirrhosis.
402 R H E U M ATO L O GY
condition. Scleromyxedema is associated with IgG mono- Anti-Jo1 is associated with polymyositis, dermatomyositis,
clonal protein. Cocaine use and appetite suppressants also pulmonary disease, and increased mortality.
cause scleroderma-like illness. Nephrogenic systemic fibrosis,
a recently described cutaneous fibrosing disorder, is caused Treatment of polymyositis includes prednisone (60 mg
by exposure to gadolinium-containing contrast agents during daily), usually for 1 to 2 months, until the muscle enzyme val-
magnetic resonance imaging, especially in patients with renal ues normalize. The dosage is slowly reduced thereafter, and the
insufficiency. clinical course and creatine kinase values are monitored. In
severe or steroid-resistant cases, either azathioprine (12 mg/
kg daily), methotrexate, or intravenous immunoglobulin can
be used.
T H E I N F L A M M ATO RY M YO PAT H I E S
Aspiration pneumonia can occur as a result of pharyngeal
weakness. If so, a liquid diet, feeding tube, or feeding gastros-
Inflammatory myopathies can be classified into several cat-
tomy is needed until there is clinical improvement.
egories, including polymyositis, dermatomyositis, myositis
associated with malignancy, childhood-type, and overlap con-
nective tissue disease. Polymyositis is an inflammatory myop- I N C LUS I O N B O DY MYO S IT I S
athy characterized by proximal muscle weakness. Patients with This usually occurs in the elderly. The onset of weakness is
dermatomyositis have an associated rash that includes a helio- more insidious, occurring over many years. The creatine kinase
trope hue of the eyelids, a rash on the metacarpophalangeal value often is only minimally to several times increased, and
and proximal interphalangeal joints (Gottron papules), and distal and proximal weakness occur. The electromyogram,
photosensitivity dermatitis of the face. Most patients have an besides showing a myopathic picture, also has an associated
increased creatine kinase level, a characteristic electromyo- neuropathic picture. The diagnosis of inclusion body myositis
gram, and a characteristic muscle biopsy. is made from biopsy. Histopathologic findings are indistin-
Electromyography is characteristic but not diagnostic guishable from those of polymyositis except for the presence
of inflammatory myopathies. It shows decreased amplitude of eosinophilic inclusions and rimmed vacuoles with baso-
and increased spike frequency, it is polyphasic, and conduc- philic enhancement. Inclusion body myositis responds poorly
tion speed is normal. Fibrillation potentials are not specific to prednisone and immunosuppressive therapy, and the course
for inflammatory myopathies, but when present they indicate is one of slow, progressive weakness.
active disease. Loss of fibrillation potentials usually means the
inflammatory myopathy is under control, but if the electro- Inclusion body myositis usually occurs in the elderly.
myographic result is still myopathic, it suggests an associated
steroid myopathy caused by treatment. The muscle biopsy, Diagnosis is made from biopsy.
which is mandatory in all patients with inflammatory myop- It responds poorly to prednisone.
athy, shows degeneration, necrosis, and regeneration of
myofibrils with lymphocytic and monocytic infiltrate in a
perivascular or interstitial distribution. D RU G -I N D U C E D M YO PAT H I E S
In patients older than 40 years, perhaps 10% to 20% of
those with dermatomyositis and polymyositis have an asso- Drugs may cause an inflammatory myopathy. The myopathy
ciated malignancy. The antibody anti-Jo1 is associated with associated with colchicine mimics polymyositis, and patients
polymyositis and dermatomyositis in approximately 25% of have muscle weakness and an increased creatine kinase level.
cases. This antibody is associated with inflammatory arthritis, This often occurs in the setting of a patient with gout and renal
progressive interstitial lung disease, Raynaud phenomenon, insufficiency receiving long-term therapy with colchicine.
and increased mortality primarily due to respiratory failure. Lipid-lowering drugs such as the statins; other drugs includ-
Mechanics hands, characterized by fissuring or cracking of ing zidovudine, d-penicillamine, and hydroxychloroquine;
the distal skin pads in the fingers, can also occur. The autoan- and addictive drugs such as heroin or cocaine have all been
tibody anti-Mi-2 is associated with dermatomyositis in 2% to associated with myopathy. Corticosteroids cause a steroid
20% of patients. myopathy with proximal muscle weakness and a normal cre-
atine kinase value.
Polymyositis is an inflammatory myopathy characterized
by proximal muscle weakness.
I N F E C T I O U S A RT H R I T I S
Dermatomyositis is an inflammatory myopathy associated
with a rash that includes heliotrope hue of the eyelids. An infectious cause should be ruled out immediately in a
patient with acute monarticular arthritis. Approximately 5%
Electromyography is characteristic but not diagnostic of
to 10% of patients with septic arthritis present with multiple
polymyositis.
joint involvement.
Perhaps 10%-20% of patients >40 years with
dermatomyositis and polymyositis have associated Infectious causes should be ruled out in patients with acute
malignancy. monarticular arthritis.
404 R H E U M ATO L O GY
MYC O BAC T E R I A L A N D F U N G A L J O I N T prophylaxis before invasive dental, gastrointestinal, or genito-
I N FEC T I O NS urinary procedures according to the recent guidelines, unless
obvious immunosuppression is present.
These types of organisms usually cause chronic bone and joint
infections. A synovial biopsy and culture may be required to
document these infections. Tuberculous arthritis is often oth- Prosthetic joint infection usually is caused by a
erwise asymptomatic and usually is caused by direct extension gram-positive organism within the first 6 months after
from adjacent bony infection. Atypical mycobacterial infec- joint replacement.
tion may cause an inflammatory arthritis and tenosynovitis Prosthetic joint infections usually are caused by
frequently involving the hand and wrist. Sporotrichosis and gram-negative or fungal organisms beyond the initial
blastomycosis are the fungi most likely to have skeletal mani- 6 months after joint replacement.
festations. The classic presentation in sporotrichosis is a gar-
dener with a rose-thorn penetration in whom a monarthritis
develops. R H E U M AT I C F E V E R A N D
P O S T S T R E P TO C O C C A L R E AC T I VE
Tuberculous arthritis is often otherwise asymptomatic and A RT H R I T I S
is caused by direct extension from adjacent bony infection.
Arthritis affects two-thirds of all patients with rheumatic
Atypical mycobacterial infection may cause an fever. One-third of patients with acute rheumatic fever have no
inflammatory arthritis and tenosynovitis most commonly obvious antecedent pharyngitis. In adults, arthritis may be the
affecting the hand and wrist. only clinical feature of acute rheumatic fever. The arthritis may
Sporotrichosis and blastomycosis are the fungi most likely be migratory, with each joint remaining inflamed for approxi-
to have skeletal manifestations. mately 1 week. The arthritis of rheumatic fever is nonerosive;
however, repeated attacks may result in a Jaccoud deformity,
in which the metacarpophalangeal joints are in ulnar devia-
tion as a result of tendon laxity rather than bony damage.
S P I NA L S E P T I C A RT H R IT I S Patients with joint symptoms without carditis may be
treated with high-dose salicylates (36 g daily). Corticosteroids
This condition should be suspected in patients with acute
may be required if patients do not respond to salicylates. Joint
or chronic, unrelenting back pain associated with fever and
symptoms may rebound when anti-inflammatory therapy is
marked local tenderness. The thoracolumbar region is most
discontinued.
commonly affected. An antecedent infection or procedure
predisposing to bacteremia may help suggest this diagnosis.
The arthritis in rheumatic fever may be migratory and
Imaging studies usually have evidence for infection crossing
usually involves the large joints, particularly the knees,
the disk space. In tuberculous spinal septic arthritis (Pott dis-
ankles, elbows, and wrists.
ease), the site of involvement is most commonly T10-L2, and
there is usually an associated paraspinal abscess. Repeated attacks of rheumatic fever may result in Jaccoud
Intravertebral disk infection is often a difficult diagnosis deformity.
to establish because pain patterns may be unusual and local-
The mainstay treatment for the arthritis of rheumatic fever
izing signs may be absent. Bone scanning may be helpful, but
is high-dose salicylates (36 g daily).
magnetic resonance imaging may be very helpful, particularly
because of the ability to show extension of infection into sur-
rounding tissues. VI R A L A RT H R I T I S
R H E U M ATO L O G I C M A N I F E S TAT I O N S O F LU P US -L I K E I L L N E S S E S I N H I V I N F E C T I O N
HIV INFECTION
Some of the features of SLE are similar to those of HIV infec-
Musculoskeletal complaints can be among the first manifes- tion. Fever, lymphadenopathy, mucous membrane lesions,
tations of HIV infection (Box 26.5). Articular manifesta- rashes, arthritis, and hematologic abnormalities are common
tions can be extremely debilitating. Epidemiologic studies to both lupus and HIV infection. HIV infection also may
have not concluded whether HIV infection predisposes to be associated with polyclonal B-cell activation resulting in
autoantibody production, including antinuclear and antiphos-
pholipid antibodies. HIV infection should be considered in
the differential diagnosis of SLE in any patient who is at risk
Box 26.5 RHEUMATOLOGIC MANIFESTATIONS OF
for HIV. Antinuclear antibodies in high titer have not been
HUMAN IMMUNODEFICIENCY VIRUS (HIV)
found in HIV infection, and antibodies to double-stranded
DNA are absent.
Arthralgia
Painful articular syndrome Although some features of HIV infection may resemble
HIV arthropathy those of SLE, antinuclear antibodies are present in low
Reactive arthritis titer only, and antibodies to double-stranded DNA are
Psoriatic arthritis absent.
Undifferentiated spondyloarthropathy
Myositis
Vasculitis
Raynaud phenomenon H I V-A S S O C I AT E D VA S C U L I T I S
Sjgren-like syndrome (diffuse infiltrative lymphocytosis
Primary angiitis of the central nervous system, angiocentric
syndrome)
lymphoproliferative vasculopathies, and polyarteritis nodosa
Septic arthritis
have been reported. Any person with known HIV infection
Fibromyalgia
who presents with new mononeuritis should be evaluated for
Serologic abnormalities
vasculitis.
406 R H E U M ATO L O GY
OT H E R H I V-A S S O C I AT E D R H EU M AT I C S U M M A RY
S Y N D RO M E S
A positive result of antinuclear antibody test alone is not
The diffuse, infiltrative lymphocytosis syndrome is mani-
specific for SLE.
fested by xerostomia, xerophthalmia, and salivary gland swell-
ing mimicking Sjgren syndrome. The glands are infiltrated Mixed connective tissue disease is defined by
with CD8 lymphocytes. In contrast to Sjgren syndrome, overlap symptoms and a strongly positive titer of
HIV-positive patients usually do not have antibodies to SS-A anti-RNP.
or SS-B and are usually rheumatoid factor-negative.
There is an inflammatory articular syndrome associated A history of thrombosis and the presence of
with HIV infection that is distinct from any resemblance to antiphospholipid antibodies define the antiphospholipid
spondyloarthropathy. Usually this is an oligoarthritis affecting antibody syndrome.
joints of the lower extremities and is short-lived. Scleroderma is defined by indurated skin of the fingers
There is an acquired immunodeficiency syndromeassoci- and the skin proximal to the metacarpophalangeal
ated myopathy that may be viral. There is also a myopathy due joints.
to zidovudine therapy. Fibromyalgia also has been reported in
up to 25% of HIV-infected patients. Polymyositis is characterized by proximal muscle weakness,
increased creatine kinase value, and myopathic findings on
electromyography.
OT H E R T Y P E S O F I N F E C T I O U S Hepatitis C infection can cause arthritis, vasculitis,
A RT H R I T I S cryoglobulinemia, and a positive rheumatoid
factor.
Whipple disease is a rare cause of arthropathy and usually is asso-
Parvovirus in adults can mimic rheumatoid arthritis. It is
ciated with constitutional symptoms, fever, neurologic symp-
diagnosed by demonstrating the presence of anti-B19 IgM
toms, malabsorption, lymphadenopathy, and hyperpigmentation.
antibodies.
There may be a slow, progressive dementia. The arthritic symp-
toms may precede the gastrointestinal manifestations. The infec- HIV infection is associated with a wide variety of
tious agent is Tropheryma whipplei. Polymerase chain reaction on rheumatologic conditions, including spondyloarth-
small bowel or synovial biopsy or synovial fluid may be necessary ropathies, vasculitis, and Sjgren and lupus-like
to establish the diagnosis. Treatment is usually with doxycycline syndromes. It should be considered in patients at risk for
or trimethoprim-sulfamethoxazole, often required for a year. the disease.
G OA L S Total Thyroxine
Review tests to assess thyroid function. Total T4 concentration is a measurement of T4 after displace-
ment from the thyroid hormonebinding proteins such as
Summarize the evaluation, causes, and management of thyroxine-binding globulin (TBG). Therefore, conditions
hyperthyroidism and hypothyroidism. that affect TBG concentration will also affect total T4 mea-
Recognize thyroid-related medical emergencies and review surements. Androgens, anabolic steroids, glucocorticoids,
their management. chronic liver disease, niacin, and familial TBG deficiency
decrease total TBG. Estrogens, pregnancy, acute hepatitis,
Explain the evaluation of thyroid nodules. and familial TBG excess increase TBG and, therefore, total
Describe thyroid malignancies. T4 concentrations.
L A B O R ATO RY A S S E S S M E N T O F T H Y R O I D TOTA L T R I I O D OT H Y RO N I N E
FUNCTION Similar to total T4, serum total triiodothyronine (T3) con-
centration is decreased in hypothyroidism, nonthyroid
S E RU M T H Y ROT RO P I N illness, and caloric deprivation and by drugs such as propra-
nolol, amiodarone, and glucocorticoids. Serum T3 levels are
Current assays measure thyrotropin (ie, thyroid-stimulating increased in thyrotoxicosis and thyroid hormone resistance.
hormone) concentrations as low as 0.01 mIU/L, allowing dif- Serum T3 concentrations should be measured to establish or
ferentiation between low-normal values and suppressed values. exclude the diagnosis of T3 thyrotoxicosis in a patient who has
Thyrotropin levels are increased in primary hypothyroidism, a decreased thyrotropin level and a normal T4 level. In sub-
during recovery from nonthyroid illness, and with thyroid clinical hyperthyroidism, the thyrotropin level is suppressed,
hormone resistance. Thyrotropin levels are low in hyperthy- but T3 and T4 levels are normal; in subclinical hypothyroid-
roidism, in nonthyroid illness, and with use of drugs such as ism, the thyrotropin level is elevated, but T3 and T4 levels are
somatostatin, dopamine, and glucocorticoids. Measurement normal (Table 27.1).
of the thyrotropin level is the best single test of thyroid func-
tion. However, thyrotropin levels are unreliable in cases of
pituitary disease since values can be inappropriately normal in T H Y RO I D H O R MO N E B I N D I N G P ROT E I N S
relation to thyroid hormone concentrations. Thus, thyrotropin
levels may be normal or increased with thyrotropin-producing Measurement of thyroid hormonebinding proteins can
tumors and normal or decreased in central hypothyroidism. be helpful when there is a discrepancy between the total
thyroid hormone concentrations and the other thyroid test
results. The concentration of these proteins can be altered
T H Y ROX I N E by medications (eg, increased by estrogens and decreased
by androgens). In addition, the concentration of available
Free Thyroxine
protein for binding can be affected by changes in thyroid
Although free thyroxine (T4) is frequently measured, there function (increased in hypothyroidism and decreased in
is substantial variability in the accuracy of the various assays hyperthyroidism) and by substances that interfere with the
available for clinical use. Serum free T4 is decreased in hypo- binding of thyroid hormones to the proteins (eg, carba-
thyroidism and nonthyroid illness and increased in hyperthy- mazepine and certain nonsteroidal anti-inflammatory drugs
roidism, nonthyroid illness, and thyroid hormone resistance. [NSAIDs]).
411
Table 27.1 INTERPRETATION OF THYROID FUNCTION absence does not exclude autoimmune thyroid disease.
TEST RESULTS Conversely, they can also be found in healthy persons. High
titers occur in more than 90% of patients with Hashimoto
SERUM CONCENTRATION
thyroiditis. When thyroglobulin antibodies are present, the
Thyrotropin Free T4 T3 DIAGNOSIS measurement of thyroglobulin is unreliable for follow-up of
thyroid malignancies.
Normal Normal Normal Normal
ET I O L O GY
T H Y RO I D S C A N N I N G
The etiology of primary thyroid disorders that cause hyperthy-
Thyroid scanning displays the distribution of functioning thy-
roidism can be divided into those characterized by increased
roid tissue. It differentiates between hyperthyroidism caused
production and release of T4 (high RAIU) and those charac-
by Graves disease and toxic thyroid nodules, ectopic thyroid
terized by unregulated release of T4 because of gland destruc-
tissue, and metastatic disease in the follow-up of patients with
tion (low RAIU) (Box 27.1).
differentiated thyroid cancer.
The most common thyroid-related cause of hyperthyroid-
ism in the United States is Graves disease. Other common
R A D I OAC T I VE I O D I N E U P TA K E causes are toxic nodular goiter and thyroiditis (lymphocytic or
Results of the radioactive iodine uptake (RAIU) test repre- subacute). Exogenous hyperthyroidism is a common cause of
sent the percentage of radioactive iodine retained for a specific nonthyroid hyperthyroidism, particularly in patients receiving
time after it is administered (usually 24 hours). RAIU is indi- combination T4 and T3 treatment.
cated during the evaluation of hyperthyroidism to distinguish
between low- and high-uptake states and to aid in dose calcula- Primary causes of hyperthyroidism are related to increased
tions when radioactive iodine is used to treat Graves disease. production and release of T4 (high-RAIU causes) or
unregulated release of T4 because of gland destruction
(low-RAIU causes).
S E RUM T H Y RO G L O BU L I N
Graves disease is the most common thyroid-related cause of
Thyroglobulin is used as a tumor marker in patients who have hyperthyroidism in the United States.
differentiated thyroid carcinoma. It is also useful in the differ-
ential diagnosis of hyperthyroidism to distinguish between an Toxic nodular goiter and thyroiditis are common causes of
endogenous hormone source (increased thyroglobulin) and hyperthyroidism.
an exogenous hormone source (suppressed thyroglobulin).
412 E N D O C R I N O L O GY
Box 27.2 SYMPTOMS AND SIGNS OF Pituitary thyrotropin-secreting tumorinappropriately
HYPERTHYROIDISM normal or high thyrotropin level with elevated levels of T4
or T3 (or both).
Symptoms
Heat intolerance A low serum thyrotropin level alone is not diagnostic of
Palpitations hyperthyroidism because a low level can also be encountered
Nervousness in nonthyroid illness, glucocorticoid therapy, dopamine ther-
Irritability apy, and secondary hypothyroidism.
Insomnia
Signs Biochemical parameters establish the diagnosis and lead to
Tachycardia the cause of hyperthyroidism.
Increased sweating
Diarrhea
Weight loss S P E C I F I C C AUS E S
Muscle weakness (proximal) Graves Disease
Graves disease is characterized by hyperthyroidism with diffuse
Exogenous hyperthyroidism commonly causes nonthyroid RAIU and the presence of TRAbs and thyroid-stimulating
hyperthyroidism in patients taking thyroid hormone immunoglobulins, which have a stimulatory effect on the
replacement. receptor causing the hyperthyroidism. The disease is more
common in young women and causes the thyroid to be mildly
enlarged and firm.
C L I N I C A L FE AT U R E S
Graves ophthalmopathy and pretibial dermopathy are usu-
Most clinical features reflect the effects of excess thyroid hor- ally associated with Graves disease. TRAbs are the pathophys-
mone. Typical symptoms and signs are listed in Box 27.2. Most iologic link between them. Treating hyperthyroidism is an
patients with hyperthyroidism have a small, firm goiter. important first step in the management of these conditions.
Graves ophthalmopathy is specific for Graves disease. The conditions associated with Graves (ophthalmopathy and
Ocular manifestations include findings due to sympathetic dermopathy) respond to treatment of hyperthyroidism when
overactivity from hyperthyroidism of any cause (retraction of initiated early in the disease process.
the upper lid, stare, and lid lag) or findings unique to Graves
ophthalmopathy (lid edema, conjunctival injection, chemosis, Graves disease is defined as hyperthyroidism with diffuse
proptosis, and extraocular muscle weakness). Patients with RAIU and TRAbs.
Graves ophthalmopathy may complain of a gritty sensation in
Young women are more commonly affected than men.
the eyes, excessive lacrimation, photophobia, and diplopia.
Elderly patients with hyperthyroidism may present with Associated conditions include a mildly enlarged and
atypical findings. Findings in patients with apathetic thyro- firm thyroid, Graves ophthalmopathy, and pretibial
toxicosis, for example, include apathy, weight loss, supraven- dermopathy.
tricular tachyarrhythmia, and congestive heart failure.
Gynecomastia may develop in younger men.
Painless Lymphocytic Thyroiditis (Postpartum
Thyroiditis or Silent Thyroiditis)
Clinical features reflect the hypermetabolic state due to
excess thyroid hormone. Painless lymphocytic thyroiditis is usually a self-limiting dis-
ease that occurs most commonly in the postpartum period
Sympathetic overreactivity due to thyroid hormone excess
and tends to recur with subsequent pregnancies. However, it
causes upper eyelid retraction, stare, and lid lag.
can also occur unrelated to pregnancy and in males.
In elderly patients, findings of apathy, weight loss, The classic presentation is a sequential triphasic pattern:
supraventricular tachyarrhythmia, and heart failure may be hyperthyroid phase (suppressed thyrotropin, low RAIU, and
from apathetic thyrotoxicosis. increased levels of free T4) is followed by a hypothyroid phase,
which is followed by a recovery phase with normal thyroid
function. This triphasic pattern may not be seen.
D I AG N O S I S Treatment is symptomatic. -Blockers may be needed dur-
ing the hyperthyroid phase, and temporary thyroid hormone
The diagnosis of hyperthyroidism is biochemical:
replacement may be necessary during the hypothyroid phase.
In some cases, the hypothyroidism may be permanent.
Overt hyperthyroidismsuppressed thyrotropin and
There is no indication for antithyroid medications or
elevated levels of T4 or T3 (or both).
radioactive iodine therapy because the hyperthyroidism results
Subclinical hyperthyroidismsuppressed thyrotropin with from the release of preformed thyroid hormone, not increased
normal levels of T4 and T3. production.
27. D I S O R D E R S O F T H E T H Y R O I D G L A N D 413
Painless lymphocytic thyroiditis is a self-limited illness that This condition is characterized by a large, solitary nodule
occurs most often in the postpartum period but which may and most commonly occurs in middle-aged women.
occur unrelated to pregnancy or in males.
The nodule demonstrates intense radioisotope uptake, with
The classic triphasic presentation includes a hyperthyroid suppressed uptake in the rest of the gland.
phase followed by a hypothyroid phase followed by the
recovery of thyroid function.
Exogenous Hyperthyroidism
Subacute Painful Thyroiditis (de Quervain Thyroiditis)
Exogenous hyperthyroidism can result from the use of T4 or
Subacute thyroiditis is characterized by a painful, tender goi- T3 (or both). It should be suspected if thyrotoxic patients have
ter. Patients often complain of fever, malaise, myalgia, and a low RAIU and no palpable goiter. Low serum levels of thyro-
history of upper respiratory tract infection. Transient hyper- globulin help to differentiate this disorder from painless lym-
thyroidism (low RAIU) is often present at diagnosis and may phocytic thyroiditis.
be followed by transient hypothyroidism. The erythrocyte
sedimentation rate is invariably increased. Thyrotoxic patients with low RAIU and a nonpalpable
Treatment is symptomatic. -Blockers and thyroid hor- goiter should be suspected of having exogenous
mone replacement are used as discussed for painless thy- hyperthyroidism.
roiditis. NSAIDs and corticosteroids are useful for pain. The
response to corticosteroid therapy is dramatic, typically with Low thyroglobulin levels differentiate this from painless
relief of symptoms within 24 hours. lymphocytic thyroiditis.
414 E N D O C R I N O L O GY
more than 1 course of treatment. Radioactive iodine therapy thyroid hormone levels from postoperative manipulation or
has not been associated with long-term risks, but pregnancy radiation-induced thyroiditis. Thyroid storm is characterized
and breast-feeding are contraindications. Radioactive iodine by delirium, fever, tachycardia, hypotension, vomiting, diar-
can worsen the course of active Graves ophthalmopathy, but rhea, and, eventually, coma. Treatment should be initiated
that worsening can be avoided with the prophylactic use of immediately in the intensive care unit. Antithyroid therapy
glucocorticoids. with propylthiouracil is preferred. Iodine solution is added
to inhibit the release of preformed thyroid hormone and
Hypothyroidism is the goal of therapy. decrease peripheral conversion of T4 to T3. -Blocker therapy,
supportive therapy directed at systemic disturbances, and
Pregnancy and breast-feeding are contraindications to the therapy directed at the precipitating event should be delivered
use of radioactive iodine, but overall no long-term risks in parallel.
have been associated with the use of radioactive iodine.
Active Graves ophthalmopathy may be worsened by Thyroid storm is a medical emergency with multisystem
radioactive iodine, but that worsening can be avoided with manifestations.
the prophylactic use of glucocorticoids.
Delirium, fever, tachycardia, hypotension, diarrhea,
vomiting, and coma characterize thyroid storm.
Surgery
Propylthiouracil is the preferred treatment, with the
Near-total or total thyroidectomy is usually unnecessary for addition of iodine solution to inhibit the release of
treatment of Graves disease or toxic multinodular goiter. If preformed thyroid hormone and decrease peripheral
nodules appear suspicious with fine-needle aspiration (FNA), conversion of T4 to T3.
surgery should be strongly considered. Thyroid lobectomy is
-Blocker therapy and supportive therapy should be
used for toxic thyroid adenoma. In addition, surgery is usu-
directed at end-organ toxicities.
ally considered when rapid restoration of a euthyroid state is
desired, when the patient is pregnant, or when the patient has
a large, compressive goiter. Damage to the recurrent laryngeal
nerves or parathyroid glands is uncommon (<1%-2%) with H Y P OT H Y R O I D I S M
experienced surgeons. To prevent thyroid storm and excessive
bleeding from the overactive friable gland, the patient should Hypothyroidism can be primary (intrinsic thyroid disease) or
be treated preoperatively with stable iodine solution in com- secondary (hypothalamic-pituitary disease). Primary hypo-
bination with antithyroid drug therapy and E-blockers. This thyroidism accounts for more than 99% of all cases.
approach should render the patient euthyroid or nearly euthy-
roid at surgery. Nearly all cases of hypothyroidism result from intrinsic
thyroid disease.
When nodules appear suspicious on FNA, surgery is
recommended. ET I O L O GY
Toxic thyroid adenoma is treated with thyroid lobectomy. The most common cause in the United States is Hashimoto
Surgical treatment is recommended when rapid restoration thyroiditis, an autoimmune thyroid disease. It tends to clus-
of a euthyroid state is desired, when the patient is pregnant, ter in families and is more common in women. Other causes
or when the patient has a large, compressive goiter. of hypothyroidism include hypothyroidism after radioactive
iodine treatment of hyperthyroidism, thyroidectomy, radio-
Thyroid storm and excessive bleeding (the gland is friable) therapy for neck malignancies, and transient hypothyroidism
can be prevented with preoperative use of antithyroid during the course of subacute or painless thyroiditis.
drugs, -blockers, and stable iodine solution.
Causes of hypothyroidism include radioactive iodine
Supportive Therapy treatment, thyroidectomy, radiotherapy for neck cancers,
and subacute or painless thyroiditis, which causes transient
Symptomatic patients should be given -blockers to control hypothyroidism.
adrenergic manifestations of hyperthyroidism while waiting
for definitive therapy to take effect.
C L I N I C A L FE AT U R E S
The clinical manifestation of hypothyroidism depends on the
T H Y RO I D S TO R M
degree and duration of the deficiency. When symptoms are
Thyroid storm is a state of life-threatening hyperthyroid- present, they are nonspecific. Many patients are asymptomatic
ism with severe multisystem manifestations. It develops in at presentation, with hypothyroidism having been diagnosed
patients who have acute illness superimposed on uncontrolled through routine screening. The most common signs and symp-
thyrotoxicosis and in patients who have a sudden increase in toms are listed in Box 27.3.
27. D I S O R D E R S O F T H E T H Y R O I D G L A N D 415
Box 27.3 SYMPTOMS AND SIGNS OF HYPOTHYROIDISM Subclinical hypothyroidism is present when thyrotropin is
elevated but T4 is normal; therapy depends on the degree
Symptoms of thyrotropin elevation.
Fatigue Secondary hypothyroidism is present when T4 is low but
Cold intolerance thyrotropin is low or normal. Magnetic resonance imaging
Muscle cramps of the head and pituitary function tests should be done.
Mental slowing
Constipation
Signs
THERAPY
Coarse skin
Dry hair Thyroid hormone replacement therapy is initiated with
Weight gain synthetic T4 (levothyroxine). The goals of therapy are to
Periorbital puffiness normalize thyrotropin in primary hypothyroidism and
Delayed ankle reflex to normalize T4 in secondary hypothyroidism. Failure to
normalize thyrotropin concentrations may indicate poor
Macrocytic anemia (due to pernicious anemia or autoim- adherence to drug therapy, decreased absorption due to
mune disease) or microcytic anemia (iron deficiency due to concomitant use of interfering medications (eg, sucralfate,
menorrhagia) may be present. Patients with dramatic increases calcium supplements, ferrous sulfate), or gastrointestinal
in thyrotropin may experience galactorrhea (thyrotropin stim- tract disease. Other possibilities include progressive thyroid
ulates prolactin secretion). Rarely, patients may have psycho- disease, increased thyroid-binding proteins (as with preg-
sis, deafness, or cerebellar ataxia (or any combination of these). nancy or estrogen use), and increased hormone clearance
If patients have respiratory depression, central hypoventila- (eg, with phenytoin or carbamazepine). It is important to
tion and apnea may be observed. Hyponatremia due to syn- assess thyrotropin annually or as indicated by the patients
drome of inappropriate secretion of antidiuretic hormone symptoms.
may be present. Associated laboratory findings include hyper-
lipidemia and increased levels of aspartate aminotransferase, In primary hypothyroidism, the goal of therapy is to
lactate dehydrogenase, or creatine kinase. The possibility of normalize thyrotropin.
associated endocrinopathies as part of a polyglandular auto- In secondary hypothyroidism, the goal of therapy is to
immune syndrome (Addison disease, type 1 diabetes mellitus, normalize T4.
hypoparathyroidism, or pernicious anemia) should be consid-
ered when hypothyroidism is identified. It may also be associ- When thyrotropin cannot be normalized, possible causes
ated with vitiligo and other autoimmune or connective tissue include poor adherence to drug therapy, decreased drug
diseases. absorption, gastrointestinal tract disease, progressive
thyroid disease, use of other drugs leading to increased
Symptoms of hypothyroidism, when present, are generally hormone clearance, and states of increased thyroid-binding
nonspecific. protein availability.
Hypothyroidism may be associated with a polyglandular
autoimmune syndrome, other autoimmune diseases, or M I S C E L L A N EO US C I RCUM S TA N C E S
connective tissue diseases.
T4 Replacement Therapy in Pregnancy
D I AG N O S I S Most women with primary hypothyroidism require an
increase in the dose of levothyroxine during pregnancy (aver-
Low T4 and increased thyrotropin levels are diagnostic of age increase, 25%-30%). Women receiving T4 replacement
overt primary hypothyroidism if nonthyroid illness has been therapy should be counseled about the importance of ensur-
excluded. Subclinical hypothyroidism is identified when the ing adequate replacement before conception because of the
thyrotropin level is elevated, but the T4 level is normal. The multiple potential complications for both mother and fetus,
decision to treat depends on the degree of thyrotropin eleva- including first-trimester spontaneous abortion, preterm deliv-
tion. Hashimoto thyroiditis is usually associated with a firm ery, and perinatal morbidity and mortality. Thyrotropin lev-
goiter and a high titer of antimicrosomal (thyroid peroxidase) els should be assessed periodically during pregnancy, and the
antibodies. A low T4 and inappropriately normal or low thy- T4 dose should be adjusted as necessary to maintain a normal
rotropin indicate secondary hypothyroidism. Magnetic reso- thyrotropin.
nance imaging of the head and pituitary function tests should
be performed.
The levothyroxine dose usually needs to be increased
during pregnancy.
Increased thyrotropin with low T4 is diagnostic of primary
hypothyroidism in the absence of nonthyroid illness as a Adequate T4 replacement therapy before conception is
potential cause. important, and patients require counseling.
416 E N D O C R I N O L O GY
T4 Replacement Therapy in Patients With Cardiac detected during a routine medical examination, or detected
Disease and in Elderly Patients during neck imaging performed for other reasons. When
nodules are identified, the primary concern is whether they
Replacement therapy for elderly patients and patients who are benign or malignant. At least 95% of palpable thyroid
have coronary artery disease should start at a low dose (2550 nodules are benign. The likelihood of malignancy increases
mcg daily) and increase gradually until thyrotropin is normal. with solitary nodules, older age, male sex, and a history
Hypothyroidism does not contraindicate cardiac interven- of radiotherapy to the head and neck (especially during
tion, although there is an increased risk of hyponatremia and childhood).
other perioperative complications.
Factors increasing the likelihood of malignancy include
For elderly patients and patients with cardiac disease, solitary nodule, older age, male sex, and a history of head
initiate low-dose thyroid hormone replacement therapy, and neck radiotherapy.
and gradually increase the dose until thyrotropin is normal.
Cardiac interventions are not contraindicated in patients Evaluation should begin with thyrotropin measurement
with hypothyroidism, but patients should be assessed for to determine whether the nodule functions autonomously.
hyponatremia and other perioperative complications. Malignancy is substantially less likely if the thyrotropin level is
suppressed, in which case ultrasonography of the thyroid and
Subclinical Hypothyroidism RAIU should be performed. A nonautonomous nodule should
be sampled by ultrasound-guided FNA if the nodule is palpa-
Subclinical hypothyroidism is a relatively common disorder, ble or larger than 1 cm. Thyroid nodule FNA has high sensitiv-
affecting 5% to 15% of elderly patients. The risk of progres- ity and specificity for excluding malignancy if performed and
sion to overt hypothyroidism increases with age, the presence interpreted by experienced personnel. If the aspirate is benign,
of thyroid antibodies, and thyrotropin levels greater than 10 annual follow-up with palpation, thyroid ultrasonography,
mIU/L. A trial of replacement therapy is indicated for symp- and thyrotropin measurement is adequate. A change in nodule
tomatic patients and for patients at risk of progressive disease. size requires consideration of another biopsy. A nondiagnostic
aspirate requires additional aspiration. If the aspirate is inter-
Risk of progression to overt hypothyroidism increases preted as suspicious or compatible with malignancy, surgical
with age, the presence of thyroid antibodies, and elevated intervention is required. Compressive symptoms (dysphonia,
thyrotropin levels. dysphagia, and dyspnea) should prompt surgical intervention
even if the nodule is benign.
Symptomatic patients and patients at risk of progressive
disease should receive a trial of replacement therapy.
A thyroid nodule is likely benign if the thyrotropin level is
suppressed.
Myxedema Coma
RAUI and thyroid ultrasonography should be performed
Myxedema coma is severe, life-threatening hypothyroidism. when the nodule is autonomous.
It occurs in patients who have severe, untreated hypothyroid-
ism with a superimposed acute illness (eg, infection, surgery, Nonautonomous nodules should be sampled by FNA if
or myocardial infarction), exposure to cold, or the use of they are palpable or >1 cm.
sedatives or opiates. The onset is insidious, with progressive Surgical intervention should be undertaken if FNA
stupor culminating in coma. Seizures, hypothermia, hypoten- findings are suspicious or compatible with malignancy, or
sion, hypoventilation, hyponatremia, and hypoglycemia may if the patient has compressive symptoms even if the nodule
be present. The mortality rate is high (20%-50%). Treatment is benign.
should be initiated promptly with intravenous T4 and sup-
portive measures.
THYROID CANCER
Patients with myxedema coma become progressively
stuporous and eventually lapse into a coma.
D I F F E R E N T I AT E D T H Y RO I D M A L I G NA N C I E S
Seizures, hypothermia, hypotension, hypoventilation,
hyponatremia, and hypoglycemia are possible findings. Papillary Thyroid Carcinoma
Mortality is high, and treatment with intravenous T4 and Papillary thyroid carcinoma is the most common type of thy-
supportive therapy must be initiated promptly. roid cancer (80%-90% of cases). It has a bimodal incidence
distribution, with increased incidence in early adulthood and
again in late adulthood. Dissemination is typically lymphatic.
THYROID NODULES Lung and bone metastases may occur. Usually found as a thy-
roid nodule, papillary thyroid carcinoma may also manifest as
Thyroid nodules are extremely common and increase in cervical adenopathy or as an incidental finding in an excised
frequency with age. They may be noticed by the patient, thyroid gland.
27. D I S O R D E R S O F T H E T H Y R O I D G L A N D 417
Follicular Carcinoma resection, extensive local invasion, large size of primary tumor,
and presence of distant metastases. Cervical lymph node
Follicular carcinoma is the diagnosis in 10% to 15% of thyroid involvement does not affect prognosis.
cancer cases. It typically spreads hematogenously. The usual
manifestation is a thyroid mass or metastases to the lungs,
Differentiated thyroid cancers and medullary thyroid
bones, or brain. Rarely, it causes thyrotoxicosis if the tumor
cancer should be treated surgically.
burden is large.
Papillary thyroid cancer carries the best prognosis of all
Papillary thyroid cancer has a bimodal incidence thyroid malignancies.
distribution: early and late adulthood.
Poor prognostic indicators include age greater than
Follicular carcinoma usually manifests as a thyroid mass or 45 years, incomplete resection, extensive local invasion,
metastases to the lung, bones, or brain. large size of primary tumor, and distant metastases.
418 E N D O C R I N O L O GY
Avoid thyroid testing in the inpatient setting unless S U M M A RY
patients have clinical features suggestive of intrinsic thyroid
disease. Primary causes of hyperthyroidism are related to increased
production and release of T4 (high-RAIU causes) or
unregulated release of T4 because of gland destruction
A M I O DA RO N E A N D T H E T H Y RO I D (low-RAIU causes).
With its high iodine content, amiodarone causes thyroid dys- Graves disease is the most common thyroid-related cause of
function in about 15% of patients; amiodarone-associated hyperthyroidism in the United States.
thyroid dysfunction is more likely in patients with thyroid
Biochemical parameters establish the diagnosis and lead to
abnormalities. The most common abnormality in iodine-
the cause of hyperthyroidism.
replete geographic areas is hypothyroidism. Hyperthyroidism
may be caused by an increase in thyroid hormone production Thyroid storm is a medical emergency with multisystem
(type 1) or a destructive thyroiditis (type 2). Medical therapy manifestations: delirium, fever, tachycardia, hypotension,
is less effective than for other causes of hyperthyroidism; in diarrhea, vomiting, and coma.
some cases, thyroidectomy is needed. Periodic monitoring of
Causes of hypothyroidism include radioactive iodine
thyroid function is essential for patients treated with amio-
treatment, thyroidectomy, radiotherapy for neck cancers,
darone, particularly elderly patients.
and subacute or painless thyroiditis, which causes transient
hypothyroidism.
Amiodarone may lead to thyroid dysfunction due to its
high iodine content. In primary hypothyroidism, the goal of therapy is to
normalize thyrotropin; in secondary hypothyroidism, the
Hyperthyroidism due to amiodarone may occur because
goal of therapy is to normalize T4.
of increased thyroid hormone production (type 1) or
destructive thyroiditis (type 2). A thyroid nodule is likely benign if the thyrotropin level is
suppressed.
Thyroidectomy may be needed to treat hyperthyroidism
since medical therapy is often less effective for Papillary thyroid cancer carries the best prognosis of all
amiodarone-induced hyperthyroidism. thyroid malignancies.
27. D I S O R D E R S O F T H E T H Y R O I D G L A N D 419
28.
LIPID DISORDER S AND DIABETES MELLITUS
Maria L. Collazo-Clavell, MD
Hyperlipidemia can be secondary to drugs or diseases. The Third Adult Treatment Panel of the National Cholesterol
Education Program recommends that adults older than 20
Hyperlipidemia may be genetic or acquired (or both). years be evaluated for hypercholesterolemia. LDL-C con-
centrations can be reliably estimated if plasma triglyceride
C L I N I C A L F E AT U R E S concentrations are less than 400 mg/dL. Nonmodifiable risk
factors for CHD include the following:
Hyperlipidemia is usually diagnosed on screening. Patients
usually do not have physical findings directly attributable 1. Age older than 45 (men) or 55 (women)
420
Table 28.1 FEATURES OF PRIMARY HYPERLIPIDEMIAS
SEVERE HYPERTRIGLYCERIDEMIA
FAMILIAL HYPERCHO- FAMILIAL COMBINED FAMILIAL DYSBETALIPO- FAMILIAL
FEATURE LESTEROLEMIA HYPERLIPIDEMIA PROTEINEMIA HYPERTRIGLYCERIDEMIA Early Onset Adult Onset
Pathophysiology Defective LDL receptor Overproduction of Defective or absent apo E; Overproduction of hepatic Lipoprotein lipase Overproduction of hepatic
or defective apo B-100; hepatic VLDL excess of CM remnants VLDLTg but not of apo deficiency VLDLTg
impaired catabolism of apo B-100 but not & VLDL in fasting state B-100 Apo C-II deficiency; Delayed catabolism of CMs
LDL of VLDL-Tg defect in CM & VLDL & VLDL
catabolism
Mode of Autosomal codominant Autosomal dominant Autosomal recessive Autosomal dominant Autosomal recessive Autosomal recessive
inheritance
Physical findings Arcus senilis Arcus senilis Arcus senilis None Lipemia retinalis Milky plasma
Tendinous xanthomas Tuberoeruptive & palmar Eruptive xanthomas Lipemia retinalis
xanthomas Eruptive xanthomas
Pancreatitis
Abbreviations: apo, apolipoprotein; CHD, coronary heart disease; CM, chylomicron; HDL-C, high-density lipoprotein cholesterol; LDL, low-density lipoprotein; Tg, triglyceride; VLDL, very low-density lipoprotein; +++, very
high; ++, high; +, moderate; , no increased risk.
Box 28.1 CAUSES OF SECONDARY HYPERLIPIDEMIA THERAPY
Lp(a) lipoprotein is an independent risk factor for vascular Limiting dietary fat intake, exercising regularly,
disease and should be measured in patients with a strong fam- and achieving and maintaining a healthy weight are
ily history of premature ischemic heart disease without con- cornerstones of lipid management.
ventional risk factors and in patients with established CHD
with disease progression despite control of conventional risk
factors.
D RU G T H E R A P Y
The decision to measure Lp(a) lipoprotein should be based Drug therapy for hyperlipidemia usually needs to be continued
on individual patient risk factors. indefinitely and thus should be initiated only after vigorous
422 E N D O C R I N O L O GY
Table 28.2 OVERVIEW OF THERAPY FOR HYPERLIPIDEMIA a
INITIATE THERAPEUTIC
CLINICAL RISK ASSESSMENT LIFESTYLE CHANGES CONSIDER DRUG THERAPY GOAL OF THERAPY
No CHD; <2 risk factorsb 160 mg/dL 190 mg/dL (160189 mg/dL: drug optional) <160 mg/dL
No CHD; 2 risk factors (10-y risk 20%) 130 mg/dL 10-y risk 10%-20%: 130 mg/dL <130 mg/dL
10-y risk <10%: 160 mg/dL
CHD or CHD risk equivalents (10-y risk 100 mg/dL 130 mg/dL (100129 mg/dL: drug optional)c <100 mg/dL
>20%)
Very high risk 100 mg/dL 130 mg/dL <70 mg/dL
efforts at dietary and lifestyle modification. Appropriate life- intolerance or diabetes mellitus is common in patients with
style modifications must be continued. The teratogenic hypertriglyceridemia, and insulin treatment may be help-
potential of most of these drugs should be considered when ful. Omega-3 fatty acids (docosahexaenoic acid [DHA] and
prescribing for women of childbearing age. Patients should eicosapentaenoic acid [EPA]) effectively reduce triglycer-
be monitored for potential side effects and for the efficacy of ides. Prescription formulations are nearly 100% omega-3
the medication in reaching the predetermined goals. Lipid fatty acid, allowing for more effective dosing compared with
concentrations should be checked approximately 3 months over-the-counter formulations.
after therapy is started. Modification of lipid-lowering therapy
may be warranted if goals are not met. Combination ther-
T R E AT M E N T O F L OW H D L- C
apy may need to be considered for some patients, especially
for secondary prevention, including CHD risk equivalents. In the absence of heart disease, lifestyle modification is
Combination therapy should be reserved for secondary pre- the intervention of choice. The use of drugs that can lower
vention in established cardiovascular disease because of the HDL-C (eg, androgens) should be discontinued when pos-
risk of myositis and hepatitis. sible. Niacin, statins, and, to a lesser extent, fibrates increase
HDL-C.
T R E AT M E N T O F I N C R E A S E D L D L- C
T R E AT M E N T O F I N C R E A S E D L P(A)
A statin is usually the drug of choice for elevated LDL-C. In
L I P O P ROT E I N
estrogen-deficient women, estrogen replacement therapy is
effective in decreasing LDL-C and increasing HDL-C, and it Niacin may produce some modest decrease, but there is no
is appropriate for women until menopause; however, estrogen proven treatment for increased Lp(a) lipoprotein. Consider
replacement therapy may increase the risk of cardiovascular lowering LDL-C to less than 100 mg/dL in these patients.
events, at least among women at high risk. There is insufficient
evidence on whether ezetimibe or a resin reduces cardiovas- Drug therapy should be reserved for patients with
cular event risk. Niacin reduces LDL-C levels, but side effects insufficient lipid lowering after therapeutic lifestyle
(flushing and worsening glucose tolerance) make it difficult to changes. Tailor the drug choice to the elevated lipid
tolerate. Flushing can be reduced by taking the drug 30 to 60 fraction and reserve combination therapy for patients with
minutes after low-dose aspirin. clear indications.
T R E AT M E N T O F H Y P E RT R I G LYC E R I D E M I A
D I A B ET E S M E L L I T U S
Extreme hypertriglyceridemia (>1,000 mg/dL) may cause
pancreatitis and thus requires treatment, including cessation ET I O L O GY A N D C L A S S I F I C AT I O N
of oral estrogen or alcohol use, improved control of diabetes,
and restriction of caloric intake, especially sources of simple Diabetes mellitus is characterized by increased levels of fast-
carbohydrates. Fibrates are the drugs of choice. Glucose ing and postprandial serum glucose and is the most common
2 8. L I P I D D I S O R D E R S A N D D I A B ET E S M E L L I T U S 423
metabolic disorder, affecting approximately 10% of the US physical stress. Severe dehydration and ketoacidosis may be
population. Type 1 diabetes mellitus (T1D) is characterized present.
by loss of function of insulin-producing beta cells of the islets T2D usually has a more insidious onset and is often
of Langerhans because of autoimmune destruction. Ten per- diagnosed during routine laboratory testing by the presence
cent to 20% of diabetic patients have T1D. T1D often mani- of glycosuria or hyperglycemia. Patients may report blurry
fests at a young age but can develop at any age. Approximately vision, myopia, recurrent skin infections, or candidal vagini-
one-third of patients with T1D present with acute hypergly- tis (females) or balanitis (males). Patients occasionally present
cemic symptoms or diabetic ketoacidosis. with chronic diabetic complications (eg, neuropathy, nephrop-
A complex interaction between genes and the environ- athy, retinopathy, or vascular disease) but without symptoms
ment leads to the development of T1D. Antibodies to islet of glucose intolerance. Polyuria, polydipsia, and polyphagia
cells or some constituent of the islets are frequently present may develop only at times of increased insulin resistance (eg,
and may help to differentiate T1D from type 2 diabetes mel- pregnancy, infection, or corticosteroid use). Patients occasion-
litus (T2D). A honeymoon period may occur soon after ally present with hyperosmolar nonketotic coma.
disease onset, with restoration of euglycemia. The duration of
this phase is highly variable, and all patients eventually require T1D has a rapid onset due to abrupt, severe insulin
insulin. deficiency, with polyuria, polydipsia, and weight loss
despite polyphagia, severe dehydration, and ketoacidosis.
T1D is characterized by immune destruction of the islets,
T2D has an insidious onset, and patients may present
leading to insulin deficiency.
with complications. Under certain conditions, polyuria,
Specific antibodies are frequently present in the early stages polydipsia, and polyphagia may develop.
of the disease.
All patients will require insulin at some point. D I AG N O S I S
T2D is characterized by abnormalities of insulin action The normal fasting plasma glucose concentration is less than
and insulin secretion in target tissues (eg, muscle and adipose 100 mg/dL. Impaired fasting glucose, or prediabetes, is defined
tissue). The ability of glucose itself to stimulate glucose uptake by fasting glucose values from 100 to 125 mg/dL. A glucose
and suppress glucose release is also defective. Suppression of tolerance test is not required for the diagnosis.
glucagon secretion after eating is also impaired, contribut-
ing to postprandial hyperglycemia. T2D is more common The diagnosis of diabetes mellitus is confirmed with the
among certain ethnic groups, and compared with T1D, the following:
pathogenesis of T2D has a significant genetic contribution.
Environmental factors contributing to obesity, and obesity a. Fasting plasma glucose values 126 mg/dL
itself, have a definite role in the development of the disease. documented on 2 occasions
b. Casual plasma glucose 200 mg/dL in the presence of
T2D is characterized by defective insulin action and classic symptoms of hyperglycemia
secretion.
c. Plasma glucose 200 mg/dL 2 hours after a 75-g oral
Obesity and environmental factors contributing to obesity glucose load
are important in T2D development.
d. Hemoglobin A1c values 6.5% documented on
T2D can occur at any age; certain ethnic groups are at 2 occasions (values of 5.7%-6.4% are consistent with
higher risk. impaired glycemia)
Secondary causes of diabetes include pancreatic disease, The diagnosis of gestational diabetes mellitus requires an
endocrinopathies, drugs or chemicals, and infections. Certain oral glucose tolerance test (see the Diabetes and Pregnancy
genetic syndromes are sometimes associated with diabetes (eg, section).
Down syndrome, Klinefelter syndrome, Turner syndrome).
Gestational diabetes mellitus is glucose intolerance that
develops or is first recognized in pregnancy. Therapy may THER APY FOR T1D
involve insulin or only dietary modification. Gestational dia-
betes mellitus may or may not persist after pregnancy. Insulin replacement is necessary for T1D treatment; oral
agents have no role in its management. Therapy is aimed at
preventing acute and chronic complications of diabetes while
C L I N I C A L F E AT U R E S allowing the patient to maintain a healthy and active lifestyle,
with optimal glycemic control and minimal hypoglycemia.
The onset of T1D is usually rapid, with weight loss, poly- Intensive insulin therapy requires considerable commitment
uria, and polydipsia due to abrupt, severe insulin deficiency. from the patient to self-monitor plasma glucose concentra-
Manifestation is often precipitated by infection or other severe tions and adjust the insulin dosage accordingly. Intensive
424 E N D O C R I N O L O GY
therapy with tight glycemic control prevents or markedly Glycemic goals are individualized according to the pres-
decreases the risks of chronic microvascular complications of ence of other disease (ischemic heart disease or cerebrovascu-
diabetes and reduces mortality. lar disease), diabetic complications, and the ability to perceive
An amylin analogue (pramlintide) can be used to manage hypoglycemia. For women with T1D who are considering preg-
both T1D and T2D. Amylin is a peptide that is cosecreted nancy, tight glucose control starting weeks to months before
with insulin by beta cells. It has several mechanisms for lower- pregnancy is critical to decrease the risk of birth defects. Tight
ing glucose levels, including delaying gastric emptying, regulat- glycemic control during pregnancy prevents macrosomia.
ing postprandial glucagon secretion, and decreasing appetite.
It is injected before meals of at least 250 kcal and always as an For T1D patients, intensive insulin therapy simulates
adjunct to insulin therapy. It shows modest efficacy at improv- normal insulin secretion with a combination of short- and
ing glycemic control (lowering hemoglobin A1c <1%), with long-acting insulin.
nausea being the most common side effect. Pramlintide ther-
apy is weight neutral and does not increase the risk of hypo- An insulin pump allows the patient to adjust basal insulin
glycemia. However, insulin doses should be decreased by 50% levels as needed.
when pramlintide therapy is initiated. Glucose and insulin management of T1D patients who are
considering childbearing or who are pregnant is essential to
An amylin analogue can be used as an adjunct to insulin prevent birth defects and other complications.
therapy, allowing insulin doses to be decreased by 50%.
Pramlintide therapy is weight neutral and does not cause G LYC E M I C G OA L S O F O P T I M A L T H E R A P Y
hypoglycemia.
The blood glucose target fasting level is 70 to 130 mg/dL, and
the target bedtime level is 100 to 140 mg/dL. Hemoglobin A1c
NU T R IT I O N should be less than 7.0%. Higher target levels are required for
Intake should allow for maintenance of a healthy weight, with patients at risk of hypoglycemia because of their inability to
10% to 20% of the total calories from protein, less than 30% recognize hypoglycemic symptoms.
of calories from fat (saturated fat <10%), and the remainder
from complex carbohydrates. Insulin doses for meals depend MO N ITO R I N G
on carbohydrate content of the meal. Patients are advised to
maintain a consistent intake of carbohydrates or adjust the Glucose concentration should be self-monitored 4 times
insulin dose according to carbohydrate intake at each meal dailybefore meals and at bedtime. If the patient has unex-
(carbohydrate counting). plained morning hypoglycemia or hyperglycemia, blood glu-
cose should be measured between 2 am and 4 am. Hemoglobin
E X E RC I S E A1c should be measured every 3 months.
2 8. L I P I D D I S O R D E R S A N D D I A B ET E S M E L L I T U S 425
A prudent exercise program facilitates weight reduction Glucagon-Like Peptide-1 (GLP1) analogues (exenatide, lira-
and improves insulin action, cardiovascular fitness, and glutide) augment insulin secretion and glucagon suppression
sense of well-being. in response to glucose. They also slow gastric emptying, reduce
appetite, and lead to moderate weight loss. They are approved
D RU G T H E R A P Y F O R T2D for use with metformin and sulfonylureas. Nausea and vomit-
ing occur in a substantial proportion of users early in therapy
Metformin is the first-line agent for managing T2D. It but often subside. Used in combination with sulfonylurea,
improves insulin-mediated glucose use in the liver. It is effec- these agents can lead to hypoglycemia. Although all the newer
tive as monotherapy and in combination therapy with other agents seem to be effective in improving hemoglobin A1c, the
glucose-lowering drugs. The main side effect is diarrhea. effect on clinical outcomes (vascular disease and microvascu-
Metformin provides multiple benefits, including less weight lar complications) is unknown. Generally, until more data are
gain compared with other oral agents and lower risk of CHD available, these agents should be reserved for patients whose
events and mortality. The risk of lactic acidosis had been a con- therapy with more traditional drugs has failed.
cern, but there is no reliable evidence that metformin increases Dipeptidyl-peptidase-4 (DPP4) inhibitors (sitagliptin,
this risk. Metformin may lead to vitamin B12 deficiency due to saxagliptin) potentiate the effect of GLP1 by inhibiting deg-
decreased absorption. The drug should generally be held when radation by DPP4. Glucose lowering occurs by enhancing
patients are hospitalized. Metformin is contraindicated in the GLP1-mediated insulin secretion. DPP4 inhibitors do not
presence of the following: have a strong effect on gastric emptying or food intake and are
considered weight neutral. They are associated with a lower
Renal impairment (creatinine 1.5 mg/dL for men and risk of hypoglycemia and are approved for use as monotherapy
1.4 mg/dL for women). and combination therapy with sulfonylureas, metformin, and
Cardiac or respiratory disease likely to cause central TZDs.
hypoxia or reduced peripheral perfusion.
Metformin is the preferred therapy for the patient with
History of lactic acidosis. T2D.
Severe infection that could lead to reduced tissue Sulfonylureas stimulate insulin secretion, so their efficacy
perfusion. depends on the presence of endogenous insulin secretion.
Liver disease. Hypoglycemia is the most important side effect.
Alcohol abuse with binge drinking. TZDs are associated with fluid retention, weight gain, and
osteoporosis.
Use of intravenous radiographic contrast agents.
Repaglinide and nateglinide are short acting and increase
Sulfonylureas are insulin secretagogues. Their efficacy insulin secretion; doses are taken before meals and skipped
depends on the presence of endogenous insulin secretion. when fasting.
Primary failure occurs in the absence of endogenous insulin GLP1 analogues are associated with weight loss and lower
secretion. Secondary failure occurs with progression of dis- risk of hypoglycemia except when used in combination
ease, when sulfonylureas become ineffective. The risk of hypo- with sulfonylureas.
glycemia from sulfonylureas increases with a longer-acting
sulfonylurea (glyburide) and in the presence of renal failure. DPP4 inhibitors promote GLP1-mediated insulin
Repaglinide and nateglinide have extremely short half-lives secretion and are associated with lower risk of
and act in a fashion similar to sulfonylureas. These agents are hypoglycemia. They are weight neutral.
taken before each meal, and the dose is skipped if the patient
misses a meal. Insulin is often reserved for patients with T2D when diet
Thiazolidinediones (TZDs) improve hepatic and peripheral and oral agents (monotherapy and combination therapy) pro-
insulin action and do not cause hypoglycemia. Pioglitazone vide inadequate glycemic control, for sick patients when oral
causes marked fluid retention, increasing the risk of heart fail- agents may be contraindicated, or for patients who require
ure, and should not be prescribed for patients who have con- rapid glycemic control. Insulin is preferred for patients who
gestive heart failure. Pioglitazone has not been associated with are pregnant, under perioperative care, or severely ill. Patients
other cardiovascular risks. Significant weight gain and osteo- with T2D often have some degree of meal-stimulated endog-
porosis have been reported with TZD use. enous insulin secretion, which allows treatment with sim-
-Glucosidase inhibitors (acarbose, miglitol) inhibit upper pler insulin regimens than for T1D. Once-daily injections of
intestinal glucosidases, limiting the conversion of complex intermediate-acting insulin in combination with an oral agent
carbohydrates to monosaccharides. Modest efficacy (lower- or twice-daily injections of intermediate-acting insulin are
ing hemoglobin A1c <1%) and significant gastrointestinal commonly used to manage T2D. Insulin therapy is associated
tract side effects (flatulence in 70% of users) limit clinical use. with some degree of weight gain in most patients. Insulin can
Glucose is necessary to treat hypoglycemia in patients taking also be given in combination with metformin. Patients who
an -glucosidase inhibitor. have a more severe insulin deficiency may use an intensive
426 E N D O C R I N O L O GY
insulin program, as in T1D. Intensive insulin therapy with AC U T E C O M P L I C AT I O N S O F D I A B ET E S
basal and bolus doses gives more flexibility with meal sched- MELLITUS
ules, while the split-mix regimen requires scheduled meals.
D I A B ET I C K ETOAC I D O S I S
Simple insulin regimens are useful for patients with T2D
who have had treatment failure with oral agents. Diabetic ketoacidosis may be the initial presentation in patients
with T1D. When diabetic ketoacidosis occurs in patients
Prescribe an intensive insulin program or a split-mix
with T2D, the patients usually also have infection, myocardial
program for patients with severe insulin deficiency.
infarction, or other major stresses. Diabetic ketoacidosis is
characterized by polyuria, polydipsia, dehydration, anorexia,
An amylin analogue (pramlintide) is also approved for nausea and vomiting, abdominal pain, tachypnea, mental
T2D patients receiving insulin therapy (see Therapy for obtundation, and coma. Physical findings include evidence of
T1D section). dehydration, decreased mentation, deep and rapid Kussmaul
respiration, and a characteristic breath odor (fruity odor of
H Y P O G LYC E M I A I N D I A B ET E S acetone). Diabetic ketoacidosis can be precipitated by a fail-
ure to take insulin or to increase the insulin dose and consume
Hypoglycemia may result from unplanned exercise, inappro- extra fluids during acute illness, infection, or other illness such
priate dosing of insulin, or inadequate carbohydrate intake. as myocardial infarction, pancreatitis, stroke, or trauma.
Patients with long-standing T1D are prone to hypoglycemia The diagnosis is based on the demonstration of moderate
unawareness due to repeated neuroglycopenia. Prevention or severe hyperglycemia, ketonemia, and metabolic acidosis.
of hypoglycemia has been shown to reverse or ameliorate Associated biochemical abnormalities include hyponatremia,
hypoglycemia unawareness in some patients. Hypoglycemia azotemia, and hyperamylasemia. Large body losses of electro-
can occur at night (nocturnal hypoglycemia) and may not be lytes occur, but often serum levels of potassium, phosphate,
apparent if glucose is checked at bedtime and at breakfast. and magnesium are normal. Concentrations of these ions
Patients may report symptoms such as nightmares, morning often decrease precipitously as the acidosis is corrected.
headache, or night sweats. Periodic monitoring of blood glu-
cose between 1 am and 3 am, especially if the patient is taking Diabetic ketoacidosis occurs with severe insulin deficiency
intermediate insulin in the evenings, is essential. Preventive and is often precipitated by intercurrent illness.
strategies include increasing the bedtime snack or modifying It may be the initial manifestation of T1D.
the insulin regimen.
In patients with long-standing T1D, inability to Diagnosis requires the presence of pronounced
secrete glucagon leads to defective counter-regulation and hyperglycemia, ketonemia, and metabolic acidosis.
patients become dependent on the autonomic nervous Serum levels of potassium and other electrolytes may be
system to respond to hypoglycemia. The use of -blockers normal despite large body losses; significant shifts can
in these situations can abolish warning palpitations with occur with correction of acidosis.
hypoglycemia.
Lower doses of insulin may be needed in patients with renal Precipitating factors should be identified and corrected.
impairment. Alcohol may interfere with gluconeogenesis and
the perception of hypoglycemic symptoms. Hypoglycemia
may also be a manifestation of cortisol deficiency (eg, Addison Treatment
disease or autoimmune hypophysitis).
Treatment of diabetic ketoacidosis requires administration of
Patients with T1D are especially prone to hypoglycemia. fluids and insulin to correct metabolic acidosis and electrolyte
depletion. Electrolyte levels should be carefully monitored
Episodes of severe hypoglycemia may occur during the and corrected and precipitating factors ameliorated. The aver-
nightcheck the blood glucose level between 1 am and 3 age fluid deficit in adults is 5 to 8 L. The risk of cerebral edema
am. is decreased through careful rehydration and correction of
ketoacidosis to avoiding a rapid decrease in osmolality.
Hypoglycemia may be precipitated by unplanned exercise,
Insulin infusion doses should be modified according to the
decreased carbohydrate intake, renal insufficiency, and
degree of glycemia and continued until the acidosis resolves.
cortisol deficiency.
This approach suppresses lipolysis and ketogenesis and stimu-
Insulin and sulfonylureas are associated with the highest lates glucose uptake.
risk of hypoglycemia. The potassium deficit is typically 300 to 500 mEq, reflect-
ing low total body stores. Serum potassium levels decrease
Metformin, TZDs, GLP1 analogues, and DPP4 inhibitors
with correction of the acidosis. Potassium should be added
are associated with less hypoglycemia.
to the intravenous fluids as soon as renal perfusion and urine
Hypoglycemia with use of -glucosidase inhibitors must be flow are assured. Phosphate repletion is indicated by phos-
treated with glucose. phate levels less than 1 mg/dL. The serum level of phosphate
2 8. L I P I D D I S O R D E R S A N D D I A B ET E S M E L L I T U S 427
must be monitored carefully owing to the risk of hypocalce- apparent during therapy. Complications include vascular
mia, seizures, and death. events such as myocardial infarction or stroke, cerebral edema,
The mortality rate is 5% to 15% among patients with coma and hypokalemia. The mortality rate can be up to 50%.
associated with diabetic ketoacidosis. For most patients, death
is due to an associated precipitating illness such as myocardial Treatment of hyperglycemic hyperosmolar nonketotic
infarction, stroke, or sepsis. After successful therapy, the goal coma includes fluid and electrolyte replacement and
is to avoid recurrence by educating the patient. management of hyperglycemia.
Hyperglycemic hyperosmolar nonketotic coma has a
Diabetic ketoacidosis is accompanied by significant fluid
significant mortality rate.
and electrolyte deficits that must be corrected while
avoiding serious complications of too rapid or excessive
replacement. C H R O N I C C O M P L I C AT I O N S O F
D I A B ET E S M E L L I T U S
H Y P E RG LYC E M I C H Y P E RO S MO L A R
N O N K ETOT I C C O M A M I C RO VA S C U L A R D I S E A S E I N D I A B ET E S
Hyperglycemic hyperosmolar nonketotic coma is character- The microcirculation is damaged by chronic hyperglycemia
ized by hyperglycemia and hyperosmolar dehydration with- and other metabolic abnormalities associated with diabetes.
out ketoacidosis. This typically occurs in poorly treated T2D Clinical manifestations include retinopathy, nephropathy,
when insulin levels are sufficient to inhibit excess lipolysis and and neuropathy. Diabetic retinopathy occurs in most patients
ketogenesis but not to suppress hepatic glucose production or with T1D within 10 years of diagnosis. Diabetic retinopathy
to stimulate glucose use. High concentrations of urinary glu- is present in 15% to 20% of patients at the time of diagnosis of
cose provoke an osmotic diuresis, with marked dehydration T2D and reaches 50% by 15 years. Background diabetic retin-
and decreased renal function. It is commonly precipitated by opathy is characterized by microaneurysms, hard exudates,
acute illness such as myocardial infarction, pancreatitis, infec- hemorrhages, and macular edema. Retinal ischemia leads to
tion, or surgery. proliferative retinopathy, stimulating the growth of new ves-
sels that are fragile and prone to hemorrhage; loss of vision
may result. It is treated with panretinal laser photocoagula-
Diagnosis tion. Patients should undergo a dilated ophthalmic exami-
Hyperglycemic hyperosmolar nonketotic coma should be nation annually. Treatment of hypertension, hyperglycemia,
suspected in any patient with diabetes who presents with glaucoma, and dyslipidemia is also important.
an altered level of consciousness and severe dehydration.
Laboratory abnormalities include hyperglycemia (blood Diabetic patients are at significant risk of neuropathy,
glucose often >600 mg/dL), absence of ketones, and plasma including peripheral and autonomic neuropathy,
hyperosmolarity (>320 mOsm/L). Always correct the under- and nephropathy, which often leads to chronic renal
lying disorder. impairment and renal failure.
Diabetes leads to microvascular disease and can cause
Hyperglycemic hyperosmolar nonketotic coma is
retinopathy, neuropathy, and nephropathy.
characterized by hyperglycemia and dehydration without
ketoacidosis.
I N FEC T I O NS A N D D I A B ET E S
The disorder should be suspected in any patient with
diabetes who has altered sensorium and severe dehydration. Skin infections can be a presenting feature of poorly con-
trolled T2D. They include carbuncles (Staphylococcus aureus),
Laboratory evaluation demonstrates marked hyperglycemia malignant external otitis (Pseudomonas), and, in diabetic
(>600 mg/dL), no significant ketosis, and plasma ketoacidosis, mucormycosis (Mucor species). Candidiasis
hyperosmolarity (>320 mOsm/L). and furunculosis also occur more frequently with poorly con-
Always search for and correct the precipitating disorder. trolled diabetes.
428 E N D O C R I N O L O GY
Persons with T2D have the same risk of myocardial infarct Early detection and optimal management of diabetes
as patients with prior myocardial infarction. Treatment of during pregnancy can prevent congenital malformations
dyslipidemia is therefore considered secondary prevention and decrease neonatal morbidity and mortality.
in this population. Patients with ischemic heart disease may
Gestational diabetes complicates 2%-3% of all pregnancies.
present with atypical symptoms; angina may manifest as epi-
gastric distress, heartburn, and neck or jaw pain. Myocardial All pregnant women older than 25 years should be
infarction may be silent (in 15% of patients), and patients evaluated at 2428 weeks.
may present with sudden onset of left ventricular failure.
Patients with diabetes have a higher risk of cerebrovascular
and peripheral arterial diseases, but the role of screening for T R E AT M E N T
vascular disease in asymptomatic patients with diabetes is Home monitoring for blood glucose and urine ketones is
uncertain. important in gestational diabetics. Postprandial glucose con-
centrations are closely associated with macrosomia and neo-
Diabetic patients have a significant risk of cardiovascular natal complications, so they are often used to guide therapy.
disease, and diabetes is considered a coronary heart disease The fasting blood glucose concentration should be between
risk equivalent. 60 and 90 mg/dL and the postprandial level should be 70 to
140 mg/dL (1 hour after a meal).
H Y P E R L I P I D E M I A I N D I A B ET E S Women with gestational diabetes who become euglycemic
in the postpartum state should institute lifestyle changes to
In poorly controlled T2D, the concentrations of prevent onset of T2D, and they should be periodically evalu-
triglyceride-rich lipoproteins are increased owing to overpro- ated. They are at high risk of T2D (diabetes develops in >50%
duction of VLDL and decreased lipoprotein lipase activity. within the 15 years after diagnosis of gestational diabetes) and
HDL-C levels are low, and control of glucose and triglyc- should be encouraged to exercise, consume an appropriate
eride levels leads to levels that are improved but usually not diet, and lose weight if appropriate.
normalized. Compositional changes in LDL (small, dense
LDL) that increase the atherogenicity of these particles are Periodic follow-up of patients with gestational diabetes is
more likely to occur in patients with T2D. Aggressive man- necessary because of the high incidence of T2D.
agement of hyperlipidemia and low HDL-C is warranted in
diabetic patients because they have a high risk of cardiovas-
cular disease. H Y P O G LYC E M I A I N N O N D I A B ET I C
PAT I E N T S
D I A B ET E S A N D P R E G N A N C Y
ET I O L O GY
Both fasting and postprandial glucose concentrations decrease Hypoglycemic disorders may be classified as insulin medi-
in normal pregnancy, and insulin secretion increases owing to ated and noninsulin mediated. Causes of insulin-mediated
increased levels of circulating hormones (eg, human placental hypoglycemia include insulinoma, sulfonylurea or exog-
lactogen, estrogen, progesterone, and cortisol), which increase enous insulin use, and autoimmune hypoglycemia mediated
insulin resistance. by insulin antibodies, which prevent insulin degradation.
Pregnancy is a diabetogenic state and may worsen glu- Noninsulin-mediated hypoglycemia may be related to drugs,
cose control in women with diabetes. Inadequate glycemic alcohol use, or cortisol insufficiency. Renal failure, liver failure,
control early in pregnancy increases the risk of congenital and sepsis are common causes of noninsulin-mediated hypo-
malformations; poor control in late pregnancy increases the glycemia in hospitalized patients. Insulinlike growth factor
risk of macrosomia, neonatal hypoglycemia, hypocalcemia, (IGF)-producing tumors, such as mesenchymal or epithelial
polycythemia, hyperbilirubinemia, and respiratory distress. tumors, may cause hypoglycemia.
Pregnancy may exacerbate diabetic retinopathy, and neph-
ropathy may lead to pregnancy-induced hypertension and
Insulin-mediated causes of hypoglycemia include
toxemia.
insulinoma, exogenous insulin use, sulfonylurea use, and
Gestational diabetes complicates 2% to 3% of all pregnan-
autoimmune hypoglycemia.
cies. All pregnant women older than 25 years should be evalu-
ated at 24 to 28 weeks with a 50-g oral glucose tolerance test. Noninsulin-mediated causes of hypoglycemia include
A glucose level higher than 140 mg/dL 1 hour after ingestion alcohol use, cortisol deficiency, renal failure, liver failure,
of the glucose drink should trigger formal testing with a 100-g sepsis, and tumors secreting IGF-2.
glucose drink. Gestational diabetes is diagnosed if the fasting
glucose is greater than 105 mg/dL and if the glucose is greater
C L I N I C A L FE AT U R E S
than 190 mg/dL at 1 hour, greater than 165 mg/dL at 2 hours,
and greater than 145 mg/dL at 3 hours. Earlier evaluations are Hypoglycemia may result in hyperadrenergic symptoms (palpi-
often needed for high-risk patients. tations, sweating, tremor, and nervousness) and neuroglycopenic
2 8. L I P I D D I S O R D E R S A N D D I A B ET E S M E L L I T U S 429
symptoms (confusion, inappropriate affect, blurred vision, diplo- P O S T P R A N D I A L H Y P O G LYC E M I A
pia, seizures, and loss of consciousness). Symptoms are relieved
Postprandial symptoms are not always caused by postprandial
promptly after oral carbohydrate intake. Patients with fasting
hypoglycemia. Postprandial hypoglycemia is defined as symp-
hypoglycemia often learn to reduce symptoms by increasing the
tomatic hypoglycemia occurring 1 to 5 hours after a meal.
frequency of their meals; as a result, they may gain weight.
Patients with noninsulinoma pancreatogenous hypoglycemia
syndrome can have postprandial hypoglycemia. The oral glu-
Hypoglycemia may cause symptoms related to activation of cose tolerance test is not reliable for diagnosing reactive hypo-
the sympathoadrenal system and neuroglycopenia. glycemia. Insulinoma usually causes fasting hypoglycemia.
D I AG N O S I S THERAPY
For all patients with suspected hypoglycemia, it is essential to Treatment is directed at correcting both the hypoglycemia
investigate the Whipple triad: low plasma glucose, symptoms and the underlying cause. For patients with serious hypo-
of hypoglycemia, and prompt resolution of symptoms after glycemia who cannot eat or drink, 1 mg of glucagon can be
normalization of plasma glucose level. administered to stimulate endogenous glucose production.
Alternatively, intravenous dextrose can be given, although this
Capillary blood glucose monitors should not be used to may be associated with superficial phlebitis and pain.
confirm hypoglycemia owing to inaccuracy.
Plasma insulin levels should be measured to determine the Injected glucagon may be used to treat hypoglycemia if the
mechanism of hypoglycemia; insulin is not appropriately oral route is not available.
suppressed in insulin-mediated causes of hypoglycemia.
C-peptide levels distinguish between exogenous and S U M M A RY
endogenous insulin; if the patient is injecting insulin,
C-peptide levels are undetectable. Hyperlipidemia can be secondary to drugs or diseases; it
can be genetic or acquired (or both).
C-peptide levels in endogenous hyperinsulinemic
hypoglycemia caused by insulinoma are indistinguishable Patients with hyperlipidemia are often asymptomatic.
from those in sulfonylurea use. Consequently, plasma The decision to measure Lp(a) lipoprotein should be based
sulfonylurea levels should be measured in all cases of on individual patient risk factors.
insulin-mediated hypoglycemia (while the patient is
hypoglycemic). Limiting dietary fat intake, exercising regularly,
and achieving and maintaining a healthy weight are
cornerstones of lipid management.
I NS U L I N O M A
Drug therapy should be reserved for patients with insufficient
Diagnostic criteria for insulinoma are plasma insulin level at lipid lowering after therapeutic lifestyle changes. Tailor
least 6 mU/mL and C peptide level at least 200 pmol/L when the drug choice to the elevated lipid fraction and reserve
plasma glucose is less than 50 mg/dL and plasma sulfonylu- combination therapy for patients with clear indications.
rea is undetectable. Ultrasonography and spiral computed
tomography of the pancreas are performed to identify and T1D has a rapid onset due to abrupt, severe insulin
localize the insulinoma; localization is successful in approxi- deficiency, with polyuria, polydipsia, and weight loss
mately 60% of cases. Arteriography and selective arterial cath- despite polyphagia, severe dehydration, and ketoacidosis.
eterization with calcium stimulation of insulin release identify
T2D has an insidious onset, and patients may present
the region of the pancreas that is the source of insulin. The
with complications. Under certain conditions, polyuria,
key to successful removal is surgical exploration of the pan-
polydipsia, and polyphagia may develop.
creas by an experienced surgeon combined with intraopera-
tive ultrasonography. Almost all insulinomas can be identified For T1D patients, intensive insulin therapy simulates
and excised in this manner. Patients with insulinoma who normal insulin secretion with a combination of short- and
decline surgical excision or who have persistent or recurrent long-acting insulin.
malignant insulinoma may be treated with diazoxide, which
The treatment goals for T2D include appropriate lifestyle
inhibits insulin secretion, but side effects (edema and malaise)
modification, cardiovascular risk factor modification, and
limit its tolerability.
optimal glycemic control.
Preoperative abdominal ultrasonography and spiral Metformin is the preferred therapy for the patient
computed tomography of the pancreas localize with T2D.
approximately 60% of insulinomas.
Diabetic ketoacidosis occurs with severe insulin deficiency
Intraoperative ultrasonography of the pancreas is a useful and is often precipitated by intercurrent illness. It may be
localization tool. the initial manifestation of T1D.
430 E N D O C R I N O L O GY
Diabetes leads to microvascular disease and can cause Hollander PA, Levy P, Fineman MS, Maggs DG, Shen LZ, Strobel
retinopathy, neuropathy, and nephropathy. SA, et al. Pramlintide as an adjunct to insulin therapy improves
long-term glycemic and weight control in patients with type 2 dia-
betes: a 1-year randomized controlled trial. Diabetes Care. 2003
Mar;26(3):78490.
Ratner RE, Dickey R, Fineman M, Maggs DG, Shen L, Strobel SA,
SUGGESTED RE ADING et al. Amylin replacement with pramlintide as an adjunct to insulin
therapy improves long-term glycaemic and weight control in Type 1
American Diabetes Association. Diagnosis and classification of diabetes diabetes mellitus: a 1-year, randomized controlled trial. Diabet Med.
mellitus. Diabetes Care. 2010 Jan;33 Suppl 1:S629. Erratum in: 2004 Nov;21(11):120412.
Diabetes Care. 2010 Apr;33(4):e57. Raz I, Hanefeld M, Xu L, Caria C, Williams-Herman D, Khatami H;
Bell DS. Metformin-induced vitamin B12 deficiency presenting as a Sitagliptin Study 023 Group. Efficacy and safety of the dipeptidyl
peripheral neuropathy. South Med J. 2010 Mar;103(3):2657. peptidase-4 inhibitor sitagliptin as monotherapy in patients with
Chiasson JL, Josse RG, Hunt JA, Palmason C, Rodger NW, Ross type 2 diabetes mellitus. Diabetologia. 2006 Nov;49(11):256471.
SA, et al. The efficacy of acarbose in the treatment of patients Epub 2006 Sep 26.
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2 8. L I P I D D I S O R D E R S A N D D I A B ET E S M E L L I T U S 431
29.
OBESIT Y
Maria L. Collazo-Clavell, MD
Identify complications of bariatric surgery and understand Implementation of healthy lifestyle changes is the key fac-
management strategies. tor to managing overweight and obesity. Dietary changes
with caloric restriction (by 250500 kcal daily) is needed to
Recognize when nutritional supplementation is
achieve weight loss. Macronutrient composition has minimal
appropriate (for micronutrients and macronutrients) and
impact on weight loss at 12 months. Regular physical activity
the role of different routes of administration.
promotes weight loss by creating an additional caloric deficit
but is insufficient alone. However, regular physical activity is a
key determinant to maintaining weight loss.
INTRODUCTION Achieving an initial weight loss goal of 5% to 10% of initial
body weight is associated with multiple benefits, including pre-
Body mass index (BMI) (calculated as weight in kilograms vention of type 2 diabetes mellitus. Predictors of weight loss suc-
divided by height in meters squared) is used to assess the health cess include having a higher initial body weight, engaging in more
risk of body weight. Waist circumference (WC), another vari- minutes of physical activity weekly, recording caloric intake, and
able used to predict health risk, is a surrogate for visceral fat. participating in group behavioral therapy. Considerable weight
WC is most useful for persons who have a BMI between 25 loss occurs with aggressive dietary restriction (very low-calorie
and 35. Persons who have an increased BMI in combination diets of <800 kcal daily) and bariatric surgery. With very
with an increased WC, which indicates excess visceral fat, have low-calorie diets, the prevalence of weight regain is high.
a greater health risk than if the BMI alone is increased. BMI val-
ues greater than 35 are associated with high health risk anyway,
Caloric restriction of 250500 kcal daily is the main
so in that BMI range, WC is less meaningful (Table 29.1).
determinant of successful weight loss.
The prevalence of overweight and obesity continues to
increase in the United States and the westernized world. Macronutrient composition without calorie restriction has
Many factors contribute to overweight and obesity, particu- no significant impact.
larly excess caloric intake and low physical activity. Additional
Initial weight loss of 5%-10% of initial body weight is
risk factors include smoking cessation, sleep deprivation, con-
recommended.
tributory social networks, lower socioeconomic status, medi-
cations, and, less commonly, health conditions. Predictors of success include having a higher initial weight,
engaging in more minutes of physical activity weekly,
recording caloric intake, and participating in group
H E A LT H R I S K A S S E S S M E N T behavioral therapy.
432
Table 29.1 BODY MASS INDEX, WAIST CIRCUMFERENCE, AND HEALTH RISK
HEALTH RISK
BMI
BMI CLASSIFICATION WC BMI Alone BMI + WC
<18.5 Underweight
18.524.9 Normal
Abbreviations: BMI, body mass index (calculated as weight in kilograms divided by height in meters squared); WC,
waist circumference in centimeters.
Adapted from National Institutes of Health, National Heart, Lung, and Blood Institute, North American Association
for the Study of Obesity. The practical guide: identification, evaluation, and treatment of overweight and obesity in
adults. Bethesda (MD): National Institutes of Health; c2000. NIH Publication No. 00-4084.
are phentermine and orlistat. Medications are generally reserved it is associated with greater weight loss than placebo. The main
for patients who are obese (BMI 30.0) or overweight (BMI side effects involve the gastrointestinal tract; diarrhea and flat-
25.029.9) and have weight-related medical complications. ulence often limit compliance. A daily multivitamin is recom-
Phentermine is a sympathomimetic agent that suppresses mended to prevent vitamin deficiencies. Concurrent use with
appetite. Few long-term studies (>12 weeks) have been per- medications influenced by fat absorption (eg, cyclosporine,
formed, and there are insufficient data detailing efficacy and amiodarone, warfarin) can limit the efficacy of those drugs.
safety. It has not been implicated in the development of cardiac
valve abnormalities and pulmonary hypertension. Patients pre- Medications for weight loss are reserved for patients
viously treated with fenfluramine or dexfenfluramine should who meet criteria for obesity or overweight and have
be evaluated for cardiac valve abnormalities. Sibutramine was weight-related medical problems.
removed from the market after it was reported to increase the risk
of nonfatal heart attacks and stroke in a high-risk population. There are insufficient long-term data on the efficacy and
Orlistat is a lipase inhibitor that limits dietary fat absorp- safety of phentermine.
tion. Administered with a low-fat diet (fat <30% of calories), Patients with a history of fenfluramine or dexfenfluramine
use should be evaluated for cardiac valve abnormalities.
Orlistat limits dietary fat absorption and should be used
Box 29.1 HEALTH RISKS ASSOCIATED WITH OBESITY
along with a low-fat diet. Patients should take a daily
multivitamin.
Type 2 diabetes mellitus
Hypertriglyceridemia Orlistat can limit the efficacy of medications influenced by
Hypertension fat absorption.
Obstructive sleep apnea
Coronary artery disease
B A R I AT R I C S U R G E RY
Congestive heart failure
Atrial fibrillation
The indications for bariatric surgery include the following:
Thromboembolic disease
Degenerative joint disease a. BMI >40 or
Gastroesophageal reflux disease
b. BMI >35 and weight-related medical comorbidities,
Nonalcoholic steatohepatitis
documented efforts at medically supervised
Cancer
weight management, absence of psychologic
Death
contraindications, and life expectancy >5 years
29. O B E S I T Y 433
Mechanisms for weight loss after bariatric surgery vary. NU T R IT I O N A F T E R BA R I AT R I C S U RG E RY
They include the following:
Nutritional deficiencies are recognized complications of
bariatric surgery; therefore, empirical vitamin supplementa-
1. Dietary restrictionvertical banded gastroplasty, tion is recommended for all patients after surgery and should
laparoscopic adjustable gastric banding include vitamin B12, a multivitamin, and calcium with vita-
2. A combination of restriction and maldigestion min D.
Roux-en-Y gastric bypass (RYGB) After any bariatric procedure, acute thiamine deficiency
can occur in a patient who is vomiting and cannot maintain
3. Malabsorptionbiliopancreatic diversion with a adequate oral intake over several days. In addition to gastro-
duodenal switch (BPD-DS) intestinal tract symptoms, neurologic complaints are com-
mon. Wernicke-Korsakoff encephalopathy may occur, so
The most commonly performed operation is the RYGB, and thiamine must be supplemented before intravenous infusion
data have demonstrated its beneficial effects, including pre- of dextrose-containing fluids.
vention and resolution of type 2 diabetes mellitus. Resolution
rates have been reported for other medical problems, includ-
ing obstructive sleep apnea, gastroesophageal reflux disease, Bariatric surgery patients should receive vitamin B12, a
hypertriglyceridemia, and hypertension. Restrictive opera- multivitamin, and calcium with vitamin D.
tions are generally associated with less weight loss and lower Acute thiamine deficiency should be suspected in the
resolution rates for most obesity-related complications, and patient who, within weeks after bariatric surgery, presents
BPD-DS is associated with the greatest reported weight loss with severe nausea and vomiting of several days duration.
and the greatest effect on the complications of excess weight.
Anemia is the most common manifestation of deficiencies
Several bariatric procedures are being used with very low of iron, vitamin B12, or folate and normalizes with appropriate
overall perioperative mortality. supplementation. Iron deficiency anemia is the most common
Weight loss after surgery leads to reduction and possible vitamin deficiency reported, especially among menstruat-
resolution of obesity-related health problems. ing women. Folate and vitamin B12 deficiencies are less com-
mon owing to empirical supplementation, but a high index
of awareness is needed owing to variable adherence to vita-
E A R LY C O M P L I C AT I O NS O F BA R I AT R I C
min supplementation regimens. Neurologic complications
S U RG E RY
resulting from vitamin B12 deficiency may not resolve. Care
Perioperative mortality is reported as less than 1%. The most must be taken to assess folate status before supplementation.
common cause of death is pulmonary embolism. Anastomotic Measuring the ferritin level is a reliable screening test for iron
leak with subsequent peritonitis is the second most common deficiency. Low vitamin B12 levels should be confirmed with a
cause of death for RYGB and BPD-DS. A high index of aware- methylmalonic acid level.
ness is critical when assessing an ill patient presenting with
dyspnea or abdominal pain within weeks after a bariatric opera- Iron deficiency anemia is the most common nutritional
tion. Sinus tachycardia is the most common physical finding in deficiency after bariatric surgery, particularly among
patients with an anastomotic leak. Risk factors associated with menstruating women. Measuring the ferritin level is the
higher perioperative morbidity and mortality are male sex, age recommended screening test.
older than 60 years, BMI greater than 60, smoking, untreated
Vitamin B12 deficiency is less common owing to empirical
obstructive sleep apnea, inactivity, and surgeon inexperience.
supplementation, but it should be suspected in patients
Anastomotic complications are also common after
who have a history of bariatric surgery and present with
RYGB. Anastomotic ulcerations and stricture of the gas-
macrocytic anemia. Folate status should be checked before
trojejunal anastomosis are the most common. Risk factors
vitamin B12 supplementation begins.
include use of nonsteroidal anti-inflammatory drugs, prior
Helicobacter pylori infection, and smoking. Presenting symp-
Inadequate diet, inadequate supplementation, and, often,
toms include epigastric pain with or without nausea and vom-
persistent gastrointestinal tract symptoms such as diarrhea
iting. Esophagogastroduodenoscopy is the diagnostic study
can lead to chronic nutritional deficiencies. Vitamin D defi-
of choice; balloon dilation of a stricture can be performed.
ciency is common among obese patients seeking bariatric sur-
Anastomotic ulcers are effectively treated with proton pump
gery and may worsen during rapid weight loss after surgery.
inhibitors with or without sucralfate.
Hypocalcemia is a late finding and is often absent with mild
or moderate deficiencies. The most common early findings
The most common causes of death after bariatric surgery
may be increased parameters of bone turnover (bone alkaline
are pulmonary embolism and anastomotic leaks.
phosphatase) and secondary hyperparathyroidism with an
If a patient presents with epigastric pain, nausea, and elevated parathyroid hormone level. Secondary hyperpara-
vomiting after bariatric surgery, anastomotic ulceration or thyroidism is also influenced by decreased dietary calcium.
stricture should be suspected. Calcium deficiency can be detected early only by identifying
434 E N D O C R I N O L O GY
hypocalciuria in a 24-hour urine collection. Long-term vita- Reported complications of RYGB and BPD-DS include
min D deficiency can lead to metabolic bone disease with renal stone disease with predominantly calcium oxalate
low bone mineral density or mineralization defects (or both) stones and rarely insulin-mediated hypoglycemia.
resulting in osteomalacia.
Other fat-soluble vitamin deficiencies (ie, vitamin A or E
deficiency) are less common but may occur. Vitamin A defi- NUTRITION
ciency is associated with night blindness. Protein malnutri-
tion is a worrisome complication of BPD-DS, which must be Ideal weight is reflected by BMI values from 18.5 to 24.9.
reversed in 1% to 2% of patients. Persons with BMI values less than 18.5 are considered under-
weight, and the risk of morbidity and mortality increases with
Vitamin D and calcium deficiencies are common in the BMI values less than 15.
obese population and can worsen after bariatric surgery. An optimal diet should provide the caloric requirements
to maintain a weight within an ideal BMI range and minimize
Malabsorptive operations (BPD-DS) carry the highest risk the risk of illness. High intakes of fruits and vegetables have
of fat-soluble vitamin and protein malnutrition. been consistently shown to provide multiple health benefits,
particularly in lowering the risk of cardiovascular disease
(Box 29.2).
L AT E C O M P L I C AT I O NS O F BA R I AT R I C
S U RG E RY
M I C RO N U T R I E N T S U P P L E M E N TAT I O N
Cholelithiasis develops in one-third of patients; 40%
become symptomatic. Prophylactic cholecystectomy was Multivitamin supplementation has not been shown to
commonly performed at bariatric surgery when it was provide health benefits to the population at large, and it
an open abdominal operation (before the laparoscopic is recommended only for persons not meeting their nutri-
approach became common). Administration of ursode- tional needs orally owing to illness or self-imposed dietary
oxycholic acid for 6 months after surgery decreases the restriction.
prevalence of gallstone development and is gaining popu- The benefits of empirical vitamin supplementation have
larity. Therefore, prophylactic cholecystectomy is no lon- been reported for folic acid in women of childbearing age
ger indicated. (to prevent neural tube defects) and for vitamin D to prevent
Bacterial overgrowth is common after RYGB and metabolic bone disease.
BPD-DS. Abdominal pain and bloating associated with diar- Empirical supplementation of antioxidant vitamins (beta
rhea are common symptoms. Esophagogastroduodenoscopy carotene and vitamin E) to prevent cardiovascular disease is
with small bowel aspirates for culture or breath tests are usu- no longer advised owing to a lack of benefit and the potential
ally diagnostic. When bacterial overgrowth is suspected or risk of lung cancer in smokers and patients who have a history
confirmed, antibiotic therapy should be instituted; various of asbestos exposure. Folic acid supplementation to decrease
regimens are available. Resolution of symptoms occurs within homocysteine levels is no longer advised owing to a lack of
1 week. Bacterial overgrowth can recur, worsening the mal- benefit in preventing cardiovascular disease.
absorption of nutrients and increasing the risk of vitamin -3 Fatty acid (docosahexaenoic acid [DHA] and eicosap-
deficiencies. entaenoic acid [EPA]) supplementation lowers cardiovascular
Other complications include renal stone disease (primar- mortality. Eating at least 1 serving of a fatty fish (rich in -3
ily calcium oxalate stones). Fat malabsorption and dietary fatty acids) weekly or supplementing with DHA and EPA is
calcium allow increased absorption of intestinal oxalate, beneficial, with studies suggesting that antiarrhythmic proper-
increasing the risk of calcium oxalate stone formation. ties contribute to a lower risk of cardiovascular death. Higher
Insulin-mediated hypoglycemia may occur in patients who doses lower triglyceride levels.
have postprandial symptoms that suggest hypoglycemia.
Symptoms may be difficult to differentiate from those of Box 29.2 DIETARY GUIDELINES TO DECREASE THE
classic dumping. Further evaluation requires documentation RISK OF CARDIOVASCULAR DISEASE
of hypoglycemia (blood glucose <55 mg/dL), endogenous
hyperinsulinemia (insulin >3 IU/mL; C-peptide >0.2 ng/ Dietary protein <20% of total calories
mL), and a negative sulfonylurea screen while the patient is Prefer lean meats
symptomatic. Dietary fat <35% of total calories
Avoid trans fats
Cholelithiasis is common after bariatric surgery. Restrict saturated fats to 10% of total calories
Prophylactic administration of ursodeoxycholic acid for Restrict dietary cholesterol to <300 mg daily
6 months after surgery decreases the risk of gallstone Prefer polyunsaturated fats
formation. Dietary carbohydrates <55% of total calories
Prefer fruits, vegetables, and whole grains
Bacterial overgrowth should be suspected in patients
Restrict refined carbohydrates, processed grains, and starches
presenting with abdominal pain and diarrhea.
29. O B E S I T Y 435
Multivitamin supplementation is advised for persons who self-imposed dietary restrictions (including vegetarians and
do not meet their nutritional needs orally or who have a vegans), patients who have gastrointestinal tract illness or have
self-imposed dietary restriction. had surgery affecting the duodenum, where iron is absorbed,
and women with heavy menses are also at risk. Unless more
Benefits of vitamin D and folic acid supplementation have
aggressive treatment with packed cell transfusion is needed or
been reported.
the patient is intolerant of oral iron, oral supplementation is
Empirical supplementation with antioxidant vitamins and sufficient.
folic acid does not provide cardiovascular health benefits.
Vitamin B12 deficiency must be suspected in any condition
-3 Fatty acids lower cardiovascular mortality and, at
(medical or surgical) that impairs absorption of intrinsic
higher doses, triglycerides.
factor or vitamin B12.
436 E N D O C R I N O L O GY
Parenteral nutrition is advised for patients who do not It is important to recognize the patient at risk of refeeding
meet their nutritional needs for 7 to 14 days and have con- syndrome so that precautions can be taken to avoid
traindications or intolerance to enteral feedings. Parenteral potentially fatal complications.
nutrition is associated with risks, and patients must be moni-
tored appropriately.
Hyperglycemia is the most common complication, and S U M M A RY
glucose monitoring is advised. Hypertriglyceridemia is a
recognized complication; limiting calories provided as fat is Caloric restriction of 250500 kcal daily is the main
advised for patients with triglyceride levels greater than 300 determinant of successful weight loss.
mg/dL. An increased risk of bloodstream infection (bacterial
Medications for weight loss are reserved for patients
and fungal organisms) is associated with parenteral nutrition.
who meet criteria for obesity or overweight and have
Patients receiving parenteral nutrition have up to a 5-fold
weight-related medical problems.
greater risk of fungal infection. Common risk factors include
poor hygiene in managing venous access and formula, severity The most common causes of death after bariatric surgery
of illness, and duration of catheter insertion. are pulmonary embolism and anastomotic leaks.
Cholelithiasis is common after bariatric surgery.
Parenteral nutrition is advised for patients who do not
Prophylactic administration of ursodeoxycholic acid for
meet their nutritional needs for 714 days and have
6 months after surgery decreases the risk of gallstone
contraindications or intolerance to enteral feedings.
formation.
Hyperglycemia, hypertriglyceridemia, and bloodstream
infection are recognized complications of parenteral Nutritional support should be considered for critically ill
nutrition. patients and for patients who have a BMI <18.5, a weight
loss >5%-10% of initial body weight, or an inability to
Ideally, nutritional needs are calculated with an accurate meet their nutritional needs for 14 days.
body weight, which is often difficult to measure if the patient is
In the absence of contraindications, enteral nutritional
critically ill. Protein needs are higher in critically ill patients, but
support is preferred.
caution must taken if patients have comorbidities contraindi-
cating a high-protein load (eg, renal insufficiency, liver disease). Parenteral nutrition is advised for patients who do not
meet their nutritional needs for 714 days and have
Calculation of nutritional needs is based on weight and contraindications or intolerance to enteral feedings.
clinical situation. Current weight is used for patients with Hyperglycemia, hypertriglyceridemia, and bloodstream
a BMI 29.9; 75% of calculated calories are provided for infection are recognized complications of parenteral
patients with a BMI 30. nutrition.
Common recommendations for nutritional support based
on patient need: SUGGESTED RE ADING
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protein Aasheim ET. Wernicke encephalopathy after bariatric surgery: a system-
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protein M, Willett WC. Dietary fat and risk of coronary heart disease in
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Barba CA, Butensky MS, Lorenzo M, Newman R. Endoscopic dilation
Refeeding syndrome is a recognized complication of aggres- of gastroesophageal anastomosis stricture after gastric bypass. Surg
sive nutritional support. It is most frequently observed in the Endosc. 2003 Mar;17(3):41620. Epub 2002 Dec 4.
Buchwald H, Avidor Y, Braunwald E, Jensen MD, Pories W, Fahrbach
significantly underweight patient (BMI <15) who is receiving K, et al. Bariatric surgery: a systematic review and meta-analysis.
parenteral nutrition. Abnormalities due to hyperinsuline- JAMA. 2004 Oct 13;292(14):172437. Erratum in: JAMA. 2005
mia occur in response to feedings and include hypokalemia, Apr 13;293(14):1728.
hypophosphatemia, hypomagnesemia, volume overload, and Dickey RA, Bartuska DG, Bray GW, Callaway CW, Davidson ET, Feld
edema, with hypophosphatemia being very common. Severe S, et al; AACE/ACE Obesity Task Force. AACE/ACE position state-
ment on the prevention, diagnosis, and treatment of obesity (1998
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mias, impaired diaphragmatic contractility, liver function test Di Stefano M, Miceli E, Missanelli A, Mazzocchi S, Corazza GR.
abnormalities, delirium, and seizures. The patient at risk of Absorbable vs. non-absorbable antibiotics in the treatment of small
refeeding syndrome must be recognized so that the necessary intestine bacterial overgrowth in patients with blind-loop syndrome.
precautions can be taken. Prevention includes gradual caloric Aliment Pharmacol Ther. 2005 Apr 15;21(8):98592.
Flum DR, Salem L, Elrod JA, Dellinger EP, Cheadle A, Chan L. Early
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438 E N D O C R I N O L O GY
30.
PITUITARY DISORDER S
Charles F. Abboud, MB, ChB, Bryan McIver, MB, ChB, PhD, and Pankaj Shah, MD
439
of the process. The most common presentation is that of a TSH deficiency: hypothyroidism and absence of goiter.
chronic process of insidious onset.
Prolactin deficiency: failure of lactation in postpartum
women.
Chronic Illness GH deficiency: ill-defined syndrome of asthenia, weakness,
Gonadotropin Deficiency and ill health.
The features of gonadotropin deficiency are those of the
loss of the steroidogenic and gametogenic functions of the Acute Illness
gonads. Female patients may have infertility, oligomenorrhea
or amenorrhea, loss of libido, vaginal dryness and dyspareunia, Adrenocortical crisis may be precipitated by the following:
involution of the uterus and genitalia, and atrophy or loss of
secondary sex characteristics. Male patients may have loss of 1. Withdrawal of prolonged glucocorticoid therapy without
libido, potency impairment, infertility, atrophy or loss of sec- proper glucocorticoid coverage during recovery of the
ondary sex characteristics, atrophy of the testes and prostate, hypothalamic-pituitary-adrenal axis
and, occasionally, gynecomastia. In both sexes, fine wrinkling 2. Pituitary surgery without optimal glucocorticoid stress
of the skin may be seen radially around the mouth or eyes and coverage
osteoporosis may occur.
3. Acute medical or surgical illness in a patient who has a
ACTH Deficiency lack of cortisol that is unrecognized or poorly managed
The features of ACTH deficiency result primarily from 4. Pituitary apoplexy
a lack of cortisol and loss of the pigmentary functions of
ACTH and related peptides. Such features may include 5. Thyroid hormone replacement therapy in a patient who
ill health, anorexia, weight loss, gastrointestinal tract dis- has an associated and unrecognized deficiency of ACTH
turbances, rheumatologic aches and pains, hypoglycemia,
hyponatremia, susceptibility to adrenocortical crises, pallor, Other acute manifestations are fasting hypoglycemia
and inability to tan or maintain a tan. The features of miner- syndrome (decreased hepatic neoglucogenesis due to lack of
alocorticoid deficiency are typically absent because aldoster- cortisol and GH), hyponatremic syndrome (renal water con-
one secretion depends on the renin-angiotensin system, not servation due to decreased glomerular filtration rate [GFR]
on ACTH. Therefore, hyperkalemia and hypovolemia with and unchecked secretion of antidiuretic hormone [ADH]ie,
orthostatism are typically absent. Partial ACTH deficiency syndrome of inappropriate secretion of ADH [SIADH]), and
may cause symptoms only during periods of acute medical or increased sensitivity to central nervous system (CNS) depres-
surgical illness. sants (decreased metabolism and clearance due to lack of
ACTH and TSH).
TSH Deficiency
TSH deficiency results in a lack of thyroid hormones (tri- Acute manifestations of hypopituitarism: adrenocortical
iodothyronine [T3] and thyroxine [T4]) and the characteristic crisis, fasting hypoglycemia syndrome, hyponatremic
features of slowing of emotional, mental, and physical func- syndrome, and increased sensitivity to CNS depressants.
tions. The thyroid gland is atrophic.
D I AG N O S I S
Prolactin Deficiency
Postpartum women who have prolactin deficiency cannot Diagnosis requires documenting the presence of hypopi-
lactate. tuitarism and identifying the cause. In the appropriate
clinical setting, provocative tests are used to accurately
diagnose deficiencies of nontropic hormones, which act
GH Deficiency
directly on target cells (eg, prolactin, oxytocin, GH).
The features of GH deficiency in adults include ill health
For deficiencies of tropic hormones, which act on other
and asthenia, fatigue, muscle weakness, osteopenia, obesity,
endocrine glands (eg, TSH, ACTH, luteinizing hormone
psychosocial difficulties, and increased cardiovascular risk.
[LH], follicle-stimulating hormone [FSH], GH), tar-
get gland function is evaluated. GH has both tropic and
Gonadotropin deficiency: failure of production of sex
nontropic functions. If target gland failure is present,
steroids and gametes; main features are hypogonadism and
tropic hormone levels must be determined to distinguish
infertility.
between primary target gland failure and failure due to
ACTH deficiency: cortisol deficiency and loss of hypothalamic-pituitary disease. Increased pituitary tropic
pigmentary effects of ACTH and related peptides. Lack of hormone levels indicate target gland failure; normal or low
cortisol is manifested as chronic ill health, hypoglycemia, tropic hormone levels indicate hypopituitarism.
hyponatremia, and susceptibility to adrenocortical crises.
Aldosterone secretion is basically normal; hyperkalemia In diagnosing hypopituitarism: hypopituitarism must be
and hypovolemia are characteristically absent. documented and its cause delineated.
440 E N D O C R I N O L O GY
Use a provocative test in the appropriate clinical setting to Growth Hormone
evaluate nontropic hormone deficiency.
GH deficiency is likely present in the patient with demon-
Evaluate target gland function for suspected tropic strable structural disease of the pituitary gland; deficiencies
hormone deficiency; test the tropic hormone level if of gonadotropins, ACTH, and TSH; and a low age-specific
target gland failure is present to distinguish between serum level of insulinlike growth factor 1 (IGF-1). In the
primary target gland failure and hypothalamic-pituitary absence of other pituitary hormone deficiency, a provoca-
disease. tive test is indicated. The preferred test uses arginine plus
GH-releasing hormone (GHRH). The insulin hypoglycemia
test is not safe and is contraindicated in patients who have sei-
Gonadotropin Axis
zures or cerebrovascular or cardiovascular disease.
Male patients have a low serum testosterone level, inappropri- GH deficiency is indicated by low serum levels of IGF-1
ately low serum LH and FSH levels, and a low sperm count. with documented structural pituitary disease and loss of other
Female patients have a low serum estradiol level and inappro- pituitary hormones. In the absence of other indicators, GH
priately low serum LH and FSH levels. Provocative tests for deficiency is confirmed by a low serum GH response to stimu-
LH and FSH with GnRH or clomiphene are rarely needed in lation. The insulin-hypoglycemia test can be hazardous and
clinical practice. should not be done.
ACTH Axis
Radiologic Evaluation
A morning plasma cortisol of less than 3 g/dL, repeated on
2 occasions, confirms adrenocortical failure. A level of more Radiologic evaluation includes imaging of the hypothalamic-
than 18 g/dL indicates a normal axis. Values of 3 to 18 g/dL pituitary region by computed tomography (CT) or magnetic
require a provocative test to assess adrenal function. resonance imaging (MRI) and, in the presence of suprasellar
In chronic ACTH deficiency, the adrenal cortices are atro- disease, neuro-ophthalmologic evaluation to assess visual fields,
phic and do not secrete cortisol in response to the short-acting visual acuity, and optic discs. MRI is preferred.
exogenous ACTH stimulation test (ie, the cosyntropin test).
Primary adrenocortical failure is confirmed by an increased Anatomical evaluation: imaging with CT or MRI
serum level of ACTH or by a lack of adrenocortical respon- (preferred) and neuro-ophthalmologic evaluation.
siveness to prolonged exogenous ACTH stimulation if cosyn-
tropin testing is not available. In adrenocortical failure due to In determining the cause of hypopituitarism, suspected
hypothalamic-pituitary disease, the levels of serum ACTH are functional causes must be removed or corrected. Normalization
inappropriately low. of pituitary function after correction of a functional cause
lends support to functional hypopituitarism. If the func-
The cosyntropin test (ie, the short ACTH stimulation test) tional causes are excluded, or if hypopituitarism persists
usually shows absence of cortisol secretory response. despite removal or correction of a functional cause, evaluation
for structural hypothalamic-pituitary disease is mandatory.
In adrenocortical failure due to hypothalamic-pituitary This evaluation is based on the clinical setting and appropriate
disease, serum levels of ACTH are inappropriately low. endocrine and anatomical studies.
Low serum free thyroxine (FT4) (or FT4 index) and an inap- If hypopituitarism persists after removal or correction
propriately normal or low serum level of TSH support of possible functional causes, evaluate for structural
the diagnosis of central hypothyroidism. In hypothyroid hypothalamic-pituitary disease on the basis of the clinical
patients, a high serum level of TSH or the presence of goi- setting and appropriate laboratory and radiologic studies.
ter points to primary hypothyroidism, and an inappropri-
ately low serum level of TSH confirms the diagnosis of TSH
THERAPY
deficiency.
Therapy includes correction of the cause and, when applica-
TSH deficiency: low serum level of FT4 or FT4 index and ble, administration of the hormones of the target glands or, in
an inappropriately normal or low serum TSH. selected cases, pituitary hormones.
3 0. P I T U I TA RY D I S O R D E R S 441
Treat the cause and, if needed, administer pituitary muscle strength and exercise capacity, increases bone min-
hormones or target gland hormones. eral density, and improves cardiac function. GH therapy
may be considered for patients with hypothalamic-pituitary
ACTH Deficiency disease and a poor GH response to a standard stimulus. The
goal of therapy is to restore serum IGF-1 to normal lev-
For ACTH deficiency, glucocorticoid replacement is critical. els and to avoid side effects. The long-term effects of such
Instruct patients in dose modification during acute illness. In therapy are unknown; thus, a benefit-risk profile cannot be
patients with a deficiency of both ACTH and TSH, initiate determined.
glucocorticoid therapy before thyroid hormone therapy to
avoid a thyroid hormoneinduced increased need for cortisol
and precipitation of an acute adrenocortical crisis. Adequacy P I T U I TA RY T U M O R S
of therapy is judged by clinical criteria, resolution of symp-
toms, and the absence of signs and symptoms of supraphysi- Pituitary tumors can be described according to size as microad-
ologic replacement. Serum ACTH levels cannot be used to enomas (10 mm) or macroadenomas (>10 mm), by extent
assess adequacy of therapy. as sellar or sellar/extrasellar, and by type as functioning or
nonfunctioning. Functioning pituitary tumors include prolac-
Instruct patients about dose modification during acute tinomas (40%-50%), GH tumors (10%-15%), ACTH tumors
illness. (10%-15%), and TSH tumors (<5%). Nonfunctioning tumors
In patients with a deficiency of both ACTH and TSH, (30%-40%) include the gonadotropinomas and null-cell
initiate glucocorticoid therapy before thyroid hormone adenomas. Pituitary tumors are usually sporadic; rarely, they
therapy. may be part of syndromes such as multiple endocrine neopla-
sia type 1 (MEN-1), McCune-Albright syndrome, or Carney
complex.
TSH Deficiency
For TSH deficiency, the drug of choice is T4. Assess the ade- Tumor size: microadenoma (10 mm) or macroadenoma
quacy of therapy by the feeling of well-being and the serum (>10 mm).
level of FT4. Serum TSH level should not be used to moni-
Tumor extent: sellar or sellar/extrasellar.
tor the adequacy of the T4 dosage since it is low in untreated
persons. Tumor type: functioning or nonfunctioning.
Tumor may be isolated or part of a syndrome such as
T4 is the drug of choice.
MEN-1.
Gonadotropin Deficiency
Gonadotropin deficiency is treated with sex steroids. In female C L I N I C A L FE AT U R E S
patients, estrogen therapy is used. Progestagens must be used
for patients with an intact uterus. The usual manifestation of a pituitary tumor is that of a
In male patients, testosterone is used to try to restore full chronic, slowly evolving disorder. Mass effects include head-
androgenicity. Assess status of the prostate in middle-aged aches and evidence of tumor extension beyond the confines of
and elderly men before therapy and follow annually. For resto- the sella as follows:
ration of fertility, FSH and LH (or GnRH therapy in patients
with hypothalamic disorders) may be indicated. Evaluate the 1. Superior tumor extension may cause the following:
patients psychosexual needs and lifestyle to assess the effect a. Chiasma syndrome (impaired visual acuity and visual
of therapy. field defects)
In hypogonadal female patients, use estrogen therapy. Use b. Hypothalamic syndrome (vegetative disturbance
supplemental progestagens for patients with an intact in thirst, appetite, satiety, sleep, and temperature
uterus. regulation and the endocrine disorder of diabetes
insipidus or SIADH)
In hypogonadal male patients, use testosterone.
c. Obstructive hydrocephalus
For restoration of fertility, consider the use of exogenous
gonadotropins (or, if feasible, GnRH therapy in patients d. Frontal lobe dysfunction
with hypothalamic disease). 2. Lateral tumor extension may cause impairment of cranial
nerves III, IV, V, and VI, with diplopia, facial pain, and
GH Deficiency temporal lobe dysfunction.
For GH deficiency, short-term GH therapy enhances a 3. Inferior tumor extension may cause nasopharyngeal mass or
sense of well-being, normalizes body composition, increases cerebrospinal fluid (CSF) rhinorrhea.
442 E N D O C R I N O L O GY
Endocrine effects include the following: TSH-producing tumors. Medical therapy is the primary ther-
apy for prolactinomas and is an adjunct to ablative therapy.
1. Hypersecretory states, in which hyperpituitarism leads to Conservative noninterventional therapy is an option for small
gigantism or acromegaly (GH excess), hyperprolactinemic tumors with no effect on quality or quantity of life.
syndrome (prolactin excess), Cushing disease and
Nelson-Salassa syndrome (ACTH excess), and Treatment options for pituitary tumors include surgical
thyrotoxicosis (TSH excess). Generally, LH or FSH excess excision, radiotherapy, or drug therapy.
is clinically silent.
Drug therapy is the primary therapy for prolactinomas and
2. Hypopituitarism can be caused by tumor growth that is a useful adjunctive therapy in the treatment of GH or
destroys the pituitary gland. TSH tumors.
3. Endocrine associations of pituitary tumors include MEN-1, Noninterventional therapy is an option for a small,
that is, parathyroid tumor or hyperplasia (primary nonfunctioning tumor or for a microprolactinoma not
hyperparathyroidism), endocrine pancreas tumor or associated with clinical features that impinge on quality of
hyperplasia (various endocrine pancreatic syndromes), life.
other endocrine gland tumors (thyroid, adrenal), and
lipomas. Transsphenoidal surgery is the operation of choice for
most tumors; the transcranial approach is used for large supra-
Rarely, pituitary tumors manifest acutely with pituitary sellar tumor extension. Surgical morbidity and mortality and
apoplexy (acute hemorrhage into the pituitary gland), which the available neurosurgical expertise should be considered.
may be the first clinical expression of the underlying tumor. Morbidity (eg, bleeding, infection, transient diabetes insipi-
dus, and CSF rhinorrhea) is less than 1% for microadenomas
Mass effects include headaches and extrasellar effects due and less than 4% for macroadenomas, and mortality is less than
to tumor extension beyond the sella. 1% with an experienced surgeon. Persistence or recurrence of
the tumor is less than 20% to 30% for microadenomas and
Endocrine effects result from hypersecretory states or 50% to 70% for macroadenomas.
hypopituitarism.
Endocrine associations of pituitary tumors include MEN-1. Transsphenoidal surgery is the operation of choice.
Pituitary apoplexy may complicate the course or be the Morbidity and mortality are low with an experienced
initial manifestation of the tumor. surgeon.
Persistence or recurrence of the tumor is moderately high.
D I AG N O S I S
The presence of a pituitary tumor is suggested by the clini- Radiotherapy results in a long latent period (a few months
cal features and confirmed by pituitary imaging. MRI is the to years) and postradiation hypopituitarism (in 10 years,
preferred imaging technique. Neuro-ophthalmologic evalua- >50% of patients, or a smaller percentage with a highly focused
tion is important, particularly if suprasellar extension is pres- modality). CNS damage and development of CNS tumors are
ent. Endocrine evaluation includes evaluation for hormonal rare.
excess or deficiency and for the presence of MEN-1. A pitu-
itary tumor is diagnosed if a sellar mass is associated with an A majority of patients have postradiation hypopituitarism.
excess of anterior pituitary hormone (except for mild hyper- CNS damage and CNS tumors due to radiotherapy are
prolactinemia, which can occur with nonpituitary masses and rare.
the stalk effect). Otherwise, the diagnosis is confirmed at
surgical exploration. Dopamine agonists are used for the management of pro-
lactinomas or GH-producing tumors. Somatostatin analogues
The presence of a pituitary tumor is suggested by clinical are used for the management of GH- or TSH-producing
assessment and radiologic imaging findings. tumors. Pegvisomant, a GH-receptor blocker, is used in the
Neuro-ophthalmologic evaluation is important, management of GH-producing tumors refractory to other
particularly with suprasellar extension. management options.
Endocrine evaluation should assess for hormonal excess or Drug therapy may be first-line (dopamine agonists for
deficiency and the presence of MEN-1. prolactinomas) or adjunctive.
3 0. P I T U I TA RY D I S O R D E R S 443
P R O L AC T I N O M A A N D T H E 1. Physiologic hyperprolactinemia may occur in pregnancy
H Y P E R P R O L AC T I N E M I C SY N D R O M E and the postpartum state and in conditions of stress, such
as surgery or acute illness.
Pituitary tumors associated with hyperprolactinemia may
2. Pathologic hyperprolactinemia may be eutopic (pituitary)
be prolactinomas, mixed tumors (eg, GH- and prolactin-
or ectopic (extrapituitary). Eutopic hyperprolactinemia
producing tumors), or nonfunctioning tumors with suprasellar
may occur in primary pituitary disease or in hypothalamic
extension and the stalk effect. In stalk-effect hyperprolactin-
or stalk disease resulting in loss of dopaminergic
emia, impingement of the mass on the pituitary stalk interferes
influence and disinhibition of prolactin secretion by
with the access of hypothalamic dopamine to the anterior pitu-
normal lactotrophs. Primary pituitary causes include
itary and results in disinhibition of prolactin secretion by nor-
prolactinoma, mixed tumors, nonfunctioning pituitary
mal lactotrophs.
tumors with suprasellar extension and stalk effect
hyperprolactinemia, hypophysitis, and primary empty
Pituitary tumors associated with hyperprolactinemia:
sella.
prolactinomas, mixed tumors, or any tumor or mass lesion
with suprasellar extension and the stalk effect. Hyperprolactinemia may be physiologic or
pathologic.
Physiologic hyperprolactinemia may occur in
C L I N I C A L FE AT U R E S pregnancy, the postpartum state, and conditions
Mass effects include hypopituitarism and expressions of extra- of stress.
sellar extension of the pituitary tumor. Persons with hyperpro- Pathologic hyperprolactinemia may be eutopic (pituitary)
lactinemia may be asymptomatic but are usually symptomatic. or ectopic (extrapituitary) in origin.
Hyperprolactinemia suppresses GnRH secretion and causes a
lactogenic effect on the breasts. Pituitary causes: most common is prolactinoma.
In women, hyperprolactinemia is usually expressed as Hypothalamic or stalk disorders can be functional or
galactorrhea, ovulatory and menstrual dysfunction (short organic. Functional hypothalamic disorders lead to hyperpro-
luteal phase or anovulation leading to infertility), oligomenor- lactinemia because of interference with the synthesis, secre-
rhea or amenorrhea and hypogonadism, and decreased libido. tion, or action of dopamine or other hypothalamic regulators
In some women, hyperprolactinemia may be associated with of prolactin secretion. These disorders may be caused by the
hirsutism and acne. following:
In men, hyperprolactinemia results in hypogonadism, infer-
tility due to oligospermia, and, rarely, galactorrhea or gyneco-
mastia. The recognition of hyperprolactinemia frequently is 1. Drugs (eg, neuroleptics, antidepressants, narcotics, and
delayed in men because decreased libido and impaired potency estrogens)
may be dismissed by the patient and physician and attributed 2. Primary hypothyroidism (15%-30%)
to psychiatric factors. In men with a pituitary tumor, marked
hyperprolactinemia and a macroprolactinoma are common at 3. Chest wall irritative lesions (eg, herpes zoster,
presentation. dermatitis, and thoracotomy)
4. Renal failure
Endocrine effects include the effects of
hyperprolactinemia, associated pituitary dysfunction, and 5. Cirrhosis or hepatic encephalopathy
associated MEN-1.
Organic hypothalamic disorders include traumatic disor-
Hyperprolactinemia exerts its clinical effects dominantly
ders (eg, surgery or radiotherapy), inflammatory disorders (eg,
on GnRH secretion and the breasts.
sarcoidosis or histiocytosis X), or neoplastic disorders (eg,
Women may have ovulatory or menstrual dysfunction, craniopharyngioma, optic glioma, meningioma, or metasta-
galactorrhea, and hirsutism. ses such as those from the breast or lungs). Ectopic hyperpro-
lactinemia (very rare) has been reported with hypernephroma,
Men may have decreased libido and impotence. gonadoblastoma, and ovarian teratomas.
In men, recognition of hyperprolactinemia is frequently
delayed, and a macroprolactinoma is common at diagnosis. Hypothalamic causes of hyperprolactinemia are functional
or organic.
D I AG N O S I S Functional disorders may be caused by drugs, primary
hypothyroidism, chest wall lesions, and chronic renal or
Prolactinoma must be distinguished from other causes of hepatic failure.
hyperprolactinemia and from other pituitary area masses.
Hyperprolactinemia can be physiologic or pathologic in Organic causes include hypothalamic disorders due to
origin: trauma, inflammation, and infiltrative processes.
444 E N D O C R I N O L O GY
Female patients with hyperprolactinemia must have preg- of prolactin-producing cells, restore gonadal function
nancy excluded. The morning basal fasting serum level of pro- (70%-80%), and decrease tumor size (>50%). Patients with
lactin should be measured. Parkinson disease who receive cabergoline should be moni-
The diagnosis of a prolactinoma is established with serum tored clinically and by echocardiography biannually because
levels of prolactin greater than 10 times the upper end of the of the possible development of cardiac valvular disease.
reference range. However, prolactinomas, particularly micro- Therapy with dopamine agonists is temporizing, and discon-
prolactinomas, may be associated with lower prolactin levels. tinuation usually leads to recurrence of tumor growth and
If the prolactin level is less than 10 times the upper end of endocrine dysfunction. However, in some patients who have
the reference range, rule out functional causes. If a functional the outcomes of normoprolactinemia and significantly smaller
cause is present, remove it or treat it if possible. If hyperpro- tumor, use of the drug can be withdrawn after 1 to 2 years. In
lactinemia does not resolve in about 3 months, evaluate for these patients, the tumor may have a long remission but need
hypothalamic-pituitary disease. If a functional cause is not careful monitoring.
present, rule out organic hypothalamic-pituitary disease by Dopamine agonist therapy should be stopped at the
imaging the hypothalamic-pituitary region, preferably by earliest sign of pregnancy. In pregnancy, the risk of micro-
MRI, and by evaluating other pituitary functions and the prolactinoma growth is less than 5%, and the risk of macro-
visual fields, if appropriate. prolactinoma growth, 20% to 40%. Observe patients closely; if
If a cause is not found, the hyperprolactinemia is consid- tumor growth is suspected, confirm with imaging (do not use
ered to be of indeterminate origin. Follow-up evaluation is gadolinium during pregnancy). If significant tumor growth
critical because some patients may harbor microadenomas or complicates pregnancy, consider surgical excision or reinstitu-
other hypothalamic-pituitary space-occupying lesions that are tion of dopamine agonist therapy.
below the limit of radiologic detection, and follow-up exami-
nations may show evidence of a mass. The serum level of pro- Dopamine agonists suppress hyperprolactinemia, restore
lactin should be checked every 6 to 12 months and imaging gonadal function (70%-80%), and decrease tumor size
should be repeated in 1 to 2 years or earlier if new symptoms (>50%).
develop.
Macroprolactinemia may account for up to 10% of patients Bromocriptine and cabergoline are safe and effective
presenting with hyperprolactinemia. Rarely, glycosylated pro- drugs. Cabergoline appears to be more effective, is more
lactin circulating in aggregates (macroprolactin) accounts for convenient to use, and is associated with lesser degrees of
most of the circulating prolactin. These aggregates are not drug intolerance or resistance.
cleared well by the kidneys. This appears to be a benign condi- Discontinuation of the use of the dopamine agonist usually
tion requiring no specific therapy. However, it can be misdiag- leads to resumption of tumor growth and endocrine
nosed and treated inappropriately. dysfunction.
Use of dopamine agonists should be stopped at the earliest
T R E AT M E N T sign of pregnancy.
Microprolactinoma or Idiopathic Hyperprolactinemia During pregnancy, the risk of microprolactinoma growth
Treatment is indicated for management of infertility, hypogo- is <5%, and the risk of macroprolactinoma growth,
nadism, or significant galactorrhea. Treatment options for 20%-40%.
infertility include dopamine agonist therapy and transsphe- If significant tumor growth complicates pregnancy,
noidal surgery for microprolactinoma. If fertility is not an consider surgical excision or reinstitution of drug therapy.
issue, estrogen therapy is indicated to prevent hypoestrogenic
manifestations, including bone loss. Otherwise, observe and
check the serum level of prolactin annually and reimage every Surgical Treatment of Prolactinomas
2 to 3 years. For microadenomas, the surgical cure rates are 60% to 80%;
for macroadenomas, 0% to 30%.
Macroprolactinoma
Therapy is indicated for all patients because of the threat of a G H T U M O R S : AC R O M E G A LY A N D
mass lesion and the effects of hyperprolactinemia. Drug therapy GIGANTISM
with a dopamine agonist is the preferred treatment. Surgical
excision or radiotherapy is reserved for the drug-intolerant or ET I O L O GY
drug-resistant cases (10%-20% for bromocriptine; 3%-7% for
cabergoline). Acromegaly is nearly always caused by a benign GH-producing
pituitary tumor. These tumors usually secrete only GH;
Dopamine Agonists infrequently, they may simultaneously secrete prolactin,
-glycoprotein, ACTH, or TSH. Rarely, acromegaly may be
Dopamine agonists are the mainstay of prolactinoma ther- caused by ectopic GH-producing tumors or hypothalamic or
apy. They suppress prolactin secretion and proliferation extrahypothalamic GHRH-producing tumors.
3 0. P I T U I TA RY D I S O R D E R S 445
GH-producing pituitary tumors are usually sporadic; suppressibility within 1 to 2 hours after a 75-g glucose load
rarely, they are familial and may occur in association with (failure of GH suppression to <1 ng/mL or a paradoxical
MEN-1, McCune Albright syndrome, or Carney complex. increase in GH secretion). A random serum level of GH is not
helpful because of the pulsatile nature of GH secretion.
C L I N I C A L FE AT U R E S
The clinical presentations are related to excess levels of GH Radiologic Diagnosis
and IGF-1, the pituitary tumor, and the associations of acro- When the diagnosis is documented biochemically, imaging of
megaly. Excess levels of GH and IGF-1 lead to gigantism in a the sella is indicated. MRI is the imaging study of choice. If a
child and to the characteristic acromegalic features in an adult. pituitary tumor is not delineated (a rare event), serum GHRH
These include the following: levels are measured to exclude a GHRH-producing tumor and a
search is made for evidence of an ectopic GH-producing tumor.
1. Bone and soft-tissue overgrowth, with coarsening of the
facial features; frontal bossing; prognathism; widened Serum IGF-1: The best screening test. Age- and
spaces between teeth; macroglossia; increased hat, glove, sex-matched serum IGF-1 is increased in all patients with
ring, or shoe size; acroparesthesias; and nerve entrapment active acromegaly.
syndromes
Glucose toleranceGH suppressibility test: failure of GH
2. Hyperhidrosis, heat intolerance, skin tags, and increased to suppress to <1 ng/mL is diagnostic of acromegaly.
skin oiliness
When acromegaly is documented biochemically, proceed
3. Carbohydrate intolerance (20%) and, rarely, frank with imaging the sella. If no tumor is visible, measure the
diabetes mellitus, hypercalciuria, and hyperphosphatemia serum level of GHRH and look for evidence of an ectopic
4. Fibromas or acanthosis nigricans GH-producing tumor.
446 E N D O C R I N O L O GY
surgical therapy is unsuccessful, medical treatment can be T H Y R OT R O P I N -P R O D U C I N G T U M O R S
used alone, as an interim therapy when postoperative radio-
therapy is given, or while awaiting the results of radiotherapy. The characteristic clinical presentations of patients who have
Three lines of medical therapy are available: somatostatin primary TSH tumors are diffuse goiter and hyperthyroid-
analogues, dopamine agonists, and pegvisomant. It is impor- ism. Other presentations include extrasellar mass effects and
tant to remember that the effects of pharmacotherapy are hypopituitarism. Laboratory evaluation reveals that, in a thy-
temporizing: they are effective only as the drug is being taken. rotoxic patient, the sensitive TSH value is normal or high,
Cessation of drug therapy leads to recrudescence of disease -glycoprotein subunit levels are high, and TSH responsive-
activity. ness to thyrotropin-releasing hormone is absent. CT or MRI
shows a sellar mass with or without extrasellar extension. The
Therapy of choice: surgical excision. For persistent disease: main differential diagnosis is Graves disease. Among patients
radiotherapy or pharmacologic therapy. with TSH-producing tumors, in contrast to Graves disease,
one finds equal incidence between the sexes, absence of oph-
Radiotherapy may be used as alternative ablative therapy. thalmopathy and dermopathy, and normal or high sensitive
Drug therapy: somatostatin analogues, dopamine TSH values in the presence of hyperthyroidism. Treatment
agonists, and GH-receptor blocker, alone or in options include ablation (surgically or with irradiation), phar-
combination, are temporizing. These are mainly used macologic therapy with octreotide, and ancillary measures for
while awaiting the full effects of primary or adjunctive the management of thyrotoxicosis.
radiotherapy or when surgical therapy has been
unsuccessful or declined.
P I T U I TA RY I N C I D E N TA L O M A S
3 0. P I T U I TA RY D I S O R D E R S 447
is the most common tumor in the pituitary region in child- 1. Decreased production of ADH in response to normal
hood but can occur at any age. Two-thirds of the tumors are osmotic stimulation
suprasellar, and one-third originate in or extend into the sella.
2. Decreased responsiveness of the distal nephron to ADH
Most are cystic, and some are solid or mixed. These tumors
(nephrogenic or vasopressin-resistant DI).
have a propensity to calcify. The clinical presentation includes
obstructive hydrocephalus, hypothalamic syndrome (diabetes
insipidus and hyperprolactinemia), chiasmal defects, hypopi-
tuitarism, or calcification in or around the sella, as seen inci- Decreased Production of ADH
dentally on radiography. Radiography shows calcification in
ADH production decreases in response to normal osmotic
intrasellar or suprasellar regions (75% of children; 25% of
stimulation most commonly from organic disorders of the
adults). CT or MRI reveals a solid or cystic mass, calcification
anterior hypothalamus, median eminence, or upper stalk
(on CT), and low attenuation values (cholesterol content).
(hypothalamic, neurogenic, central, or ADH-sensitive DI).
Surgical excision is possible for only small craniopharyn-
Infrequently, it results from functional suppression of ADH
giomas. Larger craniopharyngiomas are decompressed. A ven-
production by the ingestion of excessive volumes of fluid (pri-
triculoperitoneal shunt is used for obstructive hydrocephalus.
mary polydipsia or dipsogenic DI).
Other treatments include postoperative radiotherapy and
management of endocrine dysfunction.
Hypothalamic or Central DI
P I T U ITA RY A P O P L E X Y Hypothalamic or central DI may result from genetic or acquired
disorders of the anterior hypothalamus, median eminence, or
Pituitary apoplexy refers to hemorrhagic infarction of the
upper pituitary stalk. Genetic disorders are rare. Causes of
pituitary gland, with or without underlying disease. The usual
acquired disorders include traumatic (closed head trauma or
clinical setting is that of a pituitary tumor, irradiated pituitary
neurosurgery); inflammatory or granulomatous (sarcoidosis,
tumor, pregnancy, anticoagulation therapy, increased intrac-
tuberculosis, or histiocytosis X); primary neoplasms such as
ranial pressure, vascular disease (eg, diabetes mellitus), or vas-
craniopharyngioma, germinoma, and optic glioma; or meta-
culitis (eg, temporal arteritis). Persons are asymptomatic if the
static neoplasms primarily from the breast or lung. Idiopathic
bleeding is small or gradual. In the acute condition, hemor-
hypothalamic DI is probably the most common cause of the
rhage is sudden or large, with features such as severe headache,
syndrome and may be an autoimmune disorder.
ophthalmoplegia, visual defects, meningismus, depressed
sensorium, and acute adrenocortical crisis. Death may occur.
Diagnosis is made on the basis of the characteristic clinical, Dipsogenic DI
radiologic, and surgical findings. Therapy includes neurosurgi-
Dipsogenic DI may be idiopathic or associated with psychosis
cal decompression and hormonal support. Late sequelae may
or, rarely, organic disorders of the anterior hypothalamus such
include hypopituitarism, secondary empty sella syndrome, or
as sarcoidosis or neoplasms.
regression of hypersecretory syndrome in an infarcted func-
tioning pituitary tumor.
Nephrogenic DI
LY M P H O C Y T I C H Y P O P H Y S IT I S Nephrogenic DI, or decreased responsiveness of the distal
nephron to ADH, may also be caused by genetic or acquired
Lymphocytic hypophysitis is presumed to be of autoimmune
disorders, the most common being chronic renal disease, elec-
origin. It usually occurs in association with other autoimmune
trolyte abnormalities (hypercalcemia or hypokalemia), and
endocrinopathies and affects adults, predominantly women,
ADH-antagonist drugs such as lithium and demeclocycline.
especially during pregnancy and the postpartum period. The
clinical presentation may include hypopituitarism or the pres-
DI may result from decreased production of ADH or from
ence of a sellar mass associated with hyperprolactinemia. The
renal unresponsiveness to ADH.
major differential diagnoses are prolactinoma and Sheehan
syndrome. The diagnosis depends on the associations and the Hypothalamic DI: genetic or acquired loss of
results of surgical exploration. No specific therapy is available. ADH-secreting neurons. The most common cause is
Hormonal replacement is given as needed. idiopathic DI. Other causes include traumatic, idiopathic,
and neoplastic primary or metastatic neoplasms.
448 E N D O C R I N O L O GY
C L I N I C A L FE AT U R E S osmolality <280 mOsm/kg, in an untreated patient, points
to primary polydipsia.
The clinical manifestations include those of DI and the etio-
logic disorder. Polyuria and polydipsia, often with preference
for ice-cold water, are characteristic. Nocturia is usually pres- ET I O L O G I C D I AG N O S I S
ent and enuresis may be the presenting complaint in chil-
Look for clinical evidence of hypothalamic-pituitary or sys-
dren. An abrupt onset of symptoms usually points to central
temic disorders, examine the visual fields, assess anterior pitu-
DI. Absence of nocturia, variable intensity or intermittency
itary functions, and perform MRI. The most common causes
of symptoms, and a 24-hour urine output greater than 18
of central DI are idiopathic DI, trauma (accidental or neuro-
L suggest primary polydipsia. It is important to remember
surgical), metastases from breast or lung cancers, and hypo-
that because patients with hypothalamic or nephrogenic DI
thalamic area tumors. Systemic diseases with hypothalamic or
rely on their thirst mechanism to regulate water balance, no
stalk involvement must be considered.
other ill effects may be apparent unless the patient becomes
unconscious for any reason, is unable to obtain fluids, or has
an impaired thirst mechanism. In such circumstances, extreme THERAPY
hyperosmolar dehydration and hypertonic encephalopathy Therapy, whenever possible, is directed at the cause. For mild
may develop. central DI, free access to water is the treatment. Desmopressin
is used for moderate to severe central DI. For partial central
DI is characterized by polyuria (2.520 L daily) and DI, use ADH agonists such as chlorpropamide (250500 mg
polydipsia, often with preference for ice-cold water. daily). For nephrogenic DI, thiazides are the only treatment
Abrupt onset of symptoms usually suggests central DI, and available.
absence of nocturia suggests primary polydipsia.
When thirst sensation is impaired or access to water is A D H E XC E S S : S I A D H
restricted, a hyperosmolar state may ensue and may be
complicated by hypertonic encephalopathy and circulatory ET I O L O GY
collapse.
ADH excess, in the absence of a hyperosmolar stimulus, may
be appropriate when it occurs in response to hypovolemia or
E N D O C R I N E D I AG N O S I S hypotension and inappropriate when it occurs in the absence
of a hypovolemic or hypotensive stimulus. SIADH can result
The diagnosis depends on the use of random plasma osmo- from exogenous or endogenous disorders.
lality (or serum level of sodium) and urine osmolality levels Exogenous ADH excess may result from the inappropriate
under conditions of unrestricted fluid intake and on the use administration of ADH (or its analogues such as desmopres-
of provocative tests. The induction of plasma hyperosmolality sin) or oxytocin. Endogenous ADH excess may originate from a
(either by water deprivation or by administration of hypertonic eutopic hypothalamic or an ectopic extrahypothalamic source.
saline) is used to assess the patients ability to produce ADH Eutopic ADH excess may be a consequence of the following:
and to respond to it. The patients response can be assessed 1)
indirectly by measurements of urine volume and osmolality 1. CNS or hypothalamic disorders of various causes (eg,
before and after the administration of exogenous ADH or 2) traumatic, inflammatory, degenerative, vascular, or
directly by measurements of plasma levels of ADH in addition neoplastic disorders)
to plasma and urine osmolalities.
Although the diagnosis of severe DI of any cause can 2. Use of agonist drugs that enhance ADH secretion or
be straightforward, the diagnostic process is often difficult action (chlorpropamide, carbamazepine, vincristine,
because the extent of the disorder may be only partial and vinblastine, cyclophosphamide, phenothiazines,
because prolonged periods of polyuria, regardless of the pri- monoamine oxidase inhibitors, tricyclic antidepressants,
mary cause, may decrease the maximal urine-concentrating and clofibrate)
ability (renal medullary washout), in effect adding a nephro- 3. Neurogenic influences such as pain or nausea
genic DI component to the basic disease process.
In a patient with polyuria and dilute urine, a random
Ectopic extrahypothalamic ADH excess may result from the
plasma osmolality >295 mOsm/kg points to neurogenic or
following:
nephrogenic DI. These can be differentiated by the response to
exogenous ADH. A random plasma osmolality <280 mOsm/
1. Malignancies (cancers of the bronchus, pancreas, ureter,
kg, in an untreated patient, points to primary polydipsia.
prostate, or bladder; lymphoma; leukemia; thymoma; or
mesothelioma)
Obtain random plasma and urine osmolality values: a
random plasma osmolality >295 mOsm/kg points to 2. Benign pulmonary disorders (pneumonia, lung abscess,
neurogenic or nephrogenic DI. These can be differentiated empyema or pneumothorax, tuberculosis, cystic fibrosis,
by the response to exogenous ADH. A random plasma and the use of positive-pressure ventilation)
3 0. P I T U I TA RY D I S O R D E R S 449
PAT H O P H YS I O L O GY 2. Exclude hyperosmolar states and loss of intracellular
water to the hyperosmolar extracellular fluid, as
Continued water intake and ADH hypersecretion in the
in hyperglycemia and the use of mannitol (plasma
absence of a hyperosmolar stimulus leads to the following:
glucose, history of mannitol use, and increased plasma
osmolality).
1. Increased renal water retention, hyponatremia, and
hypo-osmolality of body fluids with inappropriately 3. In the absence of advanced renal failure, the differential
concentrated urine diagnosis is SIADH and appropriate ADH excess
associated with decreased cardiac output (volume and
2. Expansion of body fluid compartments, including
pressure stimuli). Establish the appropriateness or
extracellular fluid volume
inappropriateness of ADH hypersecretion. If the findings
3. Homeostatic adjustments that promote renal escape point to SIADH, identify the cause. If an exogenous
and natriuresis, including increased GFR, increased source is not apparent, search for a eutopic or ectopic
atrial natriuretic hormones, and suppression of the source of ADH hypersecretion.
renin-angiotensin-aldosterone axis. Natriuresis
4. The main diagnostic challenge is to differentiate SIADH
exacerbates plasma hypo-osmolality, thus explaining the
from subclinical hypovolemia. Consider urinary sodium
absence of edema despite an expanded extracellular fluid
concentration, serum creatinine or uric acid levels, and
volume.
plasma renin activity and aldosterone level. In contrast to
Physiologic or appropriate ADH hypersecretion occurs findings in SIADH, subclinical hypovolemia is associated
in response to plasma hyperosmolality, hypovolemia, or with a urinary sodium concentration less than 20 mEq/L,
hypotension. increased serum creatinine and uric acid levels, and an
increased plasma renin activity and plasma aldosterone
Pathophysiologic or inappropriate ADH excess occurs in
level.
the absence of physiologic stimuli and can have either an
exogenous or an endogenous cause. Endogenous ADH Confirm true hyponatremia and exclude hyperosmolar
excess can be from a eutopic hypothalamic source or an states, advanced renal failure, and states of appropriate
ectopic extrahypothalamic source. ADH excess.
SIADH is characterized by hypervolemia, hyponatremia, The main diagnostic challenge is to differentiate SIADH
and hypo-osmolality of body fluids, inappropriately from subclinical hypovolemia; consider urinary sodium,
concentrated urine, natriuresis, absence of edema, and low serum creatinine and uric acid, and plasma renin activity
serum creatinine and uric acid levels (a result of increased and aldosterone.
GFR).
THERAPY
C L I N I C A L FE AT U R E S Therapy for SIADH includes identifying and managing the
underlying disorder, restricting water intake to 800 to 1,000
The clinical features are a composite of the effects of the
mL daily, and monitoring the patients weight and serum
underlying disorder and those of the hyponatremic syndrome
sodium level. Combined therapy with furosemide and salt
that depend on the degree and rapidity of its development.
tablets often can increase the plasma sodium concentra-
Patients with SIADH may be asymptomatic if the hypona-
tion in SIADH. Treatment with demeclocycline, a direct
tremia is mild or has developed gradually over weeks and
cell toxin and ADH antagonist (9001,200 mg daily), may
months. When patients are symptomatic, the most frequent
be useful. This drug can be nephrotoxic, particularly in
symptoms are lethargy, fatigue, ill health, anorexia, nausea
patients with chronic liver disease. Specific ADH antago-
and vomiting, and irritability or confusion. Severe or rapidly
nists, the vaptans, have become recently available (tolvaptan
developing hyponatremia can lead to a behavioral change, a
for oral use and conivaptan for intravenous use); these will
change in the level of consciousness, or seizures.
have an increasing role in the management of SIADH in
the future.
Clinical features depend on the degree and rapidity
When acute neurologic sequelae are present, give hyper-
of the development of hyponatremia and range from
tonic saline intravenously (200300 mL of 5% saline over
asymptomatic to neurologically impaired.
34 hours). Achieve a gradual increase in serum sodium (do
not exceed 0.5 mEq/h or 12 mEq in 24 hours). Continue giv-
ing hypertonic saline until the neurologic symptoms cease
D I AG N O S I S
and a safe serum sodium level of 120 mEq/L is reached.
1. Confirm true hyponatremia. Exclude Rapid correction of hyponatremia can lead to central pontine
pseudohyponatremia associated with hyperlipidemia myelinolysis, which often is fatal.
or hyperlipoproteinemia (clinical and biochemical
features and normal plasma osmolality indicate Identify and treat the underlying disorder and manage the
pseudohyponatremia). hyponatremia.
450 E N D O C R I N O L O GY
Therapy for hyponatremia: water restriction and, if needed, hyponatremic syndrome, and increased sensitivity to CNS
an ADH antagonist (ie, demeclocycline). depressants.
For acute neurologic sequelae: hypertonic saline to increase Use a provocative test in the appropriate clinical setting to
serum sodium by 0.5 mEq/h to control symptoms and evaluate nontropic hormone deficiency.
achieve a safe serum sodium level of 120 mEq/L.
Evaluate target gland function for suspected tropic
Rapid correction of hyponatremia can lead to potentially hormone deficiency; test the tropic hormone level if
fatal central pontine myelinolysis. target gland failure is present to distinguish between
primary target gland failure and hypothalamic-pituitary
disease.
S U M M A RY Treatment options for pituitary tumors include surgical
excision, radiotherapy, or drug therapy.
Hypopituitarism can result from primary pituitary
disorders, hypothalamicpituitary stalk disorders, or SIADH is characterized by hypervolemia, hyponatremia,
extrasellar disorders. and hypo-osmolality of body fluids, inappropriately
concentrated urine, natriuresis, absence of edema, and low
Acute manifestations of hypopituitarism: adrenocortical serum creatinine and uric acid levels (a result of increased
crisis, fasting hypoglycemia syndrome, GFR).
3 0. P I T U I TA RY D I S O R D E R S 451
31.
GONADAL AND ADRENAL DISORDER S
Charles F. Abboud, MB, ChB , Bryan McIver, MB, ChB, PhD, and Pankaj Shah, MD
452
1. Cortisol deficiency: decreased vitality, energy, and secondary rests on the measurement of serum ACTH: a high
stamina; muscle weakness; anorexia, weight loss, ACTH level indicates Addison disease, and a low or inappro-
nausea, vomiting, or diarrhea (may mimic abdominal priately normal level indicates secondary failure.
malignancy); mood changes; hyponatremia, fasting A normal response to cosyntropin rules out Addison dis-
hypoglycemia, transient hypercalcemia, anemia, ease but does not exclude ACTH deficiency that is partial or
lymphocytosis, and eosinophilia of recent onset. If the diagnosis is still suspected, a metyrapone
test or an insulin-hypoglycemia test is performed: a normal
2. Aldosterone deficiency: hypovolemia, orthostatic
response to the provocative test excludes adrenocortical failure;
hypotension, hyperkalemia, hyperchloremic acidosis, and
an impaired response in a patient who has a normal response
azotemia
to cosyntropin indicates secondary failure. A low-dose cosyn-
3. Androgen deficiency: not significant in males; associated tropin test (1 g) has been advocated as a reliable alternative
with decreased libido and thinning of sexual hair in for the diagnosis of recent or partial ACTH deficiency, but its
females value for this purpose is debatable.
4. ACTH-related symptoms: ACTH excess in Addison
A plasma cortisol value <3 g/dL indicates adrenocortical
disease is associated with hyperpigmentation; pallor and
failure, whereas a value >18 g/dL excludes the diagnosis.
the inability to tan result from ACTH deficiency in
hypothalamic-pituitary disease Cosyntropin test: a subnormal cortisol response
establishes the diagnosis of adrenocortical failure but
cannot differentiate Addison disease from failure due to
Acute Adrenocortical Failure or Adrenal Crisis hypothalamic-pituitary disease. This differentiation is
Adrenal crisis is suggested in the presence of dehydration, based on serum ACTH measurements or, if not available,
hypotension, or shock out of proportion to the severity of the on the long ACTH stimulation test.
current illness; nausea and vomiting with a history of anorexia
and weight loss; abdominal pain (may mimic acute abdo- Normal cortisol response to cosyntropin excludes Addison
men); unexplained fever; and hyponatremia, hyperkalemia, disease but does not rule out secondary adrenocortical
azotemia, hypercalcemia, eosinophilia, and hypoglycemia. It failure that is partial or of recent onset. A metyrapone test
often is precipitated by an illness in a patient who has unrecog- or an insulin-hypoglycemia test is performed.
nized adrenocortical failure and who recently had glucocorti-
coid therapy withdrawn or has sustained bilateral hemorrhage
Etiologic Diagnosis
of the adrenals.
In Addison disease, an etiologic diagnosis depends on
clinical assessment and a search for other autoimmune disor-
Addison disease usually manifests as a chronic, slowly
ders, infections, and neoplasms. Autoimmune adrenalitis is
evolving syndrome; manifestations are a composite of the
diagnosed by measuring antibodies against the steroidogenic
effects of a lack of cortisol, sex steroids, and aldosterone
enzyme 21-hydroxylase (CYP21A2). Computed tomographic
and an excess of ACTH.
(CT) imaging of the adrenal glands is helpful in the diagno-
Adrenal crisis is precipitated by an illness in a patient who sis of inflammatory disorders, adrenal hemorrhage, or malig-
has unrecognized adrenocortical failure and who recently nancy. In secondary failure, pituitary function is assessed and
had glucocorticoid therapy withdrawn or has sustained magnetic resonance imaging (MRI) or CT imaging of the
bilateral hemorrhage of the adrenals. head is performed to look for a space-occupying lesion in the
hypothalamic-pituitary region.
Diagnosis Therapy
Endocrine Diagnosis Primary adrenocortical failure requires glucocorticoid and
The symptoms and signs of adrenocortical failure are vari- mineralocorticoid replacement therapy, whereas second-
able and nonspecific, and diagnosis requires a high degree ary failure requires only glucocorticoid replacement. Patient
of clinical awareness. Plasma cortisol levels (reference range, education is critical and must cover several topics: the need
727 g/dL) may be helpful in diagnosis. A value less than for disciplined daily lifelong therapy, the manner of dosage
3 g/dL indicates adrenocortical failure, and a value greater adjustments during acute illness, the use of injectable gluco-
than 18 g/dL excludes the diagnosis. corticoids when oral replacement therapy is not possible, and
The diagnosis is confirmed most reliably and effectively the use of an identification bracelet or necklace.
by the cosyntropin test, which assesses the cortisol response
to a synthetic, rapidly acting ACTH (250 g). The normal Primary Adrenocortical Failure
response to cosyntropin is an absolute value of plasma cortisol Glucocorticoid therapy consists of hydrocortisone (1020
greater than 18 g/dL. An impaired response to cosyntropin mg in the morning and 510 mg in the afternoon) or predni-
establishes the diagnosis of adrenocortical failure but does not sone (5 mg in the morning and 02.5 mg in the afternoon).
specify the type. Defining whether the failure is primary or The adequacy of therapy is assessed by the patients sense of
31. G O N A DA L A N D A D R E N A L D I S O R D E R S 453
well-being, the decrease in pigmentation, and the absence precipitating causes. After the acute illness is over, switch the
of manifestations of excessive glucocorticoid replacement; glucocorticoid therapy to dexamethasone (it will not interfere
ACTH levels are not always reliable for monitoring the ade- with plasma cortisol measurements) and perform the cosyn-
quacy of therapy. tropin stimulation test to initiate the adrenocortical diagnostic
Mineralocorticoid therapy consists of fludrocortisone process. Taper the dosage of glucocorticoids to a maintenance
(0.050.2 mg orally) and liberal salt intake. The adequacy of dosage and begin mineralocorticoid replacement, if needed,
replacement is monitored by measurement of the supine and after the saline infusion is stopped.
standing blood pressure, presence of edema, serum potassium
level, and, if needed, plasma renin activity. Prompt management is critical.
Collect blood samples for measuring electrolytes, glucose,
Primary adrenocortical failure requires glucocorticoid and
plasma cortisol, and serum ACTH, but do not wait for
mineralocorticoid therapy.
the results; begin treatment as soon as the diagnosis is
Secondary failure requires only glucocorticoid therapy. suspected.
Patient education is a critical component of effective Parenteral glucocorticoids are critical. Ensure adequate
management. fluid, electrolyte, and volume replacement. Search for
and treat any underlying precipitating disorder such as
Therapy for primary adrenocortical failure: hydrocortisone
infection.
(1020 mg in the morning and 510 mg in the afternoon)
or the equivalent; fludrocortisone (0.050.2 mg orally); After the patients condition has stabilized, continue
and liberal salt intake. infusions at a lower rate and perform the cosyntropin test.
454 E N D O C R I N O L O GY
Exogenous glucocorticoid therapy is the most common homeostatic mechanisms. These include acute illness of
cause of Cushing syndrome. any type, stress, nutritional disorders, alcoholism, and
depression.
Endogenous Cushing syndrome is best classified into
ACTH-independent and ACTH-dependent disorders. 2. Many drugs can alter diagnostic tests for cortisol
overproduction, such as oral contraceptives, which can
ACTH-independent disorders: adrenal tumors (10%) and,
increase cortisol-binding globulin, and drugs that alter
rarely, nodular hyperplasias.
dexamethasone metabolism.
ACTH-dependent disorders: Cushing disease (75%),
3. No single test is completely reliable to confirm or
ectopic-ACTH tumors (15%), adrenal tumors (10%), and,
exclude the diagnosis. Clinicians usually rely on repeated
rarely, ectopic corticotropin-releasing hormone tumors.
measurements of several tests, which are sometimes
repeated over an extended period.
Clinical Features
4. Some patients with the syndrome have only cyclic
Features of cortisol excess are the dominant features of the expression of the disease, with periods of activity
syndrome and are those of chronic indolent cortisol excess: extending over several weeks to months, interspersed with
weight gain and central obesity, thin skin with easy bruis- periods of disease inactivity. Laboratory results during
ability and wide violaceous striae, plethora, muscle weakness, periods of disease inactivity may be erroneously normal.
osteoporosis, cessation of linear growth in growing children or Only repeated testing over several months may point to
adolescents, lanugo hair, hypertension, insulin resistance and the underlying disease.
secondary diabetes, hypercalciuria and renal stones, and pro-
pensity to fungal infections. Identification of Cushing Syndrome
Features of adrenal androgen excess may be modest and The best screening tests for Cushing syndrome are the
lead to acne, hirsutism, and menstrual irregularities, as in the 1-mg overnight dexamethasone suppression test, a 24-hour
usual cases of Cushing disease and ACTH-producing bron- urine collection for free cortisol, and late-night salivary cor-
chial carcinoids, or they may be more severe and lead to viril- tisol testing. The demonstration of abnormal dexamethasone
ization, as in adrenal carcinoma. These features may be absent suppressibility or significantly increased late-night salivary
in patients with glucocorticoid-producing adrenal adenoma. cortisol and urinary free cortisol results indicate a diagnosis of
ACTH produced in significant quantities, as in the usual Cushing syndrome.
malignant causes of ectopic-ACTH tumors, may lead to The 1-mg dexamethasone suppression test is a reliable
hyperpigmentation. screening test. The normal response is a plasma cortisol value
Anatomical effects of the underlying tumor include extra- less than 5 g/dL. Patients with Cushing syndrome usually
sellar effects with pituitary macroadenomas, bronchopulmo- have values greater than 10 g/dL. False-positive test results
nary effects of lung cancer, and abdominal pain caused by occur in 13% of patients with simple obesity and in 25% of
adrenocortical carcinoma or metastatic effects of malignant patients who are chronically ill. Sensitivity of this test has
causal tumors. been improved by reducing the plasma cortisol cut-off value,
and a value less than 2 g/dL is believed to exclude Cushing
Features of cortisol excess dominate the clinical picture; syndrome.
variably, one may see the features of adrenal androgen Urinary free cortisol is increased in more than 97% of
excess, ACTH excess, and the mass effects of the patients with Cushing syndrome. It can be increased in
underlying tumor. Occasionally, attention may be drawn states of high urinary output. Importantly, it can be modestly
to the syndrome by the finding of a pituitary or adrenal increased in simple obesity, but a value greater than 300 g per
incidentaloma. 24 hours usually indicates Cushing syndrome.
Features of cortisol excess are usually chronic and slowly
evolving, giving rise to the typical cushingoid features. Screening tests: 1-mg dexamethasone test, urinary free
cortisol (most reliable), or late-night salivary cortisol.
The clinical features of malignant ectopic ACTH tumors
may be dominated by weight loss, weakness, edema, Definitive test: urinary free cortisol >300 g/24
hyperkalemia, hypertension, and secondary diabetes. h or failure of normal suppression in the 2-day
low-dose dexamethasone (2 mg daily) suppression/
corticotropin-releasing hormone test.
Diagnosis
Exclude acute illness, alcoholism, and depression.
The diagnostic approach to a patient with suspected Cushing
syndrome has 2 central components: confirming the diagnosis
of Cushing syndrome and identifying its cause. The following Etiologic Diagnosis
issues make establishing the diagnosis complex: Serum ACTH level is the test that differentiates between
ACTH-dependent and ACTH-independent causes. Plasma
1. Many non-Cushing disorders can increase cortisol ACTH levels are suppressed (<5 pg/mL) in patients with
production and impair hypothalamic-pituitary-adrenal adrenal tumors; normal (2080 pg/mL) or modestly
31. G O N A DA L A N D A D R E N A L D I S O R D E R S 455
increased (<200 pg/mL) in patients with Cushing disease or Clinical Features
ectopic ACTH caused by bronchial carcinoids; and very high
(>200 pg/mL) in most patients with the usual ectopic ACTH The prevalence of primary aldosteronism in the hypertensive
tumor. population is about 10% (5%-13%). Most patients present with
hypertension that is mild to severe (malignant hypertension is
extremely rare) and hypokalemia (>30% have normokalemia).
The most important tests to delineate the cause: serum
Hypokalemia is typically unprovoked, but it may be provoked
ACTH and radiologic evaluation.
significantly and rapidly with diuretic therapy. Most patients
Cushing syndrome caused by adrenal tumor: low or are asymptomatic, but a few report the effects of hypokalemic
undetectable ACTH level and an adrenal mass found on alkalosis (fatigue and muscle weakness, paresthesias, ortho-
abdominal CT. static hypotension, nephrogenic diabetes insipidus, and glu-
cose intolerance). Edema typically is absent.
Cushing syndrome caused by ectopic ACTH tumor:
evident ectopic tumor, rapid clinical course, very high
Presentation: usually asymptomatic hypertension and
ACTH levels (>200 pg/mL), and nonsuppressibility.
unprovoked or easily provoked hypokalemia. However,
Cushing disease: ACTH values are normal or moderately >30% of patients are normokalemic.
increased (<200 pg/mL), and CT or MRI of the sella
Absence of edema because of escape from the
may show a pituitary tumor. About 50% of patients have
salt-retaining effects; no escape occurs from the potassium
normal sellar radiographic features.
and hydrogen ion-losing state.
Therapy
Diagnosis
For Cushing disease, the treatment of choice is transsphe-
noidal surgical adenomectomy or subtotal hypophysectomy. The diagnosis of primary aldosteronism rests on documenting
For postoperative persistent disease, the therapeutic options autonomous aldosterone hypersecretion and on defining the
include pituitary radiotherapy and the interim use of steroido- underlying cause.
genesis blockers, such as ketoconazole, or bilateral adrenalec-
tomy and postoperative pituitary radiotherapy. The treatment Endocrine Diagnosis
for adrenal adenoma is unilateral adrenalectomy. For adrenal Hypokalemia is a classic finding in primary aldoster-
carcinoma, the treatment is unilateral adrenalectomy; mito- onism; however, it may be absent (>30%) and is nonspe-
tane and steroidogenesis blockers are indicated for persistent cific. In a patient with hypokalemia, a urinary potassium
or recurrent disease. Tumor excision is indicated for ectopic level greater than 30 mEq/24 h suggests renal potassium
ACTH tumor; if the tumor is incurable, steroidogenesis wasting and increases the likelihood that the patient has
blockers are used short-term. Bilateral adrenalectomy is rec- aldosteronism.
ommended for tumors with a more indolent course. The characteristic endocrine abnormalities in primary
In all cases of Cushing syndrome, surgical excision of the aldosteronism are increased production of aldosterone
causative tumor is followed by cortisol deficiency caused by the that is autonomous of regulation by the renin-angiotensin
suppressed hypothalamic-pituitary adrenal axis. It may take up system and suppressed plasma renin activity. The best
to 1 or 2 years for the axis to recover; during this period, the screening procedure is to obtain plasma measurements of
patient needs glucocorticoid replacement therapy. aldosterone (PA) (in nanograms per deciliter) and renin
activity (PRA) (in nanograms per milliliter per hour) and
After removal of a causative tumor of Cushing syndrome, to calculate the PA:PRA ratio. It is important to remember
a period of suppression of the normal axis follows and that hypokalemia should be corrected before measurements
may last up to 12 years. During this period, treat with of aldosterone levels, because hypokalemia may reduce the
glucocorticoids, as in adrenocortical failure. aldosterone production in primary aldosteronism. The test
can be done with the patient receiving antihypertensive
Patients who undergo bilateral adrenalectomy require drugs except spironolactone and eplerenone, which are
lifelong glucocorticoid and mineralocorticoid replacement. aldosterone-receptor blockers. An increased PA and a sup-
pressed PRA, with a PA:PRA ratio greater than 20, and a
P R I M A RY A L D O S T E RO N I S M plasma aldosterone concentration greater than 15 g/dL,
suggest primary aldosteronism. An increased PA and an
Etiology
increased PRA with a PA:PRA ratio less than 10 indicate
Primary aldosteronism results from an autonomous renin- secondary aldosteronism. A low PA and a low PRA suggest
angiotensinindependent disorder of the zona glomerulosa. that another mineralocorticoid is the cause of hypertension
It may be caused by idiopathic bilateral hyperplasia (65%), and hypokalemia.
an aldosterone-producing adenoma (30%), unilateral adre- The diagnosis of primary aldosteronism is confirmed by
nal hyperplasia (<5%), adrenocortical carcinoma (<3%), and, demonstrating the unsuppressible autonomous secretion of
very rarely, the familial disorder glucocorticoid-remediable aldosterone despite salt loading (oral salt loading, saline infu-
aldosteronism. sion, or fludrocortisone suppression test).
456 E N D O C R I N O L O GY
Unprovoked or easily provoked hypokalemia is with renin-dependent hyperaldosteronism with hypertension
characteristic of primary aldosteronism. and hypokalemia.
Exclude extrarenal potassium loss by checking urinary
Secondary aldosteronism: hypertension, hypokalemia,
potassium; a value >30 mEq/24 h in a patient with
increased aldosterone, increased plasma renin activity.
hypokalemia suggests a renal potassium-losing state, which
includes mineralocorticoid excess. Other types of mineralocorticoid-induced hypertension:
hypertension with hypokalemia, low aldosterone, and
The best screening test for primary aldosteronism is the
suppressed plasma renin activity.
PA:PRA ratio.
PA:PRA ratio >20: primary aldosteronism.
Therapy
PA:PRA ratio <10: secondary aldosteronism.
Therapy has 3 objectives: control or reverse hypertension, cor-
Confirm the diagnosis by demonstrating autonomous rect hypokalemia, and prevent the noxious effects of excess
aldosterone production (salt loading fails to suppress aldosterone on the cardiovascular system.
aldosterone production). Unilateral adrenalectomy is the treatment of choice for
aldosteronoma or unilateral hyperplasia unless the patient is
Etiologic Diagnosis at high surgical risk. Surgery corrects the hypokalemia in all
The major challenge is to differentiate between a unilateral patients and normalizes the blood pressure or significantly
adrenal disorder (an aldosterone-producing adenoma or uni- improves the hypertension in most (70%). Patients with per-
lateral adrenal hyperplasia) and bilateral adrenal hyperplasia. sistent postoperative hypertension should be treated with
This differentiation has important therapeutic implications. standard antihypertensive drug therapy.
Unilateral adrenal disease is treated surgically by unilateral Medical treatment is indicated for bilateral adrenal hyper-
adrenalectomy. However, bilateral hyperplasia is treated plasia and for aldosteronoma if the patient is at high surgi-
medically by the use of an aldosterone antagonist (see below). cal risk. (Surgical treatment of hyperplasia requires bilateral
This differentiation relies on CT of the adrenals and selective adrenalectomy to normalize the serum potassium level, but it
venous sampling. rarely restores blood pressure to normal levels.) Spironolactone,
CT of the adrenals is used most frequently. An adrenal an aldosterone antagonist, is given in a dosage of 25 to 100
mass usually indicates an aldosterone-producing adenoma. mg every 8 to 12 hours. It restores normokalemia and normal-
However, CT may be misleading because adenomas are small izes blood pressure in most patients. Adverse effects include
and many may be missed, an adrenal mass seen on CT may not gastrointestinal tract upset, menstrual irregularity, and, in
be an aldosteronoma but an adrenal incidentaloma, and the men, gynecomastia and impaired libido and potency. Women
mass may be a hyperplastic nodule in macronodular bilateral of childbearing age who take spironolactone should use oral
adrenal hyperplasia. contraceptives because the drug may cause feminization of the
Selective venous sampling is the most accurate localizing male fetus through its androgen-blocking effects. Eplerenone,
procedure. A unilateral gradient suggests unilateral disease, a highly selective mineralocorticoid receptor antagonist
and the absence of a gradient suggests bilateral hyperplasia. with fewer side effects, has been used as an alternative to
However, this procedure is technically difficult and requires spironolactone; it has not been approved by the US Food
radiologic expertise. and Drug Administration for the management of primary
aldosteronism.
Primary aldosteronism is due to unilateral adenoma or
hyperplasia or to bilateral adrenal hyperplasia. Surgery: unilateral adrenalectomy for patients with
aldosteronoma or unilateral adrenal hyperplasia unless the
The most reliable localizing test is selective venous
patient declines surgery or is at high surgical risk.
sampling; a unilateral gradient suggests an adenoma. The
test is difficult to perform and requires expertise. Medical therapy: for patients with hyperplasia and for
those with aldosteronoma who are at high surgical risk or
CT may demonstrate an adrenal mass but has several
who decline surgery.
pitfalls.
Medical treatment: spironolactone, an aldosterone
Differential Diagnosis antagonist, is most commonly used. Eplerenone has been
The main considerations in the differential diagnosis are used as an alternative.
hypertensive variants of secondary aldosteronism and other
causes of mineralocorticoid-induced hypertension. P H E O C H RO M O C Y TO M A A N D
Secondary aldosteronism associated with hyperten- PA R AG A N G L I O M A
sion results from increased renin production as a conse-
Etiology
quence of renal artery stenosis, malignant hypertension, or a
renin-producing tumor. Plasma renin activity, angiotensin II, Catecholamine-producing chromaffin tumors usually arise
and aldosterone production are increased, and patients present in the adrenal medulla (pheochromocytomas); they arise
31. G O N A DA L A N D A D R E N A L D I S O R D E R S 457
infrequently along the sympathetic chain in the abdomen, genetic syndromes. Normal values of plasma metanephrines
thorax, or neck (paragangliomas), and they arise rarely in exclude the diagnosis of pheochromocytoma; increased val-
sympathetic tissue in the walls of the urinary bladder. They ues, unless markedly elevated, need further confirmation with
are important because, although rare and occurring in less more specific urinary catecholamines and metanephrines. If
than 1% of all hypertensive patients, they usually occur with patients have paroxysmal symptoms, the diagnostic yield can
a distinctive recognizable clinical syndrome, they are curable, be significantly increased by initiating collection during or
and, if untreated, they can be lethal; 10% of these tumors are shortly after a paroxysm.
malignant, and 10% are familial. More than 90% of pheochro-
mocytomas are sporadic, adrenal in location, unilateral, and Document catecholamine hypersecretion. Check urinary
benign. Familial pheochromocytomas are more likely to be catecholamines and metanephrines. Normal values in a
intra-adrenal, bilateral, and malignant. Extra-adrenal tumors hypertensive patient exclude the diagnosis. In patients with
are usually located in the abdomen. Less than 1% of paragan- paroxysmal symptoms, the diagnostic yield is increased
gliomas are located in the chest or neck. significantly by initiating collection during or shortly after
a paroxysm.
458 E N D O C R I N O L O GY
excision is not successful. -Adrenergic blockade is the cor- suppression test is considered superior to measuring the
nerstone of medical therapy and should be instituted as soon 24-hour urinary free cortisol level).
as the diagnosis is made. Phenoxybenzamine is the drug of With the exception of an adrenal myelolipoma, which
choice to control the hypertension and to restore the plasma is benign and has characteristic fat-density images, imaging
volume (a high-salt diet is also important). Its major side effect studies with CT or MR may not differentiate between benign
is postural hypotension. Alternate drugs include prazosin, and malignant neoplasms. However, certain imaging charac-
terazosin, labetalol, nifedipine, and angiotensin-converting teristics make a benign disorder very likely: size less than 4 cm,
enzyme inhibitors. -Adrenergic blockers may be necessary density less than 10 Hounsfield units on CT, homogeneous
to control tachyarrhythmias, but these drugs should be used density, lack of vascularity, and a well-defined border. Bright
only after adequate -blockade to prevent exacerbation of the T2 images on MRI suggest pheochromocytoma or adrenal
hypertension. For hypertensive emergencies, phentolamine, cancer.
an -blocker, is the drug of choice and can be given in 5- to The only place for needle aspiration in the diagnosis
10-mg doses every 5 to 15 minutes as needed. Alternatively, of an adrenal mass is if adrenal metastases are a possibility.
nitroprusside or labetalol can be used. For an inoperable pheo- Pheochromocytoma must be excluded before aspiration.
chromocytoma, add metyrosine, a competitive inhibitor of
tyrosine hydroxylase, to the treatment.
Therapy
Postoperatively, in the surgically cured patient, the urinary
catecholamine and metabolite levels normalize in 2 weeks. Therapy is based on observation and follow-up. Every patient
Long-term follow-up is important to assess for persistence, with an adrenal mass that is not resected should have another
recurrence, or development of other manifestations of the CT scan within 3 to 6 months to assess for growth of the mass.
genetic syndromes mentioned above. If the mass size is stable after 3 to 6 months, additional scans
are performed 12 and 24 months after the diagnosis. Every
Surgical excision of the tumor is curative. mass lesion that demonstrably increases in size during the
observation period should be surgically excised after appropri-
Medical treatment is used in preoperative preparation to
ate biochemical studies are performed.
diminish perioperative morbidity and mortality and on a
long-term basis if surgical excision is not successful.
Exclude pheochromocytoma and a subclinical
-Adrenergic blockade is the cornerstone of medical cortisol-producing tumor before proceeding with any
therapy. It should be instituted as soon as the diagnosis is proposed surgery for an adrenal mass.
made.
Surgical excision is indicated for a functioning adrenal
-Blockade may be necessary to control tachyarrhythmias; mass, a large solid or solid-cystic mass (>6 cm), and
use only after adequate -blockade. cystic masses with blood contents on CT-guided needle
aspiration.
For hypertensive emergencies, use phentolamine (an
-blocker). Otherwise, observation is indicated with subsequent
scans done 36, 12, and 24 months after the diagnosis.
A demonstrable increase in size of the mass at any time
A D R E NA L I N C I D E N TA L O M A dictates surgical removal after appropriate screening
endocrine tests.
Etiology
Small (16 cm) adrenal masses are found in up to 9% of unse-
lected autopsies and in more than 2% of all abdominal imag- DISORDER S OF THE TESTIS
ing studies. Most are nonfunctioning adenomas; a few are
functioning adenomas or carcinomas of the adrenal cortex or
M A L E H Y P O G O NA D I S M I N T H E A D U LT
medulla. Metastatic disease to the adrenal glands is common.
Identification of the nature of the mass is important: nonfunc- Male hypogonadism refers to the clinical presentations result-
tioning adenomas are harmless, a functioning adenoma or a ing from testosterone deficiency. Such deficiency usually is
carcinoma requires surgery, and a metastasis requires onco- associated with defects in spermatogenesis and infertility.
logic care. However, spermatogenic failure may exist independently of
any testosterone deficiency.
Diagnosis
Etiology
The diagnosis of a functioning adrenal tumor rests on clini-
cal evaluation, the use of screening tests, and, when appropri- Testosterone deficiency may result from decreased testoste-
ate, confirmatory tests. For all patients, hormonal evaluation rone production by the testes or target tissue resistance to
should screen for pheochromocytoma (24-hour urinary frac- testosterone action. Decreased testosterone production may
tionated catecholamines and metanephrines) and Cushing be the consequence of primary testicular failure (hypergonado-
syndrome (in this context, a 1-mg overnight dexamethasone tropic hypogonadism) or luteinizing hormone (LH) deficiency
31. G O N A DA L A N D A D R E N A L D I S O R D E R S 459
resulting from a central hypothalamic-pituitary disorder In severe cases, men may have the characteristic facies, loss
(hypogonadotropic hypogonadism). of secondary sex characteristics, and testicular and prostate
Among the causes of primary hypergonadotropic testicular atrophy.
failure are genetic disorders such as Klinefelter syndrome;
The testes must be examined carefully.
traumatic disorders such as those resulting from physical,
radiotherapeutic, or chemotherapeutic agents; inflamma- Bone densitometry is recommended for men with
tory disorders such as those due to mumps or autoimmune long-standing hypogonadism.
endocrinopathy; and degenerative disorders such as myotonia
dystrophica.
Central hypogonadotropism may be a consequence of func-
tional hypothalamic hypogonadotropism, as in constitutional Diagnosis
delay in puberty, or the use of neuroleptic or antidepressant
The diagnosis is suspected on the basis of the clinical picture
drugs, nutritional disorders, systemic illness, stress, or other
and is confirmed by the finding of low serum levels of testoste-
endocrinopathies such as hyperprolactinemia, hyperestro-
rone. Low serum levels of total testosterone may reflect hypo-
genic states, and thyroid or adrenal disorders.
gonadism or abnormalities of sex hormonebinding globulin.
Androgen resistance may be genetic or acquired. Acquired
Most commonly, abnormal testosterone binding is related
androgen resistance may occur with the use of androgen-
to obesity (decreased binding) or aging (increased binding).
receptor blockers such as spironolactone or flutamide.
Low serum levels of free testosterone define hypogonadism.
When convenient and possible, a semen analysis is performed.
Testosterone deficiency may result from decreased In almost all cases, a normal semen analysis indicates a normal
testosterone production or target tissue resistance. hypothalamic-pituitary-gonadal axis.
Decreased testosterone production may result The etiologic diagnosis is suspected on the basis of the
from primary testicular failure (hypergonadotropic clinical picture and is confirmed by measurements of the
failure) or central hypothalamic-pituitary disorder serum levels of LH and follicle-stimulating hormone (FSH).
(hypogonadotropic failure). In primary testicular failure, the serum levels of FSH and
LH are increased (hypergonadotropic hypogonadism).
Primary testicular failure is a consequence of organic Additional tests are not indicated except for determining
diseases of the testes. karyotype (to confirm Klinefelter syndrome or its vari-
Central hypogonadotropism may result from functional or ants or mosaics) or evaluation for other endocrinopathies
organic hypothalamic disorders or from organic diseases of (in patients with autoimmune testicular failure). In central
the anterior pituitary gland. hypothalamic-pituitary hypogonadism, serum levels of LH
and FSH are low or inappropriately normal in relation
Target tissue resistance to testosterone action may be to the low level of serum testosterone (hypogonadotropic
genetic or acquired. hypogonadism). Otherwise, hypogonadotropism dictates a
complete clinical evaluation, determination of serum prolac-
tin level and other pituitary function tests, and an MRI of
Clinical Features the head to exclude mass lesions or other organic forms of
hypothalamic-pituitary disease.
The clinical manifestations of hypogonadism in men include
decreased libido and potency, decreased ejaculate volume,
Suspicion depends on clinical evaluation and the
infertility, decreased energy and stamina, decreased sexual hair
characteristic finding of low serum levels of testosterone.
growth, and gynecomastia. Hot flushes may occur if the tes-
tosterone deficiency has a rapid onset. In men with chronic or A normal semen analysis excludes hypogonadism.
severe testosterone deficiency, physical findings may include
Low serum levels of testosterone may reflect hypogonadism
the classic hypogonadal facies (with pallor and fine wrinkling
or sex hormonebinding globulin abnormalities. Check
around the mouth and eyes), altered feminine-like fat distri-
serum level of free testosterone. Low free testosterone
bution, testicular atrophy, decrease in prostate size, osteoporo-
defines hypogonadism.
sis, and gynecomastia.
The testes must be examined for size (using an orchidom- Serum levels of LH and FSH: determine whether the
eter), consistency, and evidence of structural disease such as hypogonadism is primary testicular (hypergonadotropic)
trauma, infiltrative lesions, infections, or masses. Men with or secondary to hypothalamic-pituitary
estrogen-secreting Leydig cell tumors may present with (hypogonadotropic) disease.
hypogonadism. For men with long-standing hypogonadism,
The cause of hypogonadotropism is usually obvious from
bone densitometry is recommended.
the clinical setting.
Characteristic manifestations of hypogonadism in men Hypogonadotropic hypogonadism should prompt
include decreased libido and potency, decreased ejaculate assessment of the other pituitary functions, MRI of the
volume, gynecomastia, and secondary osteoporosis. head, and consideration of functional hypogonadotropism.
460 E N D O C R I N O L O GY
Therapy most common disorder of the male breast, accounting for
more than 85% of male breast masses. The basic pathophysi-
In adults, androgen therapy is aimed at restoring and maintain- ologic mechanism is an increase in the estrogen to androgen
ing androgenic functions. In hypogonadal pubertal males, it ratio, which may result from androgen deficiency, exposure
is designed to initiate and induce full pubertal development. to exogenous estrogen, or an endogenous increase in estro-
Androgen replacement may be given in the form of parenteral gen production. Gynecomastia may have a benign or sinister
long-acting 17-hydroxyl esters of testosterone (enanthate or cypi- cause. It is always important to attempt to identify a specific
onate esters). They are effective and safe. The usual dosage for an cause. In young pubertal males, the most likely cause is physi-
adult male is 200 mg intramuscularly every 15 days. Alternately, ologic gynecomastia. In adults, the most common causes are
testosterone may be administered transdermally either in the drugs and alcohol-related liver disease. In about 10% of cases,
form of a patch (2.57.5 mg) or gel (2.57.5 mg) applied daily. the cause of gynecomastia is indeterminate or idiopathic.
This therapy is associated with stable physiologic serum testoste-
rone concentrations. Buccal testosterone given twice daily is also
available but experience with it is limited. Oral preparations avail- Diagnosis
able in the United States are all 17-alkylated derivatives of tes-
If gynecomastia is bilateral, exclude pseudogynecomastia (fatty
tosterone. They are less effective and more costly, and they can be
enlargement). If it is unilateral, exclude cancer of the breast.
associated with the potentially serious side effects of hepatotoxic-
Signs that should arouse suspicion of malignancy include an
ity, induction of peliosis hepatis, and hepatic tumors. Assessment
eccentric location in relation to the areola, unusual firmness,
of the adequacy of therapy is best done clinically and by measure-
fixation, ulceration, bloody discharge from the nipple, and the
ment of serum testosterone 2 to 3 months after the institution of
presence of axillary lymphadenopathy. Mammography and
therapy. If the patient has primary hypogonadism, normalization
excisional biopsy may be necessary for definitive diagnosis. A
of serum LH is also used as an indicator of adequacy of therapy.
complete medical history, physical examination, and appro-
Absolute contraindications to androgen therapy include
priate laboratory studies should rule out physiologic, pharma-
androgen-dependent tumors of the prostate and male breast.
cologic, alcohol-related, and refeeding types of gynecomastia.
Relative contraindications include mental retardation, psy-
Endocrine tests may include measurement of the serum levels
chopathy, and obstructive prostatism. Side effects include
of testosterone, estradiol, LH and FSH, -human chorionic
acne, mild weight gain, edema, increased erythropoiesis, and
gonadotropin, sensitive thyrotropin, dehydroepiandrosterone
induction or worsening of obstructive sleep apnea. Androgens
sulfate (DHEAS), and prolactin.
may worsen obstructive uropathy due to benign prostatic
hypertrophy. It is important to remember that prostate cancer
If gynecomastia is bilateral, rule out pseudogynecomastia.
is at least partially an androgen-dependent tumor. A digital
If unilateral, rule out tumors.
rectal examination, a serum prostate-specific antigen level
measurement, and a complete blood cell count should be done Signs that arouse suspicion of malignancy: eccentric
before the initiation of therapy, 3 months after the initiation location in relation to the areola, unusual firmness, fixation,
of therapy, and yearly thereafter. ulceration, bloody discharge from the nipple, and axillary
lymphadenopathy.
In adults, the aims of androgen therapy are to restore and
A complete medical history, physical examination, and
maintain androgenic function. In hypogonadal pubertal
appropriate laboratory studies should rule out physiologic,
males, the objectives are to initiate and induce full pubertal
pharmacologic, alcohol-related, and refeeding types of
development.
gynecomastia.
Androgen replacement therapy includes intramuscular
Endocrine tests may include measurement of the serum
testosterone enanthate or cypionate or use of a transdermal
levels of testosterone, estradiol, LH and FSH, -human
testosterone patch or gel.
chorionic gonadotropin, sensitive thyrotropin, DHEAS,
Oral preparations are all 17-alkylated derivatives of and prolactin.
testosterone. These agents have potentially serious side effects.
Absolute contraindications for testosterone therapy are
androgen-dependent tumors of the prostate and male breast. D I S O R D E R S O F T H E O VA RY
Testosterone therapy may induce erythropoiesis and
aggravate sleep apnea and obstructive prostatism. AMENORRHEA
Primary amenorrhea is present when menarche has not
occurred by age 16 in a young female patient with normal sec-
GY N E C O M A S T I A ondary sex characteristics or by age 14 in the absence of sec-
ondary sex characteristics. Secondary amenorrhea is present
Etiology
when a woman with previously established menstrual func-
Gynecomastia refers to a benign enlargement of the male breast tion experiences the absence of menstruation for more than 3
caused by an increase in glandular and stromal tissues. It is the of her previous cycle intervals or for 6 months.
31. G O N A DA L A N D A D R E N A L D I S O R D E R S 461
Etiology 1. Destruction of pituitary gonadotrophs or the
hypothalamic GnRH cell population by organic diseases
The requirements for normal regular menstrual function are of various origins
the following:
2. Functional suppression of these cells, commonly by a
1. Normal cyclic secretion of hypothalamic nutritional or psychiatric disorder, prolonged heavy
gonadotropin-releasing hormone (GnRH) and the exercise, systemic illness, and other endocrinopathies such
pituitary gonadotropins LH and FSH as uncontrolled diabetes mellitus, hyperprolactinemic
states, and thyroid and adrenal disorders
2. Normal ovarian follicular apparatus that responds to cyclic
gonadotropin stimulation by ovulation and production of Outflow tract disorders are uncommon causes and include
estrogen and progesterone in a cyclic fashion developmental abnormalities.
3. Normal endometrium capable of responding to estradiol Ovarian disorders are the most common cause of primary
(follicular proliferative endometrium) and progesterone amenorrhea; they may be genetic or acquired.
(luteal secretory endometrium) and then to their declining Hypothalamic-pituitary disease may be organic
concentrations by the initiation of menstrual shedding and caused by destructive processes affecting the
endocrine hypothalamus or the anterior pituitary,
Amenorrhea can be physiologic or pathologic. The most or it may be functional and caused by functional
common causes of amenorrhea are physiologic (pregnancy, suppression of GnRH secretion by nutritional or
lactation, and prepubertal and perimenopausal states). psychiatric disorders, systemic disease, and other
Pathologic amenorrhea may result from the following: endocrinopathies.
1. A functional or organic hypothalamic disorder leading to
loss of cyclic GnRH production Secondary Amenorrhea
2. An organic pituitary disorder resulting in loss of the Ovarian disorders are common causes of secondary amenor-
gonadotrope population rhea. The most common disorder is polycystic ovary syndrome
(PCOS). Ovarian destructive processes are an uncommon
3. An organic ovarian disorder resulting in loss of the cause of secondary amenorrhea and premature menopause.
follicular apparatus, or in anovulation, and loss of the These processes include autoimmune oophoritis, abdominal
normal sequential estradiol and progesterone secretion radiotherapy, chemotherapy with agents such as cyclophospha-
4. Organic uterine disorders and loss of the endometrium mide and vincristine, and ovarian tumors that cause secondary
or genital tract disorders preventing egress of the shed amenorrhea by hormonal abnormalities (hypersecretion of
endometrium estrogen, androgen, or human chorionic gonadotropin) or, if
bilateral, by destruction of the ovarian tissue.
Amenorrhea can result from impaired function of any Hypothalamic-pituitary disorders are the most common
component of the hypothalamic-pituitary-gonadal axis pathologic causes of secondary amenorrhea and may be either
or from an anatomical abnormality of the genital tract. functional or organic. Functional hypogonadotropism results
The most common causes of amenorrhea are physiologic: from hypothalamic dysfunction caused by a defect in the cyclic
pregnancy, postpartum lactation, and prepubertal and center, inhibition of the mid-cycle surge of GnRH and LH, and
perimenopausal states. the failure of ovulation. Mild disorders of GnRH release may be
triggered by situational stresses or mild weight loss. Moderate or
The common causes of primary amenorrhea are gonadal severe disorders of GnRH release may occur with severe weight
dysgenesis, constitutional delay in puberty, and mllerian loss, severe emotional stresses, competitive athletics, systemic
agenesis. disease, thyroid disorders, uncontrolled diabetes mellitus, or a
The most common causes of secondary amenorrhea are hyperandrogenic state caused by an adrenal or ovarian disorder.
ovarian disorders, hypothalamic dysfunction, and pituitary In organic hypothalamic-pituitary disorder, hypogonadotropism
disease. can be the only manifestation or it can occur in association with
other pituitary function abnormalities. Hypogonadotropism
can occur as a result of pituitary disorders, hypothalamic dis-
Primary Amenorrhea orders, or disorders of extrasellar structures impinging on the
Outflow tract abnormalities are uncommon causes of pri- hypothalamic-pituitary unit. Hyperprolactinemia is a common
mary amenorrhea. Developmental anomalies include imper- cause of secondary amenorrhea, accounting for 25% to 40% of
forate hymen, isolated absence of the uterus, and vaginal all cases. Postpartum pituitary necrosis (Sheehan syndrome),
aplasia or atresia. Ovarian disorders, including developmen- previously a common cause, has declined in incidence with
tal and acquired disorders, account for most of the causes improvements in obstetric care.
of primary amenorrhea. Hypothalamic-pituitary disease
can cause gonadotropin deficiency and amenorrhea by the Acquired outflow tract abnormalities are uncommon
following: causes of secondary amenorrhea.
462 E N D O C R I N O L O GY
Ovarian disorders are common causes of secondary Estrogen Replacement
amenorrhea. The most common disorder is PCOS. The goals of estrogen therapy include control of vasomotor
Ovarian destructive processes are an uncommon cause of instability, prevention of genitourinary atrophy, preservation
secondary amenorrhea and premature menopause. of secondary sex characteristics, prevention of osteoporosis,
reduction of the risk of coronary artery disease, and restora-
Hypothalamic-pituitary disorders are the most common
tion of a sense of well-being.
pathologic causes of secondary amenorrhea. They may be
Absolute contraindications to estrogen therapy include
functional or organic.
known or suspected estrogen-dependent neoplasm (breast or
uterus), cholestatic hepatic dysfunction, active thromboem-
bolic disorder, history of thromboembolic disorder associated
Clinical Features with previous estrogen use, neuro-ophthalmologic vascular
In addition to amenorrhea, findings of a hypoestrogenic state disease, and undiagnosed vaginal bleeding.
may be present: decreased vaginal secretions and dyspareunia, Estrogen therapy must be individualized and adminis-
hot flushes, osteopenia, and lack of development or loss of tered only after a thorough discussion with the patient about
the secondary sex characteristics. Other findings are related the benefits and risks of the therapy. Therapy is initiated as
to the etiologic disorder, such as hyperandrogenic features, soon as possible after the diagnosis of estrogen deficiency
expressible or spontaneous galactorrhea, shortness of stature and is continued indefinitely or until the cause has been
or Turner stigmata, thyroid dysfunction and goiter, or other reversed.
manifestations of hypopituitarism. Estrogen preparations include oral estradiol (0.52 mg
daily); conjugated estrogens (0.6251.25 mg daily); or trans-
dermal estradiol patch (0.0250.1 mg estradiol daily). Use
Diagnosis progestational agents for a woman with an intact uterus
The diagnostic approach to secondary amenorrhea is summa- (medroxyprogesterone acetate, 10 mg daily, or oral progester-
rized as follows: one, 200 mg daily) for days 1 to 12 of each month. Oral and
transdermal hormonal combinations are also available.
Rule out physiologic amenorrhea (pregnancy test), genital Complications of estrogen replacement include an
tract outflow disorders (clinical evaluation, hysteroscopy), increased risk (4- to 8-fold) of endometrial cancer (usu-
and hyperandrogenic state (clinical evaluation, serum levels ally stage I, with no excess mortality), which is dose- and
of testosterone and DHEAS). duration-dependent. This risk is prevented by progestin sup-
plementation. Other possible adverse effects include a slightly
Measure serum levels of estradiol, LH, and FSH to increased risk of breast cancer (breast examination and mam-
distinguish ovarian disease from hypothalamic-pituitary mography before treatment and annually thereafter are essen-
disease. tial) and increased risk of surgical gallbladder disease.
Low serum levels of estradiol and increased levels of
FSH and LH suggest primary ovarian failure. Obtain a The goal of estrogen therapy is to restore the estrogenic
karyotype if the patient is younger than 30 years. state.
Low serum levels of estradiol and inappropriately low Exclude the absolute contraindications.
levels of FSH and LH suggest a hypothalamic-pituitary Individualize the therapy.
disorder. Rule out a functional disorder and organic
hypothalamic-pituitary disease. Initiate therapy as soon as the diagnosis of
hypoestrogenism is made.
If organic disease is not identified, consider amenorrhea to
be of indeterminate cause and pursue long-term follow-up. Continue therapy indefinitely unless the cause is reversed
or a significant side effect or contraindication develops.
Use progestin supplementation in the woman who still has
Therapy her uterus.
Management is directed at the underlying disorder and resto- Complications of estrogen replacement therapy include
ration of a eugonadal state. It is important to identify and treat an increased risk of endometrial cancer, a possibly slightly
the cause. If the cause cannot be treated successfully, estrogen increased risk of breast cancer, and an increased risk of
replacement and, if feasible, restoration of ovulation and fer- surgical gallbladder disease.
tility potential are indicated.
31. G O N A DA L A N D A D R E N A L D I S O R D E R S 463
P O LYC Y S T I C O VA RY S Y N D RO M E Serum level of testosterone: normal or modestly increased
(70%); it almost always is <200 ng/dL.
PCOS is the most common cause of nonvirilizing hyperan-
drogenicity. It is characterized by oligo-ovulation or anovula- Serum level of DHEAS: normal or mildly increased.
tion, clinical or biochemical evidence of hyperandrogenism,
and polycystic changes in the ovaries: Modest degree of hyperprolactinemia occurs in 25%-30%
of patients.
1. In each ovary, 12 follicles measuring 29 mm in diameter The diagnosis of PCOS is one of exclusion of other causes
of hyperandrogenism.
2. Increased ovarian volume (>10 mL)
3. Increased stromal volume
S U M M A RY
The pathogenesis is poorly understood. Gonadotropin dynam-
ics are abnormal, with loss of the LH surge and increased Primary adrenocortical failure is associated with
LH levels. Hyperandrogenicity is mild to moderate and cortisol, sex steroids, and aldosterone deficiencies. It
LH-dependent. has many organic and functional causes; in the United
In many patients, there is associated obesity and insulin States, the most common causes are autoimmune
resistance and consequent hyperinsulinism, which further con- adrenalitis and bilateral adrenal hemorrhage;
tribute to the androgen excess. Insulin resistance may be present worldwide, tuberculosis-associated adrenalitis is
without obesity. The degree of insulin resistance varies. Many common.
women have a mild form; severe insulin resistance is usually
Secondary adrenal failure is due to ACTH deficiency. It
appreciated clinically by the presence of acanthosis nigricans.
affects production of cortisol and sex steroids, whereas
The onset of the disorder is at puberty, and its progression
aldosterone secretion is basically intact; it is most
is slow and of mild degree. Hirsutism (70% of patients), men-
commonly due to functional suppression of the axis by
strual abnormality (88%), infertility and anovulation (75%),
prolonged glucocorticoid therapy.
and obesity (50%) are usually present. The serum level of tes-
tosterone is normal or modestly increased (70% of patients) Adrenal crisis is precipitated by an illness in a patient
and is nearly always less than 200 ng/dL. DHEAS levels are who has unrecognized adrenocortical failure and
normal or mildly increased in 25% of patients. Changes seen who recently had glucocorticoid therapy withdrawn
on pelvic ultrasonography are characteristic (70%); hyper- or has sustained bilateral hemorrhage of the
prolactinemia may be present in 25% to 30% of patients. It is adrenals.
important to note that anovulation exposes the endometrium
Testosterone deficiency may result from decreased
to unopposed estrogen, which increases the risk of endome-
testosterone production or target tissue resistance.
trial hyperplasia and cancer.
The diagnosis of PCOS is one of exclusion of other causes Decreased testosterone production may result
of hyperandrogenism, such as late-onset congenital adre- from primary testicular failure (hypergonadotropic
nal hyperplasia, Cushing syndrome, and androgen-secreting failure) or central hypothalamic-pituitary disorder
tumors of the ovaries or adrenals. (hypogonadotropic failure).
Amenorrhea can result from impaired function of
PCOS is the most common cause of hyperandrogenicity.
any component of the hypothalamic-pituitary-gonadal
Hyperandrogenicity in PCOS is mild to moderate and axis or from an anatomical abnormality of the
LH-dependent. genital tract.
Features: onset at puberty, slow progression, hirsutism The most common causes of amenorrhea are physiologic:
(70% of patients), menstrual abnormality (88%), infertility pregnancy, postpartum lactation, and prepubertal and
and anovulation (75%), and obesity (50%). perimenopausal states.
464 E N D O C R I N O L O GY
32.
DISORDER S OF CALCIUM AND B ONE METAB OLISM
Marius N. Stan, MD
HYPERCALCEMIA Diagnosis
Elevated serum calcium and PTH levels are hallmarks
The causes of hypercalcemia are categorized as either parathy- of primary hyperparathyroidism. The serum PTH level
roid hormone (PTH) dependent or PTH independent. is usually increased but may be inappropriately normal
for the degree of hypercalcemia. Serum phosphate con-
centrations are normal or low. Urinary calcium excretion
P T H-D E P E N D E N T H Y P E RC A L C E M I A
is high-normal or elevated; this test is also useful to assess
Primary Hyperparathyroidism risk for nephrolithiasis and exclude disorders characterized
by low urinary calcium excretion (eg, familial hypocalci-
Etiology uric hypercalcemia and thiazide use). Characteristic skeletal
Primary hyperparathyroidism is the most common cause radiographic changes include subperiosteal bone resorption,
of hypercalcemia in ambulatory patients. A single parathyroid a salt-and-pepper appearance of the skull, and osteitis fibrosa
adenoma is the cause in 85% of patients, and multiglandular cystica. Renal stones or nephrocalcinosis may be visible on
disease is the cause in the remainder. Parathyroid carcinoma abdominal radiographs.
is a rare cause of hypercalcemia. Primary hyperparathyroidism
may be sporadic or familial. Familial hyperparathyroidism is
The hallmark laboratory findings are elevated serum
usually multiglandular and most commonly a manifestation
calcium and PTH levels.
of multiple endocrine neoplasia (MEN) type 1 (MEN-1) or
type 2 (MEN-2) syndromes. Serum phosphate is usually normal or low.
Urinary calcium is high-normal or elevated; this test can
Parathyroid carcinoma is a rare cause of hypercalcemia.
also help assess risk for renal stones and exclude disorders
Familial hyperparathyroidism is most often due to MEN-1 characterized by low urinary calcium excretion.
or MEN-2 and is usually multiglandular.
Therapy
Clinical Features Surgical parathyroidectomy is the treatment of choice.
Most patients with hyperparathyroidism are asymptomatic Conservative therapy may be indicated for mild uncompli-
and are identified with routine laboratory testing. Symptoms cated disease, especially in the elderly. Indications for surgical
of hypercalcemia include polyuria, polydipsia, constipa- intervention are listed in Box 32.1. Imaging studies are help-
tion, fatigue, and abdominal pain. Hypercalciuria can cause ful for guiding the surgeon, but they do not help in diagnosis.
465
Box 32.1 INDICATIONS FOR SURGICAL Lithium
INTERVENTION FOR PRIMARY Lithium raises the threshold for serum calciums inhibition
HYPERPARATHYROIDISM of PTH secretion. PTH levels are inappropriately normal or
mildly increased. The hypercalcemia resolves after discontinu-
Age <50 y ation of lithium therapy.
Serum calcium level >1 mg/dL above the upper limit of the refer-
ence range Discontinuation of lithium leads to normalization of the
Nephrolithiasis serum calcium.
Osteoporosis
Renal insufficiency (creatinine clearance <60 mL/min)
P T H-I N D E P E N D E N T H Y P E RC A L C E M I A
Preoperative imaging (parathyroid sestamibi scanning or ultra- Hypercalcemia of Malignancy
sonography) often identifies a solitary parathyroid adenoma,
Hypercalcemia of malignancy often develops acutely and may
allowing minimally invasive surgery. Transient, mild hypocal-
be severe and life-threatening. It is the most common cause
cemia is common in the early postoperative period. However,
of hypercalcemia in hospitalized patients. It results from the
in patients with severe preexisting parathyroid-induced bone
destructive effects of skeletal metastases through local cyto-
disease, correction of hyperparathyroidism may lead to marked
kines or the paraneoplastic effect of a malignancy through
and prolonged hypocalcemia due to hungry bone syndrome.
PTH-related peptide. Serum PTH is suppressed in all cases of
hypercalcemia due to malignancy.
Surgical parathyroidectomy is the treatment of choice, but
conservative therapy is reasonable for mild, uncomplicated
Serum PTH is always suppressed in hypercalcemia of
disease, particularly in the elderly.
malignancy.
Imaging studies help guide the surgeon; they are not used
in diagnosis.
Vitamin D Intoxication
Familial Hypocalciuric Hypercalcemia Hypercalcemia, hypercalciuria, renal insufficiency, and soft
Familial hypocalciuric hypercalcemia (FHH) is an autosomal tissue calcification can result from prolonged intake of high
dominant disorder resulting from an altered set point of the levels of vitamin D. Because vitamin D is stored in fat, this
calcium-sensing receptor in the parathyroid glands and renal condition may persist for months after the vitamin D supple-
tubules. It manifests as mild, asymptomatic hypercalcemia in mentation has been discontinued.
a patient with a normal or slightly increased level of PTH,
low urinary calcium, and often a family history positive for The manifestations of vitamin D intoxication may persist
hypercalcemia. The diagnosis is strongly supported by a ratio for months after supplementation is discontinued, because
of urinary calcium to creatinine clearance that is less than 0.01, vitamin D is stored in fat.
distinguishing it from primary hyperparathyroidism. Genetic
testing is clinically available. Parathyroid surgery is not indi-
cated because complications associated with hyperparathy- Sarcoidosis, Granulomatous Disorders,
roidism do not develop. and Lymphoma
The hypercalcemia and hypercalciuria in sarcoidosis, granu-
A ratio of urinary calcium to creatinine clearance <0.01 lomatous disorders, and lymphoma are due to increased
supports a diagnosis of FHH. 1-hydroxylase enzyme activity within the cells of the gran-
uloma or lymphoma, which can autonomously generate
Thiazide-Induced Hypercalcemia 1,25-dihydroxyvitamin D (the active form of vitamin D).
The serum 25-hydroxyvitamin D level is normal, whereas
Mild hypercalcemia may occur in patients taking thiazide the 1,25-dihydroxyvitamin D level is increased. The PTH
diuretics. The hypercalcemia is multifactorial (dehydration, level is low and the serum phosphorus level may be normal or
decreased renal calcium clearance, and possibly increased elevated. The hypercalcemia is responsive to treatment of the
PTH secretion). PTH levels are inappropriately normal or underlying disease and glucocorticoid therapy.
mildly increased. The hypercalcemia usually resolves within a
few weeks of discontinuation of the drug unless it is coexistent The autonomous production of 1,25-dihydroxyvitamin
with primary hyperparathyroidism. D and the 1-hydroxylase activity in granulomas or
lymphoma lead to hypercalcemia and hypercalciuria.
Thiazide diuretics may cause mild hypercalcemia, which is
generally multifactorial. The serum 25-hydroxyvitamin D level is normal,
1,25-dihydroxyvitamin D is elevated, PTH is low, and
PTH is inappropriately normal or mildly increased. phosphorus is normal or elevated.
466 E N D O C R I N O L O GY
Miscellaneous Causes Autoimmune or infiltrative processes, congenital
defect, or hypomagnesemia may lead to decreased PTH
Hyperthyroidism enhances bone turnover and may lead to net secretion.
bone loss. Hypercalcemia and, more often, hypercalciuria may
be present. The hypercalcemia resolves with the treatment of
Pseudohypoparathyroidism is characterized by end-organ
thyrotoxicosis.
(kidney and bone) resistance to the actions of PTH as a result
of a receptor or postreceptor defect. In one type, patients
Treatment of thyrotoxicosis leads to resolution of have a characteristic appearance: short stature, round face,
hypercalcemia. short metacarpals and metatarsals, and mild mental retarda-
tion (Albright hereditary osteodystrophy). A defect in the
Addison disease can cause symptomatic hypercalcemia Gs subunit of the receptor is commonly identified. Patients
related to dehydration and increased albumin concentration. have hypocalcemia, hyperphosphatemia, and elevated PTH.
The hypercalcemia is reversible with glucocorticoid therapy. Pseudopseudohypoparathyroidism is a variant in which patients
have the same characteristic phenotype as patients with
Dehydration and hyperalbuminemia may cause symptomatic Albright hereditary osteodystrophy but do not have the bio-
hypercalcemia in patients with Addison disease. chemical abnormalities.
3 2 . D I S O R D E R S O F C A L C I U M A N D B O N E M ETA B O L I S M 467
D I F F E R E N T I A L D I AG N O S I S preferred form of vitamin D therapy is calcitriol (the active
form of vitamin D). Thiazide diuretics are used to decrease the
The differential diagnosis of hypocalcemia includes hypopara-
risk of marked hypercalciuria, and oral phosphate binders may
thyroidism, decreased vitamin D production, vitamin D resis-
be given to control hyperphosphatemia. It is critical to moni-
tance, and disorders associated with decreased mobilization of
tor therapy closely since patients are at risk of hypercalciuria,
calcium from bone or increased calcium deposition in tissues.
nephrolithiasis, and nephrocalcinosis. Therapeutic doses are
Vitamin D deficiency may be caused by malnutrition, mal-
adjusted to keep the serum level of calcium just below the
absorption, and liver or kidney disease. In acute or chronic
lower limits of normal and the urinary level of calcium at less
renal failure, the pathogenesis of hypocalcemia is thought
than 300 mg in 24 hours.
to be multifactorial, resulting from hyperphosphatemia and
decreased 1,25-dihydroxyvitamin D production. In vitamin
D deficiency, hypocalcemia triggers secondary hyperparathy- Acute, severe hypocalcemia requires urgent therapy with
roidism with renal phosphate wasting. Increased tissue depo- intravenous calcium.
sition occurs in osteoblastic metastases (eg, prostate cancer) Calcitriol is necessary to treat hypoparathyroidism and
and in the hungry bone syndrome occurring after parathyroid- renal insufficiency.
ectomy for hyperparathyroidism with severe bone disease.
Hypocalcemia and soft tissue calcification may also occur in Thiazide diuretics and oral phosphate binders are needed.
acute pancreatitis. Increased calcium elimination is associated
with the use of loop diuretics.
OSTEOPOROSIS
The differential diagnosis of hypocalcemia includes
hypoparathyroidism, disorders leading to vitamin D Osteoporosis is the most common skeletal disorder encoun-
deficiency or resistance, and disorders associated with tered in clinical practice. It is characterized by decreased bone
decreased mobilization of calcium from bone or increased mass, leading to bone fragility and increased risk of fracture.
calcium deposition in tissues. Bone density can be quantified with dual energy x-ray absorp-
tiometry (DEXA). Osteopenia is defined as bone mass that is
between 1.0 and 2.5 standard deviations below the mean peak
D I AG N O S T I C A P P ROAC H bone mass of a sex-matched control population and is desig-
nated by a T score of 1.0 to 2.5. Osteoporosis is defined as
Correct assessment of calcium requires a mathematical cor-
bone mass of at least 2.5 standard deviations below the peak
rection of the total calcium value based on serum albumin
bone mass of a sex-matched control population and is desig-
level or the measurement of ionized calcium. This assessment
nated by a T score of 2.5 or less.
should be followed by measurement of the serum PTH level.
In a hypocalcemic patient, a low PTH level is diagnostic of
hypoparathyroidism. A high PTH level suggests vitamin D Osteoporosis is characterized by decreased bone mass,
deficiency or pseudohypoparathyroidism. Serum concentra- leading to bone fragility and increased fracture risk.
tions of creatinine and magnesium help identify renal failure
and magnesium deficiency states. ET I O L O GY
Mathematical correction of the total calcium value based Osteoporosis may be primary or secondary. Primary osteopo-
on serum albumin level or the measurement of ionized rosis (postmenopausal osteoporosis and senile osteoporosis,
calcium provides an accurate assessment of the serum which occurs in older men and women) is the most common.
calcium level. Secondary osteoporosis may result from endocrine, nutri-
tional, intestinal, neoplastic, or genetic disorders or from cer-
Renal insufficiency and hypomagnesemia should be tain drugs and immobilization (Box 32.2).
excluded.
468 E N D O C R I N O L O GY
C L I N I C A L FE AT U R E S symptoms and esophagitis, particularly if the medication is
taken incorrectly. Ibandronate and zoledronic acid are intrave-
Fractures can occur with minor trauma. Osteoporotic frac-
nous bisphosphonates approved for treatment of osteoporosis
tures heal normally. Vertebral fractures lead to loss of height
when oral forms are not tolerated or cannot be administered.
and spinal deformity. Serum levels of calcium, phosphate, and
Osteonecrosis of the jaw is a rare complication of bisphospho-
alkaline phosphatase are normal.
nate therapy; the risk is significantly higher among patients
given intravenous bisphosphonates while being treated for a
Serum levels of calcium, phosphate, and alkaline
malignancy. Bisphosphonates should not be given to patients
phosphatase are normal in osteoporosis.
who have creatinine clearances of less than 30 to 35 mL/min
because of the risk of renal osteodystrophy.
D I AG N O S I S
The diagnosis of osteoporosis is based on the finding of low Treatment requires adequate calcium and vitamin D
bone mass by DEXA (T score 2.5) or the presence of insuf- supplementation.
ficiency fractures. Other causes of low bone mass, such as Bisphosphonates are first-line therapy for osteoporosis;
osteomalacia, multiple myeloma, and metastatic disease, must they reduce fracture risk and prevent steroid-induced bone
be excluded. Osteomalacia may coexist with osteoporosis. loss.
Myeloma or metastatic disease should be excluded as a cause
of pathologic fracture. Estrogen replacement is effective for preventing and treat-
Secondary causes of osteoporosis should be excluded. ing osteoporosis in postmenopausal women. However, the
Evaluation should include serum levels of calcium, use of estrogen for osteoporosis treatment should be bal-
25-hydroxyvitamin D, testosterone (free, bioavailable, and anced against the risks of breast cancer, venous thrombosis,
total) for males, and thyrotropin. There should be a low thresh- and cardiovascular disease. Raloxifene is a selective estrogen
old for ruling out Cushing syndrome and multiple myeloma. receptor modulator (SERM) effective in the prevention of
DEXA should be used as a screening study for patients at both osteoporosis and breast cancer. It is less effective than
risk of osteoporosis (eg, women 65 years of age or younger bisphosphonates and estrogens with regards to bone benefits,
women or men with risk factors for osteoporosis or osteo- and it increases the risk of thrombotic events. Recombinant
porotic fracture). Routine screening in other populations (eg, PTH (teriparatide) is a potent enhancer of bone formation by
men >70 years of age) is currently debated. increasing bone turnover. Patients who have increased bone
turnover (eg, Paget disease) or an increased risk of osteosar-
Other causes of low bone mass (eg, osteomalacia, multiple coma (eg, prior radiotherapy to bone) are not candidates for
myeloma, and metastases) must be excluded. this therapy. It is administered as a daily subcutaneous injec-
Causes of secondary osteoporosis should be considered, tion for a maximum of 2 years. Nasal calcitonin is a weak anti-
and levels of calcium, 25-hydroxyvitamin D, testosterone resorptive agent with some analgesic properties.
(in males), and thyrotropin should be measured.
Raloxifene can be used to prevent osteoporosis and breast
cancer, but it is less effective than both bisphosphonates
P R EV E N T I O N A N D T R E AT M E N T O F and estrogen in terms of bone benefits.
O S T EO P O RO S I S
Recombinant PTH enhances bone formation but should
Bone loss can be prevented through adequate lifestyle activi- not be used in patients with conditions of increased bone
ties, including regular weight-bearing exercise, tobacco avoid- turnover or increased risk for osteosarcoma.
ance, and avoidance of excessive alcohol use. All adults should
consume an adequate amount of vitamin D (400800 inter-
national units) and calcium (1,0001,200 mg) daily. Estrogen O S T E O M A L AC I A
replacement in women at or after menopause is effective but
must be balanced against its known risks.
D E FI N IT I O N A N D ET I O L O GY
Weight-bearing exercise, tobacco avoidance, nonexcessive Osteomalacia is characterized by inadequate mineralization
alcohol intake, and intake of adequate amounts of calcium of newly formed bone. Normal bone mineralization requires
and vitamin D are all essential components of therapy. adequate calcium and phosphate concentrations, functional
osteoblasts, and optimal conditions for the mineralization of
Therapy requires adequate calcium and vitamin D supple- mature osteoid. Osteomalacia ensues when these conditions
mentation, similar to preventive approaches. Bisphosphonates are not met. Vitamin D deficiency is the most common cause
are considered first-line therapies for osteoporosis. Alendro- of osteomalacia. It results from inadequate oral intake, mal-
nate, risedronate, and ibandronate are oral bisphospho- absorption (celiac disease), limited sun exposure, or decreased
nates with potent antiresorptive effects that prevent bone liver production of 25-hydroxyvitamin D (due to liver dis-
loss. They reduce fracture risk and are effective in prevent- ease or drug side effect). Renal disease and inherited disor-
ing steroid-induced bone loss. Side effects include dyspeptic ders affecting activation or action of vitamin D can also cause
3 2 . D I S O R D E R S O F C A L C I U M A N D B O N E M ETA B O L I S M 469
osteomalacia. Phosphate deficiency may result from malnutri- C L I N I C A L FE AT U R E S
tion or increased renal losses. This is seen in inherited condi-
Most patients present with increased serum levels of alka-
tions such as hypophosphatemic rickets. An acquired tubular
line phosphatase or a radiographic abnormality. Serum alka-
phosphate leak can occur with some mesenchymal tumors
line phosphatase is the most useful marker of disease activity
(oncogenic osteomalacia) or with multiple myeloma (general-
and response to therapy. The main clinical features are bone
ized tubular defect in renal Fanconi syndrome).
pain and deformity. Disorganized bone remodeling results in
decreased tensile strength, skeletal pain, and bone deformities.
Vitamin D deficiency is the most common cause of Pain may also be related to fracture, degenerative changes in
osteomalacia. adjoining joints, or, rarely, the development of osteosarcoma.
Commonly affected sites include the sacrum, spine, femur,
C L I N I C A L FE AT U R E S tibia, skull, and pelvis. Other complications include nerve
Typical symptoms of osteomalacia include diffuse bone pain and entrapment, hydrocephalus due to the development of platy-
tenderness along with muscle weakness. Calcium and phospho- basia, and high-output cardiac failure due to increased vascu-
rus levels are low or low-normal, and the serum alkaline phos- larity of affected bones.
phatase level is usually increased. With vitamin D deficiency,
secondary hyperparathyroidism also occurs. Radiographs can Alkaline phosphatase is a useful marker of disease activity
display pseudofractures in later stages of osteomalacia. These and response to therapy.
are narrow lines of radiolucency perpendicular to the cortical The most commonly affected sites are the sacrum, spine,
bone surface; they are typically bilateral and symmetrical. They femur, tibia, skull, and pelvis.
are found most commonly in the pubic rami and the medial
aspect of the femur near the femoral head.
D I AG N O S I S
Calcium and phosphorus levels are low or low-normal, and Paget disease should be suspected if the serum alkaline phos-
the serum alkaline phosphatase level is increased. phatase level is increased and the serum calcium, phosphate,
and 25-hydroxyvitamin D levels are normal. A bone scan is
Secondary hyperparathyroidism occurs with vitamin D
the most sensitive test for identifying bone lesions of Paget
deficiency.
disease. Plain radiographs are best for further definition of the
affected bones (expansion, sclerosis, deformity) and surround-
THERAPY ing joints.
Effective therapy requires treating the underlying disorder
and providing adequate calcium and phosphate to the areas Consider Paget disease if the alkaline phosphatase level is
of inadequate mineralization. This usually is achieved with elevated while calcium, phosphate, and 25-hydroxyvitamin
calcium, vitamin D, and, when indicated, phosphate supple- D levels are normal.
mentation. Vitamin D dosing regimens vary, but a common A bone scan is the most sensitive test to identify lesions of
approach is 50,000 IU weekly for 8 weeks followed by 800 IU Paget disease.
daily for maintenance. Osteomalacia is considered adequately
treated when urinary calcium excretion and bone density
start to increase. The goal of therapy is to achieve bone heal- THERAPY
ing while normalizing the serum concentrations of calcium, Many patients require only monitoring of alkaline phos-
phosphate, vitamin D, and alkaline phosphatase. Alkaline phatase levels. The decision to initiate therapy relates to
phosphatase can remain elevated for several months after cor- the presence of symptoms, the location of the bone lesions,
rection of vitamin D deficiency. During therapy, serum and and the disease activity. Indications for therapy are bone
urinary calcium levels should be closely monitored to avoid pain, disease involving bones where complications could
hypercalcemia, hypercalciuria, and nephrocalcinosis. occur (skull, spine, weight-bearing bone, or near joints)
or a significant increase in the serum alkaline phosphatase
When urinary calcium excretion and bone density start to level. Medical therapy consists of oral or intravenous bis-
increase, osteomalacia is considered adequately treated. phosphonates. Alkaline phosphatase levels are used to
The goal of therapy is bone healing and normalization of monitor therapy. Orthopedic surgery may be needed to
calcium, phosphate, vitamin D, and alkaline phosphatase treat deformity, fracture, or degenerative joint disease.
levels. Neurosurgical intervention may be required for nerve
entrapment syndromes.
PAG ET D I S E A S E Monitoring alkaline phosphatase levels is sufficient for
most patients.
Paget disease affects 3% of the population older than 45 years
and is characterized by increased bone resorption with disorga- Bisphosphonates are the mainstay of therapy; monitor
nized bone remodeling. Its pathogenesis is not fully understood. therapy with alkaline phosphatase levels.
470 E N D O C R I N O L O GY
S U M M A RY The differential diagnosis of hypocalcemia includes
hypoparathyroidism, disorders leading to vitamin D
Primary hyperparathyroidism: elevated serum calcium deficiency or resistance, and disorders associated with
and PTH levels, normal or low serum phosphate, and decreased mobilization of calcium from bone or increased
high-normal or elevated urinary calcium. calcium deposition in tissues.
Serum PTH is always suppressed in hypercalcemia of Osteoporosis: serum levels of calcium, phosphate, and
malignancy. alkaline phosphatase are normal.
Treatment of the underlying cause, rehydration Osteomalacia: calcium and phosphorus levels are low or
with volume expansion to promote calciuriesis, and low-normal, and the serum alkaline phosphatase level is
administration of pamidronate are cornerstones of therapy increased.
for patients with hypercalcemia.
Consider Paget disease if the alkaline phosphatase level is
Hypocalcemia, hyperphosphatemia, and low PTH level are elevated while calcium, phosphate, and 25-hydroxyvitamin
the common findings in hypoparathyroidism. D levels are normal.
3 2 . D I S O R D E R S O F C A L C I U M A N D B O N E M ETA B O L I S M 471
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PA RT V I I
O N C O L O GY
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33.
ONCOLOGY
Timothy J. Moynihan, MD, and Michelle A. Neben Wittich, MD
475
Table 33.1 RISK FACTORS FOR BREAST CANCER
HIGH RISK: RELATIVE RISK >4.0 MODERATE RISK: RELATIVE RISK 24 LOW RISK: RELATIVE RISK 12
Older age Any first-degree relative with breast cancer Menarche before age 12 y
Personal history of breast cancer Personal history of ovarian or endometrial cancer Menopause after age 55 y
Family history of premenopausal bilateral breast Age at first full-term pregnancy >30 y White race
cancer or familial cancer syndrome
Breast biopsy showing proliferative disease with Obesity in postmenopausal women Long-duration (15 y) estrogen
atypia replacement therapy
Dense breast tissue on mammography Upper socioeconomic class
Prior history of radiation therapy
(eg, Hodgkin disease or lymphoma)
Ten percent of breast cancers found on physical not have metastatic potential because by definition it has
examination are missed by mammography. not invaded through the basement membrane. Infiltrating
ductal carcinoma is the most common histologic type (70%
Ultrasonography is recommended for a suspicious palpable
of breast cancers) of invasive breast cancer. Invasive lobu-
lump, even if mammography is negative.
lar carcinoma makes up 25% of breast cancers, is more fre-
Biopsy should be done for lumps with a solid component quently multifocal and bilateral, and is less likely to be seen
on ultrasonography. on mammography.
Ductal carcinoma in situ is noninvasive, does not have the
MRI is recommended for women at very high risk for potential for systemic spread, and is primarily treated with
breast cancer and women with dense breast tissue on local therapy only, including resection with or without breast
mammography, but it is controversial in women with irradiation. However, if left untreated, ductal carcinoma in
newly diagnosed breast cancer. situ can progress to invasive disease. Lobular carcinoma in situ
is not believed to be a precursor for invasive disease, but it is
a marker for increased risk for future development of invasive
PAT H O L O GY carcinoma in the ipsilateral or contralateral breast. Use of the
selective estrogen-receptor modulator tamoxifen after resec-
Breast cancer can be invasive or noninvasive (in situ). tion of estrogen-receptorpositive or progesterone-receptor
Ninety-five percent of breast cancers are classified as duc- positive ductal carcinoma in situ is frequently considered.
tal (70%) or lobular (25%), corresponding to the ducts and This drug does decrease the risk of a subsequent breast event
lobules of the normal breast (Figure 33.1). Invasive (some- (defined as either recurrent carcinoma in situ or development
times called infiltrating) breast cancer has the potential for of an invasive breast cancer in the ipsilateral or contralateral
systemic spread, as opposed to carcinoma in situ, which does breast) in the subsequent 10 years from 13% to 8%; however,
there is no evidence of increased survival with use of tamox-
Lobular ifen and it is associated with a substantial potential for adverse
effects.
476 O N C O L O GY
100
Box 33.1 STAGING OF BREAST CANCER
80 0 (n=279)
Primary tumor (T)
TIS Carcinoma in situ
Disease Free, %
60
T1 T = 2 cm
1-3 (n=160)
T2 T = 2.15 cm
40 4-6 (n=65)
T3 T = >5 cm
T4 T of any size with direct extension to chest wall 7-12 (n=55)
20
or skin n=614
Regional nodes (N) P=.001 13 (n=55)
0
N0 No involved nodes
0 12 24 36 48 60 72 84 96 108 120 132
N1 Movable ipsilateral axillary nodes
Months After Mastectomy
N2 Matted or fixed nodes, or in clinically apparent ipsi-
lateral internal mammary nodes in the absence of Figure 33.2 Relation of Disease-Free Survival to Numbers of Nodal
clinically evident axillary lymph node metastasis Metastases. Data are for more than 600 women with breast cancer
N3 Metastasis in ipsilateral infraclavicular lymph nodes treated with radical mastectomy alone in the early 1970s. (From Fisher
Distant metastasis (M) ER, Sass R, Fisher B. Pathologic findings from the National Surgical
Adjuvant Project for Breast Cancers [protocol no. 4]. X. Discriminants
M0 None detected for tenth year treatment failure. Cancer. 1984 Feb 1;53[3 Suppl]:71223.
M1 Distant metastasis present (includes ipsilateral Used with permission.)
supraclavicular nodes)
Stage grouping
Stage I T1 N0 for estrogen-receptorpositive disease is higher than that for
Stage IIA T0 N1 estrogen-receptornegative disease. Extent of hormone posi-
T1 N1 tivity may be very important in treatment outcome; patients
T2 N0 = Operable disease with more than 90% of tumor cells staining positive for estro-
Stage IIB T2 N1 gen receptor respond very well to hormonal therapies and may
T3 N0 be able to avoid adjuvant chemotherapy, whereas those whose
Stage IIIA T0 N2 tumors are weakly positive or negative for estrogen receptor
T1 N2 may benefit from adjuvant chemotherapy.
T2 N2 = Locally advanced disease
T3 N1,N2 HER2/neu
Stage IIIB T4, Any N
Stage IIIC Any T N3 = Advanced disease HER2/neu is a transmembrane protein that is overexpressed in
Stage IV Any T Any N M1 = Advanced or metastatic approximately 20% to 30% of breast cancers. Without the use
of anti-HER2/neudirected therapy, tumors that are HER2/
Data from Singletary SE, Allred C, Ashley P, Bassett LW, Berry D, Bland KI, neu-positive are associated with a higher risk of recurrence and
et al. Revision of the American Joint Committee on Cancer staging system for
breast cancer. J Clin Oncol. 2002 Sep 1;20(17):362836. an overall worse prognosis. Women with HER2/neu-positive
disease are usually recommended to receive adjuvant chemo-
therapy, even in the presence of otherwise good risk features
NAT U R A L H I S TO RY A N D P RO G N O S T I C (such as small tumor size and negative nodes). In addition, the
FAC TO R S
Nodal Status Table 33.2 LONG-TERM RESULTS a IN PATIENTS
The number of involved axillary lymph nodes is the most WITH NODE-NEGATIVE BREAST CANCER TREATED
important predictor of outcome (Figure 33.2). SURGICALLY
After nodal status, tumor size is the most important prognos- <1 171 88 10
tic factor (Table 33.2).
1.12.0 303 74 24
2.13.0 188 72 24
Hormone Receptor Status
3.15.0 105 61 36
In general, patients with estrogen-receptorpositive tumors
have a better prognosis, especially in the first 5 to 10 years a
Median duration of follow-up was 18 years.
after initial diagnosis. However, the difference in recur- Data from Rosen PP, Groshen S, Kinne DW. Survival and prognostic factors in
rence rates at 5 years is only 8% to 10% when compared with node-negative breast cancer: results of long-term follow-up studies. J Natl Cancer
receptor-negative disease. After 5 years, the recurrence rate Inst Monogr. 1992;(11):15962.
33. O N C O L O GY 477
use of therapies directed against the HER2/neu pathway such the sentinel lymph node does not have metastatic tumor cells,
as trastuzumab (Herceptin) greatly improve the prognosis. then the probability of other lymph nodes being affected is
HER2/neu tumors also seem to have a significantly increased less than 5%. When compared with axillary lymph node dis-
risk of recurrence within the central nervous system. section, sentinel lymph node biopsy decreases late complica-
tions such as lymphedema.
Triple-Negative Breast Cancer
Breast conservation plus radiation is equivalent to
A recently described subset of breast cancer is known as triple mastectomy in terms of overall survival.
negative, meaning that the cancer cells show no evidence of
Compared with axillary lymph node dissection, sentinel
overexpression of estrogen receptors, progesterone receptors,
lymph node biopsy is associated with less risk of
or HER2/neu. Triple-negative tumors tend to have a bet-
lymphedema.
ter response to chemotherapy than other subtypes, yet they
are associated with a poorer overall prognosis. Patients with
triple-negative disease who show no evidence of recurrence Adjuvant Treatment
after 5 years are at lower risk of late, distant recurrence.
After primary treatment of the breast, additional systemic
treatment (adjuvant) has been shown to decrease the risk
Grade of systemic recurrence and improve overall survival. The
number of involved axillary lymph nodes is the single most
Most breast cancers are high-grade. Patients with low-grade
important predictor of outcome. Women with metastatically
tumors have fewer recurrences and longer survivals.
involved axillary lymph nodes should generally be offered
adjuvant treatment: chemotherapy or hormonal therapy
The number of involved axillary nodes is the most
or both. Women with negative lymph nodes have a 25% or
important predictor of outcome.
less chance of microscopic metastatic disease. Adjuvant sys-
After nodal status, tumor size is the most important temic treatment should generally be offered to women in the
prognostic factor. intermediate- and high-risk groups. Chemotherapy has been
shown to decrease the risk of recurrence and improve over-
Patients with receptor-positive tumors have a better
all survival in both node-negative and node-positive cancer,
prognosis.
but it is associated with more toxicity than hormonal therapy.
Overexpression of HER2/neu confers a poorer prognosis Women with node-negative tumors of more than 1 centime-
if not treated with anti-HER2/neu therapies and alters ter and with node-positive cancers that overexpress HER2/
recommendations for adjuvant therapy. neu should also be offered adjuvant trastuzumab (Herceptin)
therapy.
All breast cancers should be tested for status of estrogen Long-term follow-up of women with breast cancer (espe-
receptors, progesterone receptors, and HER2/neu. cially hormone-receptorpositive disease) is essential because
Patients with low-grade tumors have a better prognosis. there are as many recurrences 5 to 15 years after diagnosis as
there are in the first 5 years after diagnosis, and metastatic dis-
ease can first become apparent 30 or more years later.
T R E AT M E N T
Women with node-positive disease are at high risk of
Primary or Local-Regional Treatment systemic disease and should be offered adjuvant treatment.
Primary local treatment for invasive breast cancer is either Women with node-negative disease have a 25% or less
lumpectomy (also known as wide local excision or breast chance of systemic disease.
conservation) followed by radiation or mastectomy. Several
randomized controlled clinical trials have shown therapeutic Adjuvant therapy decisions should be individualized on
equivalence for breast conservation compared with mastec- the basis of each persons risk of recurrence.
tomy in terms of overall survival, whereas mastectomy has a
slightly lower local recurrence rate. The outcome for women
Treatment of Advanced Disease
with invasive breast cancer depends more on the presence
of distant microscopic metastatic disease rather than on the We currently lack curative therapy for recurrent metastatic
treatment of local disease. The most important predictor for breast cancer. The median duration of survival with recur-
the presence of micrometastatic disease is involvement of rent disease is 2.5 years, but the spectrum of survival is very
axillary lymph nodes. All women with invasive breast cancer wide. Survival is generally longer with bone-only or soft tis-
should have axillary lymph node dissection or a newer proce- sue recurrence than with visceral recurrence. Because treat-
dure called a sentinel lymph node biopsy. If the sentinel lymph ment is not curative, the initial systemic treatment for
node shows histologic signs of cancer, then a complete axillary patients with estrogen-receptorpositive advanced disease
lymph node dissection should be considered based on features is usually hormonal. Chemotherapy is used once disease
that predict for involvement of additional lymph nodes. If has progressed in patients with hormone-receptorpositive
478 O N C O L O GY
disease while receiving hormonal therapy or in patients with Aromatase inhibitors increase the risk of osteoporosis,
estrogen-receptornegative breast cancer. severe arthralgias, and vaginal dryness, but they do not
increase the risk of thromboembolism risk or endometrial
There is no curative therapy for recurrent metastatic breast cancer.
cancer.
Premenopausal women with hormonally sensitive disease
The average survival with recurrent breast cancer is may also benefit from oophorectomy (either chemical or
2.5 years. surgical).
33. O N C O L O GY 479
altered sexual function, osteoporosis, myelodysplastic syn- P R EV E N T I O N
drome, and late cardiac toxicity. Exercise and maintenance of
The majority of cases of cervical cancer are associated with
ideal body weight, while not definitively proven to decrease
human papillomavirus. A recently approved vaccine (Gardasil)
cancer recurrence, should be recommended.
can provide protection against the 4 most common strains of
the virus and has shown efficacy in decreasing the risk of cer-
PAT T ER NS O F R ECU R R E N C E vical cancer. The American Cancer Society recommends this
vaccine for all females before onset of sexual activity. In 2011,
Breast cancer tends to recur in bones, liver, lungs, or brain or the US Food and Drug Administration approved use of this
locally in the chest wall or residual breast. Recurrences can vaccine for males to help prevent spread of human papilloma-
occur decades after initial diagnosis, and this possibility must virus and to prevent the relatively rare penile cancer. Other
always be kept in mind in any patient with a history of breast methods for prevention include decreasing high-risk behavior,
cancer. Hormone receptornegative disease and HER2/ such as limiting sexual partners and use of condoms.
neu-positive disease are more aggressive, and these both tend
to recur earlier than hormone receptorpositive disease.
Recent data suggest that women with HER2/neu-positive C O L O R E C TA L C A N C E R
tumors who have treatment with trastuzumab (Herceptin)
have a higher chance of recurrence in the central nervous sys-
tem. Hormone receptorpositive disease is more indolent; BAC KG RO U N D
only about 20% of recurrences happen within the first 5 years
Colorectal cancer is diagnosed in approximately 148,000
after initial diagnosis, and metastatic recurrences can occur
Americans and causes 57,000 deaths each year. Colorectal
decades later.
cancer is the second most common cause of cancer death in
North America and Europe. The incidence of colorectal can-
cer has declined during the past few years, following its peak
C E RVI C A L C A N C E R
in the late 1990s. It is associated with high-fat, low-fiber diets.
Decreased levels of physical activity and obesity are also asso-
BAC KG RO U N D ciated with an increased risk of colorectal cancer. Population
screening with fecal occult blood testing remains problematic.
In recent decades, the incidence of cervical cancer has Although one study showed a reduction in mortality from
decreased by 30% and mortality associated with cervical can- colorectal cancer with fecal occult blood screening, any partic-
cer has decreased by 40%. These changes have been attributed ipants who had positive results went on to have colonoscopy.
to widespread use of cytologic (Papanicolaou) smear screen- Another study showed that fecal occult blood tests failed to
ing. In US women each year, there are 12,200 new cases of detect 70% of colorectal cancers and 80% of large (2 cm)
cervical cancer and 4,100 associated deaths. In addition, more polyps. Although specific screening recommendations vary,
than 50,000 cases of carcinoma in situ of the cervix are diag- some form of screening should be initiated by age 50 years
nosed annually. Risk factors for cervical cancer include first regardless of risk. For high-risk patients, such as those with a
intercourse at an early age, a greater number of sexual partners, family history of colorectal cancer or a prior colorectal cancer,
smoking, history of sexually transmitted disease, especially structural studies of the entire large bowel, such as colonos-
herpesvirus or human papillomavirus, and lower socioeco- copy (every 510 years) or (less preferable) rectosigmoidos-
nomic class. It is now understood that human papillomavirus copy plus barium enema, should be performed at appropriate
is an etiologic agent for cervical carcinogenesis. intervals (such as every 13 years).
If a Papanicolaou smear shows dysplasia or malignant
cells, colposcopy with directed biopsy should be done. The
Colorectal cancer is associated with high-fat, low-fiber
Papanicolaou smear has limited sensitivity; false-negative rates
diets, decreased physical activity, and obesity.
of 20% frequently are quoted. The American Cancer Society
recommends that asymptomatic, low-risk women 20 years of Although specific screening recommendations vary, some
age or older and those younger than 20 years who are sexually form of screening process should be initiated by age 50
active have a Papanicolaou smear annually for 2 consecutive years regardless of risk.
years and, if the results are negative, at least 1 every 3 years.
For high-risk patients, the entire large bowel should be
studied at appropriate intervals.
T R E AT M E N T
Treatment for carcinoma in situ of the cervix is usually total
R I S K FAC TO R S
hysterectomy. If childbearing is desired, a more conservative
approach, such as a therapeutic conization, is another option. Approximately 10% of colorectal cancer is related to either
Early invasive carcinoma of the cervix is usually treated with defined or as yet undefined familial syndromes. High-risk
total hysterectomy. For patients with higher-stage disease, a groups include persons with 1) familial polyposis syn-
combination of chemotherapy (cisplatin-based) and radiation dromes (familial adenomatous polyposisfor which a gene
therapy is recommended. recently was identified on chromosome 5and Gardner
480 O N C O L O GY
syndromegut polyps plus desmoid tumors, lipomas, seba- standard recommendations for deeply invasive but lymph-node
ceous cysts, and other abnormalities), accounting for 1% of negative (stage II) colon carcinomas. For rectal cancers, a com-
colorectal cancer; 2) familial cancer syndromes without pol- bination of chemotherapy (5-FUbased) and pelvic irradia-
yps (hereditary nonpolyposis colorectal cancer or Lynch syn- tion, preferably administered preoperatively (neoadjuvant),
drome, which are marked by colon cancer with or without is standard for stage II and III disease followed by adjuvant
endometrial, breast, and other cancers), accounting for 3% to chemotherapy after surgery.
4% of colorectal cancer; and 3) inflammatory bowel disease
(incidence, 12% after 25 years). For stage III colon cancers, adjuvant chemotherapy is
indicated.
High-risk factors for colorectal cancer are familial
For rectal cancer, a preoperative combination of
polyposis syndromes, including familial adenomatous
chemotherapy and radiotherapy is the standard
polyposis and Gardner syndrome, both inherited as an
recommendation.
autosomal dominant trait; select familial cancer syndromes
without polyps; and inflammatory bowel disease.
Metastatic Disease
T R E AT M E N T
Certain patients with metastatic colorectal cancer may be can-
Surgery didates for an attempt at curative resection of their metastatic
disease. Of carefully selected patients with minimal meta-
Surgical resection is the preferred method of curative treat-
static disease, limited to the liver or lung, 30% to 40% survive
ment for carcinomas of the colon or rectum for all but the
beyond 5 years, many without further evidence of disease
very earliest cancers. Surgical exploration and resection allow
recurrence, after resection of metastatic lesions and systemic
for pathologic determination of tumor depth of penetration
chemotherapy.
through the bowel wall and assessment of regional lymph
Palliative chemotherapy is the only option for the vast
nodes. Prognosis is directly related to the stage of disease
majority of patients with advanced metastatic colorectal can-
(Table 33.3). Five-year survival rates for locoregional disease
cer. The median duration of survival for patients given medical
have improved in recent decades as a result of many factors,
therapy is about 24 months.
including improvements in preoperative staging, surgical tech-
nique, adequate lymph node retrieval, and the use of neoadju-
vant (preoperative) and adjuvant (postoperative) therapy. Surgical resection of metastatic disease can result in
long-term disease-free survival in a select subset of patients.
Surgical resection is the preferred treatment for colorectal Palliative conventional chemotherapy is the only option for
cancer. advanced colorectal carcinoma.
Prognosis is directly related to the stage of disease.
Five-year survival rates are improving.
Carcinoembryonic Antigen
Until recently, routine monitoring of carcinoembryonic
antigen (CEA) after curative resection of colon cancer was
Adjuvant Therapy
not recommended. Current American Society of Clinical
For colon cancers, adjuvant chemotherapy with a multidrug Oncology guidelines do recommend that the CEA level be
regimen that includes oxaliplatin, 5-fluorouracil (5-FU), checked preoperatively if it would assist in staging and surgi-
and leucovorin, given for 6 months, is recommended for cal planning. After curative treatment for colon cancer, the
node-positive (stage III) disease. Controversy exists about guidelines recommend that the CEA level be checked every
DEPTH OF NODAL
DUKES STAGE AJCC STAGE PENETRATION STATUS 5-YEAR SURVIVAL, %
A I Submucosa or Negative 90
muscularis
33. O N C O L O GY 481
3 months for at least 3 years in patients with stage II and H I S TO L O G I C T Y P E S A N D C H A R AC T E R I S T I C S
III disease, as long as the patients general medical condition
Lung cancer is divided into small cell and nonsmall cell types.
is such that the patient would be a candidate for surgical
Small cell lung cancer occurs almost exclusively in smokers.
intervention or chemotherapy. Monitoring of CEA may be
The primary tumors are often small but are associated with
useful for determining the response of metastatic disease to
bulky mediastinal adenopathy. They may be associated with
therapy.
paraneoplastic syndromes, including the syndrome of inap-
propriate secretion of antidiuretic hormone, and various
neurologic abnormalities. Nonsmall cell lung cancers can be
LU N G C A N C E R
divided into squamous, adenocarcinoma, and large cell types.
Squamous cell carcinomas may be associated with hypercalce-
M AG N IT U D E O F T H E P RO B L E M mia due to the secretion of a parathyroid hormone-like pep-
tide. Squamous carcinomas tend to occur centrally, whereas
Approximately 172,000 new cases of lung cancer are diagnosed large cell and adenocarcinoma types tend to be more periph-
in the United States annually, and approximately 157,000 eral. Adenocarcinoma is the most frequent histologic subtype
deaths from lung cancer occur. Thus, only approximately 15% in nonsmokers. Bronchoalveolar carcinoma is a low-grade
of patients with lung cancer survive the disease. Lung can- nonsmall cell carcinoma that frequently presents as a patchy
cer is the leading cause of cancer mortality in both men and infiltrate. It may be multifocal.
women.
S TAG I N G
R I S K FAC TO R S
The classic Tumor-Node-Metastasis (TNM) system is simpli-
About 95% of lung cancers in men and about 80% of lung fied in Table 33.4.
cancers in women result from cigarette smoking. Men who
smoke 1 to 2 packs per day have up to a 25-fold increased risk
for lung cancer compared with men who have never smoked. NAT U R A L H I S TO RY
The risk for lung cancer in an ex-smoker declines with time. The natural history of surgically treated lung cancer, by stage,
Passive smoking is associated with an increased risk of lung is shown in Figure 33.3.
cancer. Certain occupations (eg, smelter and iron workers),
chemicals (eg, arsenic and methylethyl ether), and exposure to
radioactive agents and asbestos are associated with increased T R E AT M E N T
risks for lung cancer.
NonSmall Cell Lung Cancer
95% of lung cancers in men and 80% in women result from Resection is the treatment of choice for clinical stages I, II, and
cigarette smoking. selected IIIA nonsmall cell lung cancer. The use of adjuvant
chemotherapy has been shown to improve survival by 10%
Men who smoke 1 to 2 packs a day have a 25-fold increased to 12% compared with operation alone. The use of adjuvant
risk for lung cancer compared with men who have never
smoked.
Passive smoking is associated with an increased risk for Table 33.4 STAGING OF LUNG CANCER
lung cancer. NONSMALL CELL TYPE
482 O N C O L O GY
100 small-dose fractions without concomitant chemotherapy. For
limited-stage small cell disease, the median duration of sur-
vival is approximately 18 months; 30% to 40% of patients sur-
80 P<.001
vive 2 years, and 10% to 20% survive 5 years.
Cumulative Proportion Surviving
60
For small cell lung cancer, treatment of limited-stage
Stage I (n=1,533) disease consists of both chemotherapy and chest radiation.
Prophylactic cranial irradiation decreases the frequency of
40 recurrence in the central nervous system.
Stage II (n=169)
Median survival is 18 months with limited-stage disease.
20 Stage IIIa (n=261)
Chemotherapy is used for extensive-stage (stage IV) small
Stage IIIb (n=543)
Stage IV (n=635) cell lung cancer. Combination chemotherapy is favored over
0
single-agent therapy. Active drugs include etoposide, cisplatin,
0 12 24 36 48 60
cyclophosphamide, doxorubicin, and vincristine. High-dose
No. of Months After Treatment
chemotherapy with or without autologous bone marrow
Figure 33.3 Survival Curves for Patients With Lung Cancer by Stage. transplant or marrow colony-stimulating factors has not yet
(From Mountain CF. A new international staging system for lung cancer. been proved superior to standard chemotherapy. The median
Chest. 1986 Apr;89[4 Suppl]:225S33S. Used with permission.) duration of survival is approximately 9 months; about 10% of
patients survive 2 years, and 1% or fewer survive 5 years.
radiation does not improve survival in resected stage II and III
For extensive-stage small cell lung cancer, treatment is
disease, but it is able to decrease the likelihood of local recur-
chemotherapy.
rence. In patients with locally advanced unresectable non
small cell lung cancer, the use of concurrent chemotherapy High-dose chemotherapy has not yet been proved superior
and radiation improves long-term survival compared with to standard chemotherapy.
radiation alone. Although patients with metastatic disease are
Median survival for patients with extensive-stage small cell
not cured, studies have shown that the use of chemotherapy
lung cancer is 9 months.
improves overall survival by several weeks and quality of life
compared with best supportive care. These studies, however,
are hampered by lack of uniform definitions of what consti- O VA R I A N C A N C E R
tutes best supportive care.
Ovarian cancer is diagnosed in 25,400 American women
Operation is the treatment of choice for stages I and II and annually. It is the leading cause of death due to gynecologic
selected IIIA nonsmall cell lung cancer. cancer, resulting in 14,300 deaths annually. There are no early
warning signs; most patients present with vague gastrointes-
There is some improvement in survival with adjuvant tinal complaints such as bloating, nausea, constipation, void-
chemotherapy. ing problems, and pain. Most patients (75%) present with
advanced disease (ie, stages III and IV, disease spread beyond
Chemotherapy is not curative for metastatic nonsmall cell
the pelvis). The term ovarian cancer refers to tumors derived
lung cancer.
from the ovarian surface epithelium, not germ cell tumors.
Chemotherapy improves overall survival by several weeks
and may improve quality of life for patients with metastatic Ovarian cancer is the leading cause of death due to
nonsmall cell lung cancer. gynecologic cancer.
There are no early warning signs.
Small Cell Lung Cancer Most patients (75%) present with advanced disease.
Treatment of limited-stage small cell lung cancer consists of
both chemotherapy and chest radiation. Surgical resection has S TAG I N G
not been shown to improve survival. For patients who have Stage I is confined to the ovary, stage II is confined to the pel-
a complete response to chemotherapy and chest radiation vis, stage III includes spread to the upper abdomen, and stage
therapy, prophylactic cranial irradiation is used to decrease IV includes spread to distant sites.
the frequency of recurrence in the central nervous system,
although there is controversy about whether this treatment
C A N C E R A N T I G E N 125
improves overall survival. Prophylactic cranial irradiation
is associated with risk for delayed leukoencephalopathy, but Cancer antigen 125 (CA 125) is expressed by approximately
this risk can be reduced by the administration of radiation in 85% of epithelial ovarian tumors and released into the
33. O N C O L O GY 483
circulation. However, it is detectable in only 50% of patients are alive at 5 years and only 5% of patients with stage IV dis-
with stage I disease. The highest serum levels of CA 125 are ease are alive.
found in patients with ovarian cancer, but the serum CA 125
level also may be increased in other malignancies and in preg-
nancy, endometriosis, and menstruation. Measurement of CA P R O S TAT E C A N C E R
125 for monitoring the course of ovarian cancer is currently
controversial. There is no clear role for CA 125 for screening
BAC KG RO U N D
purposes.
There are approximately 186,000 new cases of prostate cancer
CA 125 is expressed by about 85% of epithelial ovarian annually in the United States. It is the most common cancer in
tumors. US men and is the second leading cause of death from cancer
in US men (29,000 deaths annually). Risk factors for pros-
The CA 125 level also may be increased in other
tate cancer include older age, race (African American), fam-
malignancies and in pregnancy, endometriosis, and
ily history (first-degree relative), and possibly dietary fat. The
menstruation.
American Cancer Society recommends a digital rectal exami-
nation in men 40 years or older and determination of the
SCREENING prostate-specific antigen (PSA) value in men 50 years or older.
Use of PSA for prostate cancer screening is controversial and
Pelvic ultrasonography and serum CA 125 testing are inad-
has not been shown to reduce mortality. Screening in older
equate for screening for ovarian cancer in the general female
men should be discontinued when they have a life expectancy
population. Screening for ovarian cancer is difficult for several
of less than 10 years due to age or other comorbidities.
reasons. The incidence of the disease is low, and there are no
recognized pre-invasive lesions. Moreover, pelvic ultrasonog-
Prostate cancer is the most common cancer and the second
raphy and CA 125 testing lack sufficient sensitivity and speci-
leading cause of death from cancer in US men.
ficity. The cause of epithelial ovarian cancer is unknown. A
small subset of patients (<5%) has an inherited predisposition Risk factors for prostate cancer include older age, race
to this disease. Generally, this predisposition occurs in fami- (African American), family history, and a high-fat diet.
lies with both breast and ovarian cancer.
Screening should be stopped when advanced age or
comorbid conditions suggest a life expectancy of <10 years.
Population screening for ovarian cancer is not
recommended.
P RO S TAT E -S P EC I FI C A N T I G E N
Pelvic ultrasonography and CA 125 testing lack sufficient
sensitivity and specificity to be routinely recommended for PSA is produced by normal and neoplastic prostatic duc-
screening. tal epithelium. Its concentration is proportional to the total
prostatic mass. The inability to differentiate benign prostatic
hyperplasia from carcinoma on the basis of the PSA level ren-
T R E AT M E N T ders it inadequate as the sole screening method for prostate
The initial management of patients with epithelial ovarian cancer. PSA is useful for monitoring response to therapy in
cancer includes a thorough surgical staging and debulking cases of known prostate cancer, particularly after radical pros-
procedure. Outcome in this disease depends on the amount tatectomy, when PSA should be undetectable.
of tumor tissue remaining after initial operation. Patients with
only microscopic residual disease fare better than those with The concentration of PSA is proportional to the total
less than optimally debulked tumors. Subsequently, patients prostatic mass.
receive chemotherapy. The PSA test is inadequate as the sole screening test for
prostate cancer.
Management of ovarian cancer includes thorough surgical
staging and debulking followed by chemotherapy, both PSA is useful for monitoring response to therapy.
systemic and intraperitoneal.
Prognostic factors for prostate cancer include stage of dis-
The outcome depends on the amount of tumor tissue ease, grade of tumor, and pretreatment PSA level. Table 33.5
remaining after initial operation. simplifies the staging of prostate cancer, including the TNM
classification. The Gleason scoring system is used for patho-
logic grading of tumors. The surgical specimen is graded by
O U TC O M E
the most predominant pattern of differentiation added to the
Outcome depends on the stage of disease. At 5 years, 90% of secondary architectural pattern (eg, 3+5=8). Gleason grades 2
patients with stage I disease are alive and 80% of those with through 6 are associated with a better prognosis. Retrospective
stage II disease are alive. Unfortunately, survival with advanced results indicate that the pretreatment PSA value is a strong
disease is poor: 15% to 20% of patients with stage III disease predictor of disease outcome after operation or radiotherapy.
484 O N C O L O GY
Table 33.5 STAGING OF PROSTATE CANCER Prostatectomy is used for localized disease.
WHITMORE TNMa CRITERIA The 15-year survival rate is 85%-90% for stage A2 or B
disease.
A1 T1A Incidental focus of tumor in 5% of
resected tissue Nerve sparing operations preserve sexual function in a
A2 T1B Incidental tumor in >5% of resected tissue
majority of men.
33. O N C O L O GY 485
testosterone. They are administered as a depot injection once categories of testicular cancer are seminomas (40%) and non-
monthly. Androgen deprivation therapy, although typically seminomas. Types of nonseminomas include embryonal car-
well tolerated, is associated with considerable adverse effects, cinoma, mature and immature teratoma, choriocarcinoma,
including decreased libido, impotence, gynecomastia, osteo- yolk sac tumor, and endodermal sinus tumor. There is often
porosis, and an increased risk of myocardial infarction. an admixture of several cell types within nonseminomas. Any
nonseminomatous component plus seminoma is treated as a
Androgen deprivation is accomplished with orchiectomy nonseminoma.
or medically.
Testicular cancer is the most common carcinoma in males
Luteinizing hormone-releasing hormone agonists decrease
1535 years old.
androgen levels.
Testicular cancer is highly curable, even when metastatic.
Chemotherapy High-risk factors for testicular cancer are cryptorchid
Prostate cancer had previously been considered refractory testes and Klinefelter syndrome.
to most chemotherapy regimens. Newer combinations using The 2 broad categories of testicular cancer are seminomas
docetaxel (Taxotere) and prednisone have shown not only (40%) and nonseminomas.
considerable responses but also improved survival in men with
metastatic, hormone-refractory prostate cancer. Evaluation includes determination of -human chorionic
gonadotropin and -fetoprotein values and computed tomog-
Bisphosphonates raphy of the abdomen (retroperitoneal nodes) and chest
(mediastinal nodes or pulmonary nodules).
The use of bisphosphonates in men with prostate cancer meta-
static to bone remains controversial and does not improve
S TAG I N G
overall survival. Bisphosphonates, however, can be a useful
adjunct for treatment of painful metastases. Stage I disease is confined to the testis, stage II includes infra-
diaphragmatic nodal metastases, and stage III is spread beyond
Chemotherapy and bisphosphonates can be used for retroperitoneal nodes. About 85% of nonseminomas are asso-
palliative effects in men with prostate cancer. ciated with an increased -human chorionic gonadotropin or
-fetoprotein value. Approximately 10% of seminomas are
F O L L OW-U P R E C O M M E N DAT I O N S associated with an increased -human chorionic gonadotro-
pin level. The -fetoprotein value is never increased in pure
After curative therapy for prostate cancer (ie, prostatectomy seminoma; if it is increased, the tumor is nonseminoma and
or radiation), the PSA level can be used as a marker for recur- should be treated as such.
rence. PSA should be undetectable after successful primary
surgical therapy, but some level will persist after radiation treat- 85% of nonseminomas are associated with an increased
ment. After definitive local therapy, the median time between -human chorionic gonadotropin or -fetoprotein value.
increased PSA level (biochemical recurrence) and develop-
ment of symptoms from metastatic prostate cancer in patients 10% of seminomas are associated with an increased
receiving no ongoing therapy is 8 years, and median time to -human chorionic gonadotropin value.
death from recurrent prostate cancer is 13 years. Thus, how The -fetoprotein value is never increased in pure seminoma.
closely any individual patient is monitored depends on overall
health, comorbid conditions, and overall life expectancy.
M A NAG E M E N T
After curative treatment of prostate cancer, the median Radical inguinal orchiectomy is the definitive procedure for
time from biochemical recurrence of prostate cancer to both pathologic diagnosis and local control. Scrotal orchiec-
first symptom from metastatic disease is 8 years and the tomy or biopsy is associated with a high incidence of local
median time to death from prostate cancer is 13 years. recurrence or spread to inguinal nodes.
BAC KG RO U N D
HE AD AND NECK M ALIGNANCY
This cancer is diagnosed in 7,600 men annually. It is the most
common carcinoma in males 15 to 35 years old. It is highly
D I AG N O S I S
curable, even when metastatic. At high risk are males with
cryptorchid testes (40-fold relative risk) and Klinefelter The most common head and neck cancer is squamous cell car-
syndrome (also increased risk of breast cancer). The 2 broad cinoma. Head and neck squamous cell carcinoma can occur
486 O N C O L O GY
in the nasopharynx, oropharynx, larynx or hypopharynx, oral open biopsy is preferable to fine-needle aspiration, because a
cavity, and sinuses. Uncommon cancers of the head and neck larger specimen allows optimal histologic and immunohis-
include salivary gland cancers, esthesioneuroblastoma, mela- tochemical analysis. All patients should have a careful history
noma, lymphoma, sarcoma, and paraganglioma. Symptoms at and complete physical examination, including pelvic and rectal
presentation are related to the head and neck and can include examinations. Most patients, approximately 60%, have an ade-
throat pain, ear pain, hoarseness, trouble swallowing, and nocarcinoma. In 35% of patients, poorly differentiated carci-
enlarged lymph nodes. noma is diagnosed. Once a pathologic diagnosis is established,
additional evaluation should be tailored according to the
patients risk factors (eg, smoking, breast cancer risk), symp-
R I S K FAC TO R S
toms and signs, sites of metastasis, and the histologic diagno-
Traditional risk factors for the development of head and sis. Special consideration should be given to rule out possible
neck squamous cell carcinoma include tobacco abuse, alcohol curable malignancies such as germ cell tumors or lymphoma or
use, and chewing betel nuts. Nasopharyngeal cancer is often treatable malignancies such as breast, ovarian, or prostate can-
associated with Epstein-Barr virus. Recently, human papil- cer. Women presenting with axillary adenocarcinomas, with no
lomavirus has been implicated in oropharynx and oral cavity clear breast primary lesion, should receive treatment for breast
squamous cell carcinoma in nonsmokers. Human papilloma- cancer. Women with peritoneal carcinomatosis generally have
virusrelated tumors have a better prognosis than smoking- exploratory laparotomy with surgical cytoreduction, as for
and alcohol-related tumors. ovarian carcinoma. Men presenting with bone metastases, par-
ticularly osteoblastic metastases, should have a PSA test and
their tumor material stained for PSA expression.
SCREENING
There are no published guidelines on screening for head and
T R E AT M E N T
neck malignancy. Patients at increased risk should have a thor-
ough head and neck examination, including palpation for If a potentially treatable neoplasm is ruled out, most patients
masses in the mouth and tongue. Palpation for enlarged cervi- with metastatic cancer of an unknown primary lesion have a
cal lymph nodes should also be done. very poor prognosis, with expected survival of 4 to 6 months.
Some may benefit from palliative treatment (radiation or che-
motherapy); many are managed best with supportive care and
T R E AT M E N T A N D F O L L OW-U P
hospice care.
Treatment of head and neck cancers includes surgical resec-
tion and organ preservation with chemotherapy and radia-
tion. Recurrence can be local or distant and generally occurs PA R A N E O P L A S T I C SY N D R O M E S
within 5 years. However, follow-up by the patients oncologist
or otorhinolaryngologist should be lifelong. Patients with one
BAC KG RO U N D
head and neck cancer have a 25% chance for development of
a second head and neck cancer due to a field cancerization These conditions are the effects of a cancer occurring at a dis-
effect. Late adverse effects from treatment include skin fibro- tance from the tumor; they are called remote effects. They do
sis, decreased neck range of motion, lymphedema, xerostomia, not necessarily indicate metastatic disease. Common para-
dental problems, and swallowing difficulties. neoplastic syndromes and associated tumor types are listed in
Table 33.6.
The most common head and neck cancer is squamous cell
carcinoma.
C A RC I N O I D S Y N D RO M E
Human papillomavirus has been implicated in oropharynx
This is caused by peptide mediators secreted by carcinoid tumors
and oral cavity squamous cell carcinoma in nonsmokers.
that most frequently arise in the small intestine and that may
Recurrence can be local or distant and generally occurs have metastasized to the liver. It is less frequent with primary
within 5 years. carcinoid tumors arising from other sites such as lung, thymus,
or ovary. The most common symptoms are episodic flushing
and diarrhea; bronchospasm may occur. Flushing and diarrhea
C A R C I N O M A O F U N K N OW N P R I M A RY may occur spontaneously or be precipitated by emotional fac-
ORIGIN tors or ingestion of food or alcohol. Carcinoid heart disease
(right-sided valvular disease) is a potential late complication.
BAC KG RO U N D
L A M B E RT-E ATO N S Y N D RO M E
Patients presenting with metastatic carcinoma with an
unknown primary lesion make up 5% to 10% of general onco- This consists of muscle weakness (proximal) and gait distur-
logic practice. The first principle of management is to establish bance. Strength is increased with exercise. It is associated with
the diagnosis with a sufficient histologic specimen. In general, small cell lung cancer.
33. O N C O L O GY 487
Table 33.6 CLASSIFICATION OF PARANEOPLASTIC SYNDROMES
Endocrine
Cushing syndromea ACTH Small cell lung cancer
SIADHa ADH Lung, especially small cell
Hypercalcemiaa PTH-like peptide Lung, especially squamous; breast; myeloma
Carcinoid syndrome ? Serotonin Gut neuroendocrine tumors
? Subtance P
Hypoglycemia Insulin Gut neuroendocrine tumors; other
Insulin-like growth factors
Neuromuscular
Cerebellar degeneration Anti-Purkinje cell antibodies Lung, especially small cell; ovarian; breast
Dementia ? Lung
Peripheral neuropathya Autoantibodies Lung, gastrointestinal, breast
Lambert-Eaton Antibodies to cholinergic receptor Small cell lung cancer
Dermatomyositis ? Lung, breast
Skin
Dermatomyositis ? Lung, breast
Acanthosis nigricans ? TGF- Intra-abdominal cancer, usually gastric
Hematologic
Venous thrombosisa Activators of clotting cascade & platelets Various adenocarcinomas, especially pancreatic & gastric
Nonbacterial thrombotic endocarditis Activators of clotting cascade & platelets Various adenocarcinomas, especially pancreatic & gastric
Abbreviations: ACTH, adrenocorticotropic hormone; ADH, antidiuretic hormone; PTH, parathyroid hormone; SIADH, syndrome of inappropriate secretion of
antidiuretic hormone; TGF-, transforming growth factor-
a
Most common types.
D E R M ATO MYO S IT I S by various mediators, primarily the PTHrP. The same factors
that induce osteoclast-mediated bone resorption also stimulate
The female to male ratio is 2:1. Findings include muscle weak-
renal tubular resorption of calcium. The hypercalcemic state
ness (proximal), inflammatory myopathy, and increased cre-
interferes with renal resorption of sodium and water, leading to
atine kinase values. Skin changes are variable and include
polyuria and eventual depletion of extracellular fluid volume.
heliotrope rash, periorbital edema, and Gottron papules. An
This reduces the glomerular filtration rate, further increas-
underlying malignancy (lung, breast, gastrointestinal) is com-
ing the serum calcium level. Immobilization tips the balance
mon in patients older than 50 years.
toward bone resorption, worsening the hypercalcemia.
488 O N C O L O GY
hypercalcemia. Generally, patients with a serum calcium value Calcitonin is a relatively weak agent with a rapid,
more than 14 mg/dL, mental status changes, or an inability short-lived effect.
to maintain adequate hydration should be hospitalized for
Dialysis should be considered in hypercalcemia associated
immediate treatment. However, there is no absolute value of
with renal failure, especially if the creatinine value is more
serum calcium at which all patients become symptomatic,
than 3.0 mg/dL.
and relatively high levels may be well tolerated if the rate of
increase has been gradual. The serum calcium value should be
adjusted if the serum albumin value is abnormal. The conver- T UM O R LYS I S S Y N D RO M E
sion formula is 0.8 mg/dL of serum total calcium for every 1 g
This syndrome occurs as a result of the overwhelming release
of serum albumin more or less than 4 g/dL. If the serum albu-
of tumor cell contents into the bloodstream such that con-
min value is increased (as with dehydration), the total calcium
centrations of certain substances become life-threatening. It
value should be adjusted downward; if the serum albumin
most commonly occurs in cancers with large tumor burdens
value is reduced (as in chronic illness), the total calcium value
and high proliferation rates that are exquisitely sensitive to
should be adjusted upward.
chemotherapy. Tumor lysis syndrome can rarely occur spon-
Patients with clinically symptomatic hypercalcemia are
taneously before antitumor therapy begins. Examples include
almost always intravascularly volume-depleted. Initial ther-
high-grade lymphomas, leukemia, and, much less commonly,
apy therefore includes vigorous hydration with intravenously
solid tumors (small cell lung cancer, anaplastic thyroid cancer,
administered normal saline (up to 500 mL/h if heart function
and germ cell tumors). The syndrome is characterized by an
is normal). Loop diuretics are not used until after intravascular
increased uric acid value, which leads to renal complications;
volume expansion has been completed. Furosemide facilitates
acidosis; an increased potassium value, which can cause lethal
urinary excretion of calcium by inhibiting calcium resorption
cardiac arrhythmias; an increased phosphate value, which
in the thick ascending loop of Henle. Thiazide diuretics should
leads to acute renal failure; and a decreased calcium value,
be avoided because they can worsen hypercalcemia.
which causes muscle cramps, cardiac arrhythmias, and tetany.
Intravenous bisphosphonates (pamidronate or zoledronic
The syndrome can be prevented with adequate hydration,
acid) are helpful in the treatment of hypercalcemia of malig-
alkalinization, and administration of allopurinol before che-
nancy. Oral agents should be avoided because gastrointestinal
motherapy. Allopurinol does not lower uric acid levels that
absorption is poor. Bisphosphonates bind to hydroxyapatite
are already increased, and severe hyperuricemia can be treated
and inhibit osteoclasts. In addition to fluids, bisphosphonates
with rasburicase.
have become the mainstay of treatment for hypercalcemia.
They must be used cautiously and infused over longer periods
in the setting of renal failure. Tumor lysis syndrome is a result of the overwhelming
Calcitonin is given subcutaneously or intramuscularly; it release of tumor cell contents into the bloodstream.
is not effective at reducing calcium in its intranasal form. It It is most common in cancers with large tumor burdens
has a rapid onset of action, often lowering calcium within 12 and high proliferation rates that are exquisitely sensitive to
to 24 hours; thus, it is useful in immediate life-threatening chemotherapy.
situations. However, calcitonin is a relatively weak agent with
short-lived effect, and it should not be used as a single agent It is characterized by increased uric acid, potassium, and
due to rebound hypercalcemia. Salmon-derived calcitonin is phosphate values, acidosis, and decreased calcium value.
associated with a risk of hypersensitivity reaction, and epi-
nephrine should be given for any allergic sequelae beyond
F E B R I L E N EU T RO P E N I A
flushing. However, anaphylaxis is so rare that a test dose is no
longer recommended. This condition is defined as a temperature of 38.3C or more
Glucocorticoids are useful in hypercalcemia associated on 1 occasion or 2 episodes of 38C at least 1 hour apart and
with calcitriol production by hematologic malignancies an absolute neutrophil count of 500 109/L or less (or <1,000
and can have a direct antitumor effect on neoplastic lym- 109/L with a predicted decline to <500 within 48 hours).
phoid tissue. Calcium-free hemodialysis may be the fastest The risk of neutropenia is dependent on the type and dose of
and least hazardous method of correcting hypercalcemia in chemotherapy administered. Although a source of infection
patients with diminished kidney function. Dialysis also allows is identified in a minority of patients, at least 2 sets of periph-
calcium-lowering in the setting of congestive heart failure or eral blood samples for culture should be drawn in each patient
other conditions that prevent high-volume fluid infusion. with neutropenic fever, preferably before antibiotics are given.
In addition, at least 1 culture should be drawn through each
In patients with hypercalcemia, volume expansion must lumen of a multiple-port vascular catheter to determine
precede administration of furosemide. whether the infection is device-related.
Although management of febrile neutropenia gener-
Furosemide inhibits calcium resorption in the thick
ally involves hospitalization and institution of parenteral
ascending loop of Henle.
broad-spectrum antibiotics, recent extensive clinical experi-
Bisphosphonates bind to hydroxyapatite and inhibit ence and multiple randomized clinical trials have shown the
osteoclasts. safety and efficacy of outpatient therapy for select patients.
33. O N C O L O GY 489
Table 33.7 MEDICAL AND SOCIAL Table 33.8 REFLEXES AND THEIR CORRESPONDING
CONTRAINDICATIONS TO OUTPATIENT ROOTS AND MUSCLES
TREATMENT OF FEBRILE NEUTROPENIA
REFLEX ROOT(S) MUSCLE
S P I NA L C O R D C O M P R E S S I O N Ambulatory >80
Acute spinal cord compression is a neurologic emergency. It Paraparetic <50
results most commonly from epidural extension of vertebral
body metastases. The most common tumors include lung, Paraplegic <10
490 O N C O L O GY
or poor performance status are unlikely to be able to tolerate administration is strongly discouraged because it is pain-
an extensive operative procedure and should be treated more ful and absorption of drug is very erratic. Treatment should
conservatively. always begin with immediate-release oral or parenteral admin-
istration until the opioid requirements and effective dose for
Early diagnosis of spinal cord compression, before the individual patient are determined. Once the opioid dose
development of neurologic deficit, improves outcome. required to relieve the pain is known, then a long-acting form
should be added.
Surgical therapy is indicated for select patients with The dose of opioid used to treat acute pain is highly
neurologic deficit and spinal cord compression. dependent on whether the patient is already using opioids
because many cancer patients are opioid-tolerant. Patients
C A N C E R PA I N who are opioid-nave should be treated with 5 to 15 mg of
oral, immediate-release morphine, which is equianalgesic
More than 70% of patients with cancer have substantial pain to 2 to 5 mg given intravenously. Other opioids are equally
during the course of their disease. Multiple studies have shown effective when compared with morphine. Equianalgesic tab-
that patients with cancer-related pain are not given adequate lets are readily available and should be used to calculate an
analgesic therapy. Barriers to optimal management of cancer equivalent dose. For patients already taking opioids, the total
pain include inadequate pain assessment by health care profes- amount of opioids taken in the preceding 24 hours should be
sionals, physician reluctance and inadequate knowledge of how calculated. An immediate-release form of opioid equivalent
to prescribe opioids, and patient reluctance to take opioids. to 10% to 20% of the 24-hour total dose should be admin-
Physician reluctance to prescribe opioids stems from concern istered as initial dose to try to relieve pain. Doses will then
about addiction, lack of familiarity with the agents, problems need to be adjusted to achieve adequate analgesia. Before
with management of adverse effects of opioids, and legal or reg- adjusting the dose, one must wait until the time to peak
ulatory concerns. Psychological addiction to opioids in cancer effect has passed. For immediate-release oral agents, this is
patients is very rare, occurring in less than 1% of patients. typically 1 hour, for intravenous agents, 6 to 10 minutes, and
for subcutaneous agents, 20 to 30 minutes. Shortly after the
Evaluation time to peak effect, the patient should be reevaluated. If pain
has decreased substantially, the same dose may be repeated
Evaluation should include 1) a history regarding onset, quality, on an as-needed basis, and the duration of the effect would
severity, and location of pain; exacerbating and relieving fac- be expected to be 3 to 4 hours for most immediate-release
tors; and associated symptoms and 2) physical examination, forms. If the pain has decreased only a small amount, then
which should include a complete neurologic examination. the same dose should be repeated and the patient reassessed
Diagnostic studies are determined by the results of the history after time to peak effect. If the pain has not changed at all,
and physical examination. Administration of analgesia should the next dose should be increased by 50% to 100% and the
not be delayed while awaiting diagnostic studies or other tests. patient again reevaluated shortly after the time to peak effect
has passed. Using such an algorithm has been shown to allow
Treatment for rapid control of pain with minimal risk of adverse events
(Figures 33.4 and 33.5).
Three-Tiered Approach There is no standard opioid dosage. The dose must be
Step 1: For mild pain, administer acetaminophen or a non- increased until analgesia is achieved or adverse effects occur.
steroidal anti-inflammatory drug around the clock. Studies of Because for most patients with cancer-associated pain the
nonsteroidal anti-inflammatory drugs for cancer pain have source of the pain is unlikely to be soon eliminated, scheduled,
shown that these agents are 1.5 to 2 times more effective than around-the-clock dosing is necessary. Once the effective dose
placebo. is determined, then sustained-release or continuous-infusion
Step 2: When step 1 fails to provide adequate analgesia, or intravenous opioid should be given. When the algorithms
for moderate pain, add codeine or oxycodone. are followed, the last short-acting dose given that resulted in
Step 3: For severe pain or inadequate pain relief with steps substantial diminishment of pain should be used to calculate
1 and 2, agents include a strong opioid such as morphine, the long-acting dose. This is considered the effective 4-hour
hydromorphone, oxycodone, methadone, and fentanyl. dose because the duration of analgesia (not to be confused
with time to peak effect) would be expected to be 3 to 4 hours
General Principles for both immediate-release oral and intravenous administra-
For most cancer pain, opioids are the main treatment tion. The effective 4-hour dose should be used to calculate the
approach. Mild to moderate pain (47 on a scale of 110) 24-hour equivalent. This can then be given as either a continu-
can often be effectively treated with oral medications. Severe ous infusion intravenously or as a sustained-release oral form.
pain (>7/10) should be treated with intravenous medications An immediate-release form of an opioid should continue to be
because they allow for much more rapid titration of dose made available to the patient for unexpected exacerbations of
and more prompt pain relief. If an intravenous access is not pain. This breakthrough dose is calculated by using 10% to
available, subcutaneous administration usually works well as 20% of the total daily dose of opioid being given. Appropriate
long as the patient is reasonably well hydrated. Intramuscular equianalgesic conversions should be made when changing the
33. O N C O L O GY 491
Pain score 7-10
route or drug. Patients who require 4 or more breakthrough may be needed to determine the one best suited for any indi-
doses in a 24-hour period should have their long-acting opi- vidual patient. The fentanyl patch (a transdermal formulation)
oid dose adjusted. Each time the 24-hour dose is adjusted, the delivers drug continuously over 72 hours. It is especially useful
breakthrough dose should likewise be adjusted by using 10% for patients with poor tolerance of orally administered opioids
to 20% of the 24-hour total. or those unable to take medications orally. Because subcutane-
Adverse effects of opioids include sedation, nausea, consti- ous fat is required for absorption of the drug, this may not
pation, respiratory depression, and myoclonus. Tolerance to be a good choice in patients with severe cachexia. Likewise,
opioid-induced sedation and nausea usually develops within patients who are severely dehydrated will not have adequate
a few days. For opioid-induced constipation, docusate sodium skin perfusion to absorb the drug. Hydromorphone, fentanyl,
and senna should be used. Methylnaltrexone (Relistor) is a and methadone are the opioids preferred for use in patients
new medication for the treatment of opioid-induced consti- with renal insufficiency.
pation. It is administered as a subcutaneous injection and is
effective for producing laxation in a substantial proportion of Pain is common in patients with cancer and is often
patients, but it is not a medication used for prevention of con- undertreated.
stipation. Respiratory depression typically follows sedation;
The appropriate opioid dose for any one patient is that
if a patient is excessively somnolent and has a very low respi-
which relieves pain without excessive adverse effects.
ratory rate, doses should be held. No opioid is more or less
likely to result in a particular adverse-effect profile. However, Acute pain exacerbations should be treated with
one opioid may produce an adverse effect in a patient whereas immediate release or parenteral opioids until the effective
another will not. Thus, sequential trials of different opioids dose is determined.
Reassess in 1 h
492 O N C O L O GY
Once the effective opioid dose is known, scheduled, High-risk factors for colorectal cancer are familial
long-acting opioids should be given along with as-needed polyposis syndromes, including familial adenomatous
immediate-release opioids for breakthrough pain. polyposis and Gardner syndrome, both inherited as an
autosomal dominant trait; select familial cancer
Early referral to palliative care or hospice can improve
syndromes without polyps; and inflammatory bowel
quality of life.
disease.
For small cell lung cancer, treatment of limited-stage
OT H E R SY M P TO M S
disease consists of both chemotherapy and chest
Patients with cancer face numerous other symptoms and radiation.
challenges as they progress through the course of their ill-
CA 125 is expressed by about 85% of epithelial ovarian
ness. Dyspnea, nausea, fatigue, weight loss, depression, diffi-
tumors.
culty concentrating or thinking, and sexual dysfunction are
all common. Careful attention to symptoms and anticipation Risk factors for prostate cancer include older age,
of expected symptoms can help alleviate many of these. Early race (African American), family history, and a high-fat
referral to palliative care or hospice specialists can greatly diet.
enhance a patients quality of life. Delineation of a patients
Testicular cancer is the most common carcinoma in males
goals for care and development of advanced directives can
1535 years old.
allow the patient to remain in control and avoid unnecessary,
painful, and, at times, harmful procedures.
AC K N OW L E D G M E N T S
S U M M A RY
The authors gratefully acknowledge Charles L. Loprinzi, MD,
MRI is recommended for women at very high risk for Steven R. Alberts, MD, Roxana S. Dronca, MD, Svetomir N.
breast cancer and women with dense breast tissue on Markovic, MD, PhD, Brian A. Costello, MD, Mark Lewis,
mammography, but it is controversial in women with MD, and Heidi D. (Gunderson) Finnes, PharmD for their
newly diagnosed breast cancer. thoughtful comments and edits to the current edition.
33. O N C O L O GY 493
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PA RT V I I I
H E M ATO L O GY
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34.
BENIGN HEMATOLOGY
Alexandra P. Wolanskyj, MD
497
Table 34.1 TYPICAL FEATURES OF UNCOMPLICATED -Thalassemia
MICROCYTIC ANEMIAS (DECREASED MCV) Point mutations result in -thalassemia of varying severity.
Clinically, -thalassemia is categorized as follows:
TYPE OF ANEMIA
Abbreviations: MCV, mean corpuscular volume; RBC, red blood cell. 3. -Thalassemia major (also known as Cooley anemia)
profound anemia and lifelong transfusion dependence
The serum ferritin test is the most useful initial test for iron In -thalassemia, the hemoglobin A2 level is elevated
deficiency. (Figure 34.2). However, if the patient has iron deficiency, the
When iron deficiency anemia is discovered, identify the hemoglobin A2 level may be normal, since iron deficiency
underlying cause. decreases the hemoglobin A2 level.
-Thalassemia
Oral iron replacement therapy is the treatment of choice
Normally, a person has 4 -globin genes, but only 2 -chain
for iron deficiency. Gastric acid is required for optimal iron
loci. -Thalassemia is classifed as follows:
absorption; thus, antacids may interfere with absorption.
Reticulocytosis is seen in 4 to 7 days after initiating oral
iron replacement therapy, improvement in anemia in 3 to 1. -Thalassemia minor (-thalassemia trait)absence of
4 weeks, and correction of anemia in 6 weeksif the cause 1 or 2 of the 4 -globin genes (patients are asymptomatic,
of anemia is solely iron deficiency. Continue iron replace- usually with a low-normal MCV and normal hemoglobin)
ment therapy for another 6 months to replenish bone mar- 2. Hemoglobin H diseaseabsence of 3 -globin genes
row reserves. (patients have chronic hemolytic anemia of moderate
Indications for intravenous iron therapy include renal dial- severity, and they may benefit from splenectomy if
ysis (with recombinant erythropoietin) and inability to toler- hemolysis becomes problematic)
ate or absorb iron taken orally.
3. Absence of all 4 -globin genes is not compatible with life
Oral iron replacement therapy is the treatment of choice and results in stillbirth
for iron deficiency.
Vitamin C Deficiency
Thalassemias Patients with vitamin C deficiency (scurvy) present with micro-
cytic anemia, purpura, gingival disease, and peripheral edema.
The thalassemias are common single-gene disorders.
-Thalassemia results when -globin chains are decreased or
S I D E RO B L A S T I C A N E M I A S
absent in relation to -globin. In -thalassemia, the converse
is true: excess -globin chains precipitate as tetramers called The sideroblastic anemias are characterized by microcytic,
hemoglobin H. Genetic counseling is indicated after the diag- normocytic, or macrocytic anemia and ring sideroblasts in
nosis of - or -thalassemia has been established. the bone marrow (Figure 34.3), which are abnormal erythroid
Adapted from Savage RA. Cost-effective laboratory diagnosis of microcytic anemias of complex origin. ASCP check sample H84-10(H-153). Used with permission.
498 H E M ATO L O GY
Hypochromic microcytic anemia
Differential diagnosis:
-Thalassemia
-Thalassemia
Abnormal hemoglobin
Hemoglobin A2
Figure 34.1 Hypochromic Microcytic Anemia. The erythrocytes are 4.0% <4.0%
small with increased central pallor and assorted aberrations in size -Thalassemia
(anisocytosis) and shape (poikilocytosis). This pattern is characteristic of trait
iron deficiency rather than thalessemia; in thalassemia, red blood cells are
Hemoglobin
small but more uniform. If a mature lymphocyte is available for reference,
electrophoresis or
the diameter of a normal erythrocyte (7 m) should be similar to the
chromatography;
diameter of the nucleus of the lymphocyte (peripheral blood smear;
Wright-Giemsa). (Courtesy of Curtis A. Hanson, MD, Mayo Clinic, if normal, Southern blot
Rochester, Minnesota. Used with permission.) (-thalassemia)
3 4 . B E N I G N H E M ATO L O GY 499
MCV >100 fL
Normal reticulocyte count
No macrocytes
Oval Round
on peripheral
macrocytes macrocytes
blood smear
intrinsic factor and is absorbed in the ileum. Thus, sufficient Vitamin B12 deficiency, including pernicious anemia,
ileal mucosal surface and a normally functioning pancreas are is treated with oral or intramuscular vitamin B12. Lifelong
required for adequate absorption of vitamin B12. maintenance treatment is required. Vitamin B12 levels may
Causes of vitamin B12 deficiency include pernicious anemia be spuriously low in patients who are pregnant or using oral
(defective production of intrinsic factor, usually due to auto- contraceptives and are falsely elevated in patients who have
immune production of antiintrinsic factor or antiparietal myeloproliferative disorders, because of alterations in levels of
cell antibodies), atrophic gastritis, total or partial gastrectomy, vitamin B12-binding proteins.
ileal resection or Crohn disease involving the ileum, bacte-
rial overgrowth syndromes, infection with Diphyllobothrium Homocysteine levels are elevated in both folate deficiency
latum, and pancreatic insufficiency (most commonly from and vitamin B12 deficiency.
chronic pancreatitis or cystic fibrosis). Nitrous oxide inacti-
vates vitamin B12, and abuse of this anesthetic (eg, by dentists Methylmalonic acid levels are increased only in vitamin B12
or dental office workers) can lead to rapid development of deficiency.
severe vitamin B12 deficiency. Vitamin B12 deficiency due to
inadequate dietary intake is very rare.
The symptoms and signs of vitamin B12 deficiency include
a beefy and atrophic tongue, diarrhea, and neurologic signs
(eg, paresthesias, gait disturbance, mental status changes [B12
madness], vibratory/position sense impairment [dorsal col-
umn dropout], the absence of ankle reflexes, and extensor
plantar responses).
The MCV is increased, and hypersegmented neutrophils
are usually present (Figure 34.5). As in folate deficiency, serum
homocysteine levels are increased; however, unlike in folate
deficiency, serum and urinary levels of methylmalonic acid are
also increased. A serum vitamin B12 level less than 200 pg/mL
strongly suggests vitamin B12 deficiency. Vitamin B12 levels of
200 to 400 pg/mL (borderline or low-normal range) can also
indicate deficiency; if clinical suspicion is high, methylmalonic
acid levels can help establish the diagnosis. When present, an
abnormal intrinsic factor antibody confirms pernicious ane-
Figure 34.5 Hypersegmented Neutrophil. Polymorphonuclear leukocytes
mia as the cause of vitamin B12 deficiency. Serum gastrin levels with 5 or more nuclear lobes are characteristic of vitamin B12 or folate
are typically high. The Schilling test is frequently described in deficiency and are not typically seen in other causes of macrocytic anemia
textbooks but rarely performed in clinical practice. (peripheral blood smear; Wright-Giemsa).
500 H E M ATO L O GY
Folate Deficiency iron deficiency, total iron-binding capacity is normal or low
and ferritin is usually normal or elevated (Table 34.2).
In contrast to anemia caused by vitamin B12 deficiency, macro- In evaluating patients with suspected ACD, it is important
cytic anemia caused by folate deficiency develops quickly (ie, to exclude hemolysis and gastrointestinal tract blood loss early
within months) in patients with inadequate dietary intake of in the evaluation. No single blood test confirms ACD, but
folic acid. Folate is present in green leafy vegetables and some diagnosis is probable if 1) inflammatory markers are present; 2)
fruits. It is absorbed in the duodenum and proximal jejunum. results of iron studies are typical (ie, normal total iron-binding
Notably, folate deficiency has decreased in the United States capacity, normal or increased serum ferritin, and normal or
with folic acid fortification of grain products. Mechanisms increased transferrin saturation); 3) another cause for the nor-
of folate deficiency include increased requirements (eg, preg- mocytic anemia is not apparent; and 4) the clinical setting is
nancy, hemolytic anemia), poor folate intake (eg, alcoholics, appropriate. The sTfR concentration is normal in ACD in
persons following extremely restrictive diets), poor absorp- contrast to iron deficiency anemia, in which sTfR is usually
tion, and interference with the recycling of folate from liver elevated. Patients with ACD do not benefit from iron therapy.
stores to tissue (eg, alcohol).
Anemia due to folate deficiency is indistinguishable from
anemia due to vitamin B12 deficiency. The possibility of coex- APLASTIC ANEMIA
istent vitamin B12 or iron deficiency should be considered if Aplastic anemia is a rare disorder characterized by pancytope-
response to replacement folate therapy is not optimal. Folate nia, bone marrow hypocellularity, and absence of another
helps convert homocysteine to methionine; thus, folate defi- disorder that would explain the hypocellularity (eg, myelo-
ciency leads to an increased homocysteine level. In contrast to dysplastic syndrome, T-cell clonal disorders, or other con-
vitamin B12 deficiency, in folate deficiency the level of meth- genital bone marrow failure syndromes). Acquired aplastic
ylmalonic acid is normal. RBC folate levels are more accurate anemia is often idiopathic. Common causes include drugs
than serum folate levels in detecting true folate deficiency, (eg, chloramphenicol, sulfonamides, gold, and benzene),
since serum folate levels fluctuate quickly with dietary changes. toxins, radiation, infections (eg, hepatitis A, Epstein-Barr
A single day of healthy meals in the hospital may normalize a virus [EBV], cytomegalovirus, human immunodeficiency
patients serum folate level and lead to a false-negative result. virus [HIV], and human parvovirus B19), and autoimmune
marrow suppression. The criteria for severe aplastic anemia
If anemia due to folate deficiency does not respond include less than 25% of expected marrow cellularity and 2
optimally to folate replacement, consider coexistent of the following: 1) neutrophil count less than 0.5109/L, 2)
vitamin B12 or iron deficiency. platelet count less than 20109/L, and 3) a corrected reticu-
Unlike vitamin B12 deficiency, folate deficiency develops locyte count less than 1%.
quickly with inadequate dietary intake.
Aplastic anemia is characterized by pancytopenia,
hypocellular bone marrow, and absence of another cause of
marrow hypoplasia.
N O R MO C Y T I C A N E M I A S
Common causes of aplastic anemia include autoimmune
Normocytic anemia is defined as anemia with an MCV of 80 to marrow suppression, idiopathic causes, drug reaction,
100 fL. Diagnosing the cause of a normochromic normocytic toxins, radiation, and viral infections.
anemia can be challenging. The differential diagnosis includes
mixed nutritional deficiency (eg, concomitant folate and iron Allogeneic hematopoietic stem cell transplant is the ther-
deficiency), erythropoietic failure (aplastic anemia and RBC apy of choice for patients with an identical twin and patients
aplasia), marrow replacement (malignancy and fibrosis), kid- younger than 20 years, or high-risk patients between the ages
ney disease with lack of erythropoietin production, hemolysis, of 20 and 40 who have an HLA match. For patients older than
acute hemorrhage, some myelodysplastic syndromes, chemo- 40, the treatment of choice is antithymocyte globulin in com-
therapy, anemia of acute disease, and anemia of chronic dis- bination with corticosteroids and cyclosporine, although it is
ease (eg, infections, neoplasia, rheumatoid arthritis, and other usually not curative. Without treatment, 80% of patients who
inflammatory rheumatologic conditions). have severe aplastic anemia die within 2 years of diagnosis.
3 4 . B E N I G N H E M ATO L O GY 501
Figure 34.6 Sickle Cell Anemia. Several irreversibly sickled cells are seen. Figure 34.7 Howell-Jolly Bodies. These small, round blue inclusions are
Abundant target cells indicate hyposplenism from autoinfarction of seen with Wright-Giemsa or a comparable stain. These are characteristic
the spleen. Liver disease due to transfusional hemosiderosis was also a of hyposplenism due to splenectomy or to a functionally defective spleen.
contributing factor to these target cells (peripheral blood smear; Wright- Howell-Jolly bodies should not be confused with Heinz bodies, which
Giemsa). require a special preparation (Heinz body preparation) to observe and
are not seen on a conventional peripheral smear (peripheral blood smear;
Wright-Giemsa).
hemoglobin S), and compound states (hemoglobin S with
thalassemia or other hemoglobinopathies).
Sickle cell anemia occurs in persons of sub-Saharan Although disease manifestations do not increase during preg-
African descent and, less commonly, in persons of Middle nancy, maternal mortality is 5% to 8% and fetal mortality 20%.
Eastern or South Asian origin. Approximately 1 of every 8 Laboratory findings include severe anemia (hemoglobin,
African Americans carries 1 copy of the sickle cell gene, with 5.59.5 g/dL), sickled cells, ovalocytes, target cells, basophilic
sickle cell disease occurring in 1 of 500. Hemoglobin S sub- stippling, polychromatophilia, reticulocytosis (3%-12%), and
stitutes valine for glutamic acid at the sixth position of the hyposplenia with Howell-Jolly bodies (Figure 34.7). A per-
chain. Deoxygenated hemoglobin S distorts the cell into sistent increase in the white blood cell count to 12109/L
a sickle shape and injures the cell membrane (Figure 34.6). to 15109/L (in the absence of infection) with eosinophilia
Vasoocclusion is a function of decreased RBC deformability, is characteristic. Evidence of chronic hemolysis may be pres-
increased viscosity, and increased RBC adherence to altered ent. Liver test results are often increased. Routine diagnostic
endothelium. tests include the sickle solubility test, electrophoresis, and
Sickling is inhibited by hemoglobin F, and symptoms are chromatography.
not apparent until after 6 months of age owing to high levels
of fetal hemoglobin in early life. The first episode of vasoocclu- Acute complications of sickle cell anemia include
sive disease typically develops between the ages of 12 months vasoocclusive episodes, acute chest syndrome, dactylitis,
and 6 years and results from obstruction of the microcircula- splenic sequestration, aplastic crisis, infection, priapism,
tion by intravascular sickling. renal papillary necrosis, and cerebrovascular accidents.
Acute complications of sickle cell anemia include vasooc-
clusive episodes, acute chest syndrome, dactylitis, splenic Chronic complications include hemolytic anemia,
sequestration, stroke, aplastic crisis, infection, acute cholecys- pulmonary hypertension, folate deficiency, retinopathy,
titis, priapism, and renal papillary necrosis. Acute chest syn- chronic renal insufficiency, accelerated cardiovascular
drome, accounting for up to 25% of deaths, is the leading cause disease, transfusional hemosiderosis, nonhealing skin
of death in sickle cell anemia; clinical features include fever, ulcers, osteopenia, and growth retardation.
chest pain, tachypnea, leukocytosis, and pulmonary infil- Acute chest syndrome is the leading cause of death in sickle
trates. When infection is present, causative organisms include cell anemia.
pneumococci, Mycoplasma, Haemophilus, Salmonella, and
Escherichia coli. Aplastic crises usually follow a febrile illness Maternal and fetal mortality are increased.
and are often associated with human parvovirus B19 infec-
tion in adults. In sickle cell patients, osteomyelitis is caused by
T R E AT M E N T
Salmonella, Staphylococcus, and pneumococci.
Chronic complications include hemolytic anemia, growth Many sickle cell crises can be prevented by avoiding infection,
retardation, pulmonary hypertension, folate deficiency, retin- fever, dehydration, acidosis, hypoxemia, cold, and high alti-
opathy, chronic renal insufficiency, accelerated cardiovascu- tude. Most patients with sickle cell disease undergo autosple-
lar disease, transfusional hemochromatosis, nonhealing skin nectomy through recurrent infarction by age 5. Immunizations
ulcers, osteopenia, avascular necrosis, and growth retardation. for encapsulated organisms, penicillin prophylaxis, and folate
502 H E M ATO L O GY
supplementation are indicated. For painful crises, the corner- 1. Increased RBC destruction
stone of treatment includes gentle hydration and pain control.
a. Elevated indirect bilirubin level (>8 mg/dL suggests
Analgesics, including opioids, are essential and should not
concomitant liver disease)
be withheld because of concern about drug-seeking behav-
ior. Acetaminophen is used for fever because aspirin contrib- b. Elevated lactate dehydrogenase (LDH) level
utes to acid load. A temperature greater than 40.6C implies
infection rather than just infarction. Blood transfusion and c. Decreased haptoglobin level (haptoglobin is a
exchange transfusions are the most effective means of treat- scavenger of free hemoglobin and may be transiently
ment for severe complications. Exchange transfusion is indi- decreased after transfusion or hemodialysis)
cated for stroke, stroke prevention in patients at high risk, 2. Increased RBC production
acute chest syndrome, priapism, and progressive retinopathy.
For life-threatening complications, exchange transfusion is a. Elevated reticulocyte count
recommended with a goal for the hemoglobin S fraction of less b. Marrow erythroid hyperplasia
than 30%. Posttransfusion increases in hemoglobin to more
than 10 to 11 g/dL should be avoided except preoperatively. Peripheral smear findings such as the following can assist
Iron chelation is recommended if the transfusion requirement in making a diagnosis:
is high and the ferritin level is elevated.
Treatment with hydroxyurea decreases the frequency of 1. Spherocytes (Figure 34.8) are associated with hereditary
painful vasoocclusive crises (by about 50%), the frequency spherocytosis, alcohol, and autoimmune hemolytic
of acute chest syndrome, and the number of transfusions and anemia.
hospitalizations. It is indicated for patients who have had 2. Basophilic stippling occurs in lead poisoning,
severe complications such as acute chest syndrome and for -thalassemia, and arsenic poisoning.
patients who have frequent, painful crises.
Hematopoietic stem cell transplant with marrow or umbil- 3. Hypochromia occurs in thalassemia, sideroblastic anemia,
ical cord blood from HLA-identical siblings may be curative. and lead poisoning.
The present indications for transplant include stroke and 4. Target cells are present in thalassemia and liver disease and
recurrent acute chest syndrome. after splenectomy (Figure 34.9).
Hydroxyurea decreases the frequency of painful 5. Agglutination is present in cold agglutinin disease
vasoocclusive crises by 50% and decreases the frequency of (Figure 34.10).
acute chest syndrome. 6. Stomatocytes are associated with acute alcoholism; they
Death in sickle cell disease is associated with acute pain, also occur as an artifact.
acute chest syndrome, stroke, and infection. 7. Spur cells (acanthocytes) (Figure 34.11) are present in
Achieving a hemoglobin S level of <30% with exchange chronic severe liver disease, abetalipoproteinemia, and
transfusion is recommended for life-threatening malabsorption.
complications, including acute chest syndrome and stroke.
A posttransfusion increase in hemoglobin to >10 g/dL
should be avoided except before elective surgery.
S I C K L E C E L L T R A IT A N D C O M P O U N D S TAT E S
Sickle cell trait (heterozygous hemoglobin S) is not associ-
ated with anemia, RBC abnormalities, increased risk of infec-
tions, or increased mortality. Associations with sickle cell
trait include hematuria due to renal papillary necrosis, splenic
infarction at high altitude (>3,030 m), hyposthenuria, pyelo-
nephritis in pregnancy, and pulmonary embolism. Compound
states such as sickle cellhemoglobin C disease and hemoglo-
bin S/-thalassemia are generally milder than sickle cell dis-
ease, depending on the hemoglobin concentrations.
3 4 . B E N I G N H E M ATO L O GY 503
Figure 34.9 Target Cells. Target cells are the red blood cells with a broad Figure 34.11 Spur Cells (Acanthocytes). Note the thin, thorny, or
diameter and dark center with a pale surrounding halo. They are most finger-like projections. Spur cells are characteristic of advanced liver
commonly seen in hemoglobin C disease, thalassemia, or liver disease or disease and must be distinguished from burr cells (echinocytes) (see
after splenectomy (peripheral blood smear; Wright-Giemsa). (Courtesy Figure 34.12) (peripheral blood smear; Wright-Giemsa). (Courtesy of
of Curtis A. Hanson, MD, Mayo Clinic, Rochester, Minnesota. Used Curtis A. Hanson, MD, Mayo Clinic, Rochester, Minnesota. Used with
with permission.) permission.)
8. Burr cells (echinocytes) occur in uremia (Figure 34.12) Coombs test (also called the direct antiglobulin test [DAT])
and disappear with hemodialysis. indicates the presence of complement component C3 or IgG
(or both) on the surface of RBCs. Notably, an aplastic crisis
9. Heinz bodies are present in glucose-6-phosphate
may occur in chronic hemolytic anemia and usually results
dehydrogenase (G6PD) deficiency; they are seen with
from the development of folate deficiency or infection with
supravital stain.
parvovirus.
10. Howell-Jolly bodies indicate hyposplenism (Figure 34.7).
Hemolytic anemias may be hereditary or acquired,
11. Polychromasia indicates reticulocytosis (Figure 34.13).
from factors intrinsic or extrinsic to the RBC, and
12. Intraerythrocytic parasitic inclusions occur in malaria and Coombs-positive or Coombs-negative.
babesiosis (Figure 34.14).
Evidence of increased RBC destruction includes elevated
LDH, indirect hyperbilirubinemia, and a low haptoglobin
Hemolytic anemias may result from factors that are level.
intrinsic or extrinsic to the RBC and may be direct Coombs-
negative or Coombs-positive (Figure 34.15). A positive direct Reticulocytosis is the normal marrow response to hemolysis.
Figure 34.10 Agglutination. The random clumping of red blood cells Figure 34.12 Burr Cells (Echinocytes). Burr cell projections are much
most commonly indicates cold agglutinin disease or laboratory artifact. It smaller and more uniform in size than spur cell projections. Burr cells
is important to distinguish agglutination from rouleaux are characteristic of uremia, and the membrane abnormality is reversible
(see Figure 34.16) (peripheral blood smear; Wright-Giemsa). with hemodialysis (peripheral blood smear; Wright-Giemsa).
504 H E M ATO L O GY
which the RBCs are lysed in the macrophages of the spleen
and liver.
AU TO I M MU N E H E MO LY T I C A N E M I A
Mechanisms of Drug-Induced Hemolytic Anemia
There are 3 distinct mechanisms of drug-induced hemolytic
anemia:
3 4 . B E N I G N H E M ATO L O GY 505
Hemolytic anemia
Acquired Acquired
Congenital Acquired
Coombs-positive Coombs-negative
Autoimmune Microangiopathy
Membrane defects Paroxysmal nocturnal
Transfusion reactions (HUS/TTP)
Enzymopathies hemoglobinuria
Drugs Figure 34.15 Differential Diagnosis of
Lead poisoning
Chemical, physical Hemolytic Anemia. HUS indicates
agents hemolytic uremic syndrome; RBC,
Hypersplenism red blood cell; TTP, thrombotic
Infection
thrombocytopenic purpura.
Raynaud phenomenon, in which 1 or 2 fingers turn from fingers. The diagnosis of cold agglutinin syndrome is made
white to blue to red. by finding RBC agglutination on a peripheral blood smear
The peripheral blood smear shows RBC agglutination that only if prepared at temperatures 37C.
disappears if prepared at 37C (Figure 34.10). Agglutinated
RBCs clump together, spuriously elevating the MCV. Therapy
Autoimmune Hemolytic Anemia: Warm Agglutinins
includes avoidance of the cold. In severe cases rituximab and
cytotoxic agents are used. Agglutination should not be con- Warm agglutinins are IgG antibodies that bind to RBCs at
fused with rouleaux, in which RBCs stack in a linear pattern physiologic temperatures rather than primarily in the cold.
(Figure 34.16). The direct Coombs test is positive for both IgG and comple-
ment component C3. Associated causes include autoimmune
Cold agglutinins are often associated with Mycoplasma disorders (systemic lupus erythematosus), lymphoproliferative
pneumoniae, EBV (infectious mononucleosis), and disorders (chronic lymphocytic leukemia), drugs, and transfu-
malignancy. sion. The first general principle in the treatment of warm agglu-
tinin autoimmune hemolytic anemia is to treat the underlying
Differentiate from Raynaud phenomenon with
disease (if one can be identified) and to discontinue the use of
Coombs-positive hemolytic anemia.
drugs that have been implicated in hemolysis.
Typical clinical scenario: The patient has hemolytic anemia
and acrocyanosis of the ears, tip of the nose, toes, and Paroxysmal Cold Hemoglobinuria
(Complement-Mediated Lysis)
Paroxysmal cold hemoglobinuria is the least common cause of
autoimmune hemolytic anemia. A positive Donath-Landsteiner
test is diagnostic; it detects an IgG antibody that binds to
RBCs at low temperatures, causing hemolysis. Paroxysmal cold
hemoglobinuria is often idiopathic and can be associated with
syphilis (congenital and late), mononucleosis, mycoplasma,
and childhood exanthems. The overall prognosis is good, and
the condition usually resolves after the infection clears.
C O O M B S -N EG AT I VE H E MO LY T I C A N E M I A
The differential diagnosis of Coombs-negative hemolytic
anemia is broad and includes hereditary RBC disorders such
as enzymopathies (eg, G6PD deficiency and pyruvate kinase
deficiency), hemoglobinopathies, and membrane disorders;
Figure 34.16 Rouleaux. Stacking of red blood cells in a linear pattern paroxysmal nocturnal hemoglobinuria; Wilson disease; and
distinguishes rouleaux from agglutination (see Figure 34.10). Rouleaux microangiopathic conditions, including thrombotic throm-
are most commonly associated with hypergammaglobulinemia, especially
in human immunodeficiency virus infection or monoclonal plasma cell bocytopenic purpura (TTP). Rarely, warm autoimmune
disorders (peripheral blood smear; Wright-Giemsa). (Courtesy of Curtis A. hemolytic anemia is Coombs-negative owing to low anti-
Hanson, MD, Mayo Clinic, Rochester, Minnesota. Used with permission.) body titers.
506 H E M ATO L O GY
G6P D D E FI C I E N C Y most patients by age 50. Treatment is splenectomy after the
first decade of life for moderate or severe hemolysis, which
G6PD deficiency is the most common RBC enzyme defi-
invariably reduces hemolysis. Asymptomatic adults may be
ciency. It causes decreased levels of glutathione (an antioxi-
observed if the hemoglobin concentration is greater than 11
dant), making RBCs more sensitive to oxidative damage by
g/dL and the reticulocyte count is less than 6%.
infections, toxins (eg, naphthalene in mothballs), or drugs.
Except for G6PD and phosphoglycerate kinase deficiences,
which are sex-linked, all other RBC enzymopathies are auto- Hereditary spherocytosis: mostly autosomal dominant but
somal recessive. Rarely, a female who is heterozygous for may be autosomal recessive or sporadic.
abnormal G6PD may be clinically affected because of unfa- Splenomegaly is invariably present; pigment gallstones are
vorable lyonization. G6PD deficiency confers some protec- common.
tion against falciparum malaria and extends to both males
and heterozygous females. Features include negative direct Coombs test and increased
Anemia or RBC defects do not occur in the steady state osmotic fragility.
with the most common G6PD variants. Risk of hemolysis Treatment: splenectomy after the first decade of life for
increases with concurrent kidney or liver disease, viral or bac- patients with moderate or severe hemolysis.
terial infection, diabetic ketoacidosis, ingestion of fava beans
(seen only in G6PD Mediterranean), and drugs. Even mild Asymptomatic adults with hemoglobin >11 g/dL and a
infections can cause hemolytic anemia; this occurs more often reticulocyte count <6% may be observed.
than drug-induced hemolysis. Drugs that commonly cause
hemolytic anemia in G6PD deficiency include antimalarial PA ROX YS M A L N O C T U R NA L H E M O G L O B I N U R I A
agents (eg, primaquine and chloroquine), dapsone, sulfon-
amides, nitrofurantoin, high-dose aspirin, probenecid, and Paroxysmal nocturnal hemoglobinuria (PNH) is an acquired,
nitrites. chronic, clonal, hematologic stem cell disorder. Blood cells
Abnormal laboratory findings include intravascular hemoly- are unusually sensitive to activated complement and are
sis, methemoglobinemia, and methemalbuminemia (specific for lysed, primarily at night when plasma is more acidotic from
intravascular hemolysis due to enzymopathy). Supravital stain- sleep-related physiology (eg, relative hypoxia). The disorder is
ing for Heinz bodies is a good screening test, but their absence characterized by abnormal hematopoietic stem cells, reticulo-
does not rule out the diagnosis. The G6PD assay is the definitive cytopenia, leukopenia, or thrombocytopenia due to lysis by
test but should not be done during acute hemolysis in patients complement-mediated mechanisms.
of African ancestry. Therapy includes treating the underlying A mutation in the PIGA gene causes cells in PNH to
infection and withdrawing use of the offending drug. have a decrease or absence of glycosylphosphatidylinositol
(GPI)-linked proteins, including CD14, CD55, and CD59.
Clinically, PNH is characterized by chronic intravascular hemo-
G6PD deficiency is the most common RBC enzyme
lytic anemia, episodic abdominal pain, and venous thrombosis
deficiency and is inherited on the X chromosome.
of the portal system, brain, and extremities. Budd-Chiari syn-
G6PD deficiency provides some protection against drome (hepatic vein thrombosis) is the main cause of death. In
falciparum malaria. up to 10% of patients, myelodysplasia or acute myeloid leuke-
mia develops. PNH and aplastic anemia can coexist.
Anemia or RBC defects do not occur in the steady state
The most useful assay for diagnosis of PNH is flow cytom-
with the most common G6PD variants.
etry to establish the absence of the GPI-linked antigens. Up
Hemolysis is induced by infection more commonly than by to 60% of patients respond to prednisone; eculizumab is a
drugs. monoclonal antibody that can be used for long-term therapy
for hemolysis in PNH.
A good screening test: Heinz bodies seen on supravital
staining of peripheral blood.
PNH is associated with venous thrombosis,
Treat underlying infections and withdraw the use of especially Budd-Chiari syndrome, and is the main cause of
offending drugs. death.
Acute myelogenous leukemia or myelodysplasia occurs in
H E R E D I TA RY S P H E RO C Y TO S I S 5%-10% of patients.
Hereditary spherocytosis is typically an autosomal domi- Diagnosis: flow cytometry studies for GPI-linked
nant disorder, but it can be autosomal recessive or sporadic. proteins.
It is caused by an underlying defect in the RBC cytoskeleton
because of a partial gene deficiency (eg, in ankyrin or spec-
T H RO M B OT I C M I C ROA N G I O PAT H I E S :
trin). The osmotic fragility test is almost always abnormal and
D I FFE R E N T I A L D I AG N O S I S
is the most reliable diagnostic test. Features include jaundice,
splenomegaly, negative direct Coombs test, spherocytes, and In microangiopathic hemolytic anemia, RBCs are frag-
increased osmotic fragility. Pigment gallstones are present in mented and deformed by fibrin deposits in the peripheral
3 4 . B E N I G N H E M ATO L O GY 507
A are thrombocytopenia and microangiopathy, and these are
sufficient to establish the diagnosis. The anemia is normo-
chromic normocytic, with microangiopathic hemolytic
features (Figure 34.17). Direct Coombs test results are nega-
tive. Results of coagulation studies are normal or only mildly
abnormal, in contrast to results in disseminated intravascular
coagulopathy. The cause of TTP is unknown in more than
90% of the patients. TTP is associated with pregnancy and the
use of oral contraceptives, HIV infection, cancer, bone mar-
row transplant, certain chemotherapy drugs (especially mito-
mycin C and bleomycin), and other drugs (eg, crack cocaine,
ticlopidine, and cyclosporine).
Clinically, thrombocytopenia is associated with bleed-
ing in 96% of patients. Neurologic signs often wax and wane
and include headache, coma, mental changes, paresis, seizure
B and coma, aphasia, syncope, visual symptoms, dysarthria,
vertigo, agitation, confusion, and delirium. Kidney abnor-
malities include abnormal urinary sediment and elevated
creatinine level. Patients with TTP are deficient in the von
Willebrand factorcleaving protease ADAMTS13. Even
when ADAMTS13 assays are available, results can take days
to return; thus, the assay is not useful for initial treatment
decisions.
Without treatment, more than 90% of patients die of mul-
tiorgan failure, but with treatment, 70% to 80% survive the
disease and have few or no sequelae. The treatment of choice
is plasma exchange. Relapses are also managed with plasma
exchange. The management of refractory TTP includes intra-
venous vincristine, rituximab, splenectomy, or intravenous
high-dose -globulin. Platelet transfusion should be used only
Figure 34.17 Schistocytes. A and B, Fragmented red blood cells are when required for an invasive procedure since it can exacer-
shaped like helmets, triangles, or kites. These are characteristic of any bate the disease.
microangiopathic hemolytic process (peripheral blood smear; Wright-
Giemsa). (Courtesy of Curtis A. Hanson, MD, Mayo Clinic, Rochester, TTP: the pentad of microangiopathic hemolytic anemia,
Minnesota. Used with permission.)
fever, thrombocytopenia, neurologic signs, and renal
abnormalities.
blood (Figure 34.17). Direct Coombs testing is negative. The
associated disorders, characterized by widespread microvas- The treatment of choice is plasma exchange.
cular thrombosis leading to end-organ injury, include TTP,
hemolytic uremic syndrome (HUS), malignant hyperten- Hemolytic Uremic Syndrome
sion, pulmonary hypertension, acute glomerulonephritis,
HUS is characterized by microangiopathic hemolytic anemia,
renal allograft rejection, obstetric catastrophes, HELLP
thrombocytopenia, and acute kidney injury. Fever and neuro-
syndrome (hemolysis, elevated liver function tests, and low
logic signs are usually not present. It is associated with infec-
platelet count), disseminated intravascular coagulopathy,
tions (E coli O157:H7, Shigella dysenteriae), pregnancy, bone
collagen vascular diseases, vascular malformations including
marrow transplant, chemotherapy, and immunosuppressive
Kasabach-Merritt syndrome (giant hemangiomas that trap
medications such as cyclosporine. HUS is usually not associ-
platelets), viral infections (HIV), bacterial infections (E coli
ated with a decrease in ADAMTS13 activity. Management of
O157:H7), drug-induced disorders (eg, mitomycin C, qui-
HUS is supportive. In adults, treatment with plasma exchange
nine, ticlopidine, tacrolimus, cisplatin, and cyclosporine),
is indicated, but response is variable.
acute radiation nephropathy, bone marrow transplant, and
solid organ transplant.
HUS: hemolytic anemia, thrombocytopenia, and acute
kidney injury.
Thrombotic Thrombocytopenic Purpura
The features of TTP include the pentad of microangiopathic T R A N S F U S I O N R E AC T I O N S
hemolytic anemia, thrombocytopenia, neurologic signs, fever,
and kidney abnormalities. Most patients do not manifest all The primary cause of major transfusion reactions and
5 features before the diagnosis is made. The primary criteria transfusion-related deaths is medical error, which includes
508 H E M ATO L O GY
Table 34.3 RISKS OF COMPLICATIONS FROM ACU T E H E MO LY T I C T R A NS F US I O N
TRANSFUSIONS IN THE UNITED STATES R E AC T I O N S
COMPLICATION RISK PER UNIT Acute hemolytic transfusion reactions are the most
life-threatening tranfusion reactions and occur within minutes
Minor allergic reaction 3/100 to hours. The recipients RBC antibodies (usually IgM) react
Circulatory overload Variable against the donors RBCs and cause complement-mediated
hemolysis. The most common cause is human error, especially
Febrile, nonhemolytic 3/100 when blood is released emergently. Mortality rate is about 20%;
Delayed hemolytic transfusion reaction 1/4,000 of the fatal transfusion reactions, 85% involve ABO incom-
patibility. ABO compatibility is illustrated in Table 34.4.
TRALI 1/10,000 Other, nonclerical causes include antibodies not detected
Acute hemolytic transfusion reaction 1/2.5104 to 1/1.010 6 before transfusion, such as Kell, Duff y (Fya), and Kidd ( Jka).
Clinically, patients experience pain at the intravenous site, a
HIV infection 1/2.110 6 sense of impending doom, back pain, abdominal pain, fever,
Hepatitis B virus infection 1/2.0105 chills, chest pain, hypotension, nausea, flushing, and dyspnea.
Direct Coombs testing is positive in most cases.
Hepatitis C virus infection 1/1.9105 Complications include oliguria, acute kidney injury, and
HTLV type I or II infection 1/2.0105 disseminated intravascular coagulation. Treatment includes
immediate termination of the transfusion, vigorous admin-
West Nile virus infection Unknown istration of fluids, and furosemide to increase renal cortical
Bacterial infections 1/2,000 to 1/5.0105 blood flow.
IgA-related anaphylaxis 1/1.0105 The most common cause of acute hemolytic transfusion
Graft-vs-host disease Rare reaction is human error.
Immunosuppression Unknown Most mortality is related to ABO incompatibility.
Posttransfusion purpura Rare
Prion infection Unknown A L L E RG I C T R A N S F US I O N R E AC T I O N S
Allergic transfusion reactions are a complication in 3% of
Abbreviations: HIV, human immunodeficiency virus; HTLV, human T-cell leuke- transfusions and are caused by a recipients antibody against
mia virus; TRALI, transfusion-related acute lung injury.
foreign-donor serum proteins. Transfusion reactions can also
be associated with anti-IgA antibodies. These include anaphy-
bypassed safeguards, similar patient names, and verbal or faxed lactic reactions, which occur most commonly in patients with
communications. The major transfusion reactions include IgA deficiency who may have circulating complement-binding
acute hemolytic transfusion reactions, transfusions associated anti-IgA antibodies that react with donor IgA. Clinical fea-
with anti-IgA antibodies, transfusion-related acute lung injury tures are similar to those of an acute hemolytic transfusion
(TRALI), adult respiratory distress syndrome, delayed hemo- reaction. Treatment includes stopping the transfusion and giv-
lytic transfusion reactions, febrile transfusion reactions, urti- ing antihistamines and conventional antianaphylactic drugs.
carial (allergic) transfusion reactions, and circulatory overload Transfusion protocols for patients include use of washed
(Table 34.3). RBCs and IgA-deficient plasma.
O O AB, A, B, or O O
A A or O A or AB A
B B or O B or AB B
AB AB, A, B, or O AB AB
a
Natural alloimmunization against A and B antigens occurs in people lacking these antigens. Upon transfusion of ABO-incompatible blood, pre-
formed antibodies serve as hemagglutinins, resulting in life-threatening acute hemolysis and complement activation. Hemagglutinins are found
primarily in plasma; platelets are considered similar to plasma products with respect to ABO compatibility.
3 4 . B E N I G N H E M ATO L O GY 509
Allergic transfusion reactions are often associated with C I RCU L ATO RY OVE R L OA D
anti-IgA antibodies.
Circulatory overload may cause tightness in the chest, dry
cough, and acute edema. It occurs in patients who already have
T R A NS F US I O N-R E L AT E D AC U T E LU N G I N JU RY an increased intravascular volume or decreased cardiac reserve,
Transfusion-associated acute respiratory distress syndrome with symptoms generally developing within several hours after
or TRALI results from an interaction between the recipi- transfusion. Management includes slowing the transfusion to
ents leukocytes and donor antileukocyte antibodies. TRALI 100 mL per hour, placing the patient in the sitting position,
often is unrecognized and ranks third among causes of and giving diuretics.
transfusion-related deaths. It is characterized by acute respi-
ratory distress during transfusion or within 6 hours after Symptoms of circulatory overload develop within hours of
completion of transfusion, hypotension, bilateral pulmonary transfusion and affect patients with increased intravascular
infiltrates, normal or low pulmonary capillary wedge pressure, volume or decreased cardiac reserve.
no evidence of circulatory overload, and fever. With appro-
priate supportive care, recovery is rapid, occurring in 24 to P O S T T R A NS F US I O N P U R P U R A
48 hours.
Posttransfusion purpura is a rare syndrome in which the recipi-
ent makes antiplatelet antibodies, which cause an abrupt onset
Treatment of TRALI is primarily supportive care.
of severe thrombocytopenia 5 to 10 days after blood transfu-
sion. Most cases involve patients who lack human platelet anti-
D E L AY E D H E MO LY T I C T R A NS F US I O N gen 1a and who have an antibody from a previous pregnancy
R E AC T I O NS or transfusion.
Delayed hemolytic transfusion reactions (occurring in 1 in
Posttransfusion purpura usually occurs in patients who
4,000 transfusions) occur because of the inability to detect
have an antibody from a previous pregnancy or transfusion.
clinically significant recipient antibodies before transfusion.
They usually occur 5 to 10 days after transfusion and are less
dangerous than an acute hemolytic reaction. The recipients INFECTION
plasma contains antibody before transfusion because of a pre-
Pathogen transmission may occur with transfusions. These
vious transfusion or previous pregnancy. There is evidence of
risks and other risks of transfusion are summarized in
hemolysis and direct Coombs testing is positive. One-third
Table 34.3.
of the patients are asymptomatic, and the reactions are
detected by the recurrence of laboratory-detected anemia
without clear cause; other patients present with symptoms PORPHYRIA
of anemia, chills, jaundice, and fever. Management consists
of monitoring hemoglobin concentration and renal output The porphyrias are enzyme disorders that are autosomal
and avoiding the use of units with the offending antigen in dominant with low disease penetrance, except for congenital
the future. erythropoietic porphyria (which is autosomal recessive) and
porphyria cutanea tarda (which may be acquired and is asso-
Delayed hemolytic transfusion reactions usually occur ciated with hepatitis C and hemochromatosis). Most persons
510 days after transfusion and are less dangerous than remain biochemically and clinically normal throughout most
acute hemolytic reactions. of their lives. Clinical expression is linked to environmental
and acquired factors.
Disease manifestations depend on the type of excess por-
F E B R I L E T R A NS F US I O N R E AC T I O NS
phyrin intermediate. When there is an excess of the earlier
precursor molecules (-aminolevulinic acid and porpho-
Febrile transfusion reactions are characterized by chills, fever, bilinogen), the clinical manifestations are neuropsychiatric,
flushing, headache, tachycardia, myalgias, and arthralgias. including autonomic dysfunction (abdominal pain, vomit-
They usually begin about 1 hour after the transfusion starts ing, constipation, tachycardia, and hypertension), psychiatric
and last for 8 to 10 hours. They occur in 1% of all transfu- symptoms, fever, leukocytosis, and paresthesias. If the excess
sions. Causes include cytokines from leukocytes and platelets is in the distal intermediates (uroporphyrins, coproporphy-
against donor antigens and antiserum protein antibodies. rins, and protoporphyrins), the manifestations are cutaneous
Treatment consists of stopping the transfusion to evaluate the (photosensitivity, blister formation, facial hypertrichosis, and
patient; initially, a febrile reaction cannot be distinguished hyperpigmentation). If there is excess of both early and late
from a hemolytic transfusion reaction. Preventive methods porphyrins, there are both neuropsychiatric and cutaneous
include leukoreduction. manifestations.
Porphobilinogen production and excretion are increased
Febrile transfusion reactions usually begin about 1 hour during marked symptoms caused by the 3 neuropathic porphy-
after the start of a transfusion. rias, which include acute intermittent porphyria, hereditary
510 H E M ATO L O GY
Table 34.5 COMPARISON OF PORPHYRIAS
Features
Most common type of porphyria Increased urinary -aminolevulinic acid & porpho- Clinically: photosensitivity, abdom-
Iron overload bilinogen during acute symptomatic episodes; inal pain, neurologic problems
Skin lesions on light-exposed areas often normal levels between episodes (similar to acute intermittent
Hypertrichosis (usually mild) Neurologic symptoms: abdominal pain of 35 days porphyria)
Increased uroporphyrins in urine duration without anatomical cause, focal neuro- Increased protoporphyrin &
No neuropathic features logic problems such as polyneuropathy & motor coproporphyrin in stool
paresis, psychiatric problems with hallucinations,
confusion, psychosis, seizures
Decreased porphobilinogen deaminase activity
Normal protoporphyrin & coproporphyrin in stool
Associations
Alcoholic liver disease, chronic hepatitis C, Drugs can precipitate crises (eg, sulfonamides, barbi- Common in South Africa (due to
hemochromatosis turates, alcohol) founder effect), Holland
Estrogens: females, males treated for prostatic Menstrual cycle can exacerbate symptoms
carcinoma Infection or surgery can precipitate crisis
Hexachlorobenzene Inadequate nutrition can precipitate crisis
Treatment
Phlebotomy to remove iron Avoid prolonged fasting & crash diets Same as for acute intermittent
Chloroquine Large amounts of carbohydrate (400 g daily) porphyria
Low-dose antimalarials Intravenous hematin
Luteinizing hormonereleasing hormone agonists for
suppression of hormonal fluctuation
coproporphyria, and porphyria variegata. In hereditary Mild coproporphyrin elevation is nonspecific and not
coproporphyria and porphyria variegata, there is an accumu- diagnostic of porphyria.
lation of coproporphyrinogen/coproporphyrin or protopor-
Porphyria cutanea tarda is associated with chronic hepatitis
phyrinogen/protoporphyrin and a concomitant increase in
C and with hemochromatosis.
-aminolevulinic acid and porphobilinogen. In the acute por-
phyrias, determine the 24-hour urinary porphobilinogen level
during an attack. Patients with acute intermittent porphyria S U M M A RY
lack skin lesions. It is important to check fecal porphyrins in
protoporphyria, porphyria variegata, and coproporphyria. An Iron deficiency anemia should prompt a search for the
elevated coproporphyrin level alone, therefore, does not sup- underlying cause.
port a diagnosis of porphyria. The porphyrias are compared in
Table 34.5. Hemolytic anemias may be hereditary or acquired,
from factors intrinsic or extrinsic to the RBC, and
In suspected acute porphyria, determine the Coombs-positive or Coombs-negative.
24-hour urinary porphobilinogen level during the acute The most common cause of acute hemolytic transfusion
episode. reaction is human error.
3 4 . B E N I G N H E M ATO L O GY 511
35.
HEMATOLOGY: HEMOSTASIS a
Rajiv K. Pruthi, MBBS
512
Intrinsic Extrinsic 2. Specific factor inhibitors (eg, factor VIII [FVIII] or factor
V inhibitors)
XII
XI VII 3. Nonspecific inhibitors (eg, lupus anticoagulants)
IX
VIII
aPTT PT
Appropriate follow-up testing typically leads to the diag-
V nosis of the underlying cause of the prolongation of the PT
and aPTT.
X
II
Bleeding Disorders Not Detected With PT
Fibrinogen and aPTT
TT, RT Disorders that are not detected with the PT and aPTT include
Fibrin clot the following:
Figure 35.1 Coagulation Cascade. aPTT indicates activated partial 1. Qualitative platelet defects (requires specialized platelet
thromboplastin time; PT, prothrombin time; RT, reptilase time; TT, function testing)
thrombin time.
2. vWD (requires assays for von Willebrand factor
[vWF])
an initial screening test for the presence of lupus anticoagulant 3. FXIII deficiency (requires specialized FXIII screening or
or for patients who have bleeding symptoms. functional assays)
The aPTT assesses the intrinsic pathway. 4. Deficiency of antiplasmin and plasminogen activator
inhibitor 1 (requires specific assays)
The aPTT is commonly used to monitor UFH and DTI
therapy.
O VE RVI EW O F B L E E D I N G D I S O R D E R S
Bleeding Time Bleeding disorders consist of the following:
Use of the bleeding time (BT) test has been discontinued in
many hospitals. A review of multiple studies led to the follow- 1. Clotting factor deficiencies or inhibitors
ing conclusions: 2. Vascular bleeding disorders
1. In the absence of the clinical history of a bleeding 3. Platelet disorders (quantitative and qualitative)
disorder, BT is not a useful predictor of risk of
hemorrhage with surgical procedures. Each of these is broadly classified into congenital disorders
and acquired disorders.
2. Normal BT does not exclude the possibility of excessive
hemorrhage with invasive procedures.
C O N G E N I TA L P L A S M AT I C B L E E D I N G
3. BT cannot reliably identify patients exposed to aspirin or
D I S O R D E R S ( FAC TO R D E F I C I E N C I E S )
nonsteroidal anti-inflammatory drugs.
Of the congenital plasmatic bleeding disorders, vWD is the
most common. Others include hemophilia A, hemophilia
Approach to a Prolonged PT or aPTT B, and hemophilia C. Other factor deficiency states are rare
Step 1: Exclude artifactual causes (elevated hematocrit; (Table 35.1). All clotting factors are produced by the liver
nonfasting, lipemic sample; or heparin contamination of the except vWF, which is produced by vascular endothelial cells
specimen). and megakaryocytes.
Step 2: Perform a mixing study in a 1:1 ratio with normal
pooled plasma. von Willebrand Disease
Step 3a: Correction of the clotting time (ie, the aPTT
normalizes) implies a coagulation factor deficiency; follow-up Definition
factor assays are then performed. vWD refers to a deficiency or dysfunction of vWF.
Step 3b: Inhibition of the aPTT (ie, aPTT may shorten
but does not normalize) implies the presence of an inhibitor, Classification
including the following: vWD is classified according to whether the defect is quan-
titative (types I and III) or qualitative (types IIA, IIB, IIM,
1. Medications (eg, heparins and DTIs) and IIN).
von Willebrand disease von Willebrand factor NL NL or Prol Up to 1% Autosomal dominant or recessive
Abbreviations: aPTT, activated partial thromboplastin time; NL, normal; Prol, prolonged; PT, prothrombin time.
a
Live male births.
b
Among Ashkenazi Jews.
Biochemistry
Endothelial cells and platelets store vWF. After secretion, Variables Affecting vWF Levels
the ultra-large-molecular-weight multimers of vWF, the most Healthy people with blood group O have vWF lev-
hemostatically active, are cleaved into multimers of smaller size els that are 25% to 30% lower than in people with blood
by a protease, ADAMTS13 (ADAM metallopeptidase with groups A, B, or AB and thus may receive a misdiagnosis of
thrombospondin type 1 motif, 13). vWD. Therefore, ABO typing should be part of the initial
testing.
Acquired defects of vWF (ie, acquired von Willebrand
Function of vWF syndrome) may be seen in patients with aortic stenosis, myelo-
vWF mediates platelet adhesion and aggregation. It acts proliferative disorders, and monoclonal protein disorders. The
as a carrier protein for FVIII, protecting it from proteolytic syndrome mimics congenital type II vWD.
inactivation.
Clinical Features
Patients who have mild vWD may be asymptomatic and
bleed only when challenged with trauma or minor surgery (eg, Table 35.2 STEPWISE APPROACH TO ASSESSMENT FOR
dental extraction) or major surgery. VON WILLEBRAND DISEASE
Patients who have severe vWD may have spontaneous
bleeding. Spontaneous bleeding is typically mucocutaneous 1. Bleeding history
(bruising, epistaxis, hematuria, gastrointestinal tract hemor-
rhage); in type III vWD, bleeding occurs in joints and soft 2. Complete blood cell count
tissue. Bleeding may be exacerbated by the use of aspirin or 3. vWD profile testing
nonsteroidal analgesics. vWF:Ag
RCoF
VIII:c
Laboratory Testing
Laboratory testing (Table 35.2) includes testing for vWF 4. ABO blood group
antigen (vWF:Ag), vWF activity, and FVIII activity. If initial
5. Optional tests if initial data suggest vWD
results are abnormal, vWF multimer analyses are performed to vWF multimers
subtype vWD: vWF:CBA
vWF:VIIIB
1. Type I vWDmild to moderate reduction in vWF:Ag RIPA
level and activity
6. Genetic tests if indicated
2. Type II vWDdisproportionate reduction in activity of
the vWF called the ristocetin cofactor (RCoF) compared Abbreviations: Ag, antigen; CBA, collagen-binding assay; VIIIB, factor VIII
with vWF:Ag binding assay; VIII:c, factor VIII coagulant activity; RCoF, ristocetin cofactor;
RIPA, ristocetin-induced platelet aggregation: vWD, von Willebrand disease;
3. Type III vWDabsent vWF vWF, von Willebrand factor.
514 H E M ATO L O GY
Short-term physical exertion, inflammation, malignancy, 3. Generate treatment guidelines for managing
hyperthyroidism, estrogens, and pregnancy increase vWF levels bleeding
to normal and may mask a diagnosis of vWD. Hypothyroidism
4. Refer to a comprehensive hemophilia treatment center for
is associated with reduced vWF levels.
periodic follow-up
Type IIB vWD is associated with thrombocytopenia.
Type IIN vWD results from mutations in the FVIII binding
domain of vWF. This subtype may be mistaken for mild hemo- Specific measures include the following:
philia A.
1. Administer desmopressin
Type I vWD: mild to moderate reduction in vWF:Ag level 2. Administer adjunctive -aminocaproic acid or vWF
and activity. concentrates preoperatively to prevent bleeding or to
Type II vWD: disproportionate reduction in activity of manage bleeding
RCoF compared with vWF:Ag. 3. Administer vWF concentrates
Type III vWD: vWF is absent.
A desmopressin treatment trial should be performed for
ABO typing should be part of the initial testing. patients with types I, IIA, or IIM vWD.
Desmopressin is generally not helpful for patients with
Inheritance of vWD type IIB vWD and should not be used in patients with
Type I vWD is inherited as an autosomal dominant trait type III vWD.
with variable penetrance. Types IIA, IIB, and IIM vWD are
For patients who do not respond to desmopressin and for
inherited as autosomal dominant traits. Type III vWD and
those in whom it is contraindicated, administration of
type IIN (Normandy) vWD are inherited as autosomal reces-
purified plasma-derived vWF concentrates is the therapy of
sive traits.
choice.
Management
Upon establishment of a diagnosis of vWD, a desmopres-
sin acetate (DDAVP) treatment trial should be performed for Hemophilia A and Hemophilia B
patients with types I, IIA, or IIM vWD. Intravenous (IV) infu- Hemophilia A and hemophilia B are clinically indistinguish-
sion of 0.3 mcg/kg body weight releases vWF from its storage able X-linked recessive bleeding disorders. Hemophilia A is
sites; measure levels 60 minutes after infusion. due to a deficiency in blood coagulation FVIII, and hemo-
philia B is due to a deficiency in factor IX (FIX).
Side effects include facial flushing, headache, mild decrease
in blood pressure, mild tachycardia, and hyponatremia.
Doses repeated at intervals shorter than 24 hours may Classification
result in a decrease or loss of response (tachyphylaxis) and Hemophilia is classified according to levels of FVIII and FIX:
syndrome of inappropriate antidiuresis.
1. Severe (<1%)
Desmopressin is generally not helpful for patients with 2. Moderate (1%-5%)
type IIB vWD since the release of endogenous vWF wors-
ens thrombocytopenia. Patients with type III vWD do not 3. Mild (>5%-40%)
respond to desmopressin and should not undergo a desmo-
pressin trial.
Clinical Features
For patients who do respond, desmopressin is a reasonable
Patients who have mild hemophilia seldom experience
alternative for prevention or treatment of minor bleeding, for
spontaneous hemorrhage but will bleed after trauma or sur-
minor procedures such as dental extraction, and for the man-
gery; rarely, they may not receive a diagnosis of hemophilia
agement of menorrhagia in women with vWD. An intrana-
until adulthood.
sal formulation of desmopressin is also available. For patients
Patients who have moderate hemophilia infrequently expe-
who do not respond to desmopressin and for those in whom it
rience spontaneous bleeding but typically bleed after minor
is contraindicated, administration of purified plasma-derived
trauma and surgery.
vWF concentrates is the therapy of choice.
Patients who have severe hemophilia frequently experi-
The goals for managing vWD include preventing
ence spontaneous bleeding, including hemarthrosis, soft tis-
and treating hemorrhage. General measures include the
sue hematomas, and intracranial hemorrhage in addition to
following:
minor hemorrhage such as epistaxis and ecchymoses. Regular
prophylactic administration of vWF concentrates to patients
1. Provide patient education
with severe disease has reduced the frequency and associated
2. Recommend a medical condition identification tag chronic complications related to bleeding.
516 H E M ATO L O GY
Table 35.3 CAUSES OF ACQUIRED COAGULATION underlying disease (Box 35.1) stimulates the procoagulant
FACTOR DEFICIENCIES system, generating thrombin and resulting in consumption
of coagulation factors and platelets. The fibrinolytic system
CAUSE OF DEFICIENCY DEFICIENT FACTOR
also is activated, converting plasminogen to plasmin. Plasmin
Warfarin Vitamin Kdependent factors prevents stabilization of fibrin clots (resulting in circulat-
ing fibrin monomers) and degrades existing fibrin clots and
Decreased nutritional intake or Vitamin Kdependent factors fibrinogen-releasing cleavage products called D-dimers. The
malabsorption
circulating fibrin monomers are soluble and thus form weak
Liver failure Multiple factors clots.
Amyloid Factor X
Management
Bleeding manifestations include bleeding from surgical Principles of management include identifying and treating
wounds and venipuncture sites, ecchymoses, petechiae, hema- underlying disease while managing the coagulopathy.
tomas, vaginal bleeding, or hemorrhage from the gastrointes-
tinal tract or genitourinary system.
Thrombotic manifestations occur less frequently than Blood Component Replacement Therapy
bleeding and include necrotic skin lesions, venous throm- Observation may be reasonable for patients who have
boembolism (deep vein thrombosis and pulmonary embo- low-grade compensated DIC with mild coagulopathy and no
lism), and acute arterial occlusions (stroke and myocardial bleeding.
infarction). For patients who have symptomatic hemorrhage or abnor-
mal laboratory results and for those at risk for bleeding, ther-
apy includes transfusion of blood components:
Pathophysiology
An understanding of the pathophysiology of DIC helps
1. If fibrinogen is low (<100 mg/dL), give cryoprecipitate.
with understanding laboratory testing and management. The
2. If PT and aPTT are markedly prolonged (suggesting
significant coagulation factor deficiency states), give fresh
frozen plasma.
Box 35.1 CAUSES OF DIC
3. If the platelet count is low (<30109/L or
Acute & subacute DIC <50109/L for bleeding patients), give platelet
Malignancies (hematologic & solid organ) concentrates.
Infection or sepsis (bacterial) The target platelet count is greater than 20109/L to
Obstetric complications (placental abruption, amniotic fluid 30109/L, especially if the patient is bleeding or undergoing
embolism) procedures. Monitor transfusion therapy with a CBC, PT,
Massive trauma aPTT, and fibrinogen level 60 minutes after a transfusion and
Burns every 6 to 8 hours thereafter.
Advanced liver disease
Snake bite
Hemolytic transfusion reaction Ancillary Therapies for DIC
Chronic DIC Although UFH inhibits thrombin and interrupts the
Solid tumors cycle of consumptive coagulopathy, it is also associated with
Obstetric complications (retained dead fetus) hemorrhage, including intracranial hemorrhage. Thus, in
Advanced liver disease acute DIC, heparin usually has a limited role, if any (except
Localized causes of systemic DIC with acute DIC associated with promyelocytic leukemia),
Aortic aneurysm but it may have a role in chronic DIC as seen with solid
Giant hemangiomas tumors, the retained dead fetus syndrome, aortic aneurysm,
and giant hemangiomas. Recombinant activated protein
Abbreviation: DIC, disseminated intravascular coagulation.
C improves mortality among patients with severe sepsis.
P L AT E L ET D I S O R D E R S
Thrombocytopenia Due to Increased Platelet
Platelets are produced in the bone marrow and, after cir- Destruction
culating for about 7 to 10 days, are destroyed in the reticu-
Autoimmune Thrombocytopenic Purpura
loendothelial system. Thrombocytopenia is most commonly
Autoimmune thrombocytopenic purpura, formerly called
acquired and poses a risk of bleeding. It commonly occurs as
idiopathic thrombocytopenic purpura, is an autoimmune dis-
a result of decreased production or accelerated destruction.
ease characterized by thrombocytopenia, usually with a nor-
When thrombocytopenia occurs for the first time, the diag-
mal white blood cell count and hemoglobin concentration
nosis of pseudothrombocytopenia should be excluded with
(Table 35.4).
examination of a peripheral blood smear. Rarely, thrombocy-
The diagnosis of autoimmune thrombocytopenic purpura
topenia is congenital.
is a diagnosis of exclusion:
518 H E M ATO L O GY
Box 35.2 CAUSES OF THROMBOCYTOPENIA Antibodies to specific platelet-membrane glycoproteins, usu-
ally the glycoprotein IIb/IIIa complex, and platelet-associated
Pseudothrombocytopenia IgG can be detected in most patients but are not necessary for
Dilutional diagnosis or treatment.
Massive transfusion In patients older than 60, a bone marrow examination is
Pregnancy appropriate to rule out another disorder causing thrombocy-
Increased destruction topenia (such as a myelodysplastic syndrome, which is more
Immune common in older patients). Bone marrow examination in
Autoimmune autoimmune thrombocytopenic purpura shows a normal to
Idiopathic increased number of megakaryocytes.
Secondary (drug-induced, connective tissue diseases)
Nonimmune
Consumptive (DIC) Treatment
Sepsis The American Society of Hematology guidelines for treat-
Decreased production ment are as follows:
Bone marrow failure syndromes
Primary: anaplastic anemia 1. Patients with platelet counts of 50109/L or higher do
Secondary: metastatic disease, hematologic malignancies not routinely require treatment.
Nutritional
Vitamin B12 & folate deficiency 2. Patients with platelet counts less than 50109/L but
Infections greater than 30109/L should be treated if there is
Viral (HIV infection, CMV infection, viral hepatitis) mucous membrane bleeding or risk factors for bleeding,
including hypertension, peptic ulcer disease, and a vigorous
Abbreviations: CMV, cytomegalovirus; DIC, disseminated intravascular coag- lifestyle.
ulation; HIV, human immunodeficiency virus.
3. Patients with platelet counts less than 30109/L should be
treated.
to 60% of adults progress to a chronic state of autoimmune a. Prednisone is the mainstay of initial treatment;
thrombocytopenic purpura. Only 10% of patients have sple- initially, 70% of patients respond, with a 40% chance
nomegaly. If splenomegaly is present, one should think of of long-term remission (prednisone 1 mg/kg daily for
other causes. up to 1 month).
b. If bleeding is severe, treat with IV immunoglobulin
Laboratory Findings (1 g/kg daily for 2 days) and platelets; high-dose
In most patients, the platelet count is less than 50109/L, and IV corticosteroids can also be considered (eg,
in 30% it is less than 10109/L (spontaneous bleeding may methylprednisolone, 1 g daily for 23 consecutive
occur at this level). The mean platelet volume is increased. days; initial response rate is 80%).
Splenectomy, the treatment of choice for steroid-refractory
autoimmune thrombocytopenic purpura, removes the pre-
dominant site of antibody production and platelet destruc-
tion; the likelihood of remission is 75%, with about 60% of
patients remaining in long-term remission. Pneumococcal,
meningococcal, and Haemophilus influenzae vaccines should
be administered 2 weeks before splenectomy. Absence of
Howell-Jolly bodies on a postsplenectomy peripheral blood
smear suggests an accessory spleen, and accessory splenectomy
can result in remission. Pulsed dexamethasone (40 mg daily
for 4 sequential days every 28 days for 12 months) is an option
for the treatment of resistant autoimmune thrombocytopenic
purpura or disease relapse. Other agents used in refractory
cases include azathioprine, cyclophosphamide, colchicine,
cyclosporine, rituximab, vincristine, vinblastine, anti-RhO(D)
immune globulin, danazol, and immunoadsorption apheresis
on staphylococcal protein A columns.
Novel agents approved for use in patients with
Figure 35.3 Giant Platelets. Giant platelets may be associated with
congenital platelet synthesis disorders, acquired clonal myeloid disorders,
corticosteroid-refractory autoimmune thrombocytopenic
or immune thrombocytopenia (Wright-Giemsa). (Courtesy of Curtis A. purpura include oral (eltrombopag) and parenteral (romi-
Hanson, MD, Mayo Clinic. Used with permission.) plostim) thrombopoietin receptor agonists.
520 H E M ATO L O GY
Anticoagulant Management 2. Inflammatory or autoimmune states (eg, connective
Administer a DTI: lepirudin, bivalirudin, or argatroban tissue diseases such as systemic lupus erythematosus and
(Box 35.3). Argatroban is the treatment of choice for patients rheumatoid arthritis)
with renal insufficiency because of hepatic elimination; in
3. Nutritional deficiencies (eg, vitamin B12 or folate
contrast, for patients with hepatic failure, lepirudin (renally
deficiencies)
excreted) is preferred.
4. Bone marrow failure states such as myelodysplastic
Heparin is the drug that most commonly causes syndrome or aplastic anemia
thrombocytopenia.
Management consists of identifying and treating the
HIT type II requires discontinuation of the use of all
underlying disease.
heparin, including LMWH.
Given the high risk of thrombosis, initiation of a DTI
Congenital Platelet Disorders
should be strongly considered.
Congenital abnormalities of the platelet receptor glycopro-
Chemotherapy-Associated Thrombocytopenia teins lead to platelet dysfunction and thrombocytopenia.
The threshold for platelet transfusion is 10109/L unless Lifelong mucocutaneous bleeding and postoperative bleed-
other risk factors for bleeding (eg, fever, mucosal lesion) are ing are typical. Platelet transfusions are used for prevention
present. Interleukin 11 (oprelvekin) is modestly effective but and treatment of hemorrhage. A risk of frequent transfusions
is associated with fluid retention and atrial dysrhythmias. is platelet alloimmunization. Diagnosis is based on platelet
Pharmacologic agents stimulating the thrombopoietin recep- function testing as follows:
tor are likely to be approved soon.
1. Bernard-Soulier syndrome
522 H E M ATO L O GY
36.
HEMATOLOGY: THROMB OSIS
Rajiv K. Pruthi, MBBS
Review the evaluation and treatment of patients with Laboratory testing consists of performing the APC
venous thromboembolism (VTE). resistance assay and, if the results are abnormal, follow-up
DNA-based testing for factor V Leiden to determine whether
the person is heterozygous or homozygous.
THROMBOPHILIA: THE
The most common inherited defect of the procoagulant
H Y P E R C OAGU L A B L E S TAT E S
system is APC resistance due to the factor V Leiden
mutation.
Thrombophilia refers to the tendency for thromboembolism
(ie, having risk factors for thromboembolism), which may be Heterozygotes have an approximately 2- to 4-fold
inherited or acquired (Box 36.1). The presence of increasing increased risk of VTE, and the risk is increased 30 times
numbers of risk factors further increases the risk of venous when they take estrogen-containing oral contraceptives.
thrombosis. Lupus anticoagulant and hyperhomocysteinemia
are associated with arterial thrombosis. Prothrombin G20210A
Thrombophilic defects can be broadly classified into The next most common defect is the prothrombin
abnormalities of the procoagulant system and abnormalities G20210A mutation, which results in an elevated plasma pro-
of the anticoagulant system. thrombin level. The heterozygous mutation has a prevalence
of approximately 3% in the healthy white population and
6% to 18% among persons with VTE. Heterozygotes have an
approximately 2-fold increased risk of VTE. These defects are
D E FEC TS I N T H E P RO C OAGU L A N T SYST E M common among white people and rare among people of Asian
Inherited Risk Factors or African ancestry. Laboratory testing consists of DNA-based
testing for the presence or absence of the mutation.
Factor V Leiden
The most common inherited defect is activated protein
C (APC) resistance due to the factor V Leiden mutation Other Risk Factors
(R506Q). This causes activated factor V to be resistant to inac- Additional abnormalities of procoagulant proteins that con-
tivation by APC. fer an increased risk of VTE include increased levels of fac-
tors VIII, IX, and XI. Currently, there is no established cutoff
1. Heterozygous mutation for this increased risk and there is no known genetic basis for
a. Prevalence of 5%-7% in the healthy white population these abnormalities.
and 20%-50% among persons with VTE.
b. Heterozygotes have a 2- to 4-fold increased risk of D E FEC TS I N T H E A N T I COAGU L A N T SYST E M
VTE.
Congenital deficiencies of the anticoagulants antithrom-
c. Risk of VTE is increased 30-fold for heterozygous bin, protein C, and protein S confer an increased risk of
carriers taking estrogen-containing oral contraceptives VTE. In the majority of patients, VTE develops by 50
523
Box 36.1 INHERITED AND ACQUIRED Asymptomatic patients with antiphospholipid antibodies
THROMBOPHILIA do not need anticoagulant therapy.
Patients with antiphospholipid antibodies and
Inherited thrombophilia vascular thrombosis should be treated with long-term
Activated protein C resistance due to factor V Leiden mutation anticoagulation.
Prothrombin G20210A mutation
Anticoagulant deficiencies: antithrombin, protein C, protein S Other acquired risk factors for VTE include immobiliza-
Selected dysfibrinogenemia tion (hospitalization, paralysis, etc), orthopedic or general
Acquired thrombophilia surgery, and estrogen-containing drugs, which pose a signifi-
Lupus anticoagulant or antiphospholipid antibody syndrome cant risk of VTE. When any of these risk factors is combined
Pregnancy with an underlying inherited risk factor (eg, factor V Leiden),
Immobilization (trauma, postoperative state) the chances of symptomatic VTE increase significantly.
Estrogens (oral contraceptives, hormone replacement therapy)
Solid organ malignancy Mixed Inherited and Acquired Risk Factors
Myeloproliferative diseases In selected situations (eg, hyperhomocysteinemia), genetic
Paroxysmal nocturnal hemoglobinuria determinants (eg, MTHFR C677T mutation) pose a risk that
Prolonged travel may be compounded by acquired determinants (eg, dietary
Obesity deficiencies of folate and vitamins B6 and B12), resulting in
Age an increased risk of VTE. Patients with inherited risk factors
Mixed risk factors have a baseline increased risk; symptomatic VTE develops
Hyperhomocysteinemia when the inherited risk factors are present in combination
Elevated levels of factors VIII, IX, & XI with acquired risk factors, such as pregnancy, estrogen use, or
surgery.
524 H E M ATO L O GY
Table 36.1 RISK FACTORS AND INCIDENCE OF VTE
INCIDENCE, %
ADDITIONAL
LEVEL OF RISK SURGERY RISK FACTORS CVT Proximal DVT Clinical PE Fatal PE
Major None
Abbreviations: CVT, calf vein thrombosis; DVT, deep vein thrombosis; PE, pulmonary embolism; VTE, venous thromboembolism.
pneumatic compression if immobilized, and Step 1: Determine the Clinical Pretest Probability
pharmacologic prophylaxis (UFH and LMWH are The Wells model (Table 36.2) categorizes the pretest prob-
equivalent). ability of DVT as high (3 points), moderate (1 or 2 points),
or low (<1 point). A similar model has been applied to pulmo-
4. Very high-risk patientsSame as for moderate- or
nary embolism (Table 36.3), which stratifies patients accord-
high-risk patients but with the following differences:
ing to whether pulmonary embolism is less likely (4) or likely
UFH is not recommended; LMWH, fondaparinux, and
(>4). For patients in the low-risk category, further imaging
adjusted-dose warfarin are used to keep the international
studies are probably not needed, and determining the level of
normalized ratio (INR) between 2.0 and 3.0; and
D-dimer, a breakdown product from cross-linked stabilized
extended out-of-hospital prophylaxis may be needed.
fibrin clots, is recommended.
5. Patients with a previous history of VTE or
thrombophiliaSame as the strategies for very high-risk Step 2: Determine the D-Dimer Level
patients. In ambulatory outpatients, a negative D-dimer test has a
high negative predictive value for DVT, thus avoiding unnec-
essary additional diagnostic tests. It is most useful for ambula-
Evaluation of the Patient for VTE tory outpatients, and it should not be used to exclude VTE
in hospitalized patients, patients with malignancy or recent
Upon radiologic testing, more than 75% of ambulatory trauma, surgery, or hemorrhage. In these patients, proceeding
patients who present with symptoms worrisome for DVT are with imaging studies is appropriate.
found not to have the disease. Thus, a sensitive and specific
strategy to reduce excess radiologic imaging studies without
compromising patient safety is required. A history of the pres-
ence or absence of acquired risk factors for VTE should be Table 36.2 WELLS MODEL FOR PREDICTING
obtained. Considerations in the clinical evaluation include CLINICAL PRETEST PROBABILITY OF DEEP VEIN
patient and family history of VTE, pregnancy, recurrent THROMBOSIS
miscarriage, estrogen use, recent trauma, surgery, hospitaliza-
tion, malignancy, and travel. A physical examination should CLINICAL VARIABLE POINTS
include evaluation for venous stasis and for detection of an
Active cancer 1
underlying malignancy. The most critical initial component
of the examination is to determine the presence or absence of Paralysis or recent limb casting 1
venous limb gangrene (phlegmasia cerulea dolens), in which
Recent immobility for >3 d 1
severe obstruction of extremity venous drainage leads to con-
gestion and eventual obstruction of arterial inflow. If venous Local vein tenderness 1
limb gangrene is present, thrombolytic therapy, fasciotomy, or
Limb swelling 1
thrombectomy may be indicated.
Although important, clinical findings alone are poor Lateral calf swelling >3 cm 1
predictors of the presence or severity of VTE, and objective
Pitting edema 1
diagnostic testing may eventually be required. Initial steps,
however, consist of estimating the clinical pretest probability Collateral superficial vein 1
of VTE and using the D-dimer assay with further diagnostic
Alternative diagnoses likely 2
testing as indicated.
526 H E M ATO L O GY
Long-term Management of VTE factors (idiopathic), an additional 3 months of warfarin for
Warfarin therapy is continued for an appropriate duration. secondary prevention is recommended. For recurrent DVT,
INR is monitored every 4 to 6 weeks. Long-term outcomes consider secondary prevention with warfarin for a total of
have been shown to be superior when VTE is managed in anti- 12 months of treatment. For hemodynamically significant
coagulation clinics and with home INR devices. or idiopathic pulmonary embolism, long-term treatment
with warfarin is reasonable. Long-term treatment with
Calf Vein Thrombosis warfarin is also reasonable for VTE in patients who have
Asymptomatic calf vein thrombosis can be observed if the underlying thrombophilia (eg, from lupus anticoagulant
patient is willing and able to return for follow-up compres- or deficiency of protein C, protein S, or antithrombin) or
sion ultrasonography to document stability or progression of for patients who are compound heterozygous for factor V
the clot. For symptomatic or progressive calf vein thrombosis, Leiden and prothrombin G20210A mutation. Continuing
anticoagulation should be initiated. warfarin anticoagulation should be balanced with the risk
of hemorrhage.
Proximal DVT
LMWH and warfarin should be administered as described
above.
Pulmonary Embolism S U M M A RY
Patients with pulmonary embolism should be hospitalized
for at least 24 hours to assess clinical stability. Selected asymp- Estimating pretest probability is important in determining
tomatic, clinically stable patients may be treated as outpatients a diagnostic approach for VTE.
with LMWH and warfarin as described above. Treat DVT and pulmonary embolism for a minimum of
3 months.
Duration of Warfarin Anticoagulation
Treat with warfarin for at least 3 months for DVT and Unprovoked or recurrent VTE requires longer treatment;
pulmonary embolism. For DVT occurring without risk weigh risks and benefits of anticoagulation.
528
Table 37.2 STAGING OF CHRONIC LYMPHOCYTIC
LEUKEMIA: INTERNATIONAL WORKSHOP ON
CHRONIC LYMPHOCYTIC LEUKEMIA CLASSIFICATION
CLINICAL
STAGE FEATURES
MEDIAN SURVIVAL H A I RY C E L L L EU K E M I A
STAGE CHARACTERISTICS TIME, MO
HCL is a rare mature B-cell neoplasm characterized by an
0 Peripheral lymphocytosis >150 insidious onset of cytopenias and the presence of cells with
(>15109/L), bone marrow hairy cytoplasmic projections. The male to female ratio is
lymphocytosis (>40%)
4:1 (Figure 37.2).
I Lymphocytosis, lymphadenopathy 101 The symptoms are related to cytopenias, infections, and
splenomegaly. The bone marrow often yields a dry tap (ie,
II Lymphocytosis, splenomegaly 71
no liquid marrow is obtained); core biopsy specimens are
III Lymphocytosis, anemia (hemoglobin 19 hypercellular, with diffuse infiltration by neoplastic cells and
<11 g/dL), excluding AIHA fibrosis. With treatment, most patients live for more than 10
IV Lymphocytosis, thrombocytopenia 19 years. HCL causes immunosuppression and an increased risk
of infection. Atypical mycobacterial infections are a classic
association.
Abbreviation: AIHA, autoimmune hemolytic anemia.
Data from Rai KR, Sawitsky A, Cronkite EP, Chanana AD, Levy RN,
Pasternack BS. Clinical staging of chronic lymphocytic leukemia. Blood. 1975 Cytopenias and splenomegaly are common in patients with
Aug;46(2):21934. HCL.
530 H E M ATO L O GY
Table 37.3 COTSWOLDS STAGING CLASSIFICATION OF
HODGKIN LYMPHOMA
CLASSIFICATION DESCRIPTION
Mature T-Cell & NK-Cell Neoplams combination with a proton pump inhibitor. If this is unsuccess-
T-cell prolymphocytic leukemia ful, chemotherapy and irradiation are typically administered.
T-cell large granular lymphocytic leukemia
Chronic lymphoproliferative disorder of NK cellsa Aggressive Lymphomas
Aggressive NK cell leukemia
Systemic EBV-positive T-cell lymphoproliferative disease of In contrast to low-grade lymphomas, aggressive lymphomas
childhood are potentially curable, but the duration of survival is short if
Hydroa vacciniformelike lymphoma the patient does not have remission. Patients typically present
with symptomatic disease, including B symptoms (as in Table
532 H E M ATO L O GY
37.3: fevers, drenching night sweats, and weight loss). For M O N O C L O NA L G A M M O PAT H I E S O F
patients with aggressive lymphoma that relapses after com- U N D ET E R M I N E D S I G N I FI C A N C E
plete remission, autologous stem cell transplant is the standard
In MGUS, the most common form of dysproteinemia
therapy.
involves the serum M-protein level (typically <3 g/dL).
The standard therapy for DLBCL is R-CHOP (>50%
The bone marrow has less than 10% plasma cells. The serum
are cured). The International Prognostic Factor Index uses
creatinine, calcium, and hemoglobin levels are normal, and
age, lactate dehydrogenase level, performance status scores,
the urine has either no M protein or only a small amount.
disease stage, and extranodal involvement to predict survival
Osteolytic bone lesions are absent, and patients are usually
of patients who have DLBCL. Five-year survival ranges from
asymptomatic.
26% to 73%, depending on risk factors.
MGUS is common. In population-based studies, an M
Mantle cell lymphoma is characterized by a CD5+ and
protein was found in the serum of 3.2% of adults older than
CD20+ immunophenotype and a t(11;14) translocation,
50 years, 5.3% of those older than 70, and 7.5% of those 85
with overexpression of the cyclin D1 oncogene. Unlike
or older. MGUS progresses to a malignant monoclonal gam-
other aggressive lymphomas, mantle cell lymphoma is not
mopathy at an annual rate of about 1%. On free light-chain
curable; thus, stem cell transplant is usually incorporated
analysis, an abnormal : ratio is a risk factor for progression.
early.
Patients with MGUS should be observed.
Very aggressive lymphomas, such as Burkitt lymphoma
and lymphoblastic lymphoma, are treated with regimens
In MGUS, the serum M protein is typically <3 g/dL; bone
similar to those used for ALL. These subtypes carry a high
marrow has <10% plasma cells; and serum hemoglobin,
risk of central nervous system involvement and tumor lysis
creatinine, and calcium levels are normal.
syndrome.
Patients with human immunodeficiency virus (HIV)- Patients are observed without therapy.
related lymphoproliferative disorders with a CD4 cell count
Typical clinical scenario: A patient without symptoms has
less than 200/mL have a poor response to standard treatment.
a serum M-protein spike <3 g/dL and bone marrow plasma
Primary central nervous system lymphoma occurs with or
cells <10%. Blood counts, serum creatinine level, and bone
without HIV infection, carries a poor prognosis, and is gener-
radiographs are normal.
ally treated with high-dose methotrexate.
534 H E M ATO L O GY
Patients with AL amyloidosis may present with fatigue,
weight loss, hepatomegaly, macroglossia, renal insufficiency,
proteinuria, nephrotic syndrome, congestive heart failure,
orthostatic hypotension, carpal tunnel syndrome, or periph-
eral neuropathy. When patients have cardiac involvement,
electrocardiography may show low voltage or Q waves. The
echocardiogram is abnormal in 60%, with concentrically
thickened ventricles or a thickened intraventricular septum
and sometimes a speckled appearance. Peripheral neuropa-
thy is often associated with autonomic failure, as manifested
by diarrhea, pseudo-obstruction of the bowel, or orthostatic
syncope.
For AL amyloidosis, treatment with melphalan and dexa-
methasone is modestly effective. Autologous stem cell trans-
plant provides benefit in carefully selected patients. The
median survival for all patients with AL amyloidosis is 13
Figure 37.6 Acute Myeloid Leukemia. Blast cells are large and have an
months. With overt congestive heart failure, the median sur- open, granular nuclear chromatin, often with 1 or more nucleoli. The
vival is less than 6 months. presence of an Auer rod means that the blast is myeloid rather than
Treatment of AA amyloidosis involves correcting the lymphoid (bone marrow aspirate smear; Wright-Giemsa).
underlying disease. Liver transplant may be valuable in famil-
ial cases in which an amyloidogenic protein is made by the
abnormalities of t(8;21), t(15;17), or inv(16); and achieving
liver.
complete remission with 1 cycle of induction chemotherapy.
Poor prognostic signs include age older than 40 years (espe-
The amyloidoses are characterized by deposition of
cially >60 years); an antecedent hematologic disorder; previ-
insoluble fibrils in tissues, leading to organ dysfunction.
ous chemotherapy or radiotherapy; high-risk chromosomal
AL amyloidosis is the most common form. abnormalities (chromosome 5, 7, or 11q23, or a complex
karyotype); and poor general physical condition.
Associated clinical features: fatigue, nephrotic syndrome, For patients who present with extreme leukocytosis (WBC
congestive heart failure, sensorimotor neuropathy, and count >80109/L) and acute leukemia, the initial complica-
macroglossia. tion of most concern is cerebral hemorrhage due to leuko-
Typical clinical scenario: A 64-year-old man has stasis. Emergency treatment includes hydration, allopurinol,
weakness, weight loss, congestive heart failure, carpal hydroxyurea, and leukapheresis, followed by treatment of the
tunnel syndrome, peripheral neuropathy, and orthostatic specific type of leukemia. Patients with acute promyelocytic
hypotension. An M protein is detected on serum leukemia (AML-M3) (Figure 37.7) typically have t(15;17)
electrophoresis. and often present with disseminated intravascular coagulation
(DIC).
Treatment for AML is divided into 1) induction therapy
AC U T E L E U K E M I A S (cytarabine and an anthracycline agent) and 2) consolidation
therapy (high-dose cytarabine). Relapse occurs eventually in
Acute leukemia is defined by the presence of at least 20% most patients with AML, usually within 3 years. In patients
undifferentiated blast cells in the bone marrow. If the cells with relapsed AML, reinduction of remission is followed by
exhibit myeloid differentiation, the diagnosis is AML; if the hematopoietic stem cell transplant, if feasible. The 5-year sur-
cells have lymphoid markers, the diagnosis is ALL. vival for younger patients with a good cytogenetic profile is
60%, but for patients who have poor cytogenetics or who are
older (especially older than 70), the 5-year survival is less than
ACU T E MY E L O I D L EU K E M I A 10%.
All-trans-retinoic acid (ATRA) is the treatment of choice
The cause of AML is unknown in most cases, but there are in AML-M3 with t(15;17). Induction chemotherapy is with
many associations: previous myeloproliferative neoplasm or ATRA and an anthracycline-based program, followed by con-
MDSs; exposure to radiation or benzene; prior chemotherapy; solidation therapy. Maintenance therapy includes ATRA for
and congenital disorders such as Down syndrome, Fanconi 1 to 2 years.
syndrome, and ataxia-telangiectasia.
The median age of patients with AML (Figure 37.6) is AML: median age of patients is about 65 years.
about 65 years. Patients may present with nonspecific symp-
toms, such as fatigue and headache, or with complications of Good prognosis: being younger than 40 years; having
cytopenias. By definition, patients have 20% or more undif- chromosomal abnormalities t(8;21), t(15;17), or inv(16);
ferentiated blasts in the bone marrow. Good prognostic signs and achieving complete remission with 1 cycle of induction
include being younger than 40 years; having chromosomal chemotherapy.
Chronic myeloid disorders include MDSs, CML, and myelo- Figure 37.8 Chronic Myeloid Leukemia. Normal-appearing myeloid cells
show all stages of maturation, with a decreased number of erythropoietic
proliferative neoplasms. Patients with these disorders have less cells and 1 basophil precursor in the center (bone marrow aspirate smear;
than 20% bone marrow blasts, which distinguishes them from Wright-Giemsa). (Courtesy of Curtis A. Hanson, MD, Mayo Clinic,
AML. Chronic myeloid disorders often evolve into AML. Rochester, Minnesota. Used with permission.)
536 H E M ATO L O GY
Characteristic laboratory findings include leukocytosis. about half of those with primary myelofibrosis or essential
WBC counts of 10010 9/L are common, but leukapheresis thrombocythemia.
is not usually required since the leukocytes are mature and
do not cause leukostasis. Granulocytes in all stages of mat- Myeloproliferative neoplasms include polycythemia vera,
uration are present on peripheral blood smear, with baso- primary myelofibrosis, and essential thrombocythemia.
philia and eosinophilia and a characteristic myelocyte bulge
(ie, increased numbers of myelocytes in relation to other JAK2 mutations are universal in polycythemia vera and are
stages of granulocyte differentiation). The bone marrow is common in other myeloproliferative neoplasms.
hypercellular. Polycythemia vera and essential thrombocythemia may
progress to myelofibrosis. All myeloproliferative neoplasms
CML: clonal neoplasm due to acquired BCR-ABL fusion. can progress to AML.
Philadelphia chromosome, t(9;22), results in BCR-ABL
fusion.
Primary Myelofibrosis, Postpolycythemic Myelofibrosis,
Typical complete blood cell count finding: increased WBC and Postthrombocythemic Myelofibrosis
count, with granulocytes in all stages of maturation and
basophilia. Splenomegaly occurs in virtually all patients and is a hallmark
of primary myelofibrosis. Other features are a leukoerythro-
Patients who are resistant to tyrosine kinase inhibitors may blastic peripheral blood smear, including nucleated red blood
be eligible for allogeneic stem cell transplant or interferon and cells and dacrocytes (teardrop cells), and hypercellular mar-
cytarabine. Untreated, the chronic phase eventually progresses to row with increased fibrosis (Figure 37.9).
an accelerated phase and then a blast crisis, which is characterized Foci of extramedullary hematopoiesis can occur in any area
by blast counts greater than 20%. Blast crisis is treated like AML. of the body but are most common in the spleen, liver, lung
and pleural space, skin, eye, and central nervous system. The
Imatinib, a potent BCR-ABL inhibitor, is the treatment of median survival is 3 to 5 years.
choice in CML.
The median survival of patients with myelofibrosis is 35
years.
P H I L A D E L P H I A C H RO MO S O M E N EG AT I V E
MY E L O P RO L I FE R AT I VE N EO P L A S M S Primary myelofibrosis: hallmark is splenomegaly, often
massive.
The classic myeloproliferative neoplasms include polycythemia
vera, primary myelofibrosis, and essential thrombocythemia. Leukoerythroblastic peripheral blood smear includes
Their characteristic features are listed in Table 37.5. These teardrop cells.
disorders are interrelated: polycythemia vera progresses to
postpolycythemic myelofibrosis in 10% of patients, and essen- Asymptomatic patients should be observed. Medical ther-
tial thrombocythemia progresses to postthrombocythemic apy for anemia includes transfusion with packed red blood
myelofibrosis in 5%. AML is a complication of polycythemia cells, androgens, or erythropoietin. Some patients respond to
vera (10% of patients), essential thrombocythemia (<5%), and thalidomide or lenalidomide.
primary myelofibrosis (10%-20%) and is usually refractory to Symptoms related to the spleen, such as early satiety, infarcts,
therapy. Each of these disorders carries a risk of thrombosis and pressure, can be treated with splenectomy, hydroxyu-
and hemorrhage. rea, or splenic irradiation. DIC is common and increases the
Activating mutations involving JAK2 tyrosine kinase are risk of a complication at splenectomy. Hydroxyurea is indi-
present in almost all patients with polycythemia vera and in cated for symptomatic hepatosplenomegaly, leukocytosis, and
Polycythemia Vera
Polycythemia vera is a myeloproliferative disorder that results
from activating mutations involving JAK2 tyrosine kinase.
Clinical features include postbathing pruritus, fatigue, eryth-
romelalgia (acral dysesthesias and erythema), headache, diz-
ziness, and weight loss. More than 50% of patients have
leukocytosis and thrombocytosis in addition to erythrocyto-
sis. Polycythemia vera should be considered in the evaluation
of an idiopathic thrombosis, especially in an atypical site such
as an abdominal vessel or a dural sinus in the brain.
Bone marrow findings in polycythemia vera typically
include trilineage hyperplasia. Most bone marrow specimens
Figure 37.9 Leukoerythroblastic Blood Smear. The teardrop-shaped
erythrocytes (dacrocytes) and nucleated red blood cell are characteristic lack iron stores because the erythrocyte proliferation outstrips
of marrow fibrosis, whether due to primary myelofibrosis or a reactive the iron supply. The leukocyte alkaline phosphatase score
cause (peripheral blood smear; Wright-Giemsa). is not often measured anymore, but it is increased in poly-
cythemia vera and primary myelofibrosis and low in CML.
thrombocytosis. Bone marrow transplant may be helpful in Erythropoietin levels are low or low normal. The mainstay of
some young patients. therapy for all patients with polycythemia vera is phlebotomy,
with the goal of maintaining the hematocrit at less than 45%.
Low-dose aspirin therapy is indicated for all patients who do
Essential Thrombocythemia not have a contraindication.
Essential thrombocythemia (also called essential thrombocyto- For patients who are older than 60 or who have had prior
sis) is a clonal hematologic disorder in which patients present thrombosis, cytoreductive therapy is indicated. Hydroxyurea
with thrombocytosis and sometimes leukocytosis. Patients is often the first choice. Interferon alfa is the treatment of
may be asymptomatic, or they may have thrombosis or hem- choice for younger patients and women of childbearing age.
orrhage. Patients have a relatively long life expectancy (>10 Radiophosphorus may be useful in older patients, but it
years). Young females have a higher risk of miscarriage than increases the risk of AML.
age-matched controls. The risk of acute leukemic transforma-
tion is less than 5% at 15 years. Polycythemia vera: low erythropoietin and universal
Diagnostic features of essential thrombocythemia include finding of JAK2 mutation.
a sustained platelet count greater than 450109/L, mega-
Pruritus, unusual thrombosis, and erythromelalgia.
karyocytic hyperplasia in the bone marrow, and absence of
the Philadelphia chromosome. It may be challenging to distin- For polycythemia vera, phlebotomy is the cornerstone of
guish essential thrombocythemia from reactive thrombocyto- treatment.
sis or iron deficiency.
For patients older than 60 years or with a history of
Treatment depends on the clinical situation. All patients
thrombosis, add hydroxyurea.
who can tolerate aspirin should receive low-dose aspirin.
Platelet apheresis should be used only for emergent manage-
ment of acute bleeding or thrombosis and is not indicated from
the platelet count alone. Cytoreductive therapy (hydroxyurea S U M M A RY
is the treatment of choice; anagrelide is an alternative) is rec-
ommended for patients with acute thrombosis or a previous With treatment, more than 80% of patients with Hodgkin
history of thrombosis and for patients older than 60 years. lymphoma are now cured.
Patients who are asymptomatic and young may be observed.
In patients with very high platelet counts (>1,000109/L), NHL is a diverse group that includes low-grade
acquired von Willebrand disease can develop. For these lymphomas (which are usually not curable by the time
patients, the bleeding risk is greater than the thrombotic risk. they are diagnosed) and aggressive lymphomas (which are
potentially curable).
Essential thrombocythemia: elevated platelet count with Multiple myeloma is distinguished from MGUS and
secondary causes excluded; half of the patients have JAK2 smoldering myeloma by the presence of end-organ damage;
V617F. treatment is evolving.
Cytoreductive therapy is indicated for patients older than The median age of patients with AML is about 65 years;
60 years or for patients who have had prior thrombosis. the prognosis may be good if patients are younger than 40.
538 H E M ATO L O GY
PA RT I X
N E P H R O L O GY
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38.
ACIDBASE AND ELECTROLY TE DISORDER S
Qi Qian, MD
Define fluid, electrolyte, and acidbase disorders. For patients with volume depletion, infusion of isotonic
fluids and oral sodium restores volume status. In patients
Cite treatments for fluid, electrolyte, and acidbase with congestive heart failure, measures that optimize car-
disorders. diac function may improve renal perfusion and, therefore,
Apply these concepts to clinical scenarios. facilitate diuresis. In cirrhosis, interventions that reduce por-
tal hypertension and the need for liver transplant improve
hemodynamics. In nephrotic syndrome, correcting pro-
DISORDER S OF SODIUM BAL ANCE AND teinuria restores sodium homeostasis and volume balance.
VO LU M E R E GU L AT I O N Diuresis, in general, is unnecessary in patients with regional
fluid retention (except for regional edema involving the
Volume expansion can be general (as in patients with con- airway).
gestive heart failure, cirrhosis, and nephrotic syndrome) or
regional (as in patients with regional capillary leak, venous Sodium balance reflects the bodys volume status. Total
insufficiency, and lymphatic obstruction). Volume depletion is body sodium excess equates with volume expansion
associated primarily with gastrointestinal tract (GI) fluid loss, (hypervolemia), and total body sodium deficiency equates
excessive sweating, and renal sodium loss related to diuretic with volume depletion (hypovolemia).
use or, rarely, renal salt wasting.
D I AG N O S I S
D I S O R D E R S O F WAT E R B A L A N C E
The cause of a volume disorder can be determined by physi-
cal examination. Elevated systemic blood pressure with or H Y P O NAT R E M I A ( WAT E R E XC E S S )
without edema signifies total body sodium excess. In con-
gestive heart failure and cirrhosis, the kidneys are stimulated Hyponatremia can be categorized as hypovolemic, euv-
to retain sodium because the systemic blood pressure is low olemic, or hypervolemic. Hypovolemia is a potent stimula-
from low arterial effective volume (arterial underfill) due to tor for arginine vasopressin (AVP)-mediated renal water
pump failure and circulation derangements. Sodium retention retention, which leads to hyponatremia. Euvolemic hypona-
leads to a net positive sodium balance and edema. Regional tremia includes 1) psychogenic polydipsia and beer potoma-
volume expansion is typically obvious on physical examina- nia, in which water or hypotonic beer ingestion exceeds the
tion, showing normal vital signs and confined areas of fluid capacity of renal water excretion; 2) syndrome of inappropri-
retention. Volume depletion is manifested by hypotension ate secretion of antidiuretic hormone (SIADH), in which
and tachycardia. AVP-mediated water retention is independent of serum osmo-
lality and volume status; and, rarely, 3) hypothyroidism and
adrenal insufficiency. Hypervolemic hyponatremia mainly
THERAPY
occurs in patients with congestive heart failure or cirrhosis.
Management of volume disorders is 2-fold: Arterial underfill in both conditions signals volume deple-
tion, and activates AVP-mediated water retention, resulting
1. Volume repletion for hypovolemia and volume removal in hyponatremia. In patients with moderate to advanced
for hypervolemia with diuretics or dialysis (or both) when renal failure, dilutional hyponatremia may develop because of
appropriate the diminished capacity of renal water excretion.
541
Hyponatremia
Serum osmolality
Pseudohyponatremia Hyperglycemia
Hyperlipidemia Hypertonic infusions
Hyperproteinemia Glucose
Mannitol
Sorbitol
Glycine
<10 mEq/L >20 mEq/L <10 mEq/L >20 mEq/L <10 mEq/L >20 mEq/L
Extrarenal Renal Na+ Psychogenic SIADH Cirrhosis Renal failure
Na+ loss loss polyrapsia Hypothyroidism Heart failure
Gastro- Diuretic use Beer Adrenal Renal failure
intestinal tract Renal salt potomania insufficency
Insensible wasting Thiazide
(replete with Adrenal diuretic use
hypotonic
insufficiency
lipids)
Figure 38.1 Diagnosis of Hyponatremia. Na+ indicates sodium; SIADH, syndrome of inappropriate secretion of antidiuretic hormone.
Diagnosis Therapy
The initial step in evaluating patients with hyponatremia is For isosmotic and hyperosmotic hyponatremia, management
to determine the serum osmolality. As shown in Figure 38.1, should be directed toward correcting the underlying cause.
depending on the serum osmolality, the differential diagnosis For hypovolemic hyponatremia, restoring intravascular
is narrowed to 3 categories. volume eliminates the stimulatory signal for AVP. For patients
If hypo-osmolality is confirmed, the diagnosis can be fur- with normal renal clearance, renal water unloading normalizes
ther narrowed to hypovolemic, euvolemic, or hypervolemic serum sodium concentration and osmolality.
hyponatremia on the basis of the patients volume status, deter- For hypervolemic hyponatremia, symptomatic treatment
mined by physical examination. Urine osmolality and urinary directed toward reducing both total body water and sodium
sodium concentration can then further help with delineating (aquaresis more than natriuresis) is necessary. Loop diuretics
the underlying cause of hyponatremia. with or without vasopressin V2 receptor antagonists (vaptans)
In patients with euvolemic hyponatremia, if the urine are usually effective. Correcting the underlying cardiac and
is not maximally diluted (>150 mOsm/kg) and the uri- hepatic abnormalities, if possible, will ultimately correct the
nary sodium concentration is greater than 20 mEq/L (on water dysregulation.
a regular Western diet), thyroid disease and adrenal insuf- For euvolemic hyponatremia, SIADH, treatment options
ficiency must be ruled out before considering the diagnosis include free water restriction, vasopressin V2 receptor blocker,
of SIADH. and, when symptomatic, high-concentration (3%) saline.
Patients with thiazide diureticinduced hyponatremia Specific attention should be paid to the rate of serum sodium
may present with euvolemic hyponatremia that is indistin- correction. If hyponatremia developed over more than 2 days,
guishable from SIADH. Clinical history is critical in estab- correction should be gradual (<10 mEq daily). Rapid correction
lishing causation. Postoperative pain can be associated with could lead to central pontine myelinolysis, a devastating neuro-
transient SIADH. Drugs associated with euvolemic hypona- logic complication of the locked-in state. Underlying causes of
tremia include selective serotonin reuptake inhibitors, car- SIADH should always be sought and, when possible, corrected.
bamazepine, chlorpromazine, vasopressin analogues, and,
rarely, theophylline and amiodarone. Ecstasy intoxication can Hyponatremia can be categorized as hypovolemic,
cause hyponatremia. euvolemic, or hypervolemic.
542 N E P H R O L O GY
Hypernatremia
Fluid volume status assessed by physical examination
>20 mEq/L <10 mEq/L >20 mEq/L <10 mEq/L >20 mEq/L
Hypertonic dialysis
Hemodialysis
Peritoneal dialysis
Figure 38.2 Diagnosis and Management of Hypernatremia. D5W indicates 5% dextrose in water; GI, gastrointestinal tract; Na+, sodium; NaCl,
sodium chloride; NaHCO3, sodium bicarbonate.
H Y P E R NAT R E M I A ( WAT E R D E FI C I E N C Y ) with dilute urine and high urine volume (>3 L daily), whereas
extrarenal water loss is associated with a maximally concen-
Hypernatremia (Figure 38.2) occurs in the following settings:
trated urine (>900 mOsm/kg) and urine output is usually low
normal (<1.01.5 L daily).
1. Decreased oral water intake (insufficient water provision
Renal water wasting can be confirmed by determining ran-
or impairment of central nervous system thirst response
dom urine sodium and potassium concentrations. Renal water
2. Increased renal water loss (diabetes insipidus [DI] or wasting is signified if the sum of the urinary sodium and uri-
diuretic or aquaretic medications), GI water loss (osmotic nary potassium concentrations is less than the serum sodium
diarrhea), or insensible water loss (sweat and respiration) concentration. Investigations for osmotic diuresis and diabe-
tes insipidus are indicated.
3. Hypertonic sodiumcontaining fluid administration
(intravenous administration of concentrated sodium
Hypernatremia occurs in the setting of 1) decreased oral
bicarbonate solution)
water intake; 2) increased renal water loss, GI water loss, or
insensible water loss; or 3) hypertonic sodiumcontaining
There is almost always a degree of overlap in excessive
fluid administration.
water loss and insufficient water intake. Hypernatremia occurs
mostly in the elderly and infants and increases mortality
among hospitalized patients.
O S MOT I C D IU R E S I S
Patients with osmotic diuresis may present with polyuria and
Diagnosis
hypernatremia. The osmolality of their urine is typically nearly
Unlike hyponatremia, for which confirmation of hypo- isotonic to the plasma osmolality. Osmotic diuresis can be con-
osmolality is necessary, hypernatremia is always associated with firmed by calculating the total daily solute excretion. Normal
hyperosmolality; hence, there is no need to measure serum solute excretion for an adult is approximately 700 to 1,000
osmolality. mOsm daily (or about 10 mOsm/kg daily). If solute excretion
Urine osmolality and volume help differentiate renal from in a 24-hour urine sample is greater than normal, the presence
extrarenal water loss. Renal water wasting is typically associated of osmotic diuresis is confirmed.
3 8. AC I D B A S E A N D E L E C T R O LY T E D I S O R D E R S 543
D I A B ET E S I NS I P I D US Nephrogenic DI is due to a partial or complete
unresponsiveness of the renal tubular cells to AVP.
DI can be classified into 2 major types: central DI and neph-
rogenic DI. Central DI is due to insufficiency or absence of
endogenous AVP. Nephrogenic DI is due to a partial or com-
D I S O R D E R S O F P OTA S S I U M B A L A N C E
plete unresponsiveness of the renal tubular cells to AVP.
Nephrogenic DI can be caused by genetic disorders, but
more commonly it is caused by various acquired conditions. HYPOKALEMIA
Lithium, demeclocycline, and amphotericin B are well-known
Hypokalemia can be associated with pseudohypokalemia,
drugs that can cause renal concentration defect and nephro-
transcellular shift, inadequate intake or GI loss, and renal
genic DI.
loss. Hypokalemia (excluding pseudohypokalemia) can cause
In addition, a rare type of gestational DI exists. It occurs in
cellular hyperpolarization. Manifestations of hypokalemia
approximately 1 of every 300,000 pregnancies and is caused
include electrocardiographic (ECG) changes (blunted T wave
by placental production of vasopressinase, which degrades
and appearance of U wave), muscle weakness, ileus, polyuria
endogenous AVP and results in DI.
(functional nephrogenic DI), and, in severe cases, rhabdomy-
olysis and asystole.
Diagnosis
DI is diagnosed with a water deprivation study, during which Diagnosis
the combination of high serum sodium concentration (>145 Pseudohypokalemia due to active cellular potassium uptake in
mEq/L) and low urine osmolality (<150 mOsm/kg) consti- the test tube (leukocytosis or leukemia) should be ruled out
tutes a positive result and is diagnostic for DI. when appropriate. If the plasma is immediately separated from
If patients present with both hypernatremia (>145 mEq/L) the blood sample, this error can be avoided.
and dilute urine (<150 mOsm/kg) without receiving any Hypokalemia caused by transcellular shift is typically tran-
aquaretic medications, those findings are sufficient to establish sient. Pertinent clinical history provides key diagnostic clues,
a diagnosis of DI. A water deprivation study is not necessary. especially for rare hereditary types of hypokalemic paralysis.
After a diagnosis of DI is made, intranasal or intravenous As shown in Figure 38.3, quantifying urinary potassium is
desmopressin may be administered to differentiate central a key step in delineating the underlying (GI or renal) causes of
DI from nephrogenic DI. Desmopressin should be adminis- hypokalemia.
tered only when the serum sodium concentration is greater
than 145 mEq/L. Central DI is diagnosed if the urine osmo-
lality increases in response to desmopressin. Nephrogenic DI Therapy
is diagnosed if there is no change in urine osmolality with Potassium repletion can be achieved with oral or intravenous
desmopressin. supplementation. Intravenous potassium infusion is indicated
DI-associated polyuria should be differentiated from psy- for patients who have severe symptomatic hypokalemia or
chogenic polydipsia. The serum sodium concentration helps who lack GI access. Intravenous potassium should be given
with the differentiation. In patients with psychogenic poly- in a saline-based solution rather than a dextrose-containing
dipsia, polyuria is driven by excessive water intake; thus, serum solution because sugar stimulates insulin secretion, shifting
sodium concentration is typically in the lower end of the refer- potassium intracellularly and exacerbating hypokalemia. A
ence range (<140 mEq/L). Patients with DI, however, typi- central line is preferred for the infusion since potassium can
cally have serum sodium concentrations that are in the upper be corrosive to peripheral vessels. The rate of potassium infu-
end of the reference range (>140 mEq/L) or elevated. sion should not exceed 10 mEq hourly.
544 N E P H R O L O GY
Hypokalemia
Figure 38.3 Diagnosis of Hypokalemia. GI indicates gastrointestinal tract; HCO3, bicarbonate; HTN, hypertension; K+, potassium; Na+, sodium;
RTA, renal tubular acidosis.
with widened QRS), and muscle weakness or frank paralysis. the circulation. Hyperosmolality (hyperglycemia or
These manifestations may occur when the serum potassium administration of osmotically active solutions) can
concentration exceeds 6.5 to 7.0 mEq/L. Severe hyperkalemia shift intracellular potassium out to the extracellular
can cause lethal cardiac arrhythmia (sine wave or complete compartments through solvent drag.
absence of electrical activitycardiac standstill), although a
Hyperkalemia due to impaired potassium excretion
clear correlation between the ECG changes and serum potas-
from the collecting duct cells is common in patients
sium concentration has not been established.
with urinary outlet obstruction (eg, benign prostatic
hypertrophy).
Diagnosis Other conditions that can cause hyperkalemia include
Rule out pseudohyperkalemia due to cell lysis during hyporeninemic hypoaldosteronism and medications
or after blood sampling from using a small needle and such as potassium-sparing diuretics, nonsteroidal
inadequate technique. Use of a needle of appropriate size anti-inflammatory drugs, calcineurin inhibitors,
and optimal technique can mitigate the problem. angiotensin-converting enzyme inhibitors, angiotensin
receptor blockers, and heparin.
Impaired excretion of renal potassium occurs primarily
in patients with kidney failure and is a major cause of
persistent hyperkalemia. Therapy
Hyperkalemia caused by increased intake of potassium Therapy is dictated by the severity and underlying causes of
is seen typically in patients with some degree of kidney hyperkalemia. For patients with ECG changes, urgent intra-
dysfunction. venous administration of calcium is indicated to stabilize
the myocardium. Simultaneously, intravenous insulin, dex-
Cellular breakdown (rhabdomyolysis and tumor lysis trose solution (5% or 10%), and inhaled -agonist should
syndrome) can acutely release cellular potassium into be administered to promote an intracellular potassium shift.
3 8. AC I D B A S E A N D E L E C T R O LY T E D I S O R D E R S 545
Hyperkalemia
Figure 38.4 Diagnosis of Hyperkalemia. ACEI indicates angiotensin-converting enzyme inhibitor; GFR, glomerular filtration rate; K+, potassium;
NSAID, nonsteroidal anti-inflammatory drug; RBC, red blood cell; SLE, systemic lupus erythematosus.
Box 38.1 EXAMPLE OF ACIDBASE DETERMINATION 1. Winter formula: Expected Pco2 = (1.5 HCO3) + 8 2.
For this patient, expected Pco2 = 23 2 mm Hg. This
Patient: A 37-year-old woman with a history of Sjgren syn- formula is used when the patients serum HCO3 is in the
drome and hypothyroidism was admitted for shortness of breath. acidemic range (<20 mEq/L).
Evaluation showed significant electrolyte and acidbase imbalance.
Physical examination findings were unremarkable except for mild 2. Rule of +15: Expected Pco2 = HCO3 + 15. The value (25
tachypnea. Laboratory test results were the following: sodium 134 for this patient) should equal the last 2 digits of the pH if
mEq/L, potassium 2.6 mEq/L, chloride 115 mEq/L, bicarbonate the patient has a single acidosis with adequate respiratory
(HCO3) 10 mEq/L, and creatinine 0.6 mg/dL. Arterial blood gas compensation. The rule of +15 is relatively simple and appli-
results were pH 7.25 and Pco2 25 mm Hg. cable when the HCO3 ranges between 10 and 40 mEq/L.
Question: What is the patients acidbase status? On the basis of the calculation, this patient has a pure nonanion
gap acidosis with appropriate compensation.
Answer: With the Henderson-Hasselbalch equation, first look
at the blood pH. The patients blood pH is decreased, indicating
acidemia. Next identify which of the 2 variables (Pco2 or HCO3)
decreases like the blood pH. Her serum HCO3 is decreased, like
When appropriate, nonpotassium-sparing diuretics and
the blood pH (low HCO3 and low blood pH), indicating meta-
potassium-exchange resin (sodium polystyrene) may be used
bolic acidosis. Then look at whether the patient has an appropri-
to promote renal and GI potassium excretion. For asymptom-
ate degree of compensation, which indicates a singular metabolic
atic patients with mild to moderate hyperkalemia (<6 mEq/L),
acidosis without any other primary abnormality. If the compensa-
dietary potassium restriction, nonpotassium-sparing diuret-
tion is much more or much less than expected, there is likely a sec-
ics, and potassium-exchange resin may suffice. For patients
ond, primary respiratory abnormality. For example, if the Pco2 is
with advanced renal failure or hyperkalemia that is refractory
lower than the expected compensation, there is a primary respira-
to conservative measures, dialysis is necessary.
tory alkalosis in addition to a primary metabolic acidosis; a Pco2
While the above measures mitigate hyperkalemia,
higher than expected indicates the existence of an additional pri-
steps should be taken to correct the underlying causes.
mary respiratory acidosis.
Correcting a urinary tract obstruction can lead to kaliuresis.
One of 2 methods is used to determine the expected respira-
Medication-induced hyperkalemia should be corrected by
tory compensation (Pco2):
adjusting the medication regimen.
546 N E P H R O L O GY
Hyperkalemia can be associated with pseudohyperkalemia, N O NA N I O N G A P AC I D O S I S
excessive potassium intake, transcellular shift, and impaired
Metabolic acidoses, defined as a primary decrease in serum
secretion of renal potassium.
HCO3 and a compensatory reduction in Pco2, are classified
Therapy is dictated by the severity and underlying causes of as normal anion gap (nonanion gap) and increased anion
hyperkalemia. gap acidoses. Nonanion gap acidosis may be caused by
renal tubular acidosis (RTA) (renal hydrogen ion retention
or HCO3 wasting or both), diarrhea (GI HCO3 wasting),
AC I D B A S E D I S O R D E R S early-stage chronic kidney failure (low serum HCO3 associ-
ated with serum creatinine elevation), ureterosigmoid fistula
(enteric chloric-HCO3 exchange), and certain medications,
D ET E R M I NAT I O N O F AC I D BA S E S TAT US such as carbonic anhydrase inhibitors (eg, acetazolamide).
Examination of acidbase status should begin with the
Henderson-Hasselbalch equation:
Renal Tubular Acidoses
[ A-]
pH = pKa + log , There are 3 main types of RTA (Table 38.1):
[HA]
1. Type 1distal tubular acidosis due to defects in hydrogen
where pKa is the negative logarithm of the acid dissocia-
ion excretion in the collecting duct
tion constant and A is the concentration of the ionized form
of the acid HA. Blood pH is derived from the ratio of 2 vari- 2. Type 2proximal tubular acidosis due to defects in
ables, serum bicarbonate (HCO3) (base) and Pco2 (acid). proximal tubular HCO3 reclamation
Under conditions in which 1 of these variables increases or
3. Type 4hyporeninemic hypoaldosteronism
decreases, the other variable predictably and compensatorily
also increases or decreases and minimizes the change in the Nonanion gap acidosis may be caused by RTA, diarrhea,
ratio, hence minimizing blood pH alterations. An example early-stage chronic kidney failure, ureterosigmoid
of acidbase determination with the Winter formula and the fistula, and certain medications (eg, carbonic anhydrase
rule of +15 is shown in Box 38.1. inhibitors).
TYPE 4: HYPORENINEMIC
FEATURE TYPE 1: DISTAL TYPE 2: PROXIMAL HYPOALDOSTERONISM
Defect H+ excretion in distal tubule HCO3 reabsorption in proximal tubule Low renin, low aldosterone
Etiology & clinical setting Acquired: connective tissue Acquired: dysproteinemia (MM), DM, mild to moderate CKD
diseases, interstitial renal interstitial renal diseases (less
diseases frequently), lead or mercury toxicity
Drug: Amphotericin B Drug: ifosfamide
Hereditary: rare Hereditary: glycogen storage disease,
hereditary fructose intolerance,
mitochondrial diseases, cystinosis,
Wilson disease
Urine pH Always high (>5.3) Low (when HCO3 < Tm) Variable
Alkali treatment Small requirement Large requirement; treat the cause Small requirement
FE-HCO3 <5% Can be high with alkali treatment Variable
Abbreviations: CKD, chronic kidney disease; DM, diabetes mellitus; FE, fractional excretion; H+, hydrogen ion; HCO3, bicarbonate; MM, multiple myeloma; Tm,
tubular transport maximum.
3 8. AC I D B A S E A N D E L E C T R O LY T E D I S O R D E R S 547
Table 38.2 METABOLIC ALKALOSIS
DIAGNOSTIC FEATURES IN
ADDITION TO METABOLIC
CAUSES PATHOPHYSIOLOGY ALKALOSIS THERAPY
Vomiting & gastric secretions Net acid loss p or normal BP Normal saline
Enhanced renal proximal tubular Low urinary chloride (<20 mEq/L)
HCO3 absorption
Exogenous alkali intake (CaHCO3 & Analogous to milk alkaline Hypercalcemia Discontinue alkaline intake
NaHCO3) syndrome Usually in patients with CKD
Posthypercapnic state Net loss of carbonic acid Mechanical ventilation in patients p Ventilation
with severe COPD
Bartter syndrome Autosomal recessive inheritance Neonatal or childhood onset Sodium and potassium
with 5 types of genetic defects p BP repletion
Hypokalemia
Hypercalciuria
High urinary chloride (>20 mEq/L)
Gitelman syndrome Autosomal recessive inheritance Adolescence or adulthood onset Sodium and potassium
Mutations in distal p or normal BP repletion
sodium-chloride Hypokalemia
cotransporters Hypocalciuria
High urinary chloride (>20 mEq/L)
Abbreviations: p, decreased; n, increased; BP, blood pressure; CaHCO3, calcium bicarbonate; CKD, chronic kidney disease; COPD, chronic obstructive pulmonary
disease; H+, hydrogen ion; HCO3, bicarbonate; NaHCO3, sodium bicarbonate.
A N I O N G A P AC I D O S I S
and ingestion of toxic acids from toxic alcohol or drugs (eg,
salicylate).
Anion gap metabolic acidoses can be grouped according In recent years, several new anion gapgenerating acids
to underexcretion and overgeneration of nonvolatile acids. have been added to the list as causes of anion gap metabolic
Underexcretion occurs mainly in patients with renal failure acidosis. Accordingly, the new mnemonic for the major causes
in which nonvolatile acids from regular metabolism can- of anion gap metabolic acidosis is GOLDMARK: glycerose
not be excreted. Overgeneration is related to excessive gen- (ethylene and propylene), oxoproline, l-lactate, d-lactate,
eration of nonvolatile acid, as in lactic acidosis, ketoacidosis, methanol, aspirin, renal failure, and ketoacidosis.
548 N E P H R O L O GY
l-lactic acidoses can be subdivided into type A and type Box 38.2 RESPIRATORY ACIDBASE ALTERATIONS
B lactic acidoses. Type A lactic acidosis develops with tissue
hypoxia, as in shock, severe anemia, and hypoxia from pul- Causes of respiratory acidosis
monary diseases. Type B lactic acidosis refers to conditions of CNS respiratory depression
mitochondrial oxidative impairment, including MELAS syn- Injury: trauma, infarct, hemorrhage, tumor
drome, cyanide intoxication, and use of certain medications Drugs: opiates, sedatives, anesthetics
(metformin, linezolid, and reverse transcriptase inhibitors). Hypoventilation of obesity (eg, pickwickian syndrome)
d-lactic acidosis mainly occurs in patients with short gut Cerebral hypoxia
syndrome and overgrowth of gut bacteria. The bacteria gener- Nerve or muscle
ate d-lactate, which causes anion gap acidosis. Notably, most Guillain-Barr syndrome, myasthenia gravis, various
clinical laboratories test for only l-lactate. Therefore, when myopathies
d-lactic acidosis is suspected, measurement of d-lactate must Diaphragmatic factors: paralysis or splinting, muscle relaxants
be requested specifically. Toxins (eg, organophosphates, snake venom)
Chest wall airway lung
Diagnosis and Therapy Airway: upper and lower airway obstruction
Chest wall trauma: flail chest, contusion, hemothorax,
In most cases, clinical scenarios will reveal the cause of acidosis. pneumothorax
In addition to its use for acidbase disturbances, the osmolal gap Lung: pulmonary edema, ARDS, aspiration
should be calculated when toxic alcohol ingestion is suspected. Carbon dioxide excess
The toxic alcohols (especially methanol and ethylene glycol) are Hypercatabolic states: malignant hyperthermia
osmotically active molecules. Before their conversion to toxic Addition of CO2 to inspired gas
acids, the alcohols generate an osmolal gap (measured serum Insufflation of CO2 into body cavity (eg, for laparoscopic
osmolality is greater than the calculated serum osmolality by more surgery)
than 10 mOsm/kg). When the osmolal gap is elevated, treatment Causes of respiratory alkalosis
should be instituted immediately to block the toxic alcohols (par- CNS respiratory stimulation
ent compounds) from being metabolized. Inhibitors of alcohol Pain, hyperventilation syndrome, anxiety, psychosis, infec-
dehydrogenase (eg, 4-methylpyrazole) effectively block alcohol tion, trauma, cerebrovascular accident
metallization. In severe cases, hemodialysis is necessary. Hypoxia
Salicylate intoxication in adults typically causes anion gap High altitude, severe anemia, right-to-left shunts
acidosis and respiratory alkalosis. Anion gap acidosis is caused Drugs
by salicylic acid, its metabolites, and lactate; respiratory alka- Progesterone, methylxanthines, salicylates, catecholamines,
losis is caused by stimulation of the central nervous system nicotine
respiratory center. Endocrine conditions
Progesterone (pregnancy)
Anion gap metabolic acidoses can be grouped according to Pulmonary conditions
underexcretion and overgeneration of nonvolatile acids. Pneumonia, edema, embolism, asthma
A mnemonic for the major causes of anion gap metabolic Miscellaneous
acidosis is GOLDMARK: glycerose (ethylene and Sepsis, hepatic failure, recovery phase of metabolic acidosis
propylene), oxoproline, l-lactate, d-lactate, methanol, Abbreviations: ARDS, acute respiratory distress syndrome; CNS, central ner-
aspirin, renal failure, and ketoacidosis. vous system; CO2, carbon dioxide.
3 8. AC I D B A S E A N D E L E C T R O LY T E D I S O R D E R S 549
is regulated by the ventilatory system. The key components of serum HCO3. Respiratory alkalosis features an increase in
the ventilatory system include the respiratory center in the cen- blood pH, a decrease in Pco2, and a compensatory decrease
tral nervous system, the chest wall (ribs, nerves, and muscles), in serum HCO3. Therapy for respiratory acidbase alterations
and lung parenchyma. Central nervous system respiratory is directed to the specific causes.
drive can be affected by medications, hormones (progester-
one during pregnancy), and toxins (in patients with hepatic Respiratory acidosis is characterized by a decrease in blood
failure, uremia, or sepsis); chest wall function can be affected pH, an increase in Pco2, and a compensatory increase in
by neuromuscular diseases, paralysis, and trauma (flail chest); serum HCO3.
and lung parenchyma can be affected by infection, edema as in
acute respiratory distress syndrome, and chronic obstructive Respiratory alkalosis features an increase in blood pH, a
pulmonary disease. decrease in Pco2, and a compensatory decrease in serum
Causes of respiratory acidbase alterations and expected HCO3.
metabolic compensations for acute and chronic respiratory
acidbase alterations are summarized in Box 38.2.
S U M M A RY
Diagnosis and Therapy
In this chapter, fluid, electrolyte, and acidbase disorders
Respiratory acidosis is characterized by a decrease in blood were defined. Additionally, treatments for fluid, electrolyte,
pH, an increase in Pco2, and a compensatory increase in and acidbase disorders were explored.
550 N E P H R O L O GY
39.
ACUTE KIDNEY INJURY, GLOMERULAR DISEASE, AND
TUBULOINTER STITIAL DISEASE
Suzanne M. Norby, MD, Kianoush B. Kashani, MD, and Fernando C. Fervenza, MD, PhD
551
Table 39.1 CLASSIFICATION AND STAGING SYSTEM P R E R E NA L A K I
FOR ACUTE KIDNEY INJURY
Prerenal AKI is defined as decreased GFR due to decreased
SERUM CREATININE renal perfusion without ischemic injury to tubules, resulting
STAGE CONCENTRATION URINE OUTPUT from volume depletion, low cardiac output, drugs, or periph-
eral vasodilation (eg, sepsis). It is characterized by 1) increased
1 Increase of 0.3 mg/dL <0.5 mL/kg per hour for
or >6 h
reabsorption of sodium and water leading to concentrated
Increase to 150%-200% urine, 2) increased reabsorption of urea resulting in elevation
from baseline of SUN out of proportion to creatinine (>20:1), and 3) revers-
ibility within 3 to 4 days if the underlying cause is treated.
2 Increase to >200%-300% <0.5 mL/kg per hour for
from baseline >12 h
One cause of prerenal AKI is intravascular volume deple-
tion from external loss of fluids and electrolytes (vomiting,
3 Increase to >300% from <0.3 mL/kg per hour for diarrhea, and dehydration), loss of plasma volume (burns),
baseline 24 h or anuria for 12 h internal fluid losses (third spacing, as occurs in severe pan-
or
Concentration 4.0
creatitis), and hemorrhage. Physical findings of volume
mg/dL, with a recent depletion include orthostatic hypotension, dry mucous
increase of 0.5 mg/dL membranes, and decreased skin turgor. Management involves
or administration of oral liquids or intravenous fluids, such as
Need for renal replace- normal saline, albumin, or blood, depending on the clinical
ment therapy
situation.
A second cause of prerenal AKI is volume overload or
Adapted from Mehta RL, Kellum JA, Shah SV, Molitoris BA, Ronco C, Warnock decreased cardiac output (or both) as occurs in conges-
DG, et al; Acute Kidney Injury Network. Acute Kidney Injury Network:
report of an initiative to improve outcomes in acute kidney injury. Crit Care. tive heart failure (cardiorenal syndrome). Physical findings
2007;11(2):R31. This article is online at: http://ccforum.com/content/11/2/R31. include elevated jugular venous pressure, bibasilar crackles in
2007 Mehta et al. This is an open access article distributed under the terms of the the lungs, peripheral edema, and a third heart sound gallop.
Creative Commons Attribution License (http://creativecommons.org/licenses/
by/2.0), which permits unrestricted use, distribution, and reproduction in any Management includes optimization of hemodynamics, often
medium, provided the original work is properly cited. with diuretics.
Creatinine increase to 2x
UO <0.5 mL/kg/h
Injury baseline or GFR
x 12 h
decrease by >50%
Creatinine increase to 3x
baseline or creatinine UO <0.3 mL/kg/h
Oliguria
High
Failure value 4 mg/dL (increase x 24 h or
specificity
of 0.5 mg/dL) or GFR anuria x 12 h
decrease by >75%
Figure 39.1 The RIFLE Classification Scheme for Acute Kidney Injury. ARF indicates acute renal failure; GFR, glomerular filtration rate; RIFLE, risk,
injury, failure, loss, and ESRD. (Adapted from Bellomo R, Ronco C, Kellum JA, Mehta RL, Palevsky P; Acute Dialysis Quality Initiative workgroup.
Acute renal failure: definition, outcome measures, animal models, fluid therapy and information technology needs: the Second International
Consensus Conference of the Acute Dialysis Quality Initiative [ADQI] Group. Crit Care. 2004 Aug;8[4]:R20412. Epub 2004 May 24. Critical
Care 2004;8:R204R212. This article is online at: http://ccforum.com/content/8/4/R204. 2004 Bellomo et al. This is an Open Access article:
verbatim copying and redistribution of this article are permitted in all media for any purpose, provided this notice is preserved along with the articles
original URL.)
552 N E P H R O L O GY
A third cause of prerenal AKI is renal artery occlusion. It resulting from volume depletion, low cardiac output,
is characterized by a sudden occlusion (thrombosis, stenosis, drugs, or peripheral vasodilation (eg, sepsis).
emboli, vasculitis of the main renal arteries, or several intrare-
Causes of prerenal AKI include volume overload, renal
nal arteries) of the arteries supplying blood to the kidneys and
artery occlusion, vasoactive drugs, and HRS.
the resultant rapid decline in renal function. If not promptly
addressed, renal artery occlusion causes ischemic acute tubular
necrosis (ATN). I N T R I N S I C R E NA L A K I
Vasoactive drugs can cause intrarenal hemodynamic
changes that decrease renal blood flow, leading to prerenal
Glomerular Disease and Vasculitis
AKI. Nonsteroidal anti-inflammatory drugs (NSAIDs) inhibit Glomerular disease occurring in combination with AKI,
cyclooxygenase and decrease vasodilatory prostaglandin pro- called rapidly progressive glomerulonephritis (GN), and vas-
duction. Patients who take NSAIDs and have underlying renal culitis are discussed later in this chapter in the Glomerular
insufficiency, volume depletion, advanced liver disease, or con- Disease section.
gestive heart failure are at risk of AKI. Angiotensin-converting
enzyme inhibitors (ACEIs) and angiotensin receptor block-
ers (ARBs) increase the risk of AKI when renal blood flow Acute Tubular Necrosis (ATN)
is decreased. These medications interfere with the action of The natural history of ATN depends on its etiology and can be
angiotensin II, which serves to maintain GFR when renal blood caused by ischemia (decrease in oxygen delivery), inflamma-
flow is decreased. If AKI develops while a patient is taking an tion or nephrotoxic injury. Many toxins, both endogenous and
ACEI or ARB, use of these medications should be withheld exogenous, can cause tubular damage. Since hospital-acquired
until renal function improves. Also, the calcineurin inhibitors AKI is usually multifactorial, the timeline of development and
cyclosporine and tacrolimus cause renal vasoconstriction. recovery of ATN is based on the clinical picture. If prerenal
Hepatorenal syndrome (HRS), another cause of prerenal ischemia lasts long enough, tubular damage begins. Extension
AKI, occurs in patients with end-stage liver disease. HRS is a of the injury after reperfusion is usually from the infiltration
functional renal failure induced by intrarenal vasoconstriction of inflammatory cells. The typical course of ischemic ATN
in the setting of circulatory dysfunction with splanchnic vaso- begins with a rapid decrease in urine output, accompanied by
dilation and relatively insufficient cardiac output leading to an increase in the SCr level (Figure 39.2). During the main-
effective hypovolemia. Precipitating events may be worsening tenance phase, oliguria is usually followed by polyuria before
liver function, bleeding, infection (such as spontaneous bacte- tubules regain their concentrating capacity. The longer the
rial peritonitis), and large-volume paracentesis without albu- duration of the oliguric phase before recovery, the smaller the
min replacement. Diagnostic criteria include the following: chance of complete recovery of kidney function. In the recov-
ery phase, the SCr level begins to decrease and urine output
1. Cirrhosis with ascites normalizes.
Contrast-induced nephropathy (CIN) is typically defined
2. SCr >1.5 mg/dL as an increase in SCr of 0.5 mg/dL or 25% within 3 days after
3. No improvement in SCr after 2 days of diuretic administration of a contrast agent if there is no other cause. In
withdrawal and volume expansion with albumin
4. No recent administration of nephrotoxic drugs Pre
100 ren
al
5. Normal findings on renal ultrasonography
A
Glomerular Filtration Rate, %
80
6. Absence of shock
Initiation
y
2 HRS manifests with a more gradual decline in renal function 20 ver
sio
co
C Re
n
554 N E P H R O L O GY
Box 39.1 COMMON CAUSES OF ACUTE INTERSTITIAL hypertension, preexisting CKD, volume depletion, and the
NEPHRITIS use of ACEIs or ARBs. Calcium phosphate precipitation is
promoted by high serum phosphate concentrations that are
Drugs induced rapidly by ingestion of oral sodium phosphatebased
Antibioticspenicillin, methicillin (antitubular basement laxatives. AKI is caused by AIN due to precipitation of cal-
membrane antibodies), ampicillin, rifampin, sulfa drugs, cip- cium phosphate in the renal tubules and interstitium.
rofloxacin, pentamidine The treatment is hydration, and in the majority of cases
NSAIDsinterstitial nephritis with nephrotic syndrome removal of phosphorus is recommended. Seizures and tetany
& renal insufficiency may have a latent period; not may result from severe hypocalcemia, and calcium must be
dose-dependent; recurs; possibly T-cellmediated; allergic replaced cautiously since it may increase the chance of calcium
signs & symptoms are absent phosphate crystal precipitation. Initially, the episode of acute
Diureticsthiazides, furosemide, bumetanide (sulfa phosphate nephropathy may be unrecognized clinically, and
derivatives) it may not be diagnosed until weeks to months later. Renal
Cimetidine biopsy shows acute and chronic tubulointerstitial nephritis
Proton pump inhibitors with tubular and interstitial deposits of calcium phosphate.
Allopurinol, phenytoin, phenindione In the majority of patients, CKD develops after an episode
Cyclosporine of acute phosphate nephropathy; the chance of recovery is
Infections poor.
BacteriaLegionella, Brucella, Streptococcus, Staphylococcus,
Pneumococcus Acute phosphate nephropathy occurs in patients who
VirusEpstein-Barr, CMV, Hantavirus, HIV, hepatitis B, receive oral sodium phosphatebased laxatives.
Polyomavirus
FungusCandida, Histoplasma Acute Uric Acid Nephropathy
ParasitesPlasmodium, Toxoplasma, Schistosoma, Leishmania
Systemic diseases Acute uric acid nephropathy is associated with the tumor
Systemic lupus erythematosus lysis syndrome that develops after chemotherapy, myelo-
Sjgren syndrome proliferative disorders, heat stroke, status epilepticus, and
Sarcoidosis Lesch-Nyhan syndrome. AKI is caused by uric acid crystal
Lymphoma, leukemic infiltration formation in the renal tubular lumens, causing intrarenal
Renal transplant rejection tubular obstruction. This condition is generally completely
Idiopathic reversible. The serum uric acid level is often greater than 15
mg/dL, the 24-hour urinary uric acid is greater than 1,000
Abbreviations: CMV, cytomegalovirus; HIV, human immunodeficiency virus; mg, and the ratio of spot urinary uric acid concentration to
NSAID, nonsteroidal anti-inflammatory drug.
the spot urinary creatinine concentration is often greater
than 1.0. Prevention includes alkaline diuresis, allopurinol,
3. Eosinophiluria (>1% eosinophils)suggestive of AIN and, sometimes, hemodialysis.
but also seen in other unrelated renal diseases
4. Proteinuria that is usually mild (<1 g/1.73 m2 per 24 hours) Crystal Deposition Due to Medications or Toxins
Therapy for AIN is primarily supportive. Identification and Medications that cause crystal deposition include acyclovir,
elimination of inciting factors is important. Treatment with indinavir, sulfonamide, methotrexate (doses >50 mg/kg),
corticosteroids (prednisone 60 mg every other day) for 2 to 4 and triamterene. AKI is caused by renal tubular obstruction
weeks may hasten recovery of renal function and may benefit due to crystal formation in the renal tubular lumens and by
patients who do not regain renal function within 1 week after interstitial inflammation due to deposition in the interstitium.
discontinuing use of the offending agent. Corticosteroids are Crystal deposition is mainly a pH-dependent process, and
not indicated in infection-related AIN. Although AIN has treatment includes adequate hydration, urine alkalinization,
traditionally been considered to be a reversible process, recent and discontinued use of the offending medication. Excessive
studies have shown that impaired renal function can persist oxalate production occurs following ethylene glycol ingestion.
long-term in up to 40% of patients. Precipitation of calcium oxalate crystals contributes to AKI,
which is also mediated by direct tubular toxicity of glycolate,
Therapy for AIN is primarily supportive. Identification and another ethylene glycol metabolite. Treatment consists of urine
elimination of inciting factors is important. alkalinization, administration of the alcohol dehydrogenase
inhibitor fomepizole, and hemodialysis.
Acute Phosphate Nephropathy
Crystal deposition due to medications or toxins
Acute phosphate nephropathy cccurs in patients who receive causes AKI by renal tubular obstruction due to crystal
oral sodium phosphatebased laxatives, commonly when pre- formation in the renal tubular lumens and by interstitial
paring for colonoscopy. The main risk factors are older age, inflammation due to deposition in the interstitium.
556 N E P H R O L O GY
Table 39.3 USE OF ULTRASONOGRAPHY IN ACUTE component to the AKI by closely monitoring fluid intake,
KIDNEY INJURY urine output, and renal function. Replacing two-thirds
of the postobstructive diuresis volume is indicated if SCr
ULTRASONOGRAPHIC FINDING DIAGNOSIS
increases after relief of the obstruction.
Shrunken kidneys Chronic kidney disease 4. Avoid the use of nephrotoxic medications and intravenous
Normal-sized kidneys contrast media.
Echogenic Acute glomerulonephritis
Acute tubular necrosis 5. Identify medications that affect renal blood flow (ACEIs,
Normal Prerenal ARBs, cyclosporine, tacrolimus, cyclooxygenase 2 inhibitors,
Acute renal artery occlusion and NSAIDs) and withhold their use or carefully monitor
changes in renal function while they are being used.
Enlarged kidneys Malignancy
Renal vein thrombosis 6. Adjust dosages of medications eliminated by the kidneys
Diabetic nephropathy as renal function changes. Monitor drug levels when
Human immunodeficiency virus
indicated.
Hydronephrosis Obstructive nephropathy
7. Maintain nutritional requirements. Patients who are
seriously ill are usually catabolic. Adjust the patients
Adapted from Lameire N, Van Biesen W, Vanholder R. Epidemiology, clinical
evaluation, and prevention of acute renal failure. In: Feehally J, Floege J, Johnson diet to limit potassium, sodium, phosphorus, and fluid
RJ, editors. Comprehensive clinical nephrology. 3rd ed. Philadelphia (PA): Mosby intake. If serum phosphorus levels increase despite dietary
Elsevier; c2007. p. 77185. Used with permission. phosphorus restriction, phosphate binders should be
administered with meals.
cell casts are sometimes seen with AIN. Dysmorphic RBCs
and RBC casts indicate GN. With severe glomerular inflam-
The therapeutic approach to patients with AKI is mostly
mation, leukocytes and leukocyte casts may also be seen. RBCs
supportive.
that are not dysmorphic can be a clue to obstruction related to
genitourinary cancer or urolithiasis.
Notably, diuretic use causes an increase in FENa, even in
prerenal azotemia, since loop and thiazide diuretics act by Renal Replacement Therapy
increasing the urinary excretion of sodium. The fractional The goals for RRT in AKI are the following:
excretion of urea is not altered by diuretics; as a result, an
FENa of less than 35% indicates a prerenal state. 1. Maintain fluid, electrolyte, acid-base, and solute balance
2. Prevent further insult and promote healing
Imaging
3. Permit the use of other support measures, such as
Ultrasonography can be helpful in differentiating between the intravenous medications and parenteral nutrition
causes of AKI (Table 39.3). In postrenal AKI, ultrasonogra-
phy is the test of choice to determine whether hydronephrosis RRT should be considered for patients who have fluid over-
is present, although it may not detect early obstruction. To load unresponsive to diuretics, severe electrolyte disorders
improve the ability to detect the presence of obstruction and (typically hyperkalemia with electrocardiographic changes),
also to determine its cause, noncontrast computed tomogra- severe acid-base disorders, and uremic symptoms (metabolic
phy may be used in combination with ultrasonography. encephalopathy or other evidence of nervous system toxicity,
pericarditis and bleeding believed to be due to uremic platelet
M A NAG E M E N T O F A K I dysfunction).
The choice of RRT must be customized to the needs of the
The therapeutic approach to patients with AKI is mostly sup- patient:
portive. Determining and managing the risk factors are essen-
tial steps to decrease the extent of the injury. Management
1. Conventional intermittent hemodialysis with high-
should include the following:
or low-flux membranesThis treatment is used for
severe metabolic abnormalities (eg, hyperkalemia with
1. Avoid intravascular volume depletion. electrocardiographic changes and severe acidosis) that
2. Optimize cardiac function. While use of diuretics to require rapid, immediate correction for a short period.
maintain urine output does not expedite renal recovery, Hemodynamically stable patients who can tolerate rapid
diuretics help with volume management in some patients fluid and electrolyte shifts can undergo conventional
with AKI. Low-dose dopamine is not considered intermittent dialysis.
beneficial. 2. Continuous RRTContinuous RRT is used for severely
3. Relieve urinary obstruction, which may be followed by ill and catabolic patients who require intravenous fluids
polyuria. Therapy is aimed at preventing a new prerenal and nutrition, continuous or frequent intravenous
558 N E P H R O L O GY
G L O M E RU L A R D I S E A S E M A N I FE S T I N G WIT H IgAN is a mesangial proliferative GN characterized
N E P H R I T I C S Y N D RO M E by diffuse deposition of IgA in the mesangium of
glomeruli.
Postinfectious GN
IgAN is the most common glomerulopathy worldwide.
Classically, poststreptococcal GN develops after pharyngi-
tis (13 weeks) or skin infection (24 weeks) due to specific
(nephritogenic) strains of group A -hemolytic streptococci.
Cultures are usually negative. Titers for antistreptolysin O
Henoch-Schnlein Purpura
(ASO) and antideoxyribonuclease B (anti-DNAse B) may pro- Henoch-Schnlein purpura is a systemic form of IgAN.
vide evidence of recent streptococcal infection. Postinfectious Patients usually present with microscopic or gross hematuria
GN can occur after other infections, such as staphylococcal, (or both), RBC casts, purpura, and abdominal pain. Generally,
meningococcal, and pneumococcal infections; bacterial endo- the prognosis is good for children and variable for adults. In
carditis; and infections of ventriculoatrial shunts. patients with normal renal function, treatment is supportive
A typical manifestation is the abrupt onset of nephritic only. Patients with progressive renal failure should be con-
syndrome with active urinary sediment and proteinuria that sidered for treatment with high-dose corticosteroids with or
is usually less than 3 g/1.73 m2 per 24 hours. Treatment is without cytotoxic medication.
supportive with appropriate antibiotic therapy for persistent
infections and for persons who are contacts (to prevent new
cases). In adults, microscopic hematuria, proteinuria, hyper- Membranoproliferative GN
tension, and renal dysfunction may persist for years. Clinical presentations of all forms of membranoproliferative
GN (MPGN) are variable and include nephrotic and nephritic
features. Approximately one-third of patients present with
IgA Nephropathy
a combination of asymptomatic hematuria and proteinuria.
IgA nephropathy (IgAN) is a mesangial proliferative GN Another third present with nephrotic syndrome and pre-
characterized by diffuse deposition of IgA in the mesangium served renal function. Some patients (10%-20%) present with
of glomeruli. It is the most common glomerulopathy world- nephritic syndrome. Hypertension is common (50%-80%
wide, with an incidence approaching 1:100 in some countries of patients). The prognosis is worse with hypertension, poor
(eg, Japan). renal function, and proteinuria greater than 3 g/1.73 m2 per 24
Patients are typically young adults in the second and hours. There are 2 main types of MPGN: type I and type II.
third decades of life who present with episodic macroscopic In adults with MPGN type I, secondary forms associated
hematuria, often accompanying an upper respiratory tract with the following conditions tend to predominate: monoclo-
infection (synpharyngitic hematuria). The majority of nal gammopathies, cryoglobulinemia in patients with hepatitis
patients are asymptomatic, and the disease may be identified C virus infection, hepatitis B virus infection, subacute bacterial
when microscopic hematuria, with or without proteinuria, endocarditis, infections of shunts used to manage hydroceph-
is found on routine urinalysis. Proteinuria is common, but alus, malaria, SLE, sickle cell disease, 1-antitrypsin deficiency,
nephrotic syndrome occurs in less than 10% of all patients. and recently described abnormalities in the alternative path-
Patients with nephrotic syndrome may have minimal change way of complement activation (C3 glomerulopathy). Levels
nephropathy (MCN) superimposed on IgAN or another of C3, C4, and total hemolytic complement (CH50) may be
glomerulopathy. low in cases of MPGN type I secondary to activation of the
Patients who are normotensive and have proteinuria less classical complement pathway, whereas cases due to activation
than 500 mg/1.73 m2 per 24 hours and normal renal func- of the alternative pathway of complement activation will have
tion at presentation usually have a good long-term prognosis. low C3 but normal C4. Management includes treatment of
However, in 20% to 40% of patients, the disease progresses the underlying cause. Corticosteroids, with or without cyclo-
to end-stage renal disease (ESRD) within 10 to 25 years. phosphamide, may be used in idiopathic MPGN type I with
Progression to ESRD in patients at high risk has been shown nephrotic syndrome or rapidly progressive GN.
to be slowed by angiotensin II blockade (with ACEIs or ARBs The pathogenesis of MPGN type II involves abnormali-
or both) and administration of high doses of corticosteroids. ties of factors comprising the alternate pathway of comple-
The use of fish oil to prevent progression of IgAN is contro- ment activation, or antibodies to those factors, resulting in
versial. Persistent proteinuria of more than 1 g/1.73 m2 per 24 persistent breakdown of C3. Low levels of C3 and normal
hours, uncontrolled hypertension, impaired renal function at levels of C4 are present. MPGN type II is associated with
diagnosis, and glomerular or interstitial fibrosis identified in monoclonal gammopathies, partial lipodystrophy, and macu-
renal biopsy specimens are the most important predictors of lar degeneration. Management of MPGN type II involves
a poor outcome. Patients with IgAN and concomitant MCN plasma exchange. Pulse intravenous corticosteroids followed
typically respond to corticosteroid therapy. For patients with by tapered administration of prednisone may be considered in
rapidly progressive renal failure due to crescentic IgAN, a patients who present with a rapidly progressive course.
regimen of corticosteroids and cyclophosphamide, with the
addition of plasma exchange or pulse methylprednisolone, has MPGN occurs as a complication of other systemic
been tried with variable results. infectious and inflammatory diseases.
560 N E P H R O L O GY
infection. Diagnosis is made by finding aneurysms on angiog- toxic to glomerular epithelial cells. In some patients, MCN
raphy or nerve biopsy. Treatment of patients who do not have may have a secondary cause, such as viral infections, drugs,
evidence of hepatitis B virus infection includes high-dose tumors, or allergies.
corticosteroids and cyclophosphamide. Patients with hepati- Treatment includes high-dose corticosteroid therapy con-
tis Bassociated PAN should be treated with a short course tinued for 4 to 8 weeks after remission is achieved. In adoles-
of corticosteroids in combination with antiviral therapy and cents and adults, response to therapy is high (>80%), but the
plasma exchange. response is slow and some patients may require up to 16 weeks
of treatment to achieve remission. Of the patients who have
a response to corticosteroid therapy, 25% have a long-term
Anti-GBM AntibodyMediated GN
remission, whereas others have at least 1 relapse. Other immu-
(Goodpasture Disease)
nosuppressive agents are used in patients with frequent relapses
Goodpasture disease is a pulmonary-renal syndrome caused or corticosteroid dependence or resistance. The overall prog-
by circulating anti-GBM antibodies and linear staining seen nosis is excellent, with patients maintaining long-term renal
along the GBM and alveolar basement membrane on immu- function. If there is no response to therapy or if progressive
nofluorescence staining of a renal biopsy specimen. The anti- renal failure develops, an alternative diagnosis (such as focal
body is directed against the 3 chain of type IV collagen. segmental glomerulosclerosis [FSGS]) must be considered.
Approximately 25% to 30% of patients with anti-GBM anti-
bodies are also ANCA-positive. Pulmonary hemorrhage may MCN is defined by the absence of structural glomerular
be absent or not clinically apparent. abnormalities, except for the widespread fusion of
Treatment is with high-dose corticosteroids (oral predni- epithelial cell foot processes seen on electron microscopy,
sone or pulse intravenous methylprednisolone) in combination in a patient with nephrotic syndrome.
with oral cyclophosphamide (23 mg/kg daily up to 200 mg
MCN is the most common cause of nephrotic syndrome in
daily; the dose should be decreased by 25% for patients older
children.
than 55 or with SCr >5 mg/dL) and plasma exchange. Patients
who have 100% circumferential crescents and are receiving
dialysis do not recover renal function and should not be treated
with the immunosuppressive regimen outlined above, except
Focal Segmental Glomerulosclerosis
in the presence of pulmonary hemorrhage. The prognosis for FSGS accounts for about 25% of cases of adult nephrotic syn-
patients depends on the percentage of circumferential crescents drome. It is the most common form of idiopathic nephrotic
of the renal biopsy specimen, the presence of oliguria, and the syndrome in African Americans. FSGS is associated with
need for dialysis. Anti-GBM disease rarely recurs. variations in the apolipoprotein AI gene. Secondary causes
of FSGS include drugs (heroin abuse, pamidronate, anabolic
Goodpasture disease is a pulmonary-renal syndrome caused steroids, and interferon), infection (eg, human immunodefi-
by circulating anti-GBM antibodies and linear staining ciency virus [HIV] and parvovirus), sickle cell disease, obe-
seen along the GBM and alveolar basement membrane on sity, vesicoureteral reflux, unilateral renal agenesis, remnant
immunofluorescence staining of a renal biopsy specimen. kidneys, healed lesions of other inflammatory disorders in
glomeruli, and aging.
Patients with FSGS present with either asymptomatic pro-
G L O M E RU L A R D I S E A S E US UA L LY teinuria or full-blown nephrotic syndrome. Treatment includes
M A N I F E S T I N G A S N E P H ROT I C S Y N D RO M E prolonged (>4 months) high-dose corticosteroid therapy. The
remission rate for nephrotic syndrome is up to 40% to 60%,
Minimal Change Nephropathy
with preservation of long-term renal function. For patients
MCN is defined by the absence of structural glomerular who do not respond to corticosteroids, alternative therapy
abnormalities, except for the widespread fusion of epithelial includes the use of cytotoxic drugs (either alone or in combi-
cell foot processes seen on electron microscopy, in a patient nation with corticosteroids) or a low-dose calcineurin inhibi-
with nephrotic syndrome. It is the most common cause of tor (cyclosporine or tacrolimus). For patients with secondary
nephrotic syndrome in children. The presence of nephrotic forms of FSGS, treatment should target the primary cause, if
syndrome in a child with normal urinalysis results indicates possible. In all patients, treatment with an ACEI or an ARB,
MCN until proved otherwise. Among patients with neph- alone or in combination, may substantially reduce protein-
rotic syndrome, MCN is the cause in 70% to 90% of children uria and prolong renal survival. For patients who have protein
younger than 10 years (although rarely before the first year of excretion of less than 3 g/1.73 m2 per 24 hours, treatment with
life), 50% of adolescents and young adults, and less than 20% an ACEI or angiotensin II receptor antagonist (or both) may
of adults with primary nephrotic syndrome. be sufficient to reduce proteinuria and improve renal survival.
The typical presentation is abrupt onset of nephrotic syn- The prognosis is better for patients with a smaller degree of
drome. Hematuria is unusual. In adults, hypertension and proteinuria and for those who respond to corticosteroids.
renal insufficiency may be present. The pathogenesis of MCN
is unknown and may be a consequence of T-lymphocyte FSGS is the most common form of idiopathic nephrotic
abnormalities, with T cells producing a lymphokine that is syndrome in African Americans.
562 N E P H R O L O GY
Lupus Nephritis proteinuria (frequently massive) but often little edema.
Ultrasonography shows large echogenic kidneys. Renal biopsy
Approximately 25% of patients with SLE have substantial specimens show a collapsing form of FSGS. HIV-AN is more
renal involvement. Renal involvement usually occurs early in common and clinically more severe in African Americans than
the course of the disease and is rarely the sole manifestation in whites. Treatment includes the use of highly active antiret-
of SLE. For patients with severe lupus nephritis (LN) (classi- roviral therapy (HAART), treatment of underlying infections,
fied by renal biopsy showing focal or diffuse proliferative LN), and ACEIs to reduce proteinuria.
the use of a high-dose corticosteroid (either orally or pulse Other types of renal disease can be encountered in
intravenous methylprednisolone) in combination with intra- HIV-infected patients. These include IgAN, MPGN, MCN,
venous cyclophosphamide was the most effective form of MN, postinfectious GN, thrombotic microangiopathy, and a
therapy until recent studies demonstrated that mycopheno- lupus-like and immune complexmediated GN. Intratubular
late mofetil in combination with oral prednisone resulted in obstruction results from crystal precipitation after the admin-
fewer side effects and was as effective as cyclophosphamide istration of sulfadiazine or intravenous acyclovir. Renal calculi
in combination with prednisone. A subtype of membranous or nephropathy (or both) can occur after administration of
LN is characterized by proteinuria, weakly positive or negative indinavir.
antinuclear antibody, and no erythrocyte casts. Initial therapy
is supportive, using ACEIs or ARBs to reduce proteinuria.
Treatment of HIV-AN includes the use of HAART,
Immunosuppressive treatment should be considered for
treatment of underlying infections, and use of ACEIs to
patients who remain nephrotic for more than 6 months.
reduce proteinuria.
Cryoglobulinemic GN Associated With
Hepatitis Infection Thrombotic Microangiopathies
Type II or mixed essential cryoglobulins (Table 39.4) are Thrombotic microangiopathies are characterized by microan-
commonly found in patients with hepatitis C virus infec- giopathic hemolytic anemia and thrombocytopenia; renal
tion. Cryoglobulins contain hepatitis C virus RNA and anti thrombotic microangiopathies have various causes. It is debated
hepatitis C virus IgG, which precipitate in the glomeruli, whether hemolytic uremic syndrome (HUS) and thrombotic
bind complement, activate a cytokine cascade, and trigger an thrombocytopenic purpura (TTP) are distinct disorders,
inflammatory response. Patients may present with proteinuria, although they share a spectrum of common findings and are
microscopic hematuria, nephrotic syndrome, or renal impair- often considered together as HUS-TTP. Features include ane-
ment. Hypertension is common and may be severe, particu- mia with schistocytes on peripheral blood smear, high reticu-
larly with acute nephritic syndrome. Cryoglobulinemic GN is locyte count, elevated levels of indirect bilirubin and lactate
usually associated with low levels of C3 and C4. Cryocrits cor- dehydrogenase, decreased haptoglobin level, and presence of
relate poorly with disease activity, and 30% to 40% of patients urinary hemoglobin without RBCs on microscopy.
do not have detectable cryoglobulins. Combination treatment
with interferon alfa and ribavirin is effective in clearing the Hemolytic Uremic Syndrome
virus from the circulation and results in improvement of pro- The sporadic or diarrhea-associated form (D+HUS)
teinuria and renal function. Relapses after discontinuation of is strongly linked to ingestion of meat or other foods con-
the antiviral therapy are common. Treatment with prednisone, taminated with Escherichia coli O157:H7, which produces a
cytotoxic agents, and plasmapheresis is indicated for patients Shiga-like toxin that binds to a glycolipid receptor on renal
with acute nephritis. The renal prognosis is usually good, with endothelial cells and triggers endothelial damage. The treat-
few patients progressing to ESRD. ment is supportive, and antibiotics should not be used.
The nondiarrhea-associated form (DHUS) occurs in
HIV-Associated Nephropathy association with the use of various medications (oral contra-
ceptives, cyclosporine, tacrolimus, mitomycin C, bleomycin,
HIV-associated nephropathy (HIV-AN) is characterized by ticlopidine, or quinine), antiphospholipid antibody syndrome,
progressive renal insufficiency in patients with nephrotic-range underlying malignancy, or radiotherapy.
II. Mixed cryoglobulins with monoclonal M/G>>G/G Sjgren syndrome, Waldenstrm macroglobulinemia,
immunoglobulins lymphoma, essential cryoglobulinemia
III. Mixed polyclonal immunoglobulins M/G Infection, SLE, vasculitis, neoplasia, essential
cryoglobulinemia
564 N E P H R O L O GY
chloride (eg, after the use of a loop diuretic) in the urine; condi- A NA L G E S I C N E P H RO PAT H Y
tions that reduce flow rates (eg, intravascular depletion and the
Analgesic nephropathy is a slowly progressive chronic inter-
use of NSAIDs); and use of radiocontrast agents.
stitial nephritis due to the long-term consumption of mixed
Treatment of cast nephropathy includes the following:
analgesic preparations, frequently complicated by papillary
necrosis and resulting in bilateral renal atrophy. Renal damage
1. Vigorous hydration with normal saline can develop from the use of acetaminophen in combination
2. Correction of hypercalcemia with aspirin and from long-term use of NSAIDs. Papillary
necrosis may occur. Noncontrast computed tomography
3. Avoidance of nephrotoxic or precipitating agents imaging of the kidneys has become the standard method
4. Alkalinization of the urine to maintain pH >7 for diagnosing analgesic nephropathy. No specific treatment
(possibly beneficial in some patients) is available. Patients with analgesic nephropathy are at an
increased risk of uroepithelial tumors, particularly transitional
5. Plasmapheresis, which quickly removes light chains from cell carcinomas (renal pelvis, ureter, bladder, and proximal
the circulation and should be considered for patients urethra). Tumors frequently occur simultaneously at different
with AKI and high serum levels of free light chains or sites in the urinary tract, and close follow-up with regular uri-
hyperviscosity syndrome nary cytologic examination is recommended.
AKI in multiple myeloma occurs as a result of intraluminal
precipitation of proteinaceous casts (cast nephropathy) and OT H E R C AUS E S
the resulting acute noninflammatory interstitial nephritis
Other causes of chronic tubulointerstitial damage include the
(myeloma kidney).
following:
C YS T I C R E N A L D I S E A S E S U M M A RY
Autosomal dominant polycystic kidney disease (ADPKD) is AKI denotes a rapid deterioration (within hours to
the most common hereditary renal disease. It occurs in both weeks) of kidney function, resulting in the accumulation
males and females and is characterized by multiple, bilateral of nitrogenous metabolites and fluid, electrolyte, and
renal cysts and cysts in other organs (eg, liver, spleen, and pan- acid-base imbalances.
creas). ADPKD is most often associated with mutations in 2
genes that code for interacting proteins found in renal tubular The key diagnostic tests for evaluating AKI are urinalysis
cells and in primary cilia: with microscopy and renal ultrasonography.
Nephritic syndrome is characterized by oliguria, edema,
1. PKD1 gene, localized on chromosome 16p, encodes hypertension, proteinuria (usually <3.5 g/1.73 m2 per 24
polycystin 1 (85%-90% of cases) hours), and an active urinary sediment.
2. PKD2 gene, localized on chromosome 4, encodes Nephrotic syndrome is defined as the presence of urinary
polycystin 2 protein >3.5 g/1.73 m2 per 24 hours, hypoalbuminemia
(<3.0 g/dL), peripheral edema, hypercholesterolemia, and
Diagnosis is made through genetic testing. Additionally, lipiduria.
the diagnosis of ADPKD can be made through renal imag-
ing. Ultrasonographic criteria for diagnosis have been recently IgAN is the most common glomerulopathy worldwide.
revised (age 1539: 3 cysts in 1 or both kidneys; age 4059: MPGN occurs as a complication of other systemic
2 cysts in each kidney; age 60: 4 cysts in each kidney). infectious and inflammatory diseases.
Manifestations of renal involvement can include hyperten-
sion, flank or back pain, macroscopic hematuria, CKD, uri- FSGS is the most common form of idiopathic nephrotic
nary tract infection, and inferior vena cava obstruction. syndrome in African Americans.
Extrarenal manifestations of ADPKD include polycystic
MN is the most common cause of nephrotic syndrome in
liver disease (most common) and intracranial aneurysm (ICA).
white adults.
The incidence of ICA is 5% to 22%, depending on whether
there is a positive family history of ICA. Risk of rupture DN is the most common cause of ESRD in the United States.
566 N E P H R O L O GY
40.
EVALUATION OF KIDNEY FUNCTION AND CHRONIC
KIDNEY DISEASE
Axel Pflueger, MD, PhD
Discuss the definition, causes, and treatment of chronic The kidneys normally maintain a constant extracellular
kidney disease (CKD). environment, secrete multiple hormones, and catabolize
peptide hormones in fasting conditions.
N O R M A L K I D N EY F U N C T I O N
E VA LUAT I O N O F K I D N EY F U N C T I O N
The kidneys normally perform several essential functions:
Kidney function is characterized by GFR and the functional-
1. Maintain a constant extracellular environment, which
ity of the filtering structures of roughly 1 million nephrons in
is required for adequate cell function and is achieved
each kidney. Kidney function is assessed by the estimated and
by excreting numerous metabolic waste products (eg,
measured GFR. The functionality of the filtering structures
urea, creatinine, and uric acid) and by adjusting urinary
is assessed by analysis of the urine (microscopic urine analysis
excretion of water and electrolytes to match net intake
and protein excretion) and by imaging studies of the kidney to
and endogenous production. The kidneys regulate the
determine structural abnormalities.
excretion of water and solutes (eg, sodium, potassium, and
hydrogen) by changing tubular reabsorption or secretion.
E S T I M AT E D G F R
2. Secrete multiple hormones that participate in the
regulation of systemic and renal hemodynamics (eg, renin, The GFR can be estimated by measuring the concentration
angiotensin II, adenosine, prostaglandins, nitric oxide, of molecules in the blood that are primarily filtered by the
endothelin, and bradykinin); red blood cell production glomerulus. Typically, the concentration of serum creatinine
(erythropoietin); and calcium, phosphorus, and bone is measured. In recent years, cystatin C has been used to esti-
metabolism (1,25-dihydroxyvitamin D3). mate GFR.
The initial step in urine formation is the separation of an
3. Catabolize peptide hormones. ultrafiltrate of plasma across the wall of the glomerular cap-
4. Synthesize glucose (gluconeogenesis) in fasting conditions. illary. Fluid movement across the glomerulus is governed by
Starling forces, which are proportional to the permeability of
The kidneys help maintain normal body function and the membrane and to the balance between the hydraulic and
homeostasis by directly interacting with other organ systems, oncotic pressure gradients:
including the cardiovascular, nervous (eg, brain), gastrointesti-
nal tract (eg, liver), blood, pulmonary, and muscular systems. GFR = LpS ( Hydraulic Pressure Oncotic Pressure),
In patients with kidney disease, some or all of these func-
tions may be diminished or entirely absent. As an example, where Lp is the unit permeability (or porosity) of the capil-
patients with nephrogenic diabetes insipidus are less able to lary wall, S is the surface area available for filtration, and is
567
Box 4 0.1 DRUGS THAT CAUSE PSEUDOELEVATION OF The MDRD Study equation has been found to have greater
CREATININE AND SERUM UREA NITROGEN precision and accuracy than the CG formula, but it has not
been validated in children, pregnant women, persons older
Competitive tubular secretion of creatinine than 70 years, and other racial and ethnic groups. Neither
Trimethoprim equation provides accurate results if patients have extreme lev-
Cimetidine els of creatinine (eg, patients with muscle-wasting conditions,
Probenecid very high or low protein intake, an amputaed limb, or large or
Triamterene small body size).
Amiloride
Spironolactone Cystatin C
Interference with laboratory determination of creatinine
Ascorbic acid Cystatin C is a small protein excreted by all human nucleated
Cephalosporins (cefoxitin and cephalothin) cells, and it is filtered solely by the glomerulus. Therefore, it is
Flucytosine less dependent on muscle mass and tubular function and has
Levodopa been shown to provide a more precise estimation of GFR than
Methyldopa creatinine-based estimated GFR. It may eventually replace
Hypercatabolic effect creatinine for estimating GFR.
Corticosteroids
Tetracycline MEASURED GFR
Adapted from Choudhury D, Ahmed Z. Drug-associated renal dysfunction and Clearance of p-aminohippurate is a measure of renal blood
injury. Nat Clin Pract Nephrol. 2006 Feb;2(2):8091. Used with permission.
flow. Orthoiodohippurate is used in renal scans. The clearance
rates of inulin, iothalamate, diethylenetriamine pentaacetic
acid (DTPA), and creatinine are measures of the GFR.
change. The GFR in healthy adults is approximately 9520 Measurements of GFR are typically based on the urinary
mL/min in women and 12025 mL/min in men. concentration of a glomerular-filtered substance (eg, SCr)
divided by its plasma concentration expressed as follows:
568 N E P H R O L O GY
Table 4 0.1 CAUSES OF URINE DISCOLORATION characterize mass lesions (eg, solid or cystic angiomyolipoma)
and to screen for polycystic kidney disease. Ultrasonography
COLOR CAUSE
may also be used to assess for renal vein thrombosis (ie, to
Dark yellow or brown Bilirubin assess for the presence or absence of blood flow), but it is not a
screening test for renal artery stenosis.
Brown-black Homogentisic acid (ochronosis)
Melanin (melanoma)
Metronidazole Computed Tomography
Methyldopa/levodopa
Phenothiazine Computed tomography shows calcification patterns. It is used to
stage neoplasms, help determine the cause of obstruction (without
Red Beets contrast medium), and assess cysts, abscesses, and hematomas.
Rifampin
Porphyria
Hemoglobinuria or myoglobinuria Magnetic Resonance Imaging
Phenazopyridine hydrochloride (Pyridium)
Urates Magnetic resonance imaging may be used to identify adrenal
hemorrhage and assess a mass in patients sensitive to contrast
Blue-green Indomethacin
Amitriptyline dyes. Magnetic resonance angiography is a promising screening
method for renal artery stenosis. Extreme caution should be used
Turbid white Pyuria to ensure that gadolinium-containing contrast material is not
Chylous fistula
Crystalluria
used in patients with stage 4 or 5 CKD, renal and hepatic trans-
plant recipients, patients with severe acute renal insufficiency or
hepatorenal syndrome, and intensive care unit patients.
Urine pH also varies (47.5 pH) and depends on the Nephrogenic systemic fibrosis (also called nephrogenic fibro-
dietary intake in healthy persons. Acidic urine is indicative of a sing dermopathy) has been directly associated with exposure to
high-protein diet, acidosis, and potassium depletion. Alkaline gadolinium-containing contrast material in patients with stage 4
urine is associated with a vegetarian diet, alkalosis (unless or 5 CKD. Nephrogenic systemic fibrosis is a painful skin disease
there is potassium depletion), and urease-producing bacteria. characterized by thickening of the skin that can involve the joints
A urine pH less than 5.5 generally excludes type 1 renal tubu- and significantly limit motion within weeks to months.
lar acidosis. A pH greater than 7 may suggest infection. The National Kidney Foundation recommends that alter-
native imaging techniques be attempted when patients have
an estimated GFR of 30 mL/min per 1.73 m2 or less and that
R E NA L I M AG I N G
if patients need a gadolinium-based contrast material, the low-
Radiography est possible dose should be used. In patients with stage 5 CKD
who are receiving dialysis, a reduced dose of gadolinium-based
Plain radiographs magnify the kidneys 30%. Normal renal size contrast material should be used only if absolutely unavoid-
is 3.5 times the height of vertebra L2 (>11 cm). The left kid- able, and the patients should receive hemodialysis immedi-
ney is up to 1.5 cm longer than the right kidney. An enlarged ately afterward. Patients receiving peritoneal dialysis should
kidney indicates obstruction, infiltration (eg, amyloidosis, leu- not be given gadolinium.
kemia, or diabetes mellitus), acute glomerulonephritis, acute
tubulointerstitial nephropathy, renal vein thrombosis, or poly-
The choice of renal imaging technique is determined by the
cystic kidney disease. Calcifications are associated with stones,
potential disease process being investigated.
tuberculosis, aneurysms, and necrosis of the papillary tips.
Other Tests
Excretory Urography
Arteriography and venography are used to evaluate arterial
Excretory urography provides a detailed definition of the col-
stenosis, aneurysm, fistulas, vasculitis, and mass lesions and to
lecting system and can be used to assess renal size and contour
assess living related donor transplants. Gallium and indium
and to detect and locate calculi. It is also used to assess renal func-
scans are used to evaluate acute interstitial nephritis, abscess,
tion qualitatively. Rapid sequence excretory urography is a poor
pyelonephritis, lymphoma, and leukemia. Diethylenetriamine
screening test for renovascular hypertension. Complications
pentacetic acid (also called pentetic acid or DTPA) and hip-
include a large osmotic load (congestive heart failure) and reac-
puran renal scanning are useful in assessing a transplanted
tions (5% of patients). An iodine load may occur and is a con-
kidney, obstruction (before and after furosemide), and infarct
sideration if the patient has hyperthyroidism.
(presence or absence of blood flow).
Ultrasonography
C H R O N I C K I D N EY D I S E A S E
Ultrasonography is used to measure renal size (>9 cm) and to
screen for obstruction, but the results may be negative early More than 20 million people in the United States have CKD,
in the course of obstruction. Ultrasonography can be used to including 11 million with stage 3 CKD (GFR <60 mL/min
4 0. E VA LUAT I O N O F K I D N EY F U N C T I O N A N D C H R O N I C K I D N EY D I S E A S E 569
Table 4 0.2 CAUSES OF CHRONIC KIDNEY DISEASE renal tubular involvement is greater than glomerular involve-
ment, such as in type 4 renal tubular acidosis. To prevent
CAUSE CASES, %
hyperkalemia, the recommended dietary potassium restric-
Diabetes mellitus 42 tion is 70 mEq daily.
Hypertension 26 Hyperkalemia usually occurs when the GFR is less than 20
Glomerulonephritis 11 mL/min per 1.73 m2.
Other or unknown 20 Hyperkalemia can occur at higher GFRs when renal
tubular involvement is greater than glomerular
involvement, such as in type 4 renal tubular acidosis.
per 1.73 m2) (Table 40.2). The goals of recognizing and treating
CKD are to prevent the morbidity and mortality associated Sodium restriction of 90 mEq daily is recommended to
with the progression of renal dysfunction, delay progression prevent hypertension and fluid overload. In addition, usually
of kidney disease, and allow adequate time to educate the after the patients GFR has decreased to the range of stage 4
patients and their families about the patients kidney disease (GFR 1529 mL/min per 1.73 m2) or stage 5 (GFR <15 mL/
and options for renal replacement therapy (RRT). min per 1.73 m2) disease and urine output has decreased, the
CKD has been categorized into 6 stages (Table 40.3). patient may also require fluid restriction.
When renal function decreases to stage 3 (GFR 3059 mL/ Protein loading can lead to accumulation of acid, phospho-
min per 1.73 m2), the complications of CKD become evident. rus, and uric acid. A protein restriction of 0.8 to 1.0 g/kg daily
These complications include hypertension, cardiovascular may be needed to prevent these complications. The benefits
disease, lipid abnormalities, anemia, metabolic bone disease, of protein restriction must be balanced against the morbid-
and electrolyte disturbances. To prevent the progression of ity and mortality associated with protein malnutrition. If the
CKD, therapy must be directed toward preventing these com- patients protein stores are normal, a protein-restricted diet is
plications and achieving adequate glucose control in diabetic recommended. If the patient becomes protein malnourished
patients with CKD. or the serum albumin decreases, the protein restriction should
be liberalized.
D I ETA RY R E C O M M E N DAT I O N S
A protein restriction of 0.8 to 1.0 g/kg daily may be needed
Dietary adjustments are an important part of the care plan for to prevent accumulation of acid, phosphorus, and uric acid
patients with CKD. Dietary restrictions are directed at pre- in CKD.
venting electrolyte abnormalities and unwanted weight loss.
As GFR decreases, the nephron is less able to handle potas- Phosphorus retention can lead to metabolic bone disease
sium, phosphorus, sodium, and acid loads. and cardiovascular disease. If hyperphosphatemia develops, a
As their renal function changes, patients should be moni- dietary phosphorus limit of 1,200 mg daily is recommended.
tored for hyperkalemia and other electrolyte abnormalities, Decreased vitamin D production in CKD can lead to
and their dietary prescription should be changed as indicated. decreased calcium absorption and hypocalcemia. Maintaining
Hyperkalemia usually occurs when the GFR is less than 20 a calcium intake of 1.0 to 1.2 g daily will help hypocalcemia and
mL/min per 1.73 m2, but it can occur with higher GFRs when parathyroid stimulation. Unwanted weight loss, anorexia, and
cachexia are complications of uremia and should be avoided
by prescribing a diet that provides 35 kcal/kg daily.
Table 4 0.3 STAGES OF CHRONIC KIDNEY DISEASE
Phosphorus retention can lead to metabolic bone disease
GFR , mL/min per and cardiovascular disease.
STAGE DESCRIPTION 1.73 m 2
570 N E P H R O L O GY
angiotensin receptor blockers (ARBs) are excellent choices for Hyperphosphatemia and secondary hyperparathyroidism
decreasing both systemic hypertension and proteinuria. The are risk factors for metabolic bone and mineral disease as
goal blood pressure is less than 130/80 mm Hg for patients well as for cardiovascular disease in persons with stage 3, 4,
with CKD and less than 120/75 mm Hg for those with CKD or 5 CKD.
and proteinuria.
Osteitis fibrosa cystica is the classic form of renal failure
associated bone disease with overactive osteoclastic and
Thiazide diuretics are useful until the GFR is <45 mL/min osteoblastic activity.
per 1.73 m2.
The goal blood pressure is <130/80 mm Hg for patients Recognizing and treating secondary hyperparathyroid-
with CKD and <120/75 mm Hg for those with CKD and ism and vitamin D deficiency early in the course of CKD can
proteinuria. prevent or minimize these complications. Treatment and pre-
vention of renal osteodystrophy and CKD-associated mineral
Proteinuria is a marker of renal dysfunction and a risk fac- and bone disorders focus on the suppression of parathyroid
tor for progression of CKD. ACEIs and ARBs are beneficial hormone production by maintaining a normal calcium and
in delaying the progression of renal disease not only by con- phosphorus balance. Treatment begins with a low-phospho-
trolling blood pressure but also by decreasing proteinuria. The rus diet. If the serum level of phosphorus remains elevated,
goal is to decrease urinary protein excretion by 35% to 40% of adding enteric phosphate binders is the next step. A low
the baseline level with an ideal goal of decreasing the urinary serum calcium level or a high parathyroid hormone level or
protein excretion to less than 0.3 g/1.73 m2 per 24 hours. both are indications for the addition of calcitriol or vitamin
D analogues. An elevated calcium-phosphorus product has
Proteinuria is a marker of renal dysfunction and a risk been associated with increased morbidity and mortality. The
factor for progression of CKD. goal is a calcium-phosphorus product of less than 55. Further
treatment of secondary hyperparathyroidism involves calcit-
ACEIs and ARBs are beneficial in delaying the progression riol, vitamin D analogues, or a calcimimetic agent to inhibit
of renal disease not only by controlling blood pressure but parathyroid hormone production. If the above measures fail
also by decreasing proteinuria. to adequately suppress the parathyroid, a parathyroidectomy
Decreasing the urinary protein excretion to <0.3 g/1.73 m2 may be indicated.
per 24 hours is the ideal goal in CKD. Osteomalacia (low-turnover bone disease due to 1,25-
dihydroxyvitamin D deficiency) is characterized by increased
The use of ACEIs, ARBs, and -blockers can lead to hyper- osteoid activity and diminished or absent osteoclastic and
kalemia, which may cause rhythm disturbances. Therefore, all osteoblastic activity. Osteoporosis occurs rarely in ESRD and
patients with progressive renal dysfunction who are receiving advanced CKD. Oversuppression of parathyroid hormone
these medications should be monitored for rhythm distur- production with vitamin D analogues or calcimimetic agents
bances and electrolyte abnormalities. is the most common cause.
Treating hyperlipidemia is also an important step in slow-
ing the progression of CKD and in decreasing cardiovascu- Osteomalacia results from 1,25-dihydroxyvitamin D
lar risks. Statins (3-hydroxy-3-methylglutaryl coenzyme A deficiency.
[HMG-CoA] reductase inhibitors) not only improve lipid
profiles but also may slow the progression of ESRD; however, With avoidance of aluminum phosphate binders and
the data are inconclusive. other aluminum-containing medications, aluminum bone
disease occurs infrequently in CKD and ESRD. Aluminum
Statins not only improve lipid profiles but also may slow bone disease is characterized by low levels of parathyroid
the progression of ESRD. hormone and 1,25-dihydroxyvitamin D in a patient present-
ing with microcytic anemia and bone fractures. Aluminum
Hyperphosphatemia and secondary hyperparathyroidism toxicity can also cause severe neurotoxicity. Thus, aluminum-
are risk factors for metabolic bone and mineral disease as well containing medications should be avoided in all patients with
as for cardiovascular disease in persons with stage 3, 4, or 5 stage 4 or stage 5 CKD. Aluminum osteodystrophy is diag-
CKD. In addition, through a complex feedback system, renal nosed with an iliac crest bone biopsy and treated with defer-
disease leads to phosphate retention, hypocalcemia, acidosis, oxamine chelation.
decreased 1,25-dihydroxyvitamin D production, and increased Anemia due to a decrease in erythropoietin production
parathyroid hormone production. Relatively early in advanc- is another complication of CKD. This anemia is a normo-
ing renal insufficiency, hyperphosphatemia and a decreased cytic normochromic anemia that is multifactorial; decreased
level of 1,25-dihydroxyvitamin D begin the cascade leading erythropoietin production, hemolysis, and blood loss may
to secondary hyperparathyroidism and the development of help contribute to the low hemoglobin concentration.
bone and systemic mineral disease. Osteitis fibrosa cystica is Bleeding is common in CKD because of platelet dysfunc-
the classic form of renal failureassociated bone disease with tion, but treatment with desmopressin is helpful in reversing
overactive osteoclastic and osteoblastic activity. the bleeding tendency quickly. If the GFR decreases to less
4 0. E VA LUAT I O N O F K I D N EY F U N C T I O N A N D C H R O N I C K I D N EY D I S E A S E 571
than 33 mL/min per 1.73 m2, erythropoietin production by and debilitating arthritis. Residual GFR is the most impor-
the renal parenchyma is not sufficient to prevent anemia. tant factor in this phenomenon and is inversely related to
Treatment with erythropoiesis-stimulating agents should 2-microglobulin deposition. Pseudogout and periarthritis are
be started if anemia develops in patients who have CKD other musculoskeletal complications in patients with stage 4
and ESRD. Studies, however, have shown an increased risk or 5 CKD.
of thromboembolic events when erythropoiesis-stimulating
agents were given to patients who had hemoglobin levels of 2-Microglobulin deposition occurs in persons with stage
11 g/dL or more. Other studies have shown decreased sur- 4 or 5 CKD and results in carpal tunnel syndrome and
vival and progression of cancer when the target hemoglobin debilitating arthritis.
is between 12 and 14 g/dL in women with breast and ovarian
cancer and in men and women with advanced head and neck Many abnormalities of the gastrointestinal tract can occur
cancer or with gastric and small cell lung cancer. On the basis with advanced CKD, including gastritis, colitis, ileitis, consti-
of these findings, the recommended optimal hemoglobin tar- pation, peptic ulcer disease, and gastrointestinal tract bleeding.
get level is 10 to 12 g/dL. Erythropoiesis-stimulating agents Anorexia is a multifactorial complication leading to protein
have also been recognized as contributing to systemic neph- and caloric malnutrition.
rogenic fibrosis. Thus, the goal is to use the smallest possible Neurologic complications commonly occur in persons
dose of erythropoiesis-stimulating agents to achieve hemo- with stage 3, 4, or 5 CKD. These include peripheral neuropa-
globin levels of 10 to 12 g/dL. Iron deficiency, which occurs thies, sleep disorders, restless legs, and eventually cognitive
in 25% to 38% of patients with CKD, is the most common impairment and central nervous system irritability with sei-
cause of resistance to erythropoiesis-stimulating agents, so it zures and coma in severe uremia.
should be corrected before starting erythropoiesis-stimulating
therapy. Other causes of resistance to erythropoiesis-stimu-
C K D A N D C A R D I OVA S CU L A R D I S E A S E
lating agents include inflammation, malignancy, secondary
hyperparathyroidism, hematologic disorders, and increasing Many large studies of patients with CKD have shown increased
uremia. mortality and morbidity from cardiovascular disease. The
nontraditional risk factors for cardiovascular disease associ-
In anemia of CKD, the goal is to use the smallest possible ated with CKD include lipid abnormalities, endothelial dys-
dose of erythropoiesis-stimulating agents in CKD to function, anemia, inflammation, and abnormal metabolism of
achieve hemoglobin levels of 1012 g/dL. phosphorus and calcium. The presence of proteinuria is evi-
dence of endothelial dysfunction and is an independent risk
The complications of progressive renal dysfunction and factor for cardiovascular disease. Lipid abnormalities associated
uremia involve all organ systems. Uremic symptoms and signs with CKD begin with mild abnormalities in GFR. These lipid
may occur at different levels of GFR depending on the patients abnormalities include hypertriglyceridemia, decreased high-
comorbid illnesses and the management of the patient begin- density lipoprotein, and increased levels of very low-density
ning dialysis. lipoprotein, remnant-like particles, intermediate-density lipo-
Metabolic acidosis begins in the early phases of CKD, protein, lipoprotein(a), and small dense low-density lipopro-
initially as a nonanion gap acidosis due to decreased ammo- tein. As kidney disease progresses and approaches ESRD (stage
nium secretion. As renal dysfunction progresses, phosphate 5 CKD), a progressive decrease in the total cholesterol level is
and sulfate accumulate and the acidosis becomes a high anion associated with increased cardiovascular events and all-cause
gap acidosis. mortality. This is the low-cholesterol paradox of chronic mal-
Although hyperkalemia can occur with a GFR less than nutrition and signifies a state of inflammation. Stage 5 CKD is
20 mL/min per 1.73 m2 and oliguria, hyperkalemia can also a state of increased levels of proinflammatory cytokines with
occur with a GFR much greater than 20 mL/min per 1.73 m2 elevated levels of C-reactive protein, increased oxidative stress,
as a result of distal tubular dysfunction (type 4 renal tubu- and decreased clearance of proinflammatory substances. This
lar acidosis or aldosterone deficiency) and medications that state of inflammation increases cardiovascular risks.
interfere with potassium handling (ACEIs, ARBs, -blockers, Additional factors contributing to increased cardio-
and potassium-sparing diuretics). Hyperkalemia associated vascular risks include anemia and altered metabolism of
with electrocardiographic changes should be treated emer- calcium, phosphorus, and vitamin D. Anemia in patients
gently with intravenous calcium to protect the myocardium with CKD contributes to the development of left ventricu-
and then with an infusion of insulin to redistribute the potas- lar hypertrophy. Vitamin D improves blood pressure and
sium; however, if the patient has electrocardiographic changes decreases inflammation, and decreased vitamin D produc-
and a low GFR, dialysis is indicated. Resins and dialysis are tion in CKD leads to increased cardiovascular risks. The
used to eliminate potassium. Chronic hyperkalemia can be mechanisms are thought to involve downregulation of the
treated with a scheduled dose of a resin, a low-potassium diet, renin-angiotensin system and a decrease in cellular cytokine
and the avoidance of medications that interfere with potas- production. An elevated calcium-phosphorus product and
sium handling. hyperparathyroidism are associated with increased inflam-
2-Microglobulin deposition occurs in persons with mation and systemic metastatic calcification leading to car-
stage 4 or 5 CKD and results in carpal tunnel syndrome diovascular disease.
572 N E P H R O L O GY
Cardiovascular disease in CKD is multifactorial and complain of muscle cramps, pain (back, chest, or abdominal),
is accompanied by lipid abnormalities, endothelial nausea and vomiting, pruritus, or urticaria. These symptoms
dysfunction, anemia, inflammation, and abnormal may be accompanied by fever, hypotension, or hypertension.
metabolism of phosphorus and calcium. Treatment is usually symptomatic and involves using another
type of dialysis membrane.
All patients with ESRD are at increased risk of hepatitis
L O N G -T E R M D I A LY S I S
B and C. They should receive hepatitis B vaccine. Infections
The number of patients reaching ESRD and beginning dialy- involving the dialysis access are mostly seen with central
sis continues to increase while diabetes mellitus and hyper- venous catheters or arteriovenous grafts and peritoneal dialy-
tension continue to be the leading causes of renal failure. sis tunneled catheters. Early detection and treatment with
Dialysis should be initiated before uremic symptoms develop. antibiotics is critical. Complications specific to peritoneal
Indications for dialysis include fluid overload, systemic acido- dialysis include catheter leaks, obesity, hyperlipidemia, and
sis, hyperkalemia, and uremic symptoms. hyperglycemia.
If the GFR is less than 30 mL/min per 1.73 m2, the patient Selecting the appropriate medications in the appropriate
should be told about options for RRT, which include in-center doses for patients receiving dialysis is essential to avoid adverse
hemodialysis, home hemodialysis, peritoneal dialysis, and reactions and accumulation of drugs leading to toxicity. Many
renal transplant. Innovative dialysis prescriptions include drugs are not removed by hemodialysis or peritoneal dialysis
daily hemodialysis and nocturnal hemodialysis. The choice of and should be avoided or their doses adjusted as the patients
dialysis type in chronic nonemergent renal failure depends on residual GFR decreases. Conversely, toxicity from some
many clinical and mechanical factors and on patient choice. All ingested drugs can be treated with hemodialysis (Box 40.2).
types of dialysis can be done at home. Peritoneal dialysis offers
a continuous ultrafiltration and solute clearance, avoiding Patients receiving dialysis should have all vaccinations
rapid fluid shifts and hemodynamic instability. Hemodialysis up to date and be monitored carefully for concurrent
offers more efficient clearance of solutes. Selected patients who infection.
have poor hemodialysis access options, cardiomyopathy, or a
scheduled transplant may be candidates for peritoneal dialysis.
Peritoneal dialysis will fail in patients with a history of recur-
rent abdominal operations or diseases that lead to fibrosis of
Box 4 0.2 DIALYSIS AND OVERDOSES
the peritoneal lining. Frequent hemodialysis methods such as
daily or nightly hemodialysis in a dialysis center or at home
have been shown to improve blood pressure, control bone dis- Drugs removed with dialysis
ease, and improve overall well-being. Methanol
Aspirin
Ethylene glycol
If the GFR is <30 mL/min per 1.73 m2, the patient should
Lithium
be told about options for RRT.
Sodium
Mannitol
Theophylline
Complications of Dialysis Drugs not removed with dialysis
Tetracycline
Intradialytic hypotension is a common complication of hemo-
Benzodiazepines
dialysis. Rapid removal of fluid, osmolar shifts, and abrupt
Digoxin
changes in calcium, bicarbonate, and potassium can lead to
Phenytoin
hemodynamic instability and arrhythmias. Rapid changes in
Phenothiazines
electrolytes or fluid removal can also lead to nausea, vomiting,
Drugs to avoid in patients receiving dialysis
and muscle cramps.
Tetracycline
The rapid removal of solutes, specifically urea in patients
Nitrofurantoin
with high urea values, can lead to neurologic consequences
Probenecid
known as dialysis dysequilibrium syndrome. The symptoms
Neomycin
include headaches, nausea and vomiting, decreased or altered
Bacitracin
mental status, seizures, and death. This syndrome is thought to
Methenamine
be caused by rapid shifts in urea and osmolality leading to fluid
Nalidixic acid
shifts into the central nervous system and cerebral edema. The
Clofibrate
best way to avoid this complication in patients with excessively
Lovastatin
high urea levels is to limit the efficiency of the dialysis session
Magnesium
by dialyzing with low flows of blood and dialysate for short
Oral hypoglycemic agents
periods.
Antiplatelet drugs
Allergic reactions to the hemodialyzer membrane can
Renally excreted -blockers
occur. Overt anaphylactic reactions are rare, but patients may
4 0. E VA LUAT I O N O F K I D N EY F U N C T I O N A N D C H R O N I C K I D N EY D I S E A S E 573
S U M M A RY through analysis of the urine (microscopic urine
analysis and protein excretion), and by imaging studies
The kidneys normally maintain a constant extracellular of the kidney to determine structural
environment, secrete multiple hormones, and catabolize abnormalities.
peptide hormones in fasting conditions.
If the GFR is <30 mL/min per 1.73 m2, the patient should
Kidney function is assessed by the estimated and measured be told about options for RRT.
GFR, by the functionality of the filtering structures
574 N E P H R O L O GY
PA RT X
A L L E R GY
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41.
ALLERGYa
Gerald W. Volcheck, MD
PATC H T E S TS A N D P R I C K (CU TA N EO US ) T E S T S Intradermal skin tests are more sensitive but less specific
Patch testing of skin is not the same as immediate than skin prick tests for airborne allergens.
wheal-and-flare skin testing. Patch testing is used to investi- Intradermal skin testing is used to investigate allergy to
gate only contact dermatitis, a type IV hypersensitivity skin insect venoms and penicillin.
reaction. Patch tests require 72 to 96 hours for complete eval-
uation. Many substances cause contact dermatitis. Common
contact sensitivities include nickel, formaldehyde, fragrances,
I N VIT RO A L L E RGY T E S T I N G
and latex.
Inhalant allergens, in comparison, cause respiratory symp- In vitro (blood) allergy testing initially involves chemically
toms, such as allergic rhinitis and asthma, and are identified by coupling allergen protein molecules to a solid-phase sub-
skin prick testing. Their sources include dust mites, cats, dogs, stance. The test is then conducted by incubating serum (from
cockroaches, molds, and tree, grass, and weed pollens. Food the patient) that may contain IgE antibody specific for the
allergy is also assessed by skin prick testing. allergen that has been immobilized to the membrane for a
standard time. The solid phase is then washed free of non-
Patch testing is used to investigate contact dermatitis. binding materials from the serum and incubated in a second
solution containing a reagent (eg, radiolabeled anti-IgE anti-
a
body). The measured radioactivity is correlated directly with
Portions previously published in Volcheck GW. Clinical allergy: diagnosis and
management. Totowa (NJ): Humana; c2009. Used with permission of Mayo the preparation of a standard curve in which known amounts
Foundation for Medical Education and Research. of allergen-specific IgE antibody were incubated with a set of
577
standard preparations of a solid phase. Labeled anti-IgE can Triggers of vasomotor rhinitis include strong odors and
also be measured with colorimetry, fluorometry, or monoclo- changes in humidity and temperature.
nal and polyclonal anti-IgE antibodies.
This test only identifies the presence of allergen-specific Factors common to allergic rhinitis and nonallergic rhini-
IgE antibody in the same way that the allergen skin test does. tis (thus, without differential diagnostic value) include peren-
Generally, in vitro allergy testing is not as sensitive as skin nial symptoms, intolerance of cigarette smoke, and history of
testing and has some limitations because of the potential for dust sensitivity. Factors that suggest fixed nasal obstruction
chemical modification of the allergen protein while it is being (which should prompt physicians to consider other diagno-
coupled to the solid phase. Generally, it is more expensive ses) include unilateral nasal obstruction, unilateral facial pain,
than allergen skin tests and has no advantage in routine clini- unilateral nasal purulence, nasal voice but no nasal symptoms,
cal work. In vitro allergy testing may be useful clinically for disturbances of olfaction without any nasal symptoms, and
patients who have been taking antihistamines and are unable unilateral nasal bleeding. Further evaluation with computed
to discontinue their use or for patients who have primary tomographic (CT) scan of the sinuses or rhinolaryngoscopy
cutaneous diseases that make allergen skin testing impractical is indicated.
or inaccurate (eg, severe atopic eczema with most of the skin
involved in a flare). Perennial symptoms, intolerance of cigarette smoke, and
history of dust sensitivity are common to allergic and
Skin testing is more sensitive and less expensive than in nonallergic rhinitis.
vitro allergy testing.
House dust mite sensitivity is a common cause of perennial
allergic rhinitis.
CHRONIC RHINITIS Rhinoscopy or CT scan of the sinuses should be performed
to evaluate unilateral symptoms.
M E D I C A L H I S TO RY
The differential diagnosis of chronic rhinitis is given in Box 41.1.
A L L E RGY S K I N T E S TS I N A L L E RG I C R H I N I T I S
Nonallergic rhinitis is defined as nasal symptoms occurring in
response to nonspecific, nonallergic irritants. Vasomotor rhin- The interpretation of allergy skin test results must be tailored
itis is the most common form. Common triggers of vasomotor to the unique features of each patient.
rhinitis are strong odors, respiratory irritants such as dust or
smoke, changes in temperature, changes in body position, and 1. For patients with perennial symptoms and negative results
ingestants such as spicy food or alcohol. on allergy skin tests, the diagnosis is nonallergic rhinitis.
Nonallergic rhinitis is defined as nasal symptoms occurring 2. For patients with seasonal symptoms and appropriately
in response to nonspecific stimuli. positive allergy skin tests, the diagnosis is seasonal allergic
rhinitis.
Historical factors favoring a diagnosis of allergic rhinitis 3. For patients with perennial symptoms, allergy skin tests
include a history of nasal symptoms that have a recurrent seasonal positive for house dust mite suggest house dust mite
pattern (eg, every August and September) or symptoms pro- allergic rhinitis. In this case, dust mite allergen avoidance
voked by being near specific sources of allergens, such as animals. should be recommended. Patients should encase their
Factors favoring vasomotor rhinitis include symptoms provoked bedding with allergy-proof encasements, wash sheets and
by strong odors and changes in humidity and temperature. pillowcases in hot water weekly, and keep the relative
humidity in the house at 40% to 50% or less.
Allergic rhinitis has a recurrent seasonal pattern and may
be provoked by being near animals.
C O RT I C O S T E RO I D T H E R A P Y F O R R H I N I T I S
Box 41.1 DIFFERENTIAL DIAGNOSIS OF CHRONIC
The need for systemic corticosteroid treatment for rhinitis is
RHINITIS
limited. Occasionally, patients with severe symptoms of aller-
gic rhinitis may benefit greatly from a short course of pred-
Allergic rhinitis
nisone (10 mg 4 times daily by mouth for 5 days). This may
Vasomotor rhinitis
induce sufficient improvement so that topical corticosteroids
Rhinitis medicamentosa
can penetrate the nose and satisfactory levels of antihistamine
Sinusitis
can be established in the blood. Severe nasal polyposis may
Nasal polyposis
warrant a longer course of oral corticosteroids. Sometimes
Nasal septal deviation
the recurrence of nasal polyps can be prevented by continued
Foreign body
use of topical corticosteroids. Polypectomy may be required if
Tumor
nasal polyps do not respond to treatment with systemic and
578 A L L E R GY
intranasal corticosteroids, but nasal polyps often recur after the market because of its association with hemorrhagic stroke
surgical intervention. in women. Several prescription and nonprescription combi-
nation agents combine an antihistamine and a decongestant.
Treatment of nasal polyposis can include oral prednisone, Saline nasal rinses may provide symptomatic improvement
followed by topical corticosteroids. in patients with chronic rhinitis by helping to remove mucus
from the nares.
In contrast to systemic corticosteroids, topical corticoster-
oid agents for the nose are easy to use and have few adverse Pseudoephedrine is the most common decongestant in
systemic effects. nonprescription and prescription preparations.
Topical corticosteroid agents are helpful for allergic nasal In men who are middle-aged or older, urinary retention
congestion. may be caused by antihistamines (principally the older drugs
that have anticholinergic effects) and decongestants. Although
Long-term treatment with decongestant nasal sprays may there has been concern for years that decongestants may exac-
have addictive potential (a vicious cycle of rebound con- erbate hypertension because they are -adrenergic agonists, a
gestion called rhinitis medicamentosa caused by topical vaso- clinically significant hypertensive response is rare in patients
constrictors). In contrast, intranasal corticosteroid does not with hypertension that is controlled medically.
induce this type of dependence.
Antihistamines and decongestants may cause urinary
Unlike decongestant nasal sprays, intranasal corticosteroid retention in men.
does not induce tachyphylaxis and rebound congestion.
The elderly are more sensitive to the anticholinergic effects
A substantial number of patients with nonallergic rhinitis of antihistamines.
also have a good response to intranasal (topical aerosol) corti-
costeroid therapy, especially if they have the nasal eosinophilia
form of nonallergic rhinitis. I M MU N OT H E R A P Y F O R A L L E RG I C R H I N I T I S
Until topical nasal glucocorticoid sprays were introduced,
Many patients with nonallergic rhinitis have a good
allergen immunotherapy was considered first-line therapy for
response to topical intranasal corticosteroid therapy.
allergic rhinitis when the relevant allergen was seasonal pollen
of grass, trees, or weeds. Immunotherapy became second-line
A patient who has allergic rhinitis and does not receive
therapy after topical corticosteroids were introduced because
adequate relief with topical corticosteroid plus antihistamine
immunotherapy 1) requires a larger time commitment during
therapy may need systemic corticosteroid treatment and
the build-up phase and 2) carries a small risk of anaphylaxis to
immunotherapy. Unilateral symptoms suggest anatomical
the immunotherapy injection itself. However, immunother-
causes, including polyps, septal deviation, and tumor.
apy for allergic rhinitis can be appropriate first-line therapy for
selected patients and is highly effective.
If pharmacologic management fails, allergy
Immunotherapy is often reserved for patients who do not
immunotherapy should be considered for patients with
receive satisfactory relief from intranasal corticosteroids or
allergic rhinitis.
who cannot tolerate antihistamines. Controlled trials have
shown a benefit for pollen, dust mite, and cat allergies and a
An unusual side effect of intranasal corticosteroids is nasal
variable benefit for mold allergy. Immunotherapy is not used
septal perforation. Spray canisters deliver a powerful jet of
for food allergy or nonallergic rhinitis. Immunotherapy has
particulates, and a few patients have misdirected the jet to the
been shown to decrease the incidence of the development of
nasal septum.
asthma in children with allergic rhinitis and to decrease the
onset of new allergen sensitivities in those treated for a single
Rarely, topical corticosteroid nasal sprays cause perforation
allergen.
of the nasal septum.
Immunotherapy is often reserved for patients who do
A N T I H I S TA M I N E S A N D OT H E R T R E AT M E N TS not receive relief from intranasal glucocorticoids or who
cannot tolerate antihistamines.
Antihistamines antagonize the interaction of histamine with
its receptors. Histamine may be more causative than other Controlled trials have shown that immunotherapy is
mast cell mediators of nasal itch and sneezing. These are symp- very effective for allergic rhinitis and results in prolonged
toms most often responsive to antihistamine therapy. symptom improvement.
Pseudoephedrine is the most common decongestant agent
Anaphylaxis is a risk of immunotherapy.
in nonprescription drugs for treating cold symptoms and
rhinitis and usually is the active agent in widely used prescrip- Immunotherapy for allergic rhinitis can be first-line
tion agents. Phenylpropanolamine has been removed from therapy for selected patients.
41. A L L E R GY 579
Box 41.2 DUST MITE CONTROL removal is not tenable, some partial measures must be consid-
ered. Recommendations include keeping the animal out of the
Encase bedding & pillows in mite-impermeable encasements bedroom entirely and attempting to keep the animal in 1 area
Remove carpeting from bedroom of the home. A high-efficiency particulate air (HEPA) room
Remove upholstered furniture from bedroom air purifier should be placed in the bedroom. Naturally, the
Remove all carpeting laid on concrete person should avoid close contact with the animal and should
Discontinue use of humidifier consider using a mask if handling the animal or entering the
Wash bedding in hot water weekly room where the animal is kept. Bathing cats about once every
Run dehumidifier other week may reduce the allergen load in the environment.
580 A L L E R GY
Box 41.4 CAUSES OF PERSISTENT OR RECURRENT U RT I C A R I A A N D A N G I O E D E M A
SINUSITIS
D U R AT I O N O F U RT I C A R I A
Nasal polyposis
Mucormycosis The distinction between acute urticaria and chronic urticaria is
Allergic fungal sinusitis arbitrary and based on duration. If urticaria has been present
Ciliary dyskinesia for 6 weeks or longer, it is called chronic urticaria.
Wegener granulomatosis
Hypogammaglobulinemia
S EC O N DA RY U RT I C A R I A
Tumor
Most patients simply have urticaria as a skin disease (chronic
idiopathic urticaria). Many of these patients have an anti-
Persistent, refractory, and complicated sinusitis should be body that interacts with their own IgE or IgE receptor
evaluated by a specialist. Sinus CT is the preferred imaging that produces the urticaria. Occasionally urticaria is the
study for these patients (Figure 41.1). presenting sign of more serious internal disease. It can be
Amoxicillin (500 mg 3 times daily) or trimethoprim- a sign of lupus erythematosus and other connective tis-
sulfamethoxazole (1 double-strength capsule twice daily) for sue diseases, particularly the overlap syndromes that are
10 to 14 days is the treatment of choice for uncomplicated more difficult to categorize. Thyroid disease, malignancy
maxillary sinusitis. (mainly of the gastrointestinal tract), lymphoproliferative
Plain radiography of the sinuses is less sensitive than CT diseases, and occult infection (particularly of the intestines,
(using the coronal sectioning technique). CT scans show greater gallbladder, and dentition) may be associated with urti-
detail about sinus mucosal surfaces, but CT usually is not neces- caria. Immune-complex disease has been associated with
sary in acute uncomplicated sinusitis. CT is indicated, though, urticaria, usually with urticarial vasculitis; hepatitis B virus
for patients being considered for a sinus operation and for those has been identified as an antigen in cases of urticaria and
in whom standard treatment of sinusitis fails. However, patients immune-complex disease.
with extensive dental restorations that contain metal may gen-
erate too much artifact for CT to be useful. For these patients, Urticaria can be associated with lupus erythematosus
magnetic resonance imaging techniques are indicated. and other connective tissue diseases, thyroid disease,
malignancy, infection, and immune-complex disease.
Sinus imaging is indicated for recurrent sinusitis.
Sinus CT is preferred to sinus radiography for complicated A common cause of acute urticaria and angioedema
sinusitis. (other than the idiopathic variety) is drug or food allergy.
However, drug or food allergy usually does not cause chronic
urticaria.
R E L AT I O N B ET WE E N U RT I C A R I A A N D
ANGIOEDEMA
In common idiopathic urticaria, the hives last 2 to 18 hours,
and the lesions itch intensely because histamine is the primary
cause of wheal formation.
41. A L L E R GY 581
C1 E S T E R A S E I N H I B ITO R D E FI C I E N C Y patient to create enough pressure to cause symptoms in those
with delayed pressure urticaria. Unlike most cases of common
Hereditary angioneurotic edema (HANE) is characterized by
idiopathic urticaria, in which the lesions affect essentially all
recurrent episodes of angioedema, typically without urticaria.
skin surfaces, many cases of physical urticaria seem to involve
If HANE is strongly suspected, the diagnosis can be proved
only certain areas of skin. Thus, challenges will be positive
by the appropriate measurement of complement factors
only in the areas usually involved and negative in other areas.
(decreased levels of C1 esterase inhibitor [quantitative and
Directing challenges to the appropriate area depends on the
functional] and C4 [also C2, during an episode of swelling]).
history.
Levels of C1 esterase inhibitor and C4 are decreased in
For physical urticaria, the history is the only way to suspect
HANE.
the diagnosis, which can be confirmed by applying stimuli
to the patients skin.
Treatment of C1 esterase inhibitor dysfunction includes
the following:
F O O D A L L E RGY I N C H RO N I C U RT I C A R I A
1. Plasma-derived C1 esterase inhibitor given intravenously
indicated for prophylaxis and acute attacks Food allergy almost never causes chronic urticaria. However,
urticaria (or angioedema or anaphylaxis) can be an acute man-
2. Kallikrein inhibitor (ecallantide) given subcutaneously ifestation of true food allergy.
indicated for acute attacks
3. Bradykinin B2 receptor antagonist (icatibant) given Food allergy almost never causes chronic urticaria.
subcutaneouslyindicated for acute attacks Food allergy may cause acute urticaria, angioedema, or
anaphylaxis.
The duration, size, and location of individual swellings
vary. Many patients with HANE have also had symptoms
resembling intestinal obstruction. These symptoms usually H I S TO PAT H O L O GY O F C H RO N I C U RT I C A R I A
resolve in 3 to 5 days. Chronic urticaria is characterized by mononuclear cell perivas-
Lesions in HANE do not itch. The response to epineph- cular cuffing around dermal capillaries, particularly involving
rine is also a useful differential point: HANE lesions do not the capillary loops that interdigitate with the rete pegs of the
respond well to epinephrine, but common angioedema usually epidermis. Urticarial vasculitis shows the usual histologic fea-
resolves in 15 minutes or less. Laryngeal edema almost never tures of leukocytoclastic vasculitis.
occurs in the common idiopathic type of disease (although
it may occur in allergic reactions, most often in insect-sting The characteristic histopathologic feature of chronic
anaphylaxis cases); however, it is relatively common in HANE urticaria is a mononuclear cell perivascular cuff around
(earlier articles cited a 30% mortality rate in HANE, with capillaries.
all deaths due to laryngeal edema). HANE episodes may be
related to local tissue trauma in a high percentage of cases, with
dental work often regarded as the classic precipitating factor. M A NAG E M E N T O F U RT I C A R I A
The history is of utmost importance for discovering the 2%
Many patients with HANE have been hospitalized for to 10% of cases of chronic urticaria due to secondary causes.
intestinal obstruction. A complete physical examination is needed, with particular
HANE lesions do not respond well to epinephrine. attention paid to the skin (including testing for dermatogra-
phism) to evaluate for the vasculitic nature of the lesions and
In HANE, laryngeal edema is relatively common. to the liver, lymph nodes, and mucous membranes. Laboratory
Dental work is the classic precipitating factor for HANE. testing need not be exhaustive but may include the following:
chest radiography, a complete blood cell count with differen-
tial count (to discover eosinophilia), liver enzymes, tests for
thyroid function and antibodies, erythrocyte sedimentation
P H Y S I C A L U RT I C A R I A
rate, serum protein electrophoresis (in patients older than 50),
Heat, light, cold, vibration, and trauma or pressure can cause urinalysis, and stool examination for parasites. Allergy skin
hives in susceptible persons. Obtaining the history is the only testing is indicated only if the patient has an element in the
way to suspect the diagnosis, which can be confirmed by apply- history suggesting an allergic cause. However, patients with
ing each of the stimuli to the patients skin in the laboratory. idiopathic urticaria often have fixed ideas about an allergy
Heat can be applied by placing coins (soaked in hot water for causing their problem, and skin testing often helps to dissuade
a few minutes) on the patients forearm. Cold can be applied them of this idea.
with coins kept in a freezer or with ice cubes. For vibration, a
laboratory vortex mixer or any common vibrator can be used. The history is of utmost importance in diagnosing chronic
A pair of sandbags connected by a strap can be draped over the urticaria due to secondary causes.
582 A L L E R GY
Laboratory testing may include chest radiography, 3. Insect stings (bee, fire ant, and vespid)
eosinophil count, liver enzymes, tests for thyroid function
4. Latex
and antibodies, erythrocyte sedimentation rate, serum
protein electrophoresis, urinalysis, and stool examination 5. Aspirin and other nonsteroidal anti-inflammatory agents
for parasites.
The vast majority of anaphylactic events occur within 1
Management of urticaria and angioedema consists of hour, often within minutes, after exposure to the offending
blocking histamine, beginning usually with nonsedating H1 agent.
antagonists. The addition of leukotriene antagonists may be
helpful. The role of H2 antagonists is unclear; they may help
a small percentage of patients. Tricyclic antidepressants, such F O O D A L L E R GY
as doxepin, have potent antihistamine effects and are useful.
Systemic corticosteroids can be administered for acute urti-
C L I N I C A L H I S TO RY
caria and angioedema.
The clinical syndrome of food allergy may include the fol-
Urticaria and angioedema: management is usually with H1 lowing: Very sensitive persons experience tingling, itching,
antagonists. and a metallic taste in the mouth while the food is still in the
mouth. Within 15 minutes after the food is swallowed, epigas-
Urticaria and angioedema: systemic corticosteroids are
tric distress may occur. There may be nausea and rarely vomit-
used for acute cases.
ing. Abdominal cramping is felt chiefly in the periumbilical
area (small-bowel phase), and lower abdominal cramping and
A N A P H Y L AX I S watery diarrhea may occur. Urticaria or angioedema may occur
in any distribution, or there may be only itching of the palms
There is no universally accepted clinical definition of ana- and soles. With increasing clinical sensitivity to the offending
phylaxis. The manifestations of anaphylaxis vary, depending allergen, anaphylactic symptoms may emerge, including tachy-
on the severity, and can include any combination of urticaria, cardia, hypotension, generalized flushing, and alterations of
angioedema, flushing, pruritus, upper airway obstruction, consciousness.
lower airway obstruction, diarrhea, nausea, vomiting, syn- In extremely sensitive persons, generalized flushing,
cope, hypotension, tachycardia, and dizziness. Approximately hypotension, and tachycardia may occur before the other
90% of anaphylactic episodes include urticaria or angioedema. symptoms. Most patients with a food allergy can identify
A cellular and molecular definition of anaphylaxis is a gener- the offending foods. The diagnosis should be confirmed by
alized allergic reaction characterized by activated basophils skin testing or in vitro measurement of allergen-specific IgE
and mast cells releasing many mediators (preformed and antibody.
newly synthesized). The dominant mediators of acute anaphy-
laxis are histamine and prostaglandin D2. The serum levels of Allergic reactions to food usually include pruritus,
tryptase peak at 1 hour after the onset of anaphylaxis and may urticaria, or angioedema.
stay elevated for 5 hours. Physiologically, the hypotension of
anaphylaxis is caused by peripheral vasodilatation and not by C O M M O N C AUS E S O F F O O D A L L E RGY
impaired cardiac contractility. Anaphylaxis is characterized by
a hyperdynamic state. For these reasons, anaphylaxis can be Items considered to be the most common causes of food
fatal in patients with preexisting fixed vascular obstructive dis- allergy are listed in Box 41.5.
ease in whom a decrease in perfusion pressure leads to a critical
reduction in flow (stroke) or in patients in whom laryngeal F O O D -R E L AT E D A NA P H Y L AX I S
edema develops and completely occludes the airway.
Food-induced anaphylaxis is the same process involved in acute
The clinical hallmarks of anaphylaxis are urticaria, flushing, urticaria or angioedema induced by food allergens, except that
hypotension, and tachycardia.
Histamine and prostaglandin D2 are the dominant
mediators of acute anaphylaxis. Box 41.5 COMMON CAUSES OF FOOD ALLERGY
41. A L L E R GY 583
the severity of the reaction is greater in anaphylaxis. Relatively Anaphylaxis caused by allergy to stinging insects is similar
few foods are commonly involved in food-induced anaphy- to all other forms of anaphylaxis. Thus, the onset of anaphy-
laxis; the main ones are peanuts, shellfish, and nuts, although laxis may be very rapid, often within 1 or 2 minutes. Pruritus
any food has the potential to cause anaphylaxis. In patients of the palms and soles is the most common initial manifesta-
with latex allergy, food allergy can develop to banana, avo- tion. Frequently, 1 or more of the following occur next: gen-
cado, kiwifruit, and other fruits. eralized flushing, urticaria, angioedema, or hypotension. The
reason for attaching importance to whether a stinging insect
Anaphylaxis to food can be life-threatening. reaction is a large local or a generalized one is that allergy skin
testing and allergen immunotherapy are recommended only
There is cross-sensitivity between latex and banana, for generalized reactions. Patients who have a large local reac-
avocado, and kiwifruit. tion are not at increased risk of future anaphylaxis.
584 A L L E R GY
Box 41.6 INDICATIONS FOR VENOM Box 41.7 DOS AND DONTS FOR PATIENTS WITH
IMMUNOTHERAPY HYPERSENSITIVITY TO INSECT STINGS
History of mild, moderate, or severe anaphylaxis to a sting Avoid looking or smelling like a flower
Positive results on skin tests to the venom that was implicated his- Avoid flowered prints for clothes
torically in the anaphylactic reaction Avoid cosmetics & fragrances, especially ones derived from flower-
Urticaria distant from the site of the sting (adults only) ing plants
Never drink from a soft-drink can outdoors during the warm
correlate with the clinical history are sufficient evidence for monthsa yellow jacket can land on or in the can while you
considering Hymenoptera venom immunotherapy. are not watching, go inside the can, & sting the inside of your
mouth (a dangerous place for a sensitive patient to be stung)
Skin testing should be delayed for at least 1 month after a when you take a drink
sting-induced general reaction. Avoid doing outdoor maintenance & yard work
Never reach into a mailbox without first looking inside it
Patients with clinical anaphylaxis and positive results on Never go barefoot
venom skin tests benefit from venom immunotherapy. Always look at the underside of picnic table benches & park
benches before sitting down
V E N O M I M MU N OT H E R A P Y Never attempt to eject a stinging insect yourself from the interior
of a moving automobile; pull over, get out, & let someone else
The decision to undertake venom immunotherapy can be remove the insect
reached only after a discussion between the patient and the
physician. General indications for venom immunotherapy are
Stevens-Johnson Syndrome
listed in Box 41.6. Patients must understand that after immu-
notherapy is begun, the injection schedule must be maintained Stevens-Johnson syndrome is a bullous skin and mucosal reac-
and that there is a small risk of immunotherapy-induced allergic tion; very large blisters appear over much of the skin surface,
reaction. Patients also need to understand that despite receiv- in the mouth, and along the gastrointestinal tract. Because
ing allergy immunotherapy, they must carry epinephrine when of the propensity of the blisters to break down and become
outdoors because of the possibility (from 2% with vespid stings infected, the reaction often is life-threatening. Treatment
to 10% with apid stings) that immunotherapy will not provide consists of stopping use of the drug that causes the reaction,
suitable protection. Most, but not all, patients can safely dis- giving corticosteroids systemically, and providing supportive
continue venom immunotherapy after 5 years of treatment. care. The patients are often treated in burn units. Penicillin,
sulfonamides, barbiturates, diphenylhydantoin, warfarin,
There is a small risk that venom immunotherapy will and phenothiazines are well-known causes. A drug-induced
induce an allergic reaction. Stevens-Johnson reaction is an absolute contraindication to
administering the causative drug to the patient in the future.
There is a 2%-10% chance that venom immunotherapy will
not provide adequate protection.
Stevens-Johnson syndrome is life-threatening and is an
absolute contraindication for rechallenge with the drug.
AVO I DA N C E
The warnings that every patient with stinging insect hypersen- Toxic Epidermal Necrolysis
sitivity should receive are listed in Box 41.7. A patients specific
circumstances may require additional entries to this list. Also, Clinically, toxic epidermal necrolysis is almost indistinguish-
patients need to know how to use self-injectable epinephrine able from Stevens-Johnson syndrome. Histologically, the cleav-
in its several forms. Many patients wear an anaphylaxis identi- age plane for the blisters is deeper than in Stevens-Johnson
fication bracelet. syndrome. The cleavage plane is at the basement membrane
of the epidermis, so even the basal cell layer is lost. This
All patients with stinging-insect sensitivity should carry an makes toxic epidermal necrolysis even more devastating than
epinephrine kit. Stevens-Johnson syndrome because healing occurs with much
scarring. Often, healing cannot be accomplished without
skin grafting, so the mortality rate is even higher than for
D RU G A L L E R GY Stevens-Johnson syndrome. Patients with toxic epidermal
necrolysis should always be cared for in a burn unit because of
full-thickness damage over 80% to 90% of the skin. The very
D RU G A L L E RGY N OT I N VO LVI N G IgE O R
high mortality rate is similar to that for burn patients with
I M M E D I AT E -T Y P E R E AC T I O NS
damage of this extent.
Patients with drug allergy not involving IgE or immediate-type
reactions have negative results on skin prick and intradermal Toxic epidermal necrolysis is a life-threatening exfoliative
testing. dermatitis.
41. A L L E R GY 585
Morbilliform Skin Reaction It is associated with several connective tissue diseases, viral
infections, and drug allergy.
Morbilliform skin reaction is the most common dermatologic
manifestation of a drug reaction. It is an immune-mediated
drug rash without IgE involvement, manifested by a Contact Dermatitis
macular-papular exanthem. The rash can be accompanied
Contact dermatitis can occur with various drugs. Commonly,
by pruritus but has no other systemic symptoms. It typically
it is a form of drug allergy that is an occupational disease in
occurs more than 5 days after use of a medication was begun. It
medical or health care workers. In some patients receiving
is not associated with anaphylaxis or other serious sequelae.
topical drugs, allergy develops to the drug or to various ele-
ments in its pharmaceutical formulation (eg, fillers, stabilizers,
Morbilliform skin reaction is the most common antibacterials, and emulsifiers). Contact dermatitis is a mani-
dermatologic manifestation of a drug reaction and is not festation of type IV hypersensitivity. Clinically it appears as
associated with anaphylaxis. an area of reddening on the skin that progresses to a granular
weeping eczematous eruption with some dermal thickening;
Ampicillin-Mononucleosis Rash the surrounding skin has a plaque-like quality. When patients
are receiving treatment for dermatitis, and contact hypersensi-
Ampicillin-mononucleosis rash is a unique drug rash that
tivity develops to corticosteroids or other drugs used in treat-
occurs when ampicillin is given to an acutely ill, febrile patient
ment, a particularly difficult diagnostic problem arises unless
who has mononucleosis. The rash is papular, nonpruritic,
the physician is alert to this possibility. When contact hyper-
and rose-colored. It occurs usually on the abdomen and feels
sensitivity to a drug occurs, it does not increase the probabil-
granular when the fingers brush lightly over the surface of
ity of acute type I hypersensitivity and is not associated with
the involved skin. It is not known why the rash is specific for
serious exfoliative syndromes. However, exquisite cutaneous
ampicillin and mononucleosis. This rash does not predispose
sensitivity of this type can develop in patients so that almost
to allergy to penicillin.
no avoidance technique in the workplace completely elimi-
nates dermatitis; even protective gloves are only partly helpful.
Ampicillin-mononucleosis rash is papular, nonpruritic, and Thus, it can be occupationally disabling.
rose-colored, and it occurs on the abdomen.
This rash does not predispose to penicillin allergy. Contact dermatitis is a form of drug allergy.
It is a manifestation of type IV hypersensitivity.
Fixed Drug Eruptions
Fixed drug eruptions are red to red-brown macules that D RU G A L L E RGY I N VO LV I N G IgE O R
appear on a certain area of the patients skin; any part of the I M M E D I AT E -T Y P E R E AC T I O N S
body can be affected. The macules do not itch or have other Penicillin Allergy
signs of inflammation, although fever is associated with
their appearance in a few patients. The unique aspect of this Penicillin can cause anaphylaxis in sensitive persons. It is an
phenomenon is that if a patient is given the same drug in IgE-mediated process that can be evaluated with skin testing
the future, the rash develops in exactly the same skin areas. to the major and minor determinants of penicillin. Patients
Resolution of the macules often includes postinflammatory with positive results on skin testing and a clinical history of
hyperpigmentation. Except for cosmetic problems due to penicillin allergy can be desensitized to penicillin in a super-
skin discolorations, the phenomenon does not seem serious. vised setting.
Antibiotics and sulfonamides are the most frequently recog-
nized causes. Penicillin can cause anaphylaxis.
Both major and minor determinants of penicillin should
In fixed drug eruptions, the same area of skin is always be tested in suspected penicillin allergy.
affected.
Patients can be desensitized under supervision.
Erythema Nodosum
Penicillin skin tests can be helpful in determining
Erythema nodosum is a characteristic rash of red nodules about whether it is safe to administer penicillin to a patient with
the size of a quarter, usually nonpruritic and appearing only suspected penicillin allergy. About 85% of patients who
over the anterior aspects of the lower legs. Histopathologically, give a history of penicillin allergy have negative results with
the nodules are plaques of infiltrating mononuclear cells. skin tests to the major and minor determinants of penicil-
Erythema nodosum is associated with several connective tis- lin. These patients are not at increased risk of anaphylaxis
sue diseases, viral infections, and drug allergy. and can receive penicillin safely. If penicillin skin test results
are positive, there is a 40% to 60% chance that an allergic
Erythema nodosum rash is usually nonpruritic, appearing reaction will develop if the patient is challenged with peni-
only over the anterior aspect of the lower legs. cillin. These patients should avoid penicillin and related
586 A L L E R GY
drugs. However, if there is a strong indication for penicillin OT H E R A L L E R G I C O R I M MU N O L O G I C
treatment, desensitization can be performed. The desensi- CONDITIONS
tization procedure involves the administration of progres-
sively increasing doses of penicillin. Desensitization can be
M A S TO C Y TO S I S
accomplished by the oral or intravenous route and is usually
performed in a hospital setting. Systemic mastocytosis is a disorder of abnormal prolifera-
Ampicillin, amoxicillin, nafcillin, and other -lactam tion of mast cells. The skin, bone marrow, liver, spleen, lymph
antibiotics cross-react strongly with penicillin. Early studies nodes, and gastrointestinal tract can be affected. The clinical
suggested that up to 20% to 30% of patients with penicillin manifestations vary but can include flushing, pruritus, urti-
allergy were also allergic to cephalosporins. More recent stud- caria, unexplained syncope, fatigue, and dyspepsia. Bone mar-
ies have suggested that the cross-sensitivity of penicillin with row biopsies with stains for mast cells (toluidine blue, Giemsa,
cephalosporins is much less (about 5%). Most studies have or chloral acetate esterase) and immunochemical stains for
suggested that aztreonam does not cross-react with penicillin. tryptase are the most direct diagnostic studies. Serum levels of
tryptase and urinary concentrations of histamine, histamine
About 5% of patients with penicillin allergy are also metabolites, and prostaglandins are typically increased.
allergic to cephalosporins. Treatment initially consists of antihistamines. Cromolyn
sodium given orally can be beneficial, especially in patients
Aztreonam does not cross-react with penicillin.
with gastrointestinal tract symptoms. Corticosteroids should
be considered in severe cases, and interferon is a promising
Radiographic Contrast Media Reactions investigational treatment.
41. A L L E R GY 587
Box 41.8 COMMON CAUSES OF EOSINOPHILIA Autoimmune anemia, thrombocytopenia, or neutro-
penia is present in 10% to 50% of the patients and typically
Atopic occurs before CVID is diagnosed. Inflammatory arthritis and
Allergic bronchopulmonary aspergillosis lymphoid interstitial pneumonia are other associated condi-
Asthma tions. Also, patients have an increased risk of a malignancy,
Atopic dermatitis particularly a lymphoid malignancy such as non-Hodgkin
Drug hypersensitivity lymphoma.
Pulmonary The diagnosis of CVID should be considered if patients
Eosinophilic pneumonia have recurrent pyogenic infections and hypogammaglobuline-
Lffler syndrome mia. Associated gastrointestinal tract or autoimmune disease
Proliferative/neoplastic and the exclusion of hereditary primary immunodeficiencies
Idiopathic hypereosinophilic syndrome support the diagnosis. Treatment is with intravenous or subcu-
Eosinophilic leukemia taneous -globulin. The typical dosage is 400 mg/kg monthly.
Vasculitis/connective tissue
Churg-Strauss vasculitis T E R M I NA L C O M P L E M E N T C O M P O N E N T
Eosinophilic fasciitis D E FI C I E N C I E S
Eosinophilic gastroenteritis
Infectious Patients with deficiency of the terminal complement com-
Visceral larva migrans ponent C5, C6, C7, or C8 have an increased susceptibil-
Helminth ity to meningococcal infections. The terminal complement
Toxic components form the membrane attack complex that causes
Eosinophilia-myalgia syndrome cell lysis; hence, deficiency of 1 of these components results
Toxic oil syndrome in defective microbial killing. The terminal component C9
participates in membrane pore formation but is not essential
for complement-mediated cell lysis. Thus, patients with the
echocardiography, complete blood cell count, and liver rare C9 deficiency have a limited increased susceptibility to
enzyme and serum tryptase levels). The differential diagnosis infections.
of eosinophilia is given in Box 41.8. Terminal complement component deficiency should be
Hypereosinophilia syndrome is treated with prednisone, suspected if patients have recurrent meningococcal disease,
1 mg/kg daily, alone or in combination with hydroxyurea. a family history of meningococcal disease, systemic menin-
Second-line therapy includes recombinant interferon-alfa. gococcal infection, or infection with an unusual serotype of
meningococcus. Diagnosis is confirmed with assay of total
C O M M O N VA R I A B L E I M MU N O D E FI C I E N C Y hemolytic complement and measurement of individual com-
plement components.
Common variable immunodeficiency (CVID) affects males
and females of all ages. It is the most common primary immu-
nodeficiency in adults. Patients have recurrent sinopulmo- S U M M A RY
nary infections, primarily with encapsulated organisms. The
primary laboratory abnormality is hypogammaglobuline- Patch testing is used to investigate contact dermatitis.
mia (low IgG levels). IgA and IgM levels may be normal or
decreased. Recurrent pyogenic infections include chronic Skin prick (immediate) testing is used to investigate
otitis media, chronic or recurrent sinusitis, pneumonia, and respiratory allergy to airborne allergens and food allergy.
bronchiectasis.
Allergic rhinitis has a recurrent seasonal pattern and may
Patients with CVID often have autoimmune or gastroin-
be provoked by being near animals.
testinal tract disturbances. About one-half of patients have
chronic diarrhea and malabsorption. They may have steator- Triggers of vasomotor rhinitis include strong odors and
rhea, protein-losing enteropathy, ulcerative colitis, or Crohn changes in humidity and temperature.
disease. Other gastrointestinal tract problems associated with
Urticaria and angioedema: management is usually with H1
the disease are atrophic gastritis, pernicious anemia, giardiasis,
antagonists.
and chronic active hepatitis. Pathologic changes in the gastro-
intestinal tract mucosa include loss of villi, nodular lymphoid Urticaria and angioedema: systemic corticosteroids are
hyperplasia, and diffuse lymphoid infiltration. used for acute cases.
588 A L L E R GY
42.
ASTHMA a
Gerald W. Volcheck, MD
G OA L S PAT H O P H YS I O L O GY
Recognize the pathophysiology and triggers of asthma. Bronchial hyperresponsiveness is common to all forms of
Categorize asthma by severity. asthma. It is measured by assessing pulmonary function before
and after exposure to methacholine, histamine, cold air, or
Define testing and treatment strategies for asthma patients. exercise. A decrease in forced expiratory volume in 1 second
(FEV1) of 20% or more with challenge is considered a sign of
airway hyperreactivity.
PAT H O L O GY Persons who have allergic asthma generate mast cell
and basophil mediators that have important roles in the
The pathologic features of asthma have been studied chiefly in development of endobronchial inflammation and smooth
fatal cases; some bronchoscopic data are available for mild and muscle changes that occur after acute exposure to aller-
moderate asthma. The histologic hallmarks of asthma include gen. Mast cells and basophils are prominent during the
mucous gland hypertrophy, mucus hypersecretion, epithelial immediate-phase reaction. In the late-phase reaction to
desquamation, widening of the basement membrane, and allergen exposure, the bronchi show histologic features of
infiltration by eosinophils (Box 42.1). chronic inflammation and eosinophils become prominent
in the reaction.
The histologic hallmarks of asthma include mucous Patients who have chronic asthma and negative results on
gland hypertrophy, mucus hypersecretion, epithelial allergy skin tests usually have an inflammatory infiltrate in the
desquamation, widening of the basement membrane, and bronchi and histologic findings dominated by eosinophils
infiltration by eosinophils. when asthma is active. Patients with sudden asphyxic asthma
may have a neutrophilic rather than an eosinophilic infiltra-
tion of the airway.
Box 42.1 HISTOLOGIC HALLMARKS OF ASTHMA
Important characteristics of cytokines are summarized
in Table 42.1. Interleukin (IL)-1, IL-6, and tumor necro-
Mucous gland hypertrophy sis factor are produced by antigen-presenting cells and start
Mucus hypersecretion the acute inflammatory reaction against an invader; IL-4
Alteration of tinctorial & viscoelastic properties of mucus and IL-13 stimulate IgE synthesis; IL-2 and interferon-
Widening of basement membrane zone of bronchial epithelial stimulate a cell-mediated response; and IL-10 is the primary
membrane anti-inflammatory cytokine.
Increased number of intraepithelial leukocytes & mast cells
Round cell infiltration of bronchial submucosa
IL-4 stimulates IgE synthesis.
Intense eosinophilic infiltration of submucosa
Widespread damage to bronchial epithelium IL-5 stimulates eosinophils.
Large areas of complete desquamation of epithelium into air-
Helper T cells produce IL-4 and IL-5.
way lumen
Mucous plugs filled with eosinophils & their products
G E N ET I C S
a
The genetics of asthma is complex and confounded by envi-
Portions previously published in Volcheck GW. Clinical allergy: diagnosis and
management. Totowa (NJ): Humana Press; c2009. p. 189278. Used with permis- ronmental factors. No asthma gene has been discovered. The
sion of Mayo Foundation for Medical Education and Research. gene encoding the subunit of the high-affinity IgE receptor
589
Table 42.1 CHARACTERISTICS OF CYTOKINES Box 42.2 INDUSTRIAL AGENTS THAT CAN CAUSE
PRIMARY
ASTHMA
CYTOKINE MAJOR ACTIONS SOURCES
Metals
IL-1 Lymphocyte activation Macrophages Salts of platinum, nickel, & chrome
Fibroblast activation Endothelial cells
Wood dusts
Fever Lymphocytes
Mahogany
IL-2 T- & B-cell activation T cells (TH1) Oak
Redwood
IL-3 Mast cell proliferation T cells
Neutrophil & macrophage Mast cells Western red cedar (plicatic acid)
maturation Vegetable dusts
Castor bean
IL-4 IgE synthesis T cells (TH2)
Cotton
IL-5 Eosinophil proliferation & T cells (TH2) Cottonseed
differentiation Flour
Grain (mite & weevil antigens)
IL-6 IgG synthesis Fibroblasts
Lymphocyte activation T cells Green coffee
Gums
IL-8 Neutrophil chemotaxis Fibroblasts Industrial chemicals & plastics
Endothelial cells
Ethylenediamine
Monocytes
Phthalic & trimellitic anhydrides
IL-10 Inhibition of IFN- & IL-1 T cells Polyvinyl chloride
production Macrophages Toluene diisocyanate
IL-13 IgE synthesis T cells Pharmaceutical agents
Phenylglycine acid chloride
IFN- Antiviral activity Leukocytes Penicillins
IFN- Macrophage activation T cells (TH1) Spiramycin
Stimulation of MHC expression Food industry agents
Inhibition of TH2 activity Egg protein
Polyvinyl chloride
TNF- Antitumor cell activity Lymphocytes
Macrophages Biologic enzymes
Bacillus subtilis (laundry detergent workers)
TNF- Antitumor cell activity T cells Pancreatic enzymes
GM-CSF Mast cell, granulocyte, Lymphocytes Animal emanations
& macrophage stimulation Mast cells Canine or feline saliva
Macrophages Horse dander (racing workers)
Rodent urine (laboratory animal workers)
Abbreviations: GM-CSF, granulocyte-macrophage colony-stimulating factor;
IFN, interferon; IL, interleukin; MHC, major histocompatibility complex; TH,
helper T cell; TNF, tumor necrosis factor. performed in the workplace and away from the workplace aid
in the diagnosis.
is located on chromosome 11q13 and is linked to total IgE, Every patient evaluated for allergy or asthma must be asked
atopy, and bronchial hyperreactivity. Polymorphic variants of to provide a detailed occupational history.
the 2-adrenergic receptor are linked to bronchial hyperreac-
tivity. The gene for IL-4 is located on chromosome 5q31 and
is linked to total IgE. G A S T R O E S O P H AG E A L R E F LUX A N D
ASTHM A
590 A L L E R GY
Patients with asthma who have glaucoma treated with oph- exposed to aeroallergens and often have seasonal variation
thalmic preparations of timolol or betaxolol may experience of symptoms. If allergy skin test results are negative, one can
bronchospasm. -Blockers are not absolutely contraindicated be reasonably certain that the patient does not have allergic
in asthma, but observation is warranted. asthma. Respiratory infections (particularly viral), cold dry
air, exercise, and respiratory irritants can trigger allergic and
-Blockers, including those in eyedrops, can cause severe nonallergic asthma.
adverse responses in patients with asthma.
In allergic asthma, symptoms can be perennial (eg, from
1-Selective blockers such as atenolol may also provoke
dust mites or pets), or sporadic (eg, from seasonal pollens).
asthma.
Patients with allergic asthma are likely to react to many
A chronic, dry cough that mimics asthma may develop in nonimmunologic triggers.
persons taking angiotensin-converting enzyme inhibitor drugs.
Cold dry air and exercise can trigger asthma.
Wheeze and dyspnea, however, do not accompany the cough.
Aspirin ingestion can cause acute, severe, and fatal asthma
in a small subset of patients with asthma. Most of the affected
A S S E S S M E N T O F C O N T R I B U TO R S TO
patients have nasal polyposis, hyperplastic pansinus mucosal
ASTHM A
disease, and moderate to severe persistent asthma. However,
not all asthma patients with this reaction to aspirin fit the pro-
The mnemonic AIR-SMOG provides a concise checklist
file. Many nonsteroidal anti-inflammatory drugs can trigger
of possible contributors to asthma (Box 42.3). In addition,
the reaction; the likelihood correlates with a drugs potency
patient compliance with medications and ability to use the
for inhibiting cyclooxygenase. Only nonacetylated salicylates
inhaler correctly should be reviewed for all patients with per-
such as choline salicylate (a weak cyclooxygenase inhibitor)
sistent asthma.
seem not to provoke the reaction. Leukotriene-modifying
drugs may be particularly helpful in aspirin-sensitive asthma.
Traditionally, asthma patients have been warned not to take
A S S E S S M E N T O F S E VE R I T Y
antihistamines because the anticholinergic activity of some
antihistamines was thought to cause drying of lower respira-
Asthma is intermittent if 1) the daytime symptoms are inter-
tory tract secretions, further worsening the asthma. However,
mittent (<2 times weekly), 2) continuous treatment is not
antihistamines do not worsen asthma, and some studies have
needed, and 3) the flow-volume curve during formal pulmo-
shown a beneficial effect.
nary function testing is normal between episodes of symptoms.
Even for patients who meet these criteria, inflammation (albeit
Aspirin and other nonsteroidal anti-inflammatory drugs patchy) is present in the airways and corticosteroid inhaled on
can cause acute, severe asthma. a regular basis diminishes bronchial hyperresponsiveness.
Asthma, nasal polyposis, and aspirin sensitivity form the
aspirin allergy triad. Corticosteroid inhaled on a regular basis diminishes
bronchial hyperresponsiveness.
Leukotriene modifiers may be helpful in aspirin-sensitive
asthma.
Asthma is mild persistent or moderate persistent when 1)
Antihistamines are not contraindicated in asthma. the symptoms occur with some regularity (>2 times weekly)
or daily, 2) there is nocturnal occurrence of symptoms, or
C I G A R ET T E S M O K I N G A N D A S T H M A 3) asthma exacerbations are troublesome. For many of these
patients, the flow-volume curve is rarely normal and complete
A combination of asthma and cigarette smoking leads to accel- pulmonary function testing may show evidence of hyperinfla-
erated chronic obstructive pulmonary disease. Because of the tion, as indicated by increased residual volume or an increase
accelerated rate of irreversible obstruction, all asthma patients
who smoke should be counseled to stop smoking.
Environmental tobacco smoke is an important asthma Box 42.3 AIR-SMOG : A MNEMONIC FOR A CHECKLIST
trigger. In particular, children with asthma who are exposed OF CONTRIBUTORS TO ASTHMA
to environmental smoke have more respiratory infections and
asthma attacks. Aallergy
Iinfection, irritants
Rrhinosinusitis
M E D I C A L H I S TO RY
Ssmoking
Mmedications
A medical history for asthma includes careful inquiry about
Ooccupational exposures
symptoms, provoking factors, alleviating factors, and severity.
Ggastroesophageal reflux disease
Patients with marked respiratory allergy have symptoms when
4 2. A S T H M A 591
above expected levels for the diffusing capacity of the lung for E X H A L E D N I T R I C OX I D E
carbon dioxide. Asthma is severe persistent when symptoms are
present almost continuously and the usual medications must Exhaled nitric oxide has been studied as a noninvasive mea-
be given in doses at the upper end of the dose range to control sure of airway inflammation. The fraction of nitric oxide in
the disease. the exhaled air increases in proportion to inflammation of
Patients with mild, moderate, or severe persistent asthma the bronchial wall, sputum eosinophilia, and airway hyper-
should receive treatment daily with anti-inflammatory medi- responsiveness. Exhaled nitric oxide levels increase with dete-
cations, usually inhaled corticosteroids. Most patients with rioration in asthma control and decrease in a dose-dependent
severe asthma require either large doses of inhaled cortico- manner with anti-inflammatory treatment. The usefulness of
steroid or oral prednisone daily for adequate control. A major- measuring exhaled nitric oxide may be in monitoring asthma
ity have been hospitalized more than once for asthma. The control, guiding therapy, and predicting response to cortico-
severity of asthma can change over time, and an early sign that steroid therapy.
asthma is not well controlled is the emergence of nocturnal
symptoms. Elevated exhaled nitric oxide levels are associated with
eosinophilic respiratory inflammation and decreased
Patients with mild, moderate, or severe persistent asthma asthma control.
should receive treatment daily with anti-inflammatory
medications.
D I F F E R E N T I A L D I AG N O S I S
Nocturnal symptoms suggest that asthma is worsening.
The differential diagnosis of wheezing is given in Box 42.5.
M ET H AC H O L I N E B R O N C H I A L
CHALLENGE
M E D I C AT I O N S F O R A S T H M A
If a patient has a history suggestive of episodic asthma but has
Medications for asthma are listed in Box 42.6. They can be
normal results on pulmonary function tests on the day of the
divided into bronchodilator compounds and anti-inflamma-
examination, the patient is a reasonable candidate for a metha-
tory compounds.
choline bronchial challenge. The methacholine bronchial chal-
lenge is also useful in evaluating patients for cough if baseline
pulmonary function appears normal. Positive results indicate B RO N C H O D I L ATO R C O M P O U N D S
that bronchial hyperresponsiveness is present, although results
Currently, the only anticholinergic drug available in the United
can be positive in conditions besides asthma (Box 42.4). Some
States for treating asthma is ipratropium bromide, although it
consider isocapnic hyperventilation with subfreezing dry air
is approved for treating only chronic obstructive pulmonary
(by either exercising or breathing a carbon dioxideair mixture)
or exercise testing as alternatives to a methacholine challenge.
Do not perform a methacholine challenge in patients who
have severe airway obstruction or a clear diagnosis of asthma. Box 42.5 DIFFERENTIAL DIAGNOSIS OF WHEEZING
Usually, a 20% decrease in FEV1 is considered a positive
result. Pulmonary embolism
Cardiac failure
Patients with suspected asthma and normal results on Foreign body
pulmonary function tests are candidates for methacholine Central airway tumors
testing. Aspiration
Carcinoid syndrome
Chondromalacia or polychondritis
Lffler syndrome
Box 42.4 MEDICAL CONDITIONS ASSOCIATED Bronchiectasis
WITH POSITIVE FINDINGS ON METHACHOLINE Tropical eosinophilia
CHALLENGE Hyperventilation syndrome
Laryngeal edema
Current asthma Vascular ring affecting trachea
Past history of asthma Factitious (including psychophysiologic vocal cord adduction)
Chronic obstructive pulmonary disease 1-Antitrypsin deficiency
Smoking Immotile cilia syndrome
Recent respiratory infection Bronchopulmonary dysplasia
Chronic cough Bronchiolitis (including bronchiolitis obliterans), croup
Allergic rhinitis Cystic fibrosis
592 A L L E R GY
Box 42.6 MEDICATIONS FOR ASTHMA mild persistent asthma. These agents work by decreasing
the inflammatory effects of leukotrienes. Zileuton can cause
Bronchodilator compounds increased liver function test results. Cases of Churg-Strauss
Anticholinergic drugs (ipratropium bromide) vasculitis have also been linked to zafirlukast and montelu-
2-Agonist drugs kast, although a clear cause-and-effect relationship has not
Short-acting (albuterol, pirbuterol, levalbuterol) been established.
Long-acting (salmeterol, formoterol)
Methylxanthines (theophylline) C O RT I C O S T E RO I D S
Antiallergic compounds
Cromolyn
Many experts recommend inhaled glucocorticoids for all
Nedocromil
severities of persistent asthma because of the potential
Glucocorticoids
long-term benefits of reduced bronchial hyperresponsiveness
Systemic
and reduced airway remodeling (fibrosis). Long-term use of
Prednisone
-agonist bronchodilators alone may adversely affect asthma;
Methylprednisolone
this also argues for earlier use of inhaled glucocorticoids.
Topical
Asthma mortality has been linked to the heavy use of -agonist
Beclomethasone
inhalers. This association may simply reflect that patients with
Budesonide
more severe asthma (who are more likely to die of an asthma
Ciclesonide
attack) use more -agonist inhalers. However, prolonged and
Flunisolide
heavy use of inhaled -agonists may have a direct, deleterious
Fluticasone
effect on asthma. Asthma patients with regularly recurring
Mometasone
symptoms should receive inhaled corticosteroids as part of
Triamcinolone acetonide
the treatment.
Antileukotrienes
Leukotriene receptor antagonists (zafirlukast, montelukast) Prescribe inhaled glucocorticoids for mild, moderate, and
Lipoxygenase inhibitors (zileuton) severe persistent asthma.
Glucocorticoids in combination with long-acting 2-agonists Long-term and heavy use of -agonist bronchodilators may
Budesonide with formoterol worsen asthma.
Fluticasone with salmeterol
The inflammatory infiltrate in the bronchial submucosa
disease. Several short-acting -adrenergic compounds are of asthma patients probably depends on cytokine secretory
available, but albuterol, levalbuterol, and pirbuterol are pre- patterns. Corticosteroids may interfere at several levels in the
scribed most. More side effects occur when these medications cytokine cascade, and they offer several benefits:
are given orally rather than by inhalation. Nebulized -agonists
are rarely used long-term in adult asthma, although they may 1. Corticosteroids reduce airway inflammation by
be used in acute attacks. For home use, the metered-dose modulating cytokines IL-4 and IL-5.
inhaler or dry powdered inhalation is the preferred delivery 2. Corticosteroids can inhibit the inflammatory properties
system. Salmeterol and formoterol are 2 long-acting inhaled of monocytes and platelets.
-agonists. Both should be used only in combination with
inhaled corticosteroids. Theophylline is effective for asthma, 3. Corticosteroids have vasoconstrictive properties.
but it has a narrow therapeutic index, and interactions with 4. Corticosteroids decrease mucous gland secretion.
other drugs (cimetidine, erythromycin, and quinolone antibi-
otics) can increase the serum level of theophylline. The most common adverse effects of inhaled corticoster-
oids are dysphonia and thrush. These unwanted effects occur
-Agonists are best delivered by the inhaler route for in about 10% of patients and can be reduced by using a spacer
long-term use. device and rinsing the mouth after administration. Usually, oral
Theophylline is effective for asthma but has a narrow thrush can be treated successfully with oral antifungal agents.
therapeutic index. Dysphonia, when persistent, may be treated by decreasing or
discontinuing the use of inhaled corticosteroids.
Detailed study of the systemic effects of inhaled corticoster-
oids shows that these agents are much safer than oral corticos-
A N T I-I N F L A M M ATO RY C O M P O U N D S
teroids. Nevertheless, there is evidence that high-dose inhaled
Cromolyn and nedocromil are inhaled anti-inflammatory corticosteroids can affect the hypothalamic-pituitary-adrenal
(mast cell stabilizing) medications that are appropriate for axis and bone metabolism. Also, high-dose inhaled corticos-
treatment of mild or moderate asthma. The 5-lipoxygenase teroids may increase the risk of future development of glau-
inhibitor zileuton and the leukotriene receptor antagonists coma, cataracts, and osteoporosis. Inhaled corticosteroids
zafirlukast and montelukast are approved for treatment of can decrease growth velocity in children and adolescents. The
4 2. A S T H M A 593
effect of inhaled corticosteroids on final adult height is not
Symptoms of asthma
known, but it appears to be minimal.
Poor inhaler technique and poor compliance can result
in poor control of asthma. Therefore, all patients using a
metered-dose inhaler or dry powder inhaler should be taught Previous
No
diagnosis of Establish diagnosis of asthma
the proper technique for using these devices. Most patients asthma?
using metered-dose inhaled corticosteroids should use a spacer
device with the inhaler. Yes
M A NAG E M E N T O F C H RO N I C A S T H M A
Schedule regular follow-up visits
Baseline spirometry is recommended for all patients with
asthma, and home peak flow monitoring is recommended
for those with moderate or severe asthma (Figure 42.1). Figure 42.1 Diagnosis and Management of Asthma. PEFR indicates peak
Environmental triggers should be discussed with all asthma expiratory flow rate.
patients, and allergy testing should be offered to those with
suspected allergic asthma or with asthma that is not well con- Home peak flow monitoring is recommended for patients
trolled. Although allergy immunotherapy is effective, it is rec- with moderate or severe asthma.
ommended only for patients with allergic asthma who have
had a complete evaluation by an allergist.
M A NAG E M E N T O F AC U T E A S T H M A
Spirometry is recommended for all asthma patients. Inhaled -agonists, measurements of lung function at presen-
tation and during therapy, and systemic corticosteroids (for
most patients) are the cornerstones of managing acute asthma
Box 42.7 GOALS OF ASTHMA MANAGEMENT
(Figure 42.2). Generally, nebulized albuterol, administered
repeatedly if necessary, is the first line of treatment. Delivery
No asthma symptoms
of -agonist by metered-dose inhaler can be substituted in less
No asthma attacks
severe asthma attacks. Inhaled -agonist delivered by continu-
Normal activity level
ous nebulization may be appropriate for more severe disease.
Normal lung function
It is important to measure lung function (usually peak
Use of safest & least amount of medication necessary
expiratory flow rate but also FEV1 whenever possible) at pre-
Establishment of therapeutic relationship between patient &
sentation and after administration of bronchodilators. These
provider
measurements provide invaluable information that allows the
594 A L L E R GY
Patient in ED with acute
exacerbation of asthma
Assess severity of
asthma exacerbation
Poor response
Hospitalize patient
Figure 42.2 Management of Acute Asthma in Adults. ED indicates emergency department; FEV1, forced expiratory volume in 1 second; IV,
intravenous; MDI, metered-dose inhaler; O2, oxygen; PAP, positive airway pressure; PE, physical examination; PEFR, peak expiratory flow
rate. (Adapted from Sveum R, Bergstrom J, Brottman G, Hanson M, Heiman M, Johns K, et al. Diagnosis and management of asthma. 10th ed.
Bloomington [MN]: Institute for Clinical Systems Improvement [updated 2012 Jul]. Available from: http://www.icsi.org/asthma__outpatient/
asthma__diagnosis_management_of__guideline_.html. July c2012. Used with permission.)
physician to assess the severity of the asthma attack and the Most patients with acute asthma need a course of systemic
response (if any) to treatment. corticosteroids.
Patients who do not have a prompt and full response to
inhaled -agonists should receive a course of systemic corti-
costeroids. Patients with the most severe and poorly responsive A L L E R G I C B R O N C H O P U L M O N A RY
disease (FEV1 <50%, oxygen saturation <90%, and moderate ASPERGILLOSIS
to severe symptoms) should be treated on a hospital ward or
in an intensive care unit. Allergic bronchopulmonary aspergillosis is an obstructive
lung disease caused by an allergic reaction to Aspergillus
Measure pulmonary function at presentation and after in the lower airway. The typical patient presents with
giving bronchodilators. severe steroid-dependent asthma. Most patients with this
4 2. A S T H M A 595
Box 42.8 DIAGNOSTIC FEATURES OF ALLERGIC
BRONCHOPULMONARY ASPERGILLOSIS
Clinical asthma
Bronchiectasis (usually proximal)
Increased total serum IgE
IgE antibody to Aspergillus (by skin test or in vitro assay)a
Precipitins or IgG antibody to Aspergillus
Radiographic infiltrates (often upper lobes)
Peripheral blood eosinophilia
a
Required for diagnosis.
596 A L L E R GY
PA RT X I
P SYC H I AT RY
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43.
PSYCHIATRY
Brian A. Palmer, MD
This chapter reviews common psychiatric illnesses and Weight loss, fatigue, feelings of worthlessness, excessive
emphasizes diagnosis and management. Since 30% to 40% of guilt, loss of interest, and decreased ability to concentrate
ambulatory primary care visits have a psychiatric component, are hallmark symptoms of depression if they last >2 weeks.
successful patient management often hinges on successful
treatment of comorbid psychiatric illness. Seasonal Affective Disorder
The key concept when assessing psychiatric symptoms Seasonal affective disorder is a subtype of major depres-
is whether the symptom interferes with a patients functioning sion characterized by the onset of symptoms in autumn or
or causes distress. For example, a patient may have a fear of winter. It is twice as common among women compared with
heights. If this acrophobia never causes an alteration in activ- men and is associated with psychomotor retardation, hyper-
ity, intervention is unnecessary. If, however, this acrophobia somnia, overeating (carbohydrate craving), and weight gain
causes distress and interferes with the patients functioning, (resembling hibernation). Diagnosis requires 3 consecutive
intervention may be warranted. years of autumn or winter episodes that resolve by spring or
summer. Treatment has relied primarily on phototherapy with
a full-spectrum light source of 10,000 lux, which must be used
MOOD DISORDER S for a minimum of 30 minutes daily. Antidepressant agents are
also of benefit in treating this disorder.
Mood disorders are common, with a prevalence of 8% in the
general US population. The essential feature is disturbance Recurrent depression in the winter must occur in 3
of mood in a constellation of other symptoms (mood change consecutive winters to be classified as seasonal affective
alone, such as sadness, is not an illness). Mood disorders are disorder.
accompanied by related cognitive, psychomotor, vegetative,
and interpersonal difficulties. Mood disorders may be related
Postpartum Depression
to a general medical condition or be substance induced.
Postpartum depression affects 10% of mothers. Although
it occurs in all socioeconomic groups, single or poor moth-
D E P R E S S I VE D I S O R D E R S ers are at greatest risk. Untreated postpartum depression can
adversely affect parent-child bonding. Treatment with antide-
Major Depression
pressants, although effective, must be balanced with the pos-
Major depression is a serious psychiatric disorder with pri- sible effect on a developing fetus or breast-fed infant, but it
mary symptoms that include 5 of the 9 criteria in Box 43.1 for is generally accepted that in moderate to severe depression,
599
Box 43.1 CRITERIA FOR A MAJOR DEPRESSIVE the stress. In general, these reactions are relatively transient.
EPISODE a Although patients generally can be managed by an empathetic
primary care physician, the development of extreme with-
Depressed mood (feeling sad or empty; tearful)b drawal, suicidal ideation, or failure to improve as the circum-
Diminished interest or pleasure in many activitiesb stances improve may prompt psychiatric referral. Treatment
Notable weight loss or weight gain (>5% of body weight in 1 mo) includes supportive psychotherapy, psychosocial interven-
or decreased or increased appetite tions, and, sometimes, use of antidepressant agents.
Insomnia or hypersomnia nearly every day
Psychomotor agitation or retardation Principles of Depression Treatment
Fatigue or loss of energy
Feelings of worthlessness or inappropriate guilt (which may be There are 3 common major groups of treatment modalities
delusional) for depression: psychotherapy, pharmacotherapy, and ECT.
Diminished ability to think or concentrate, or indecisiveness Generally, these therapeutic modalities are used in some
Recurrent thoughts of death, including suicidal ideation or combination. Although internists rarely conduct formal psy-
planning chotherapy, brief cognitive interventions, such as challenging
overly perfectionistic beliefs, can be helpful.
a
Symptoms must be present every day or nearly every day for at least 2 weeks. A The selection of medication is based on the side-effect pro-
diagnosis of major depression requires 5 of the 9 criteria.
file of the medication and on the personal or family history
b
A diagnosis of major depression requires either a depressed mood or a loss of of a good response to a particular agent. Initially, the patient
interest or pleasure in activities. should use a low dose, followed by titration to a therapeutic
dose based on clinical assessment. Blood level determinations
of a drug are meaningful only for tricyclic antidepressants
the risks of not treating depression outweigh the risk of treat-
used at higher doses. Treatment duration usually extends for
ment with most antidepressants. Prescribing clinicians should
a minimum of 6 to 12 months after the patient noticeably
be cognizant of the pregnancy category of the agent they pre-
improves. Patients who have a severe depressive episode or
scribe in this patient group. Bipolar disorder is overrepresented
who have experienced 2 or more depressive episodes are at high
in patients with postpartum mood disorders.
risk of symptom recurrence without prophylactic medication.
Use of antidepressants should be tapered rather than stopped
Dysthymia abruptly when treatment is discontinued. If the response to
the first antidepressant agent is minimal, reevaluate the diag-
Dysthymia is chronic depression that is milder in severity than
nosis, change to a different class of drug, or consider ECT.
major depression. It can be disabling for the person because the
depressed mood is present most of the time during at least a
2year period. Many patients have 1 or 2 associated vegetative MANIA AND BIPOLAR DISORDER
signs, such as disturbance of sleep and appetite. Also, patients
The essential features of a manic episode are the presence of an
often feel inadequate, have low self-esteem, and struggle with
abnormally euphoric, expansive, or irritable mood associated
interpersonal relationships. If onset is in late adolescence, the
with 3 of the criteria in Box 43.2 (4 criteria are required if the
dysthymia may become intertwined with the persons person-
mood is only irritable). For a diagnosis of bipolar disorder, the
ality, behavior, and general attitude toward life. Treatment is
patient must have had at least 1 episode of mania (bipolar I
usually a combination of psychotherapy and pharmacother-
disorder) or hypomania (bipolar II disorder). Most patients
apy. Pharmacotherapy may be particularly useful for patients
with bipolar disorder have had recurrent depressive episodes
with a family history of mood disorders or for those who have
the early-onset form of dysthymia. In patients with dysthymia,
superimposed major depressive episodes may develop. Box 43.2 CRITERIA FOR A MANIC EPISODE a
600 P SYC H I AT RY
in addition to manic episodes, although rarely patients have sedative hypnotics, benzodiazepines, and narcotics. Long-term
mania exclusively. The prevalence of bipolar disorder is esti- use or abuse of alcohol or hallucinogens has also been impli-
mated to be about 1%. Bipolar disorder occurs about as fre- cated in inducing mood disturbances.
quently in women as in men, and the usual age at onset is
from the teens to 30 years. A family history of bipolar or other
mood disorder is more common among patients with bipo- A N X I ET Y D I S O R D E R S
lar disorder than among patients with other mood disorders.
Some patients do not experience a fully developed manic epi- Anxiety symptoms may be misinterpreted as those of medical
sode but have fewer symptoms. The term hypomania has been illness because many of the symptoms overlap (eg, tachycar-
introduced to describe this form of bipolar disorder (bipolar II dia, diaphoresis, tremor, shortness of breath, nausea, abdomi-
disorder), which generally is challenging to clinicians because nal pain, and chest pain). Autonomic arousal and anxious
its subtle features make it more difficult to recognize and it agitation in a medically ill patient can also be attributed
may be confused with other psychiatric disorders. quickly to stress or anxiety when the symptoms may repre-
sent pulmonary embolus or cardiac arrhythmia. Common
A patient with mania may present with a euphoric mood, sources of anxiety in the medical setting are related to fears of
flight of ideas, decreased need for sleep, and unrestrained death, abandonment, loss of function, pain, dependency, and
buying sprees. loss of control. When to treat or to seek psychiatric consulta-
tion depends on the assessment of the degree of anxiety. Is the
Treatment is aimed at mood stabilization with medica- patient able to function in his or her role without distress or
tion and improved social and occupational functioning. avoidance?
Pharmacotherapy of mania includes lithium carbonate, val-
proic acid, other mood stabilizers, and atypical antipsychotics.
PA N I C D I S O R D E R A N D AG O R A P H O B I A
Lithium has the added benefit of being useful in preven-
tion or treatment of bipolar depression. Lamotrigine is also Panic disorder refers to recurrent, discrete episodes of extreme
effective in treating bipolar depression. Patients with bipo- anxiety accompanied by various somatic symptoms such as
lar depression may be treated with ECT, lithium carbonate, dyspnea, unsteady feelings, palpitations, paresthesias, hyper-
lamotrigine, or an antidepressant (used simultaneously with a ventilation, trembling, diaphoresis, chest pain or discomfort,
mood-stabilizing agent to help prevent mania). or abdominal distress. Agoraphobia refers to extreme fear of
being in places or situations from which escape may be dif-
ficult or embarrassing. This may lead to avoidance, ultimately
M O O D D I S O R D E R S C AUS E D BY A G E N E R A L
causing severe limitations in daily functioning for the patient.
M E D I C A L C O N D IT I O N
Panic disorder is more common in women (prevalence,
Mood disorders can be caused by medical illness. Many medi- 2%-3%) than in men (prevalence, 0.5%-1.5%). The usual age at
cal conditions may induce mood changes, so the clinical inter- onset is from the late teens to the early 30s. A history of child-
view should identify coexisting symptoms such as excessive hood separation anxiety is reported in 20% to 50% of patients.
guilt, social withdrawal, or suicidal ideation, which are more The incidence is higher in first- and second-degree relatives.
specific for a primary depressive disorder. Medical conditions Most patients describe their first panic attack as spontaneous.
that may cause mood symptoms include endocrinopathies They generally go to an emergency department after the first
(Cushing syndrome, Addison disease, hyperthyroidism, hypo- attack, believing that they are having a heart attack or a severe
thyroidism, hyperparathyroidism, and hypoparathyroidism), medical problem.
certain malignancies (lymphomas, pancreatic carcinoma, and Patients with panic attacks may be prone to episodes of major
astrocytomas), neurologic conditions (Parkinson disease, depression. The differential diagnosis of panic disorder includes
Huntington disease, and Alzheimer disease), autoimmune several medical disorders, such as endocrine disturbances (eg,
conditions (systemic lupus erythematosus), and infections hyperthyroidism, pheochromocytoma, and hypoglycemia), gas-
(chronic hepatitis C, encephalitis, mononucleosis, and human trointestinal tract disturbances (eg, colitis and irritable bowel
immunodeficiency virus infection). syndrome), cardiopulmonary disturbances (eg, pulmonary embo-
lism, exacerbation of chronic obstructive pulmonary disease, and
acute allergic reactions), and neurologic conditions (especially
S U B S TA N C E -I N D U C E D MO O D D I S O R D E R S
conditions such as seizures that are episodic or are associated with
The essential feature of a substance-induced mood disorder paresthesias, faintness, or dizziness).
is a mood disturbance, either depressed or manic, due to the Several substances of abuse may cause or exacerbate anxi-
direct physiologic effects of a substance. Many substances can ety symptoms. Stimulants (eg, cocaine, amphetamines, and
induce mood changes, including medications, toxins, and caffeine) can fuel anxiety, as can withdrawal from sedating
drugs of abuse. The mood symptoms may occur during the use agents (eg, alcohol, benzodiazepines, and narcotics). Patients
of or exposure to the substance or during withdrawal from the may use alcohol or benzodiazepines to prevent or treat panic
substance. Medications that have been implicated in inducing symptoms, but regular or high-dose use may result in a cycle
mood disturbances include corticosteroids, interferon, reser- of tolerance and withdrawal, paradoxically causing an increase
pine, methyldopa, carbonic anhydrase inhibitors, stimulants, in anxiety symptoms.
602 P SYC H I AT RY
evident initially in the teenaged years. Symptoms have been 30s or 40s. It is diagnosed twice as often in women as in men
subdivided into positive (delusions and hallucinations) and and is characterized by preoccupation with pain for at least 6
negative (apathy and amotivational) symptoms. Diagnostic months. No organic lesion is found to account for the pain,
criteria include the presence of delusions and hallucinations; or if there is a related organic lesion, the complaint of pain or
marked decrement in functional level in areas such as work, resulting interference with usual life activities is in excess of
school, social relations, and self-care; and continuous signs what would be expected from the physical findings. A thor-
of the disturbance for at least 6 months. Exclusion criteria ough assessment is essential before this diagnosis can be estab-
include a consistent mood disorder component and evidence lished. Treatment is usually multidisciplinary (eg, primary care,
of an organic factor that produces the symptoms. psychiatry, psychology, and physiatry) and focused on helping
Brief psychotic disorder describes a primary psychotic illness the patient manage or live with the pain rather than continu-
lasting less than 1 month; schizophreniform disorder is a pri- ing with the expectation of cure. Avoidance of long-term
mary psychotic illness lasting 1 to 6 months. dependence on addictive substances is an important goal.
604 P SYC H I AT RY
racial groups. Despite high lifetime prevalence (up to 20%), dependence often have an iatrogenic component. Five char-
less than 10% of persons with substance use disorders are acteristics may help distinguish medical use from nonmedical
involved in treatment (either self-help groups or professional use:
care).
Several pharmacologic agents are available to help 1. Intent: What is the purpose of the use?
diminish the craving for alcohol and other drugs or to
deter relapse. Although several medications, including 2. Effect: What is the effect on the users life?
disulfiram, acamprosate, and naltrexone, may help pre- 3. Control: Is the use controlled by the user only or does a
vent relapse, they are adjunctive and not a substitute for physician share in the control?
treatment.
Substance dependence is typified by the following criteria (3 4. Legality: Is the use of the drug legal or illegal? Medical
of the 7 are required for diagnosis): drug use is legal.
5. Pattern: In what settings is the drug used?
1. Tolerance
2. Withdrawal Withdrawal of the use of benzodiazepines and barbitu-
rates, in particular, may be serious because of the increased
3. Increasing amount of use risk of withdrawal seizures; slowly tapered doses are indicated,
4. Unsuccessful efforts to stop particularly for long-term use.
606 P SYC H I AT RY
involuntary movements of the face, trunk, or extremities. trimester of pregnancy is associated with Ebstein anomaly.
The most consistent risk factors for its development are Renal effects generally can be reversed with discontinued use
long-term medication use (>6 months) and older age. It of lithium; renal function should be followed. A hematologic
is best if treatment with the antipsychotic agent can be side effect is benign leukocytosis. Hypothyroidism is com-
discontinued at an early sign of tardive dyskinesia because mon, and thyroid function should be monitored.
the dyskinesia is sometimes reversible. It is rarer with Lithium has a narrow therapeutic index (typically 0.51.0
atypical antipsychotics. mEq/L), and toxicity (typically >1.52.5 mEq/L) can cause
renal failure and death. Signs of toxicity include abdomi-
6. Glucose intolerance, weight gain, and electrophysiologic
nal pain and vomiting, dry mouth, nystagmus and blurred
cardiac changes have been associated with atypical
vision, delirium, ataxia, hyperreflexia and fasciculations, and
antipsychotics. Additionally, several studies have shown a
seizures.
lack of efficacy for off-label use in dementia patients, and
Lithium levels are increased by angiotensin-converting
safety concerns have arisen related to an increased risk of
enzyme inhibitors, thiazide diuretics, nonsteroidal
death among these patients.
anti-inflammatory drugs, dehydration, overheating or
7. Clozapine side effects: Clozapine is an atypical antipsychotic increased perspiration, and certain antibiotics (tetracycline,
that can increase the risk of seizures, orthostasis, and spectinomycin, and metronidazole). Levels can be decreased
myocarditis, and it has a 1% to 2% risk of producing by caffeine and theophylline.
agranulocytosis, which is reversible if use of the medication
is withdrawn immediately. Because of this serious potential
side effect, a specific requirement is that white blood cell E L E C T R O C O N V U L S I VE T H E R A P Y
counts be made regularly (weekly for the first 6 months).
ECT is the most effective treatment for severely depressed
patients, especially those with psychotic features. It is also
BENZODIAZEPINES
helpful in treating catatonia and mania and may be used in
Benzodiazepines are used most appropriately to treat children and adults. ECT can be administered safely to preg-
time-limited anxiety or insomnia related to an identifiable nant women if fetal monitoring is available. A usual course of
stress or change in sleep cycle. After long-term use (>23 treatment is 6 to 12 sessions given over 2 to 4 weeks.
months), therapy with benzodiazepines and related substances ECT no longer has any absolute contraindications,
should be tapered rather than discontinued abruptly to avoid although it has several relative contraindications related to
relapse, rebound, and withdrawal. anesthesia risks, intracranial space-occupying lesions, and
Relapse is the return of the original anxiety symptoms, increased intracranial pressure. Before ECT is administered,
often after weeks to months. Rebound is the intensification the patient should be assessed for cardiovascular function,
of the original symptoms, which usually last several days and pulmonary function, electrolyte balance, neurologic sta-
appear within hours to days after abrupt cessation of drug tus (eg, history of epilepsy), and previous experiences with
use. Withdrawal includes autonomic and central nervous sys- anesthesia.
tem symptoms that are different from the original presenting
symptoms of the disorder.
Several benzodiazepines have metabolites with long S U M M A RY
half-lives, so smaller doses are needed in the elderly, patients
with cognitive dysfunction, and children. These patient Weight loss, fatigue, feelings of worthlessness, excessive
groups, especially patients with known brain damage, are guilt, loss of interest, and decreased ability to concentrate
prone to paradoxical reactions (anxiety, irritability, aggression, are hallmark symptoms of depression if they last >2 weeks.
agitation, and insomnia). Dysthymia is characterized by disturbed sleep, appetite
changes, low self-esteem, and issues with interpersonal
L IT H IU M relationships for 2 years.
Lithium is used for bipolar disorder and recurrent depression A patient with mania may present with a euphoric mood,
and as an adjunct for depression treatment after ECT. Peak flight of ideas, decreased need for sleep, and unrestrained
levels occur in 1 to 2 hours, and its half-life is about 24 hours; buying sprees.
levels are generally checked 10 to 12 hours after the last dose Patients with chronic pain disorder are preoccupied with
and 4 to 5 days after a dose change. Common side effects pain for 6 months. The pain interferes with normal
include resting tremor, diarrhea, polyuria, polydipsia, thirst, function, but no organic cause is found on careful medical
and nausea (give lithium on a full stomach). Use in the first evaluation.
611
Box 44.1 NEUROLOGIC HISTORY infarction, MRI and CT provide roughly equivalent informa-
tion. Vasculitic lesions or microinfarcts, as in systemic lupus
Temporal profile: When did the symptoms begin? erythematosus, are often seen on MRI but missed on CT.
Acute (seconds to hours) Subacute and chronic intracerebral hemorrhages are better
Subacute (days to weeks) defined by MRI, especially with gradient echo (GRE) MRI,
Chronic (months to years) which is sensitive for acute hemorrhage and old hemosiderin.
Progression: How have the symptoms changed? Magnetic resonance angiography (MRA) is noninvasive
Improving and has replaced standard angiography for many indications.
Static, unchanged, plateaued It is quite sensitive in defining the degree of stenosis in the
Progressive, worsening carotid or vertebrobasilar system. However, MRA does not
Fluctuating adequately evaluate more distal intracranial arteries, and arte-
Episodic, spells riography is required for this indication. MRA is also used as
Character: What are the features of the symptoms? a screening study for aneurysms. Formal angiography still may
Positive symptoms (tremor or other abnormal movements, par- be needed to examine the anatomical details of aneurysms
esthesia, pain, behavioral outbursts) or vascular malformations or when cerebral vasculitis is sus-
Negative symptoms (weakness, incoordination, anesthesia, pected. CT angiography is another sensitive test for determi-
amnesia, or cognitive deficit) nation of vascular disease and anatomical features.
Ill-defined symptoms (fatigue or imbalance, which frequently
have a nonneurologic basis) For evaluating acute hemorrhage in the brain and
subarachnoid space, CT is better than standard MRI.
During evolution of an acute ischemic cerebral infarct,
N E U R O L O G I C D I AG N O S T I C T E S T I N G MRI is better than CT.
For evaluating subacute and chronic stages of an ischemic
C O M P U T E D TO MO G R A P H Y A N D M AG N ET I C
cerebral infarct, CT and MRI are equivalent.
R E S O NA N C E I M AG I N G
MRA and CT angiography are useful noninvasive studies
Vascular Diseases to evaluate for vascular pathology.
Computed tomography (CT) is a good initial test for evaluat-
ing a patient who may have cerebral ischemia (transient isch-
emic attack or stroke) because it can quickly identify acute Trauma
hemorrhage in brain parenchyma or the subarachnoid space MRI is competitive with but not comparable to CT for assess-
(Box 44.3). CT (even with contrast enhancement) often gives ing the brain after craniocerebral trauma. Soon after injury,
equivocal or negative results in the first 24 to 48 hours after an CT is preferable because the examination time is shorter.
ischemic cerebral infarction. In these situations, magnetic res- Standard radiographic examination or CT is necessary to
onance imaging (MRI) is the first neuroimaging test to show evaluate skull fractures because bone cortex is not well visual-
abnormalities during the evolution of an ischemic cerebral ized with MRI.
infarct. With diffusion and perfusion MRI scanning, cere- CT is highly dependable for demonstrating subdural and
bral ischemia can be delineated within minutes of the onset other intracranial hematomas, which are also visualized with
of symptoms, before CT or routine MRI shows any abnor- MRI. Coronal MRI sections are usually best for visualizing the
mality. In subacute and chronic stages of an ischemic cerebral size, shape, location, and extent of subdural hematomas. In trau-
matic brain injury (TBI) patients, conventional MRI can show
changes from diffuse axonal injury that are not visible on CT.
Box 44.2 LOCALIZATION OF NEUROLOGIC
This is often the pathologic substrate for mental status changes
DISORDERS
or coma after head trauma when intracerebral hemorrhage is
excluded. Newer MRI techniques, such as diffusion tensor
Level of nervous system
imaging (DTI), may offer more sensitive assessments of TBI.
Supratentorial (cerebral hemispheres)
In adults and children with TBI, recovery of consciousness
Posterior fossa (brainstem and cerebellum)
is unlikely after 12 months. Recovery is rare after 3 months in
Spinal cord
adults and children with nontraumatic brain injury.
Peripheral (peripheral nerves, neuromuscular junction, &
muscle)
Soon after traumatic head injury, CT of the brain is
Extent of the process
recommended to exclude intracranial hemorrhage and
Focal: Can the symptoms be explained with a single lesion?
skull fracture.
Multifocal: Can the symptoms be explained by multiple lesions
at 1 or more levels? CT is dependable for showing subdural and other
Diffuse: Does widespread dysfunction at 1 or more levels intracranial hematomas.
account for the symptoms?
MRI is most sensitive in detecting diffuse axonal injury.
612 N E U R O L O GY
Table 44.1 FORMULATING A NEUROLOGIC DIFFERENTIAL DIAGNOSIS
PROCESS ACUTE (SECONDS TO HOURS) SUBACUTE (DAYS TO WEEKS) CHRONIC (MONTHS TO YEARS)
Focal Vascular (eg, MCA stroke) Infection (eg, cerebral abscess) Neoplasm (eg, low-grade glioma)
Migrainous Autoinflammatory (eg, multiple sclerosis) Degenerative (eg, carpal tunnel syndrome)
Epilepsy (eg, complex partial seizure)
Diffuse Vascular (eg, SAH) Infection (eg, bacterial meningitis) Degenerative (eg, Alzheimer dementia)
Epilepsy (eg, GTC seizure) Autoinflammatory (eg, Guillain-Barr Metabolic (eg, diabetic sensorimotor
Metabolic (eg, hypoglycemic coma) syndrome) peripheral neuropathy)
Abbreviations: GTC, generalized tonic-clonic; MCA, middle cerebral artery; SAH, subarachnoid hemorrhage.
Intracranial Tumors are often perpendicular to the lateral ventricles). MRI evi-
dence of multiple subcortical ischemic cerebral infarctions
A wide spectrum of intracranial tumors is visualized with may be the cause of adult-onset dementia. However, white
MRI and CT. Often MRI shows more extensive involvement matter changes in the elderly must be interpreted carefully
(of 1 lesion or multiple smaller lesions) than CT, especially because MRI shows some changes in the white matter of most
in gliomas or metastasis. MRI is superior in demonstrating neurologically normal elderly persons.
diseases of the meninges (eg, carcinomatous meningitis). CT
with a contrast agent and MRI with gadolinium are both
MRI is the test of choice in multiple sclerosis, with
excellent for detecting meningiomas. MRI is superior to CT
periventricular white matter lesions (often perpendicular
for identifying all types of posterior fossa tumors and is the
to the lateral ventricles) being the most common finding.
study of choice for identifying brainstem gliomas.
MRI shows some changes in the white matter of most
MRI is favored over CT for the evaluation of tumors neurologically normal elderly persons.
because it shows more anatomical detail and allows
detection of smaller lesions.
MRI is superior to CT for identifying posterior fossa Spinal Cord
tumors and brainstem gliomas. A wide spectrum of lesions at the cervicomedullary junction
and in the spinal cord can be seen more clearly with MRI
because CT of these structures is obscured by bony artifact.
White Matter Lesions Thus, MRI is the study of choice for assessing the cervicomed-
ullary junction and spinal cord. Generally, MRI is better than
MRI is superior to CT in detecting abnormalities of the white CT for identifying intramedullary and extramedullary lesions
matter, as may be seen in multiple sclerosis (in which lesions of the spinal cord. CT can be helpful if bony detail is impor-
are most commonly periventricular white matter lesions and tant (eg, fractures and spurs).
Dementia
CT advantages
Evaluation of suspected acute hemorrhage In assessing dementia, either CT or MRI can demonstrate
Evaluation of skull fractures or bony spine trauma potentially reversible lesions (ie, subdural hematoma, brain
Lower cost tumor, or hydrocephalus), but MRI is more sensitive for deter-
Wider availability mining the presence of multiple infarcts in vascular demen-
MRI advantages tia. MRI can assess atrophy more accurately, especially in the
Evaluation of subacute & chronic hemorrhage mesial temporal lobes, a common finding in Alzheimer dis-
Evaluation of acute ischemic cerebral infarction ease. This is best viewed with thin-slice coronal imaging.
Evaluation of primary & metastatic CNS tumors
Diagnosis of multiple sclerosis
Spine
Evaluation of posterior fossa & brainstem tumors & lesions
Evaluation of the spine & spinal cord Protruding intervertebral disks are well visualized on MRI
Safety (no ionizing radiation) sagittal sections, which show the relation of the disk to the
spine and nerve roots. CT myelography occasionally shows
Abbreviation: CNS, central nervous system.
far lateral disk herniations that are not apparent with MRI, so
4 4 . D I AG N O S I S O F N E U R O L O G I C D I S O R D E R S 613
that there are rare circumstances in which a clear radiculopa- EEG is valuable for evaluating various encephalopathies.
thy with no structural cause evident on MRI would be appar- Some drugs (especially benzodiazepines) cause an unusual fast
ent with CT myelography. pattern, and many metabolic encephalopathies cause a dif-
fuse slow or triphasic pattern. Diffuse slow patterns are seen
MRI is the study of choice for most degenerative spinal also in degenerative cerebral disease (eg, Alzheimer disease).
disorders. Unusual, periodic, high-amplitude sharp wave activity helps
define Creutzfeldt-Jakob disease and subacute sclerosing pan-
encephalitis. EEG is often valuable in diagnosing certain infec-
E L E C T RO MYO G R A P H Y A N D N E RVE tious encephalopathies (eg, herpes simplex encephalitis).
CONDUCTION STUDIES EEG is essential for diagnosing various sleep disorders and
is an adjuvant tool for diagnosing brain death. Brain death is a
Nerve conduction studies (NCS) involve electrically stimulat- clinical diagnosis. EEG may be used as an intraoperative mon-
ing nerves and measuring certain electrophysiologic variables itoring procedure (eg, during carotid endarterectomy).
(amplitude of responses, conduction velocities, and distal By 24 to 48 hours after a hypoxic insult, the EEG assists
latencies). Electromyography (EMG) is performed by inserting in predicting the likelihood of neurologic recovery. Poor out-
a small needle into the muscle and recording electrical activity come is seen with alpha coma, burst suppression, periodic pat-
at rest and with light muscle contraction. These tests are excel- terns, and electrocerebral silence.
lent for identifying diseases of the anterior horn cell, nerve root,
peripheral nerve, neuromuscular junction, or muscle. They also
EEG is valuable in diagnosing certain infectious
assess the large-fiber sensory peripheral nervous system. They
encephalopathies (eg, herpes simplex encephalitis).
give little information, however, on small-fiber function, which
requires specific testing of the autonomic nerves and sweating EEG is an adjuvant tool for diagnosing brain death.
pathways. In addition, EMG does not thoroughly assess type
Brain death is a clinical diagnosis.
2 muscle fibers, which can be affected in myopathies caused
by corticosteroid use or deconditioning. By helping to localize
and to better define further diagnostic studies, EMG and NCS
are an extension of the neurologic examination. LU M BA R P U N C T U R E A N D C E R E B RO S P I NA L
FLU I D A NA LYS I S
NCS and EMG are valuable for identifying neuromuscular
Lumbar puncture should be performed only after a thorough
disorders affecting the anterior horn cell, nerve root,
clinical evaluation and after consideration of the potential
large-fiber sensory peripheral nerve, neuromuscular
value compared with the hazards of the procedure. Imaging of
junction, or muscle.
the brain (CT or MRI) is mandatory if there is any suspicion
NCS and EMG do not exclude small-fiber dysfunction. of a focal cerebral or cerebellar process.
614 N E U R O L O GY
indications in non-Hodgkin lymphoma, and certain neu- Perform lumbar puncture only after a thorough clinical
ropathies (Guillain-Barr syndrome, acute inflammatory evaluation.
demyelinating polyneuropathy, and chronic inflammatory
Increased IgG synthesis and oligoclonal banding in the
demyelinating polyradiculopathy).
CSF are nonspecific findings, but they are most suggestive
Postdural puncture headache occurs in approximately
of multiple sclerosis.
one-third of patients who undergo lumbar puncture. These
headaches relate to some degree to the size of the needle CSF pressure is high in pseudotumor cerebri (idiopathic
used and the leakage of CSF through a dural rent or tear. A intracranial hypertension).
20-gauge needle is recommended.
CSF pressure is low with CSF hypovolemia.
Lumbar puncture is dangerous when an intracranial mass is
Contraindications for Lumbar Puncture present, with or without papilledema.
Suppuration in the skin and deeper tissues overlying the spi- Lumbar puncture is safe in pseudotumor cerebri, and it is
nal canal, anticoagulation therapy, or bleeding diathesis are therapeutic.
contraindications for lumbar puncture. A minimum of 1 to 2
hours should elapse between lumbar puncture and initiation Lumbar puncture aggravates the signs of spinal cord disease
of heparin therapy. If the platelet count is less than 20 109/L, in complete spinal block.
platelets should be transfused before lumbar puncture is per-
formed. The use of aspirin is not a contraindication to lumbar
puncture. Use of other antiplatelet agents, such as clopidogrel, S U M M A RY
may increase the risk of bleeding; if possible to do so safely,
discontinue use of the drug for 5 to 7 days before perform- The history and examination findings suggest localization
ing lumbar puncture. If this is not possible, lumbar puncture to the level and side of the nervous system.
is still safe; we have not found any complications from this The temporal profile is then used to determine a
procedure in patients who are using clopidogrel or aspirin (or differential diagnosis.
both).
Increased intracranial pressure due to a focal intracranial MRI is the study of choice for most degenerative spinal
mass lesion is a contraindication. Lumbar puncture is danger- disorders.
ous when papilledema is due to an intracranial mass, but it is Epilepsy is a clinical diagnosis, not an EEG diagnosis.
safe (and has been used therapeutically) in pseudotumor cere-
bri, in which the increased pressure is diffusely distributed and A normal EEG does not rule out epilepsy.
changes in the pressure due to CSF removal do not increase
CSF pressure is high in pseudotumor cerebri (idiopathic
the risk of cerebral herniation. In complete spinal block or
intracranial hypertension).
stenosis, lumbar puncture may aggravate the signs of spinal
cord disease. CSF pressure is low with CSF hypovolemia.
4 4 . D I AG N O S I S O F N E U R O L O G I C D I S O R D E R S 615
45.
NEUROLOGIC DISORDER S CATEGORIZED BY
ANATOMICAL INVOLVEMENT
Lyell K. Jones Jr, MD, Brian A. Crum, MD, Eduardo E. Benarroch, MD,
616
P E R S I S T E N T VEG ETAT I VE S TAT E (oculocephalic reflexes) and the cold caloric response (oculo-
vestibular reflex), is fully intact, at least early in the disease.
Persistent vegetative state is the absence of cerebral cortex
function with normal brainstem function (deafferentated
state). The patient has no detectable awareness and no pur- Patients with systemic encephalopathies typically have no
poseful interaction with the environment but, unlike a patient focal signs.
in a coma, is wakeful and has sleep-wake cycles.
ACU T E C O N F US I O NA L S TAT E S
L O C K E D -I N S Y N D RO M E Acute confusional state is a manifestation of malfunction of
Locked-in syndrome is characterized by normal cerebral the cerebral cortex and reticular activating system. Acute con-
cortex function with no brainstem function. The lesion usu- fusional states are abrupt, of recent onset, and often associated
ally is in the pons and causes quadriplegia and the inability with fluctuations in the state of awareness and cognition. They
to speak, swallow, and move the eyes horizontally (ie, the are manifested by confusion, inattention, disorientation, and
de-efferentated state). The patient, however, is wakeful and delirium. Thus, patients may be inattentive, dazed, stuporous,
aware but cannot communicate verbally because of the neu- restless, agitated, or excited and may have marked autonomic
rologic deficits. Often, though, these patients can communi- dysfunction and visual and tactile hallucinations. Abnormal
cate with eye blinks and vertical eye movements. This can also motor manifestations are common, including paratonia,
occur with severe neuromuscular weakness, such as in myas- asterixis, tremor, and myoclonus. The usual etiologic factors
thenia gravis, Guillain-Barr syndrome, and botulism. of acute confusional states are toxic, metabolic, traumatic,
or infectious conditions; organ failure of any sort; or ictal or
postictal encephalopathies. Withdrawal states from alcohol,
STUPOR AND COMA benzodiazepines, and barbiturates are also important causes
For a person to stay awake, the cerebral hemispheres and of acute confusion or delirium.
reticular activating system must be intact. Patients with dys-
function of only 1 cerebral hemisphere have a focal neurologic DEMENTIA
deficit but are awake. Patients with a large unilateral cerebral
lesion may go into stupor or coma if the lesion causes shifting Dementia is chronic malfunction of the cerebral cortex or
and pressure changes in other parts of the brain, such as the subcortical structures (or both) with normal function of the
opposite hemisphere or brainstem. These patients can have brainstem. It is a clinical state characterized by a marked loss
focal neurologic signs. Patients with brainstem lesions that of function in multiple cognitive domains and not resulting
directly affect the ascending reticular activating system are in from an impaired level of arousal. Besides memory, other
coma but, again, have focal brainstem signs. Persons who feign higher cognitive functions are impaired, including visuospa-
coma have no focal signs, no abnormal reflexes, normal caloric tial, calculation, language, judgment, personality, and motor
responses, and a normal EEG. They account for a small per- planning. The presence of dementia does not necessarily imply
centage of patients with stupor and coma. The most common, irreversibility, a progressive course, or any specific disease.
potentially reversible causes of stupor and coma are toxic, Dementia is not a disease but an entity with various causes
metabolic, and infectious problems that affect both cerebral (Box 45.1). The most common causes of degenerative demen-
hemispheres diffusely (the famed toxic/metabolic enceph- tia are Alzheimer disease (AD), dementia with Lewy bodies,
alopathy). Thus, most patients in stupor or coma have an and frontotemporal dementias.
underlying systemic problem. A small percentage of patients have reversible causes of
dementia. These include the effects of medications, depression,
thyroid disease, central nervous system (CNS) infections, vita-
Large unilateral cerebral lesions that cause a shift and
min deficiencies, and structural brain lesions (eg, neoplasms,
pressure changes in the other hemisphere or brainstem
subdural hematomas, and symptomatic hydrocephalus).
produce focal neurologic signs together with coma.
Brainstem lesions that cause coma also produce focal signs. Dementia is the potential result of many different diseases,
a minority of which are reversible.
Persons who feign coma have no focal signs, no abnormal
reflexes, normal caloric responses, and a normal EEG.
The most common reversible causes of stupor and coma are
toxic, metabolic, and infectious problems that affect both Alzheimer Disease
cerebral hemispheres diffusely. AD is the most common cause of dementia. Generally, patients
present first with difficulties of memory (anterograde amnesia),
Patients with toxic or metabolic encephalopathies have but eventually difficulties develop in other cognitive domains,
changes in mental status and awareness before going into stu- including aphasia, apraxia, or agnosia. These patients may also
por or coma, but they typically have no focal neurologic signs. have various behavioral and psychiatric manifestations.
Corneal reflexes are lost early in the process, but pupillary Mild cognitive impairment (MCI) consists of loss of mem-
reflexes remain. Ocular motility, tested with the dolls eye sign ory (usually anterograde amnesia) or other cognitive function
618 N E U R O L O GY
Box 45.3 CLASSIFICATION OF SEIZURES and the type of epilepsy are related to age at onset. However,
the cause may not be found in many patients. Neonatal sei-
Partial (focal) seizures zures are often due to congenital defects or prenatal injury, and
Simple partial seizures head trauma is often the cause of focal seizures in young adults.
Partial simple sensory Brain tumors and vascular disease are major known causes of
Partial simple motor seizures in later life. Seizures often occur during withdrawal
Partial simple special sensory (unusual smells or tastes) from alcohol, barbiturates, or benzodiazepines in young and
Speech arrest or unusual vocalizations old adults. Seizures also occur with the use of drugs such as
Complex partial seizures cocaine, usually in young adults. Metabolic derangements
Consciousness impaired at onset (eg, hypoglycemia, hypocalcemia, hyponatremia, and hyper-
Simple partial onset followed by impaired consciousness natremia) can occur at any age, as can infections (eg, menin-
Evolving to generalized tonic-clonic convulsions (secondary gitis and encephalitis). Metabolic abnormalities usually cause
generalized tonic-clonic seizures) primary generalized tonic-clonic seizures and rarely focal or
Simple evolving to generalized tonic-clonic multifocal seizures. CNS infections usually cause partial and
Complex evolving to generalized tonic-clonic (including secondary generalized tonic-clonic seizures.
those with simple partial onset)
True auras (actually, simple partial seizures) Pseudoseizures
Generalized seizuresconvulsive or nonconvulsive (primary gen-
eralized seizuresgeneralized from onset) Psychogenic spells (ie, pseudoseizures or nonepileptic seizures)
Absence and atypical absence are sudden changes in behavior or mentation not associated
Myoclonic with any physiologic cause or abnormal paroxysmal discharge
Clonic of electrical activity from the brain. They are often the cause
Tonic of so-called intractable seizures. Effective treatment is elusive.
Tonic-clonic A favorable outcome may be associated with an independent
Atonic lifestyle, the absence of coexisting epilepsy, and a formal psy-
Unclassified epileptic seizures (includes some neonatal seizures) chologic approach to therapy.
Use of other drugs metabolized in the liver Drugs that do not affect metabolism of other drugs Gabapentin, tiagabine, lamotrigine,
zonisamide, levetiracetam
Avoidance of oral contraceptive pill failure Drugs with no or minimal effect on contraceptive VPA, clonazepam, gabapentin, tiagabine,
metabolism lamotrigine, zonisamide, levetiracetam
Abbreviations: CBZ, carbamazepine; GTCS, generalized tonic-clonic seizure; PB, phenobarbital; PHT, phenytoin; VPA, valproic acid.
620 N E U R O L O GY
Gabapentin has the advantage of fewer drug interactions consequences. In adults, relapse occurs in 26% to 63% of
because it is eliminated primarily by renal excretion. It may patients within 1 to 2 years after therapy is discontinued.
be safer than other anticonvulsants in the management of sei- Predictors of relapse are an abnormal EEG before or during
zures in patients with porphyria. medication withdrawal, abnormal findings on neurologic
Special issues must be considered when managing epilepsy examination, frequent seizures before entering remission,
in pregnancy. Seizure control is attempted first with mono- or mental retardation. To lessen the chance of seizures after
therapy, with the lowest possible dose of anticonvulsant and discontinuing therapy, withdrawal should not proceed faster
monitoring of drug levels. Essentially all anticonvulsant drugs than a 20% reduction in dose every 5 half-lives.
have the potential to cause developmental abnormalities.
Valproic acid and, to a lesser extent, carbamazepine are selec- Anticonvulsant Blood Levels
tively associated with an increased risk of neural tube defects. Measurement of anticonvulsant blood levels is read-
ily available and helps attain the best control of seizures.
The treatment of choice for seizures is monotherapy. It is important to remember that therapeutic levels are
represented by a bell-shaped curve and that patients with
All anticonvulsant drugs have the potential to cause well-controlled seizures are included under the bell-shaped
developmental abnormalities. curve. Seizures are well controlled in many patients who
Valproic acid (and, to a lesser extent, carbamazepine) is have anticonvulsant blood levels below or above the ther-
associated with a higher likelihood of birth defects than apeutic range. The anticonvulsant dose should never be
the other anticonvulsants. changed on the basis of blood levels alone. Remember that
toxicity is a clinical phenomenon, not a laboratory phenom-
enon. Measurement of anticonvulsant blood levels ensures
When to Start and Stop Anticonvulsant Therapy that patients are taking their medication and helps deter-
Decisions about when to start and stop anticonvulsant mine whether new symptoms might be related to toxicity
therapy are difficult and there is simply no easy algorithm from the medication.
on which to rely. The decision to begin anticonvulsant
therapy after a first seizure should be individualized for each Therapeutic levels are represented by a bell-shaped curve.
patient. The decision depends on the risk of additional sei- The dose of anticonvulsant should never be changed on the
zures, the risk of seizure-related injury, the loss of employ- basis of blood levels alone.
ment or driving privileges, and other psychosocial factors.
An important decision is whether a single generalized tonic Toxicity is a clinical phenomenon, not a laboratory
seizure is provoked, for example, by sleep deprivation, alco- phenomenon.
hol, or concurrent illness. After the first seizure, the risk of
recurrence ranges from 30% to 60%, with higher risks for If a patient is receiving therapy for epilepsy and has break-
patients with an abnormal EEG and a remote symptomatic through seizures, several factors should be considered, includ-
cause (Box 45.4). After a second seizure, the risk of recur- ing the following:
rence increases to 80% to 90%.
For many patients who have been seizure free for 1 to 2 1. Compliance issues
years, anticonvulsant therapy can be discontinued. The ben- 2. Excessive use of alcohol or other recreational drugs
efit of discontinuing therapy should be weighed against the
possibility of seizure recurrence and its potential adverse 3. Psychologic and physiologic stress (eg, anxiety or lack of
sleep)
Box 45.4 RISK FACTORS FOR RECURRENCE AFTER THE 4. Systemic disease of any type, organ failure of any type, or
FIRST SEIZURE systemic infection
5. A new cause of seizures (eg, neoplasm)
Age >60 y
No precipitating factor identified (eg, no sleep deprivation or alco- 6. Newly prescribed medication, including other
hol use) anticonvulsants (ie, polypharmacy) and over-the-counter
Partial seizure drugs
Abnormal neurologic examination 7. Toxic levels of anticonvulsants (with definite clinical
Abnormal electroencephalogram (spikes or nonspecific) toxicity)
Abnormal imaging study
Other factors 8. Nonepileptic spells (eg, psychogenic spells)
Family history of seizures (in first-degree relative)
9. Progressive CNS lesion not identified previously with
History of febrile seizures
neuroimaging or lumbar puncture
Onset during sleep
Postictal Todd paralysis
If no cause is found, the anticonvulsant dosage must be
Occupational risk
readjusted or the drug replaced with another.
If status persists after 20 mg/kg of fosphenytoin, give additional drug up to a maximum of 30 mg/kg
If status persists, transfer patient to ICU because intubation, ventilation, or vasopressor may be needed Figure 45.1 Algorithm for the Management of Status
Phenobarbital 20 mg/kg IV, up to 60 mg/min Epilepticus. ECG indicates electrocardiographic; ICU,
If status persists, give general anesthesia with pentobarbital, midazolam, or propofol intensive care unit; IV, intravenous.
Status epilepticus is a medical emergency and a life-threatening Headache may indicate intracranial or systemic disease, but
condition. It can be defined by the duration of the seizure (eg, more commonly it is a primary disorder. Some headaches have
>5 minutes) or by whether repetitive seizures occur without a readily identified organic cause. Classic migraine and cluster
recovery between seizures. The most common causes of sta- headaches form distinctive and easily recognized clinical enti-
tus epilepticus include stopping the use of an anticonvulsant ties, although their pathophysiologic mechanisms are not fully
agent, alcohol toxicity or withdrawal, recreational drug tox- understood. The major challenge is that often neither the loca-
icity, and CNS trauma or infection. Rarely, status epilepticus tion nor the intensity of the pain is a reliable clue to the nature
is the initial presenting sign of epilepsy. The management of of the problem. Episodic tension headache and migraine can
status epilepticus is summarized in Figure 45.1. be difficult to distinguish.
Nonconvulsive status epilepticus may cause an acute con-
fusional state or stupor and coma, especially in the elderly. In Neither location nor intensity of headache pain is a reliable
these cases, there is often very subtle rhythmic motor activity clue to the nature of the problem.
in the limbs or face. EEG is a critical diagnostic tool because
nonconvulsive status epilepticus must be treated as quickly Conditions alerting physicians that a headache may have
and vigorously as convulsive status epilepticus. a serious cause are listed in Box 45.5. Chronic recurrent head-
aches are rarely, if ever, caused by eye strain, chronic sinusitis,
Status epilepticus is a life-threatening medical emergency. dental problems, food allergies, high blood pressure, or tem-
poromandibular joint syndrome. Headache without other
The seizure lasts >5 minutes, or there are repetitive seizures
neurologic signs or symptoms is rarely caused by a brain
without recovery.
tumor. Serious causes of headache in which neuroimaging
Administer 100 mg of thiamine intravenously and then 50 findings may be normal and lead to a false sense of reassurance
mL of 50% dextrose intravenously. are listed in Box 45.6.
Slowly administer lorazepam intravenously.
Any worst headache of my life or headache that is
Antiepileptic treatment should begin with a loading dose maximal at instantaneous onset warrants urgent
of fosphenytoin. evaluation.
Cardiorespiratory monitoring is required if fosphenytoin Headache with abnormal neurologic findings, papilledema,
or phenytoin is infused rapidly. obscuration of vision, or diplopia warrants further
evaluation.
Nonconvulsive status epilepticus may be a cause of acute
confusional state and is manifest with subtle rhythmic Headache without other neurologic signs or symptoms is
motor activity; EEG is required for diagnosis. rarely caused by a brain tumor.
622 N E U R O L O GY
Box 45.5 CONDITIONS INDICATING THAT A Box 45.7 TREATMENT OF MIGRAINE
HEADACHE MAY HAVE A SERIOUS CAUSE
Abortive medications
Worst headache of my life Triptans
Headache that is maximal at instantaneous onset Ergotamine
Headache in a person not prone to headache, especially a Nonsteroidal anti-inflammatory drugs
middle-aged or elderly patient Dihydroergotamine mesylate (DHE-45)
Headache associated with abnormal neurologic findings, papille- Prochlorperazine, metoclopramide, chlorpromazine
dema, obscurations of vision, or diplopia Magnesium sulfate (1.0 g intravenously)
Headache that changes with different positions or increases with Methylprednisolone
exertion, coughing, or sneezing Prophylactic medications
Changes in headache patternscharacter, frequency, or severi- -Blockers
tyin someone who has had chronic recurring headaches Tricyclic antidepressants
Headache that awakens one from sound sleep Valproic acid
Headache associated with trauma Topiramate
Headache associated with systemic symptoms (eg, fever, malaise, Gabapentin
or weight loss) Verapamil
Botulinum toxin type A
624 N E U R O L O GY
Tension headache: A young patient has a 3-year history Migraine and other headaches can become a refractory,
of headaches, which occur almost every month and last intense headache.
several days. They are bilateral and are not associated with
Overuse of medications causes daily headache and prevents
any neurologic deficit, nausea, or vomiting.
the effective action of other drugs.
Cluster headache: A 27-year-old man has a 1-month
Nonsteroidal anti-inflammatory drugs, -blockers, calcium
history of severe, excruciating headaches that occur daily
channel blockers, and tricyclic antidepressants do not cause
and last for approximately 1 hour. He had a similar episode
transformation or withdrawal syndrome.
1 year ago, in which the headache lasted 3 months and
then resolved completely. The pain is unilateral and worse
behind the right eye. The right eye becomes red and teary Trigeminal Neuralgia
during the headache. Patients with trigeminal neuralgia usually have symptoms in
the second or third division of the trigeminal nerve. The idio-
pathic variety occurs in middle-aged and elderly patients and
Analgesic-Overuse Headache is heralded by a sharp, lancinating pain that usually can be trig-
Chronic daily headache may occur de novo, probably as a gered. Chewing, talking, or touching the skin or teeth often
form of tension headache or, more importantly, it may be part precipitates the pain of trigeminal neuralgia, and swallowing
of an evolution from periodic migraine or tension headache. often precipitates the pain of glossopharyngeal neuralgia.
Chronic daily headache is often accompanied by sleep distur- In the elderly, trigeminal neuralgia may be caused by an
bances, depression, anxiety, and overuse of analgesics; most enlarged or tortuous artery (rarely a vein) that compresses the
patients with this disorder have a family history of headache. trigeminal nerve. This can be seen on MRI or magnetic reso-
Episodic migraine and other episodic benign headaches can nance angiography. Importantly, in idiopathic trigeminal neu-
evolve into a daily refractory, intense headache. This syndrome ralgia, sensory and motor functions of the trigeminal nerve are
is usually due to the overuse (>23 days weekly) of ergotamine normal. If there are signs or symptoms other than pain, evalu-
tartrate, triptans, analgesics (especially analgesics combined ate for other compressive lesions (eg, neoplasm). Consider the
with barbiturates), narcotics, and perhaps even benzodiaz- possibility of multiple sclerosis if trigeminal neuralgia occurs in a
epines. To control the headache, the use of these medications young person or if it occurs bilaterally. Treatment options include
has to be discontinued. Two points must be stressed: the over- carbamazepine, phenytoin, baclofen, gabapentin, and clonaze-
use of these medications causes daily headache, and the daily pam. Carbamazepine is the most effective. Surgical treatment
use of these medications prevents other useful medications includes alcohol blocks, radiofrequency ablation of the gasserian
from working effectively. ganglion (cranial nerve [CN] V), Gamma Knife radiosurgery,
The treatment of daily refractory headaches may require and an open craniotomy with microvascular decompression.
hospitalization and withdrawal of the overused medication,
with repetitive intravenous administration of dihydroergot- Chewing, talking, or touching often precipitates
amine together with an antiemetic drug such as metoclopr- pain in trigeminal neuralgia, as does swallowing in
amide or prochlorperazine. glossopharyngeal neuralgia.
-Blockers, calcium channel blockers, and tricyclic anti- In idiopathic trigeminal neuralgia, there should be no
depressants do not cause transformation or withdrawal other neurologic signs or symptoms when the patient is
syndrome. Also, analgesic or rebound headache does not examined during an asymptomatic period.
develop in patients who do not have headache but who take
large amounts of analgesics for other conditions (eg, arthri- Consider multiple sclerosis if trigeminal neuralgia occurs
tis). Simple withdrawal of analgesics produces improvement in a young person or if it is bilateral.
in patients with chronic daily headache. A nonprescription
medication can be withdrawn abruptly. However, prescrip- I N T R AC R A N I A L L E S I O N S
tion medications (eg, ergotamine tartrate, narcotics, and
Leptomeningeal Lesions
barbiturates) must be withdrawn gradually. When narcotics
or compounds containing codeine and ergotamine tartrate Patients with inflammation, infection, or neoplastic inva-
are withdrawn, clonidine may be helpful in repressing with- sion of the leptomeninges may present with similar signs and
drawal symptoms. Some physicians think that even simple symptoms, as follows:
analgesics (eg, aspirin and acetaminophen) taken for more
than 2 to 3 days weekly can cause daily headache syndrome. 1. Cerebralheadache, seizures, and focal neurologic signs
The overuse (>3 days weekly for 2 weeks) of triptan drugs
is now becoming a common cause of medication-overuse 2. Cranial nerveany cranial nerve can be affected,
syndrome. especially CN III, IV, VI, and VII (CN VII is often
affected in Lyme disease)
Chronic daily headache is often accompanied by a family 3. Radicular (radiculoneuropathy or radiculomyelopathy)
history of headache, sleep disturbances, depression, anxiety, neck and back pain as well as radicular pain and spinal
and analgesic overuse. cord signs
CEREBELLAR LESIONS
VEN T R I CU L A R SYST E M
Hydrocephalus Problems with equilibrium and coordination suggest a cerebel-
lar lesion. Lesions of the cerebellar hemisphere usually produce
A combination of signs and symptomsimpaired mental ipsilateral ataxia of the arm and leg. Lesions restricted to the
status, gait disturbance, and urinary problemssuggests anterior superior vermis, as in alcoholism, usually cause ataxia
hydrocephalus. of gait (ie, a wide-based gait and heel-to-shin ataxia), with rela-
Obstructive hydrocephalus (also called noncommunicating tive sparing of the arms, speech, and ocular motility. Lesions of
hydrocephalus) results from an obstructive lesion anywhere in the flocculonodular lobe cause marked difficulty with equilib-
the ventricular system. Patients with the obstructive type may rium and walking but not much difficulty with finger-to-nose
have signs of increased intracranial pressure, including leth- and heel-to-shin tests if the patient is lying down.
argy, nausea, vomiting, and headache; obscurations of vision
are often associated with changes in position.
V E RT I G O A N D D I Z Z I N E S S
Communicating hydrocephalus includes the following 3
types: Accurate visual, vestibular, proprioceptive, tactile, and audi-
tory perceptions are necessary for normal spatial orientation.
1. Hydrocephalus ex vacuoresults from the loss of These inputs are integrated in the brainstem and cerebral
parenchyma, either gray or white matter, and is not hemispheres. The outputs are the cortical, brainstem, and
associated with the signs listed above (if the cause of cerebellar motor systems. The impairment of any of these
hydrocephalus is aging, the neurologic examination functions or their input, integration, or output causes a com-
findings are normal; if the cause is AD, clinical plaint of dizziness (a sensation of altered orientation or
examination shows signs of dementia) space). Dizziness, vertigo, and dysequilibrium are common
complaints. The results of diagnostic tests are often normal.
2. NPHdue to decreased reabsorption of CSF
Diagnosis depends mainly on the medical history, with physi-
3. Hydrocephalus due to overproduction of CSFrare and cal examination findings required in some cases. Vestibular
controversial; supposedly occurs with choroid plexus tests rarely provide an exact diagnosis. The types of dizziness
tumors are listed in Box 45.8.
626 N E U R O L O GY
Box 45.8 TYPES OF DIZZINESS vertigo; they typically present with unilateral hearing loss
and tinnitus. Vertigo frequently occurs in episodes. Common
Vertigo vestibular disorders with a genetic predisposition include
Peripheral migraine, Mnire disease, otosclerosis, neurofibromatosis,
Central and spinocerebellar degeneration.
Presyncopal light-headedness
Orthostatic hypotension Benign Positional Vertigo
Vasovagal attacks Benign positional vertigo (BPV) is the most common
Impaired cardiac output cause of vertigo. Symptoms include brief episodes of vertigo
Hyperventilation that usually last less than 30 seconds with positional change
Psychophysiologic dizziness (eg, turning over in bed, getting in or out of bed, bending over
Acute anxiety and straightening up, and extending the neck to look up).
Agoraphobia (fear & avoidance of being in public places) The usual cause is a misplaced otolith in a semicircular canal.
Chronic anxiety In about half the patients who do not have BPV, no cause is
Dysequilibrium found. For the other half, the most common causes are post-
Lesions of basal ganglia, frontal lobes, & white matter traumatic and postviral neurolabyrinthitis.
Hydrocephalus Typically, bouts of BPV are intermixed with variable peri-
Cerebellar dysfunction ods of remission. Periods of vertigo rarely last longer than
Ocular dizziness 1 minute, although after a flurry of episodes, patients may
High magnification & lens implant complain of more prolonged nonspecific dizziness that lasts
Imbalance in extraocular muscles hours to days (eg, light-headedness or a swimming sensation
Oscillopsia associated with nausea). Management includes reassurance,
Multisensory dizziness positional exercises (ie, vestibular exercises), and the canalith
Physiologic dizziness repositioning maneuver. Drugs are not very useful, but mec-
Motion sickness lizine and promethazine may help with nausea and nonspe-
Space sickness cific dizziness. Rarely, in intractable cases, surgical treatment
Height vertigo (section of the ampullary nerve) may be needed.
Cerebellar Lesions
Vertigo Vertigo of CNS origin is caused by acute cerebellar lesions
(hemorrhages or infarcts) or acute brainstem lesions (espe-
Vertigo is an illusion of movement (usually that of rotation) cially the lateral medullary syndrome [also called Wallenberg
and the feeling of vertical or horizontal rotation of either the syndrome]). Vertebrobasilar arterial disease is also a cause,
person or the environment around the person. Most patients but vertigo by itself is almost never indicative of a transient
report this as spinning or rotational feelings. Others expe- ischemic attack. Other symptoms are necessary to make the
rience mainly a sensation of staggering. In contrast to vertigo, diagnosis of vertebrobasilar insufficiency, such as dysarthria,
dysequilibrium is a feeling of unsteadiness or insecurity about dysphagia, diplopia, facial numbness, crossed syndromes,
the environment, without a rotatory sensation. Vertigo occurs hemiparesis or alternating hemiparesis, ataxia, and visual field
when there is imbalance, especially acute, between the left defects.
and right vestibular systems. The sudden unilateral loss of ves-
tibular function is dramatic; the patient complains of severe
vertigo and nausea and vomiting and is pale and diaphoretic. P R E S Y N C O PA L L I G H T-H E A D E D N E S S
With acute vertigo, the patient also has problems with equilib- Presyncopal light-headedness is best described as the sensation
rium and vision, often described as blurred vision, or diplo- of impending faint. It results from pan cerebral hypoperfusion.
pia. Autonomic symptoms are commonsweating, pallor, Presyncopal light-headedness is not a symptom of focal occlu-
nausea, and vomitingand occasionally can cause vasovagal sive cerebrovascular disease, but it may indicate orthostatic
syncope. hypotension, usually due to decreased blood volume, chronic
use of antihypertensive drugs, or autonomic dysfunction.
M ni re Disease Symptoms of vasovagal attacks are induced when emotions
Fluctuating hearing loss and tinnitus are characteristic of such as fear and anxiety activate medullary vasodepressor cen-
Mnire disease. Abrupt complete unilateral deafness and ters. Vasodepressor episodes can also be precipitated by acute
vertigo occur with viral involvement of the labyrinth or CN visceral pain or sudden severe attacks of vertigo. Impaired
VIII (or both) and with ischemia of the inner ear. Patients cardiac output causes presyncopal light-headedness, as does
who slowly lose vestibular function bilaterally, as may happen hyperventilation. Chronic anxiety with associated hyperven-
with the use of ototoxic drugs, often do not complain of ver- tilation is the most common cause of persistent presyncopal
tigo but have oscillopsia with head movements and instability light-headedness in young patients. In most persons, a moder-
with walking. Even if unilateral vestibular loss occurs slowly ate increase in respiratory rate can decrease the Paco2 level to
(eg, acoustic neuroma), patients usually do not complain of 25 mm Hg or less in a few minutes.
628 N E U R O L O GY
noted. The findings on examination include limb weakness, Many drugs have been studied, including gabapentin, lamotrig-
spasticity, and increased muscle stretch reflexes below the level ine, insulinlike growth factor 1 (IGF-1), celecoxib, and lithium,
of the lesion. Extensor plantar reflexes (Babinski signs) may but none have shown a benefit. Treatment of ALS focuses on
also be elicited. Sensory findings are often noted. rehabilitation issues, nutrition, mobility, and communication; a
The most common noncompressive lesion is transverse multidisciplinary approach is useful. Many agents hold promise
myelitis, usually of unknown cause. Some patients have a his- and are being studied, including stem cells, although no clear
tory of vaccination or symptoms suggestive of viral disease that indication exists for their use outside of a clinical trial.
usually precede the neurologic symptoms by a few days to 1 or 2
weeks. Up to 50% of these patients have antibodies, which were
described from patients with neuromyelitis optica (NMO), to Multifocal Motor Neuropathy
a water aquaporin channel (NMO IgG). They have recurrent Multifocal motor neuropathy is a rare syndrome of purely lower
episodes of severe myelitis and optic neuritis; consequently, motor neuron weakness that can mimic ALS. Treatment of mul-
long-term immunomodulatory therapy is usually indicated. tifocal motor neuropathy with intravenous immunoglobulin
Compressive myelopathy is commonly due to degenera- (IVIG) can be very effective in slowing the progression of weak-
tive spine or disk disease or to metastatic epidural neoplasm. ness. It is often distal and asymmetrical, accompanied by motor
The patients usually present with local vertebral column pain conduction block on nerve conduction studies (NCS) and elec-
at the level of the spinal cord lesion. This symptom is pres- tromyography (EMG), and may be associated with high titers
ent for weeks to months before the gross neurologic deficits of serum antibodies to GM1 gangliosides. Kennedy disease (or
occur, although occasionally bony pain may antedate other spinobulbar muscular atrophy) is a pure lower motor neuron
symptoms by only a few hours. degenerative process that is X-linked and caused by an excess
of CAG repeats in the androgen receptor gene. This most com-
Upper motor neuron pattern muscle weakness may be monly affects elderly men and also leads to gynecomastia, diabe-
associated with a compressive or noncompressive spinal tes mellitus, and a sensory peripheral neuropathy. Genetic testing
cord lesion. is widely available. There is no effective treatment, although the
Transverse myelitis is the most common noncompressive disease is much more slowly progressive than ALS.
lesion.
R A D I CU L O PAT H Y
M OTO R N EU RO N D I S E A S E
Nerve root lesions usually are indicated by pain that is often
Amyotrophic Lateral Sclerosis sharp and lancinating, follows a dermatomal or myotomal
pattern, and is increased by increasing intraspinal pressure
Degenerative disorders that affect the motor neurons in the (eg, sneezing and coughing) or by stretching of the nerve
cerebral cortex and the anterior horn cells are called motor neu- root. Paresthesias and pain occur in a dermatomal pattern.
ron diseases. The most common is amyotrophic lateral sclerosis Findings are in the root distribution and include weakness,
(ALS). This disorder should be considered in any patient who sensory impairment, and decreased muscle stretch reflexes.
has progressive, painless weakness. Typically, patients present Radiculopathies have many causes, including compressive
with asymmetric weakness that begins distally and is associated lesions (eg, osteophytes, ruptured disks, and neoplasms) and
with cramps and fasciculations. Footdrop and hand weakness noncompressive lesions (eg, postinfectious and inflammatory
are the most common first complaints. Often the initial (but radiculopathies and metabolic radiculopathies, as in diabetes).
incorrect) diagnosis is stroke, radiculopathy, carpal tunnel syn- Indications for emergent neurologic and neurosurgical consul-
drome, or ulnar neuropathy. The diagnosis is often delayed. tation are increasing weakness, bowel or bladder dysfunction,
Bulbar weakness (eg, dysarthria and dysphagia) can be the pre- or intractable pain with an appropriate lesion seen on MRI.
senting problem and is always eventually present. Bowel and Large disk protrusions can cause minimal symptoms and are
bladder difficulties are very uncommon, and sensory abnor- not by themselves grounds for urgent surgical intervention.
malities are rare. Findings on examination include weakness,
atrophy, fasciculations, spasticity, and abnormal muscle stretch Nerve root lesions are indicated by sharp, lancinating pain
reflexes and extensor plantar responses. The hallmark is the with a dermatomal or myotomal pattern.
mixture of both upper and lower motor neuron signs. Because
of the progressive weakness affecting the limbs, bulbar muscles, Pain is increased by sneezing and coughing.
and diaphragm, the disease is devastating, and patients have an Pain often has a dermatomal pattern.
average life span of about 3 years after the onset of symptoms.
ALS is sporadic in 80% to 90% of cases. In those that are Findings are weakness, sensory impairment, and decreased
familial, 10% of the patients harbor a mutation in the oxygen muscle stretch reflexes.
radical detoxifying enzyme superoxide dismutase (SOD-1). No
Radiculopathies have many causes.
drug has been found to be effective in reversing the progressive
course of this disease. Some beneficial effect has been noted Surgery is considered for increasing weakness, bowel
with riluzole, especially in patients with bulbar onset of the or bladder dysfunction, or intractable pain with an
disease. This drug prolongs ventilator-free survival by 3 months. appropriate lesion seen on MRI.
3. The symptoms are usually bilateral but can be Mononeuropathy multiplex Diabetes mellitus
asymmetrical or unilateral Vasculitis
Lyme disease
4. The pain usually has a dull, aching quality HIV neuropathy
Sarcoidosis
5. The whole lower extremity is generally involved Leprosy
Multifocal motor neuropathy
6. The pain is provoked while walking or standing HNPP
7. Sitting or leaning forward provides relief Acute motor AIDP (Guillain-Barr
polyradiculoneuropathy syndrome)
8. There is often a dead feeling in the legs. Lyme disease
HIV neuropathy
Bicycling causes little or no pain, unlike with vascular clau- Porphyria
dication. Decompressive operations for lumbar stenosis can Toxins (arsenic, thallium)
Carcinomatous or lymphomatous
be performed with low morbidity despite the advanced age of meningitis
most patients. A very high initial success rate can be expected,
although about 25% of patients become symptomatic again (Continued)
630 N E U R O L O GY
Table 45.4 (CONTINUED) Box 45.9 EVALUATION OF PERIPHERAL NEUROPATHY
PATTERN OF COMMON OR IMPORTANT
NEUROPATHY CAUSES Basic laboratory investigations
CBC with platelets
Chronic motor or sensorimotor CIDP
polyradiculopathy Paraproteinemia (eg, osteoscle-
Erythrocyte sedimentation rate
rotic myeloma) Fasting blood glucose
Hereditary neuropathy (eg, Serum electrolytes
Charcot-Marie-Tooth Serum creatinine
disease) Liver function tests
Lead toxicity
Diabetes mellitus
Serum & urine electrophoresis & immunoelectrophoresis
Amyloidosis Urinalysis
Chest radiography
Length-dependent distal Diabetes mellitus Electromyography
(stocking-and-glove) Alcoholism
sensorimotor neuropathy Uremia
Special investigations
Toxins (hexacarbons) Thyroid function test
Hereditary neuropathy Vitamin B12
Vitamin B12 deficiency Vitamin E
Hypothyroidism Cholesterol & triglycerides
Gluten sensitivity
Copper deficiency
HIV serology
Lyme serology
Sensory ataxic neuropathy Sjgren syndrome Hepatitis serology
Paraneoplastic disorder Cryoglobulins
Diabetes mellitus
Paraproteinemia
Angiotensin-converting enzyme
Vitamin B12 deficiency Antineutrophil cytoplasmic antibodies
HIV infection Antinuclear antibodies
Cisplatin Antibodies against extractable nuclear antigens
Vitamin B6 excess Gliadin antibodies, endomysial & tissue transglutaminase
Hereditary neuropathy
antibodies
Painful peripheral neuropathy Diabetes mellitus Paraneoplastic antibodies
Vasculitis GM1 antibodies
Hereditary amyloidosis Porphyrins
Toxins (arsenic, thallium)
Hepatitis C
Heavy metal screen
Cryoglobulinemia Serum copper & ceruloplasmin
HIV neuropathy Investigations in selected cases
CMV polyradiculoneuropathy in Autonomic function tests
HIV-positive patients Cerebrospinal fluid analysis
Alcoholism
Fabry disease
Sural nerve biopsy
Investigation for inborn errors of metabolism
Neuropathy with prominent auto- Acute or subacute Genetic studies
nomic involvement Guillain-Barr syndrome MRI of nerve roots or plexus
Subacute pandysautonomia
Paraneoplastic Abbreviations: CBC, complete blood cell count; HIV, human immunodefi-
pandysautonomia ciency virus; MRI, magnetic resonance imaging.
Porphyria
Vincristine neuropathy
Botulism
hereditary neuropathy. Also, examination or close questioning
Chronic of family members may secure a diagnosis.
Diabetes mellitus
Amyloidosis
Sjgren syndrome The pattern of neuropathy and the time course suggest the
cause.
Abbreviations: AIDP, acute inflammatory demyelinating polyradiculoneuropathy;
CIDP, chronic inflammatory demyelinating polyradiculoneuropathy; CMV, cyto- Peripheral neuropathy: distal weakness and sensory
megalovirus; HIV, human immunodeficiency virus; HNPP, hereditary neuropathy changes more in the legs than in the arms, usually
with liability to pressure palsies.
symmetrical, and with distal muscle stretch reflexes
impaired or absent.
cases of idiopathic neuropathy referred to specialty centers
are in fact hereditary neuropathies. On examination, the find- The cause of peripheral neuropathy is usually found in
ing of high arches (ie, pes cavus) or fallen arches (ie, pes planus) 70%-80% of cases; hereditary causes may explain many
with hammertoe deformities is a clue to a long-standing or cases of idiopathic neuropathy.
632 N E U R O L O GY
are useful when these agents are not useful or when they lead a microvasculitis of the nerve. Patients with diabetes (often
to side effects include carbamazepine, lidocaine patch (5%), mild and well controlled) may have bilateral proximal and
narcotics, lamotrigine, mexiletine, and venlafaxine. pelvic girdle weakness, wasting, weight loss, and autonomic
dysfunction. A course of intravenous corticosteroids may
speed the recovery.
Autonomic Neuropathy
Neuropathy with autonomic dysfunction (eg, orthostatic Neuromuscular Transmission Disorders
hypotension, urinary bladder and bowel dysfunction, and
impotence) suggests Guillain-Barr syndrome, acute pan- Patients with neuromuscular transmission disorders (classi-
dysautonomia, paraneoplastic dysautonomia, porphyria, dia- cally, myasthenia gravis) present with fluctuating weakness
betes mellitus, amyloidosis, or familial neuropathy. manifested as fatigable weakness in the limbs, eyelids (ie,
Acute pandysautonomia is a heterogeneous, monopha- ptosis), tongue and palate (ie, dysarthria and dysphagia), and
sic, usually self-limiting disease that involves the sympa- extraocular muscles (ie, diplopia). Sensation, muscle tone, and
thetic and parasympathetic nervous systems. It may produce reflexes usually are normal except in Lambert-Eaton myas-
orthostatic hypotension, anhydrosis, diarrhea, constipation, thenic syndrome (LEMS), in which the weakness is more
urinary bladder atony, and impotence. The syndrome usu- constant and the reflexes are diminished. Drugs may cause
ally evolves over a few days to a few months, with a recov- problems at neuromuscular junctions; for example, penicilla-
ery that is generally prolonged and partial. This may be mine can cause a syndrome that appears similar to myasthenia
an immunologic disorder, but it is indistinguishable from gravis. Three major clinical syndromes of the neuromuscular
paraneoplastic autonomic neuropathy. Some patients may junction are myasthenia gravis, LEMS, and botulism. Several
have antibodies against the ganglion-type nicotinic ace- drugs adversely affect neuromuscular transmission and may
tylcholine receptor. IVIG treatment limits the duration exacerbate weakness in these disorders. They include amino-
and reduces the long-term disability of patients with acute glycoside antibiotics, quinine, quinidine, procainamide,
pandysautonomia. propranolol, calcium channel blockers, and iodinated radio-
contrast agents.
Motor polyneuropathy: inflammatory demyelinating
polyradiculoneuropathy, hereditary neuropathy, Myasthenia Gravis
osteosclerotic myeloma, porphyria, and lead poisoning. Myasthenia gravis (MG) usually occurs in young women
and older men and is often heralded by such cranial nerve
Sensory polyneuropathy: diabetes mellitus, paraneoplastic findings as diplopia, dysarthria, dysphagia, and dyspnea.
disorder, Sjgren syndrome, dysproteinemias, HIV The deficits are usually fatigable, worsening with repetition
infection, vitamin B12 deficiency, cisplatin toxicity, vitamin or late in the day. However, muscle stretch reflexes, sensa-
B6 excess, and some hereditary neuropathies. tion, mentation, and sphincter function are normal. The
Neuropathy with autonomic dysfunction: amyloidosis, diagnosis of MG is based on the detection of nicotinic
diabetes mellitus, Guillain-Barr syndrome, porphyria, and acetylcholine receptor antibodies and the presence of dec-
some familial neuropathies. remental responses to repetitive electrical stimulation of
motor nerves. Administration of a short-acting acetylcho-
line esterase inhibitor (eg, edrophonium) can immediately
Diabetic Neuropathy reverse weakness due to MG; this can be used as a diagnostic
Diabetes mellitus may cause CN III neuropathy. Affected test. Acetylcholine receptor antibodies are rare in conditions
patients usually present with sudden diplopia, eye pain, impair- other than MG (ie, they do not occur in patients with con-
ment of the muscles supplied by CN III, and relative sparing of genital MG and they occur in only about 50% of those with
the pupil. With compressive CN III lesions, the pupil usually purely ocular MG). Striational antibodies are highly associ-
is involved early. Painful diabetic neuropathies include CN III ated with thymoma in younger patients and sometimes occur
neuropathy, acute thoracoabdominal (ie, truncal) neuropathy, in LEMS or small cell lung carcinoma. They can occur in
acute distal sensory neuropathy, acute lumbar radiculoplex- penicillamine recipients, bone marrow allografts, and auto-
opathy, and chronic distal small-fiber neuropathy. immune liver disorders. Some myasthenic patients without
acetylcholine receptor antibodies have muscle-specific kinase
Diabetes mellitus may cause CN III neuropathy, often with (MuSK) antibodies that are also diagnostic for MG. These
relative sparing of the pupil. patients may have more severe weakness, often bulbar, and
may be more resistant to treatments. Of the 30% of patients
The pupil is involved early in compression of CN III. who have MG without acetylcholine receptor antibodies,
half have antibodies to MuSK.
Acute or subacute muscle weakness can occur in vari- Treatment strategies for MG include the use of anticho-
ous forms of diabetic neuropathy. Weakness, atrophy, and linesterase and immunomodulatory agents. Cholinesterase
pain affect the pelvic girdle and thigh muscles (asymmetri- inhibitors, such as pyridostigmine bromide, are often given
cal or unilateraldiabetic amyotrophy). This has been as initial therapy for MG. This therapy provides symp-
termed diabetic polyradiculoplexus neuropathy and is due to tomatic improvement for most patients. Thymectomy
634 N E U R O L O GY
Box 45.10 CLASSIFICATION OF MYOPATHIES Acute Alcoholic Myopathy
Patients with acute alcoholic myopathy have acute pain, swell-
Dystrophic myopathies (childhood or adult onset, progressive) ing, tenderness, and weakness of mainly proximal muscles.
Congenital myopathies (congenital onset; slowly progressive or Gross myoglobinuria may cause renal failure.
nonprogressive)
Inflammatory myopathies Gross myoglobinuria often occurs in acute alcoholic
Infectious & viraltoxoplasmosis, trichinosis myopathy.
Granulomatoussarcoidosis
Idiopathicpolymyositis, dermatomyositis, IBM
Inflammatory myopathy with collagen vascular disease Statin-Induced Myopathy
Metabolic myopathies
Statin drugs (HMG-CoA reductase inhibitors) may produce
Glycogenoses
an acute necrotizing myopathy characterized by myalgia,
Mitochondrial disorders
weakness, myoglobinuria, and a marked increase in creatine
Defects of fatty acid oxidation
kinase. This toxic effect is potentiated by fibric acidderivative
Endocrinopathy
drugs and cyclosporine. A more subacute to chronic myo-
Periodic paralyses
pathy can also occur with statins. Symptoms of cramps and
Toxicstatin drugs, emetine, chloroquine, vincristine
myalgias can occur, occasionally with little or no muscle weak-
Miscellaneous
ness or creatine kinase elevation. How soon symptoms abate
Amyloidosis
after discontinuing use of the drug is unknown, although 3 to
Abbreviation: IBM, inclusion body myositis. 6 months may be needed. It is also likely that in some patients
statins unmask a presymptomatic acquired or genetic myopa-
thy. The myopathic symptoms persist in some patients even
Prednisone is the cornerstone for treatment of other after they discontinue the use of the statin medication.
inflammatory myopathies such as polymyositis and dermato-
myositis. The most common pitfall in treating these conditions Electrolyte Imbalance
is treating with doses of prednisone that are too low and are
given for an insufficient time. Dermatomyositis, unlike IBM Severe hypokalemia (<2.5 mEq/L) and hyperkalemia (>7
or polymyositis, responds to IVIG. In both polymyositis and mEq/L) produce muscle weakness, as do hypercalcemia,
dermatomyositis, other immunomodulatory agents (includ- hypocalcemia, and hypophosphatemia. Familial periodic
ing azathioprine, methotrexate, mycophenolate mofetil, paralysis of the hypokalemic, hyperkalemic, or normokalemic
cyclosporine, cyclophosphamide, and chlorambucil) are type consists of episodes of acute paralysis that last 2 to 24
indicated if relapse occurs while the prednisone dose is being hours and can be precipitated by a carbohydrate-rich meal or
tapered, if unacceptable side effects develop from prednisone, strenuous exercise; cranial or respiratory muscle paralysis does
or if there is no response to prednisone or the response is slow. not occur. The diagnosis is difficult to make and is based on
Plasma exchange is ineffective for polymyositis, dermatomyo- the potassium levels during an attack, family history, EMG,
sitis, and inclusion body myositis. A regular exercise program and, occasionally, genetic testing for certain sodium and cal-
is important, and it has been shown that physical therapy and cium channel mutations.
exercise are not detrimental to patients with myopathies.
Endocrine Diseases
Myopathy refers to muscle disease.
Hyperthyroidism and hypothyroidism, hyperadrenalism and
If the disease is progressive and genetic, it is called hypoadrenalism, acromegaly, and primary and secondary
dystrophy. hyperparathyroidism cause muscle weakness.
Myotonic dystrophy: atrophy and weakness begin in the
face and sternocleidomastoid muscles.
ACU T E MUS C L E WE A K N E S S
Myotonia (ie, normal contraction with slow relaxation) is
a feature of myotonic dystrophy; a patient with myotonia Physicians may overlook serious underlying diseases in
cannot let go quickly during a handshake. patients whose chief or only complaint is weakness, espe-
cially if there are few or no obvious clinical signs. A delayed
Acquired myopathy: no underlying cause is found in many or missed diagnosis can lead to life-threatening complications,
adults. such as respiratory failure, irreversible spinal cord dysfunc-
tion, and acute renal failure. In some patients with neuromus-
Patients with dermatomyositis: increased incidence of
cular weakness, respiratory muscles may be affected, although
occult carcinoma.
strength in the extremities is relatively normal. Patients with
Causes of myopathies: collagen vascular disease, early Guillain-Barr syndrome may have distal paresthesias
paraneoplastic changes, amyloidosis, endocrinopathy, and increased respiratory effort and be given the diagnosis of
sarcoidosis. hysterical hyperventilation.
636 N E U R O L O GY
46.
NEUROLOGIC DISORDER S CATEGORIZED
BY MECHANISM
Lyell K. Jones Jr, MD, Brian A. Crum, MD, Eduardo E. Benarroch, MD,
The causes of ischemic cerebrovascular disorders, including In young adults, illicit drug use is a risk factor for stroke.
transient ischemic attack (TIA) and cerebral infarction, can
be classified according to the site of the source for the arterial
blockage within the vascular system, from most proximal to Risk Factors
distal: Risk factors for atherosclerotic occlusive disease are similar
to those for coronary artery disease: hypertension, male sex,
1. Cardiac source (most proximal source of emboli): advanced age, cigarette smoking, diabetes mellitus, and hypercho-
arrhythmias and structural disease (eg, valve disease, lesterolemia. Emboli from intracardiac mural thrombi also cause
dilated cardiomyopathy, recent myocardial infarction); TIA and cerebral infarction. Proven cardiac risk factors are atrial
paradoxical emboli with a right-to-left shunt through a fibrillation (including paroxysmal atrial fibrillation), atrial flutter,
patent foramen ovale (PFO), although most patients with dilated cardiomyopathy, mechanical valve, rheumatic valve dis-
PFO are asymptomatic; the aorta ease, recent myocardial infarction, and others (Box 46.1).
2. Large-vessel disorders: most commonly atherosclerosis or Hypertension is the most important modifiable risk factor
dissection in the carotid or vertebrobasilar system for stroke, but other modifiable risk factors include cigarette
smoking, diabetes mellitus, hypercholesterolemia, metabolic
3. Small-vessel occlusive disease: inflammatory syndrome, sedentary lifestyle, obesity, obstructive sleep apnea,
or noninflammatory arteriopathies (eg, and, possibly, elevated homocysteine levels. Although low lev-
hypertension-induced disease, isolated central els of alcohol consumption appear to have a protective effect
637
Box 46.1 CARDIAC RISK FACTORS FOR CEREBRAL Carotid Endarterectomy and Carotid Angioplasty With
INFARCTION OR TRANSIENT ISCHEMIC ATTACK Stent Placement
Carotid endarterectomy markedly decreases the risk of stroke
Proven cardiac risk factors and death of symptomatic patients who have a 70% to 99%
Atrial fibrillation stenosis of the carotid artery. For a 50% to 69% stenosis,
Paroxysmal atrial fibrillation carotid endarterectomy is moderately efficacious in selected
Atrial flutter symptomatic patients. Medical treatment alone is better than
Dilated cardiomyopathy carotid endarterectomy for patients with a stenosis of 49% or
Mechanical valve less. Symptoms must be those of a carotid territory TIA or
Rheumatic valve disease minor stroke and must be of recent onset (<4 months). To
Recent (within 1 mo) myocardial infarction have a favorable risk-benefit ratio, the perioperative complica-
Intracardiac thrombus tion rate must be low (<6%).
Intracardiac mass (ie, atrial myxoma or papillary fibroelastoma) Carotid angioplasty with stent placement may be used
Infectious endocarditis as an alternative to carotid endarterectomy, particularly for
Nonbacterial thrombotic endocarditis high-risk patients, such as those who previously had carotid
Putative or uncertain cardiac risk factors endarterectomy, radiotherapy to the neck, or neck dissection;
Sick sinus syndrome those with a stenosis high in the internal carotid artery; or
Patent foramen ovale with or without atrial septal aneurysm those otherwise deemed at high risk for the operation. The
Atherosclerotic debris in the thoracic aorta safety and durability of the endovascular approach compared
Spontaneous echocardiographic contrast with endarterectomy are not clear, and the available data are
Myocardial infarction 26 mo earlier somewhat conflicting.
Hypokinetic or akinetic left ventricular segment Selected patients with an asymptomatic carotid stenosis of
Calcification of mitral annulus at least 60% benefit from carotid endarterectomy (ie, they have
a decreased risk of future ipsilateral stroke or related death).
for ischemic stroke, heavy alcohol consumption increases a In the Asymptomatic Carotid Atherosclerosis Study (ACAS),
persons risk for all types of stroke, particularly intracerebral medical patients were treated with aspirin and risk-factor reduc-
and subarachnoid hemorrhage. tion therapy. The risk of stroke was low for patients treated
surgically and for those treated medically (5-year risk of ipsi-
Transient Ischemic Attacks lateral stroke or death was 11% for those treated medically and
6% for those treated surgically). No trend was noted among
Patients who experience TIA are at high risk for subsequent the various degrees of stenosis, but the number of events was
cerebral infarctions: 4% to 10% within 1 year to 33% within the small in each stenosis subdivision. Surgeons and hospitals were
patients lifetime. Most TIAs last less than 15 minutes; about chosen for having reported perioperative complication rates of
90% resolve within 1 hour. Patients with cerebral infarcts, less than 3% in asymptomatic patients. In the Asymptomatic
hemorrhages, and mass lesions can present with symptoms Carotid Surgery Trial, the efficacy of surgery was similar to
like those of TIAs. that noted in the ACAS trial outlined above. The primary end
Amaurosis fugax is defined as temporary, partial, or com- point was ipsilateral stroke or any perioperative stroke or death
plete monocular blindness and is a classic symptom of carotid (within 30 days of the procedure or entry into the study). The
artery TIA. Glaucoma, vitreous hemorrhage, retinal detach- risk was 12% over 5 years among patients treated medically
ment, papilledema, migrainous aura, temporal arteritis, and and 6.4% among patients receiving surgical management.
even ectopic floaters can mimic amaurosis fugax. Patients with asymptomatic carotid occlusive disease who
The long-term prognosis for patients who have TIA gener- require an operation for another reason (eg, coronary artery
ally follows the rule of 3s: one-third will have cerebral infarc- bypass graft or abdominal aortic aneurysm repair) usually can
tion, one-third will have at least 1 more TIA, and one-third have that procedure performed without prophylactic carotid
will have no more TIAs. The following features help to deter- endarterectomy, because in this context the risk of stroke in
mine the risk of stroke after TIA: age older than 60 years, asymptomatic persons is quite low. For patients with symptoms
hypertension, weakness or speech disturbance with TIA, TIA in the distribution of a stenotic carotid artery, the decision is
duration more than 60 minutes, and diabetes mellitus. more complicated. Generally, if a patient with an asympto-
matic carotid stenosis has cardiac symptoms (eg, angina), coro-
Most TIAs last <15 minutes. nary artery bypass grafting or angioplasty is performed first and
carotid endarterectomy or angioplasty with stent placement is
Patients with cerebral infarcts, hemorrhages, and mass
performed if the patient is otherwise a good surgical candidate.
lesions can present with symptoms like those of TIA.
Amaurosis fugax is a classic symptom of carotid artery TIA.
Antiplatelet Agents
The rule of 3s for patients with TIA: one-third will have
cerebral infarction, one-third will have 1 more TIA, and Aspirin, aspirin in combination with extended-release
one-third will have no more TIAs. dipyridamole, and clopidogrel are all effective for secondary
638 N E U R O L O GY
prevention of stroke. The optimal dose of aspirin is uncer- intracranial hemorrhage, mass effect, early evidence of signifi-
tain, with ranges recommended from 30 to 1,300 mg daily. cant cerebral infarction (greater than one-third distribution
Clopidogrel is given as a single dose, 75 mg daily. A combina- of the cerebral hemisphere), or midline shift. Patients may be
tion of low-dose aspirin and extended-release dipyridamole excluded by the following clinical criteria: rapidly improving
is well tolerated and provides another useful alternative to deficit, obtunded or comatose status or presentation with sei-
aspirin for prevention of stroke. The combination may be zure, history of intracranial hemorrhage or bleeding diathesis,
slightly more effective than aspirin alone in secondary stroke blood pressure elevation persistently greater than 185/110 mm
prevention. Hg, gastrointestinal tract hemorrhage or urinary tract hemor-
Ticlopidine is also an effective antiplatelet agent, but it is rhage within the previous 21 days, traumatic brain injury or
rarely given now because of associated neutropenia (thus, a com- cerebral infarction within 3 months, or mild deficit. Eligible
plete blood cell count must be monitored every 2 weeks for the patients should have marked weakness in at least 1 limb or
first 3 months of treatment) and thrombotic thrombocytopenic severe aphasia. Laboratory abnormalities that may preclude
purpura, which has rarely been reported with clopidogrel. treatment are heparin use within the previous 48 hours with
There is evidence that the use of clopidogrel in combi- an increased activated partial thromboplastin time, interna-
nation with aspirin does not provide additional prevention tional normalized ratio (INR) greater than 1.5, or blood glu-
for ischemic stroke but does increase the risk of significant cose concentration less than 50 mg/dL.
bleeding; therefore, the combination is not commonly used In a treatment trial of intravenous tPA, the efficacy in
for stroke prevention. When clopidogrel was compared with improving neurologic status at 3 months was defined for tPA
aspirin in combination with extended-release dipyridamole compared with placebo, with the agent administered within
for the secondary prevention of stroke in a large randomized 3 hours after the onset of symptoms. Although a greater pro-
clinical trial, the study did not demonstrate any difference in portion (about 12% greater) of subjects in the tPA group had
effectiveness. minimal or no deficit at 3 months after the event, there was no
increase in the proportion of persons who died. This is partic-
ularly important because there was an increased occurrence of
Warfarin symptomatic hemorrhage in the tPA group (6.4% compared
Warfarin is used for secondary prevention in selected patients with 0.6%).
who have TIA or cerebral infarction and 1) specific cardiac Intravenous tPA should be given in a 0.9-mg/kg dose
sources of embolus (eg, atrial fibrillation, left atrial or ven- (maximum, 90 mg), with 10% given as a bolus and the rest
tricular clot, dilated cardiomyopathy with markedly reduced over 60 minutes.
ejection fraction, mechanical heart valves, recent myocardial
infarction with left ventricular thrombus, valvular thrombus) Intravenous tPA should be considered for patients
or 2) hypercoagulable states. Warfarin may also be recom- evaluated within 3 hours after the onset of symptoms of
mended for patients with TIA or cerebral infarction and aor- severe cerebral infarction.
tic arch thrombus and for those with extracranial dissection;
Do not treat with tPA if CT shows hemorrhage, mass
no clinical trial data support this treatment approach, though,
effect, or midline shift.
and aspirin is sometimes recommended for these conditions
instead of warfarin. In a clinical trial with patients who had
symptomatic intracranial stenosis, warfarin was not more
Stroke Risks With Nonvalvular Atrial Fibrillation
effective than aspirin in reducing ischemic stroke risk and was
associated with a higher risk of hemorrhage. Atrial fibrillation is associated with up to 24% of ischemic
strokes and 50% of embolic strokes. The stroke rate for the
entire cohort of patients with chronic atrial fibrillation is gen-
Management of Acute Cerebral Infarction
erally about 5% per year. However, patients younger than 60
If a patient has a severe neurologic deficit caused by an acute with lone atrial fibrillation have a lower risk for stroke than
cerebral infarction, the immediate decision in the emergency other patients with atrial fibrillation and are often treated
department is whether the patient is a candidate for throm- with only aspirin, depending on their CHADS2 score (con-
bolytic therapy (tissue plasminogen activator [tPA]). The initial gestive heart failure, hypertension, age >75 years, diabetes
therapeutic approach to ischemic infarction depends greatly on mellitus, and previous stroke) (see Table 2.8). Stroke risk fac-
the time from the onset of symptoms to the presentation for tors with atrial fibrillation include a history of hypertension,
emergency medical care. If the onset of symptoms was less than recent congestive heart failure, previous thromboembolism
3 hours before the evaluation, emergent thrombolytic therapy (including TIAs), left ventricular dysfunction identified on
should be considered. If a patient awakens from sleep with the 2-dimensional echocardiography, and increased size of the left
deficit, thrombolytic therapy should not be considered unless atrium identified on M-mode echocardiography. Patients with
the duration of the deficit is clearly less than 3 hours. Some data atrial fibrillation who have 1 or more risk factors generally
do suggest, however, that patients may benefit from the use of should receive anticoagulation with warfarin (INR, 2.03.0)
tPA up to 4.5 hours after symptom onset. and those at low risk should receive aspirin.
Computed tomographic (CT) findings are important in For patients receiving anticoagulant therapy, the dominant
selecting patients for tPA. CT should not show any evidence of risk factor for intracranial hemorrhage is the INR, but age is
4 6. N E U R O L O G I C D I S O R D E R S C AT E G O R I Z E D BY M E C H A N I S M 639
another risk factor for subdural hemorrhage. An INR of 2.0 to Vomiting and the inability to walk are important findings
3.0 is probably an adequate level of anticoagulation for nearly in cerebellar hemorrhage.
all warfarin indications except for preventing embolization
Long-tract signs usually are not present.
from mechanical heart valves. Generally, the lowest effective
intensity of anticoagulant therapy should be given. Cerebellar hemorrhage may cause obstructive hydrocephalus.
640 N E U R O L O GY
Table 46.1 DIFFERENTIAL DIAGNOSIS OF SUBTYPES with low-grade astrocytomas, median survival is 6 to 8 years;
OF HEMORRHAGIC CEREBROVASCULAR DISEASE among patients with oligodendrogliomas, about 10 years.
Clinical and radiologic observation is a reasonable approach
Hemorrhage into parenchyma for patients with stable lesions in a nonresectable area of the
Hypertension brain. Patients with large lesions and mass effect are candidates
Amyloid angiopathy
Aneurysm for surgical resection. The role of postoperative radiotherapy is
Vascular malformation still controversial.
Arteriovenous malformation High-grade astrocytomas, including anaplastic (grade III)
Cavernous malformation astrocytoma and glioblastoma multiforme (grade IV) are asso-
Venous malformation (rare cause of hemorrhage) ciated with low survival (about 17.7% at 1 year). Surgical therapy
Traumaprimarily frontal & temporal
Hemorrhagic infarction is important for obtaining a tissue diagnosis, reducing the mass
Secondary to brain tumors (primary & secondary neoplasms) effect, and removing the majority of the lesion. Surgical therapy
Inflammatory diseases of vasculature is followed by radiotherapy at the site of the lesion. Patients who
Disorders of blood-forming organs (blood dyscrasia, especially leu- receive concurrent temozolomide and radiotherapy have longer
kemia & thrombocytopenic purpura) survival than those who receive radiotherapy alone.
Anticoagulant or thrombolytic therapy
Increased intracranial pressure (brainstem) (Duret hemorrhages) Primary CNS lymphoma is becoming more common in
Illicit drug use (cocaine or amphetamines) patients with AIDS and in immunocompetent patients. Median
Postsurgical survival has increased with the combination of radiotherapy
Fat embolism (petechial) and chemotherapy (mainly intravenous methotrexate).
Hemorrhagic encephalitis (petechial)
Undetermined cause (normal blood pressure & no other recogniza-
ble disorder) N EU RO L O G I C M A N I F E S TAT I O N S I N PAT I E N T S
Hemorrhage into subarachnoid space (subarachnoid hemorrhage) WI T H S YS T E M I C C A N C E R
Trauma The most common neurologic symptoms of patients with sys-
Aneurysm
Saccular (berry, congenital) temic cancer are back pain, altered mental status, and head-
Fusiform (arteriosclerotic)rarely causes hemorrhage ache. However, the most common neurologic complication
Mycotic of systemic cancer is metastatic disease, of which cerebral
Arteriovenous malformation metastasis is most frequent. In patients with cancer and back
Many of the same causes listed under Hemorrhage into paren- pain, epidural metastasis and direct vertebral metastasis are
chyma above
common, but 15% to 20% of patients have no malignant diag-
Subdural & epidural hemorrhage (hematoma) nosis. Nonstructural causes are the most common reasons for
Mainly traumatic (especially during anticoagulation) headache. Identified causes include fever, side effects of ther-
Many of the same causes listed under Hemorrhage into paren-
apy, lumbar puncture, metastasis (cerebral, leptomeningeal, or
chyma above
Hemorrhage into pituitary (pituitary apoplexy) base of skull), and intracranial hemorrhage (thrombocytope-
nia or hemorrhage due to intracranial metastasis). The most
common cause of altered mental status is toxic-metabolic
vomiting, and papilledema), new-onset seizures, or progres- encephalopathy, which is also the most common nonmeta-
sive cognitive and behavioral changes. The most common static manifestation of systemic cancer. Less common causes
primary brain tumors in adults are meningioma, astrocytoma, include intracranial metastatic disease (parenchymal and
oligodendroglioma, and lymphoma. meningeal), paraneoplastic limbic encephalitis, intracranial
The main risk factors associated with meningioma are sex hemorrhage, primary dementia, cerebral infarction, psychiat-
steroid hormones and ionizing radiation. Treatment options ric disorder, known primary brain tumor, bacterial meningitis,
vary according to patient age, comorbid conditions, and and transient global amnesia.
tumor size, location, progression, and histologic characteris- Many neurologic problems in patients with cancer can
tics. Small asymptomatic tumors in older patients should be be diagnosed from the medical history and findings on
observed with follow-up CT or magnetic resonance imag- neurologic examination and require knowledge of both
ing (MRI) every 6 to 12 months. If symptoms develop or nonmetastatic- and noncancer-related neurologic illness.
there is clear tumor growth, surgical resection is indicated. Neurologic complications of systemic cancer are catego-
Postoperative radiotherapy is indicated after incomplete resec- rized as follows:
tion or for tumors with aggressive histologic features (anaplas-
tic or malignant meningiomas). Stereotactic radiosurgery is a 1. Metastatic: parenchymal, leptomeningeal, epidural,
treatment option in some cases. subdural, brachial plexus, lumbosacral plexus, and nerve
Of all primary CNS neoplasms, 40% are gliomas, which infiltration; these complications are common
occur in all areas of the brain and spinal cord. They are clas-
2. Infectious: unusual CNS infections because of
sified as grades I through IV according to their histologic fea-
immunosuppression
tures. Patients with gliomas, which are infiltrative tumors, may
present with seizures. The prognosis depends on the patients 3. Complications of systemic metastases: hepatic
age at diagnosis and on the tumor type. Among patients encephalopathy
4 6. N E U R O L O G I C D I S O R D E R S C AT E G O R I Z E D BY M E C H A N I S M 641
4. Vascular complications: cerebral infarction from or renal carcinoma. About 60% of all cases involve the tho-
hypercoagulable states, nonbacterial thrombotic racic spine, and multiple sites are involved in one-third of
endocarditis, and radiation damage to carotid arteries; the patients. The cardinal symptom is back pain, followed
cerebral hemorrhage (eg, from thrombocytopenia and by weakness, sensory loss, and bladder or bowel dysfunction.
hemorrhagic metastases) Epidural spinal cord compression should be considered in
all patients with any type of cancer and back or radicular
5. Toxic-metabolic encephalopathies: usually from multiple
pain.
causes, hypercalcemia, syndrome of inappropriate
Dexamethasone is highly effective at ameliorating symp-
secretion of antidiuretic hormone, medications, and
toms. In many patients, radiotherapy is efficacious for prevent-
systemic infections
ing further tumor growth and neural damage. The therapeutic
6. Complications of treatment (radiotherapy, chemotherapy, response is better with radiosensitive tumors (eg, multiple
or surgery): radiation necrosis of the brain, radiation myeloma, lymphoma, and prostate, breast, and small cell lung
myelopathy, radiation plexopathy, fibrosis of the carotid carcinoma) than with relatively radioresistant tumors (eg, mel-
arteries, neuropathies, encephalopathies, and cerebellar anoma, renal cell carcinoma). Surgery is indicated for patients
ataxia with spinal instability, bone impingement on the spinal cord,
worsening deficits during or despite radiotherapy, radioresis-
7. Paraneoplastic (ie, nonmetastatic or remote effect tant epidural tumors with limited tumor elsewhere, or a diag-
of cancer): rare syndromes have been described from nosis that is in doubt.
the cerebral cortex through the central and peripheral Meningeal metastases occur in lung and breast cancer, mel-
neuraxes to muscle anoma, leukemia, and lymphoma. Patients typically present
8. Miscellaneous: various systemic and neurologic illnesses with symptoms and signs reflecting involvement at many lev-
unrelated to cancer els of the nervous system: headache, encephalopathy, seizures,
cranial nerve involvement (most commonly diplopia or facial
weakness), back pain, or spinal root involvement. Diagnosis
M ETA S TA S I S TO T H E B R A I N
is suggested by the presence of meningeal enhancement on
Brain metastases are the most common brain tumors. gadolinium MRI and is confirmed by CSF cytologic findings.
Approximately 30% of cancer patients have brain metas- Subsequent CSF samples may be necessary; the yield is 90%
tasis at presentation or later. Metastatic lung cancer is the after the third lumbar puncture.
most common (40%-50% of cases), followed by breast can- Intramedullary spinal cord metastases are much less fre-
cer, colon cancer, melanoma, and unknown primary cancer. quent than epidural metastases and most commonly result
Melanoma produces a disproportionate number of metas- from small cell lung carcinoma. Brachial plexus involvement
tases in the CNS. Evaluation includes detailed history and is most frequent with lung and breast cancer. Colorectal can-
examination, assessment of medical and neurologic perfor- cer causes local pelvic metastasis and is the most frequent
mance status, and imaging studies (MRI of the brain with cause of neoplastic plexopathy. Head cancer and neck cancer
gadolinium; CT of the chest, abdomen, and pelvis; posi- are the most frequent sources of metastasis to the base of the
tron emission tomography). Brain metastases are frequently skull.
associated with surrounding edema. Dexamethasone (2 mg
24 times daily) is indicated in these cases, but additional Cancers commonly causing neurologic problems are lung,
treatment is required to prolong survival. Among untreated breast, and colorectal cancers, leukemia, lymphoma, and
patients, median survival is 1 to 2 months; among treated melanoma.
patients, 2 to 10 months. Common metastatic sites are the parenchyma of the
Survival depends on patient age, performance status, pres- cerebral hemispheres and cerebellum, leptomeninges,
ence or absence of extracranial metastasis, and control of the epidural and subdural spaces, brachial and lumbosacral
primary tumor. Surgical resection of single accessible lesions plexuses, and nerves.
increases survival among patients with good prognostic fac-
tors. Most patients receive postoperative whole-brain radio- Cerebral metastasis is the most common neurologic
therapy. Stereotactic radiosurgery can be used to treat multiple complication of systemic cancer.
lesions in a single session in conjunction with whole-brain
Epidural spinal cord compression should be considered for
radiotherapy.
all patients with any type of cancer and back or radicular
pain.
M ETA S TA S I S TO T H E S P I NA L C O R D,
The most frequent cause of tumor plexopathy is colorectal
L E P TO M E N I N G E S , O R P E R I P H E R A L N E RVE S
cancer.
Epidural spinal cord compression is the most common cause
Melanoma produces a disproportionate number of
of spinal cord dysfunction in patients with cancer and is
metastases in the CNS.
frequently preceded by vertebral metastasis. The most com-
mon causes are lung, breast, and prostate cancer, followed by Toxic-metabolic encephalopathy is the most common
non-Hodgkin lymphoma, multiple myeloma, and colorectal nonmetastatic manifestation of cancer.
642 N E U R O L O GY
Box 46.2 CLASSIFICATION OF PARANEOPLASTIC Table 46.2 PARANEOPLASTIC ANTIBODIES
NEUROLOGIC DISORDERS ASSOCIATED WITH CANCER AND SYNDROMES
ASSOCIATED ASSOCIATED
Central nervous system ANTIBODY CANCER SYNDROMES
Encephalomyelitis
Limbic encephalitis Anti-Hu (ANNA-1) SCLC Encephalomyelitis
Cerebellar degeneration Limbic encephalitis
Cerebellar degeneration
Brainstem encephalitis SSN
Opsoclonus-myoclonus Autonomic ganglionopathy
Stiff person syndrome
Chorea Anti-Ri (ANNA-2) Breast, gyneco- Ataxia
logic, SCLC Opsoclonus-myoclonus
Necrotizing myelopathy Brainstem encephalitis
Motor neuronopathy
Dorsal root ganglion & peripheral nerves Anti-Yo (PCA-1) Breast, ovary Cerebellar degeneration
Subacute sensory neuronopathy CRMP-5 SCLC, Chorea, myelopathy, optic
Gastroparesis or intestinal pseudo-obstruction thymoma neuritis, retinopathy, &
Acute autonomic ganglionopathy others
Acquired neuromyotonia
Amphiphysin Breast, SCLC Stiff person syndrome
Neuropathy associated with plasma cell dyscrasia or lymphoma Encephalomyelitis
Vasculitis of nerve or muscle
Neuromuscular junction Anti-Ma2 Testicular Limbic encephalitis
Lambert-Eaton myasthenic syndrome germinoma Brainstem encephalitis
Myasthenia gravis P/Q type VGCC SCLC LEMS
Muscle
Dermatomyositis Muscle nAChR Thymoma Myasthenia gravis
Polymyositis Ganglionic nAChR SCLC Autonomic ganglionopathy
Acute necrotizing myopathy
Eye and retina Voltage-gated Thymoma, SCLC Neuromyotonia
potassium channel Limbic encephalitis
Cancer-associated retinopathy
Optic neuropathy NMDA receptor Ovarian Limbic encephalitis
teratoma Rigidity
Hypoventilation
PA R A N E O P L A S T I C D I S O R D E R S Dysautonomia
Paraneoplastic disorders are associated with increased levels
of circulating antibodies (onconeural antibodies) directed Abbreviations: ANNA, antineuronal nuclear antibody; CRMP, collapsin response
mediator protein; LEMS, Lambert-Eaton myasthenic syndrome; nAChR, nico-
against neoplastic cells and attacking membrane ion chan- tinic acetylcholine receptor; NMDA, N-methyl-d-aspartate; PCA, Purkinje cell
nels or intracellular (nuclear or cytoplasmic) proteins in antibody; SCLC, small cell lung carcinoma; SSN, subacute sensory neuronopathy;
neurons. The most common underlying malignancies are VGCC, voltage-gated calcium channels.
small cell lung carcinoma and breast cancer. Others include
ovarian or testicular carcinoma, thymoma, Hodgkin disease,
and parotid tumors. Paraneoplastic syndromes can affect any paraneoplastic disorders related to antibodies against mem-
level of the CNS or peripheral nervous system (Box 46.2). brane antigens such as P/Q type voltage-gated calcium chan-
Important examples include limbic encephalitis (character- nels (LEMS) or voltage-gated potassium channels (limbic
ized by behavioral and memory abnormalities and seizures), encephalitis).
brainstem encephalitis, opsoclonus-myoclonus, cerebel-
lar ataxia, myelopathy, peripheral neuropathy, stiff person Paraneoplastic neurologic syndromes typically precede the
syndrome (with axial and limb rigidity), sensory ganglion- diagnosis of the underlying cancer.
opathies, Lambert-Eaton myasthenic syndrome (LEMS),
dermatomyositis, and retinopathy. These syndromes are A paraneoplastic syndrome should be suspected in any
characterized by an acute or subacute onset and increased patient with a subacute inflammatory disorder affecting
levels of 1 or more antibodies (Table 46.2). A paraneoplas- any level of the central or peripheral nervous system.
tic neurologic syndrome precedes the diagnosis of cancer in
60% of cases and develops after tumor diagnosis or at tumor N EU RO L O G I C C O M P L I C AT I O NS O F C A N C E R
recurrence in 40%. T R E AT M E N T
Treatment of the underlying neoplasm is the main fac-
tor associated with neurologic stabilization. Immunotherapy Treatment of cancer with chemotherapeutic and biologic
with corticosteroids, intravenous immunoglobulin, plasma agents is frequently complicated by the development of neu-
exchange, cyclophosphamide, or rituximab may be helpful in rotoxicity. Typical examples are listed in Table 46.3.
4 6. N E U R O L O G I C D I S O R D E R S C AT E G O R I Z E D BY M E C H A N I S M 643
Table 46.3 EXAMPLES OF NEUROTOXICITY OF mainly with the arms outstretched, although there is often
CHEMOTHERAPEUTIC AGENTS a kinetic component as well. Postural tremor is physiologic,
but it is also noted pathologically in essential tremor. Drugs
TYPICAL MANIFESTATIONS OF
AGENT NEUROTOXICITY
such as methylxanthines, -adrenergic agonists, lithium, and
amiodarone may produce postural tremor. Kinetic tremor is
Platinum compounds (cis- Sensory (large fiber) neuropathy (sensory seen mainly in action, as in finger-to-nose testing. This type of
platin, oxaliplatin) ataxia) tremor occurs with cerebellar disease and diseases of the cer-
Autonomic neuropathy ebellar connections in the brainstem.
Ototoxicity
Encephalopathy, cortical blindness,
seizures E S S E N T I A L T R E MO R
Retrobulbar neuritis
Retinal injury Essential tremor is the most common movement disorder and
Vinca alkaloids Sensorimotor peripheral neuropathy should be differentiated from tremor observed in Parkinson
Autonomic neuropathy disease (Table 46.4). Essential tremor is a monosymptomatic
condition manifested by rhythmic oscillations of various
Taxanes (eg, paclitaxel) Predominantly sensory peripheral parts of the body. Middle-aged and older persons are most
neuropathy
Occasional motor neuropathies
commonly affected, and there is often a genetic component.
Transient scotomata The hands are affected most, with the tremor present in the
postural position and often having a kinetic component. The
Methotrexate Acute chemical arachnoiditis (intrathecal head and voice can be affected. Head tremor can be either hor-
administration)
Acute, reversible, stroke-like syndrome
izontal (no-no) or vertical (yes-yes). Head tremor almost
Subacute encephalopathy never occurs in Parkinson disease, but parkinsonian patients
Transverse myelopathy may have tremor of the mouth, lips, tongue, and jaw. The legs
Chronic demyelinating encephalopathy and trunk (affected in orthostatic tremor) are affected less fre-
5-Fluorouracil Cerebellar dysfunction
quently in essential tremor. Essential tremor is a slowly pro-
Acute encephalopathy gressive condition; its pathophysiologic mechanism is not
Subacute extrapyramidal syndrome known.
Leukoencephalopathy (when combined The agent most effective in decreasing essential tremor is
with levamisole) alcohol. Drinking a beverage containing alcohol can substan-
Cytarabine (ara-C) Cerebellar dysfunction tially reduce the tremor for 45 to 60 minutes. Notably, the
Cognitive impairment prevalence of alcoholism among patients with essential tremor
Necrotizing leukoencephalopathy is no different from that of the general population. Propranolol
Peripheral neuropathy (80320 mg daily), other -blockers, and primidone (25250
Seizures, parkinsonism, myelopathy
mg at bedtime) are also effective. Other drugs that have been
Ifosfamide Encephalopathy with agitation, visual & prescribed are clonazepam, gabapentin, and topiramate. Deep
auditory hallucinations, behavioral & brain stimulation (DBS) of the thalamus is effective for all
memory changes
Hemiparesis, seizures, coma
Cerebellar, extrapyramidal, or cranial
Table 46.4 DIFFERENTIAL DIAGNOSIS OF TREMOR
nerve dysfunction
FEATURE PARKINSON DISEASE ESSENTIAL TREMOR
Nitrosoureas Encephalopathy
Busulfan Seizures Tremor type & Rest >> postural; Postural, kinetic;
frequency 35 Hz 812 Hz
l-Asparaginase Encephalopathy
Cerebral venous thrombosis Affected by Hands, legs, chin, jaw Hands, head, neck,
tremor voice
Tremor is an oscillatory rhythmic movement disorder. A sim- Therapy Levodopa, dopamine Propranalol, primidone,
ple classification of tremor is rest tremor and action tremor. agonists, gabapentin, botuli-
anticholinergics num toxin type A
Rest tremor is observed while the patient is sitting with the
arms lying in the lap or walking with the arms at the side. Rest Surgical Subthalamic Thalamic (Vim)
tremor occurs in Parkinson disease. Action tremor occurs when treatment stimulation stimulation
there is muscle contraction. It includes postural tremor and
kinetic tremor. Postural tremor affects the hands and is seen Abbreviation: Vim, subnucleus ventralis intermedius.
644 N E U R O L O GY
types of tremor and is indicated for patients with functional Box 46.4 NONMOTOR MANIFESTATIONS OF
disability that does not respond to drug therapy. PARKINSON DISEASE
Essential tremor affects the hands most and occurs mostly Autonomic
in middle-aged and older persons. Constipationa
There is often a genetic component. Orthostatic hypotension
Bladder dysfunction
Head tremor almost never occurs in Parkinson disease. Sleep disorders
Excessive diurnal somnolence
Insomnia
PA R K I NS O N D I S E A S E REM sleep behavior disordera
Periodic leg movement disorder
Patients with Parkinson disease present with tremor (the ini- Cognitive symptoms
tial symptom in 50%-70%, but 15% never have tremor), rigid- Depressiona
ity, and bradykinesia. The gait is unsteady, slow, and shuffling. Anxiety
Decreased blinking rate, lack of change in facial expression, Hallucinations
small handwriting, and asymptomatic orthostatic hypotension Abnormal behavior
are also common. Parkinson disease includes motor manifes- Sensory symptoms
tations (Box 46.3) and nonmotor manifestations (Box 46.4). Impaired olfactiona
The classic motor manifestations of Parkinson disease, includ-
ing rest tremor, muscle stiffness (rigidity), and slowness of Abbreviation: REM, rapid eye movement.
a
movement initiation and execution (hypokinesia and bradyki- May precede the diagnosis of disease.
nesia), typically start asymmetrically and respond to levodopa
therapy. Late motor manifestations, including difficulty swal- (increased deep tendon reflexes, spasticity, or extensor plan-
lowing, postural instability, and freezing of gait, are much less tar response), and early dementia. Although dementia is more
responsive to treatment. At late stages of the disease in patients frequent among patients with Parkinson disease, it is noted in
who have received prolonged levodopa therapy, motor fluctu- only about 25% of those in whom the disease develops after
ations develop. Some nonmotor manifestations may precede age 60.
the diagnosis of Parkinson disease (Box 46.4).
The differential diagnosis of Parkinson disease includes Tremor does not occur in 15% of patients with Parkinson
disorders caused by drugs (Box 46.5) or toxins (eg, carbon disease.
monoxide, manganese), potentially treatable neurometabolic
disorders (particularly Wilson disease in patients younger
than 50 years), and other neurodegenerative disorders in
which parkinsonism is a prominent feature (Parkinson plus Box 46.5 DRUGS THAT INDUCE PARKINSONISM OR
syndromes) (Table 46.5). Conditions that should each suggest TREMOR
a disorder other than Parkinson disease as a cause of parkin-
sonism include the lack of response to levodopa, the presence
Antagonist of dopamine D2 receptors
of early postural instability or orthostatic hypotension, the
Neuroleptics (haloperidol, risperidone, resperine, etc)
detection of cerebellar findings (ataxia) or corticospinal signs
Antiemetics (metoclopramide, prochlorperazine)
Other psychiatric drugs
Selective serotonin reuptake inhibitors
Box 46.3 MOTOR MANIFESTATIONS OF PARKINSON Tricyclics
DISEASE Lithium
Cardiovascular drugs
Early manifestations (typically asymmetric in onset & responsive Amiodarone
to levodopa) Calcium channel blockers (flunarizine)
Rest tremor Atorvastatin
Rigidity Anticonvulsants
Bradykinesia Valproate
Late manifestations (less responsive to levodopa) Others
Gait & postural instability Cyclosporine
Dysphagia Metronidazole
Motor fluctuations (in patients with severe disease & long-term Caffeine & other methylxanthines
levodopa therapy) -Adrenergic agonist
Wearing-off & on-off phenomena Thyroxine
Levodopa-induced dyskinesia Prednisone
4 6. N E U R O L O G I C D I S O R D E R S C AT E G O R I Z E D BY M E C H A N I S M 645
Table 46.5 DIFFERENTIAL DIAGNOSIS OF PARKINSON If ataxia, increased deep tendon reflexes, spasticity, extensor
PLUS SYNDROMES plantar responses, or lower motor neuron findings are
present, consider Parkinson plus syndromes.
MANIFESTATION SUSPECT
Poor response to levodopa Any Parkinson plus syndrome The treatment of the motor manifestations of Parkinson
(MSA & PSP may respond) disease is summarized in Table 46.6. The initial treatment
Early falls PSP or MSA options include dopaminergic agonists and a combination of
levodopa and carbidopa (Sinemet). Anticholinergic agents
Severe OH, urologic symptoms, MSA were used in the past for young patients with mild symptoms
anosmia, or DEB
(predominantly tremor), but they are rarely used now and
Cerebellar signs MSA or spinocerebellar degeneration should not be given to patients older than 65 years because of
the high incidence of side effects, such as memory loss, delir-
Vertical gaze palsy PSP
ium, urinary hesitancy, and blurred vision.
Asymmetric apraxia Corticobasal degeneration Patients with disabling symptoms should receive
carbidopa-levodopa. The initial dosage is a 25/100 tablet (25
Early dementia Lewy body dementia
Creutzfeldt-Jakob disease mg carbidopa/100 mg levodopa) by mouth 3 times daily on
an empty stomach. Although monotherapy with dopamin-
ergic agonists carries a smaller risk of delayed motor com-
Abbreviations: DEB, dream enactment behavior; MSA, multiple system atrophy;
OH, orthostatic hypotension; PSP, progressive supranuclear palsy. plications than long-term levodopa therapy, these agents are
less efficacious than levodopa. Dopaminergic agonists can be
used as initial treatment in young patients to reduce the dose
The effects of drugs should be excluded in all patients
of levodopa. Dopaminergic agonists include pramipexole and
presenting with parkinsonism.
ropinirole. Bromocriptine and pergolide, ergot derivatives, are
Wilson disease should be considered in all patients younger no longer used because of the risk of retroperitoneal or cardiac
than 50 years who present with parkinsonism (or dystonia, valvular fibrosis. The main side effects of levodopa and dop-
cerebellar ataxia, or cognitive or psychiatric manifestations). aminergic agonists are nausea, orthostatic hypotension, and
Dopaminergic agonists Early use in young patients, either alone or Nausea, vomiting, OH
Pramipexole associated with small dose of levodopa More likely than Sinemet to produce excessive diurnal somnolence,
Ropinirole Motor fluctuation in patients taking Sinemet impulse control disorder, hallucinations, or peripheral edema
Rotigotine (patch)
MAO-B inhibitors Delay the need to start levodopa therapy Insomnia (with selegiline); nausea, hallucinations, confusion,
Selegiline May be neuroprotective dyskinesias, OH
Rasagiline
Abbreviations: COMT, catechol O-methyltransferase; DBS, deep brain stimulation; GPi, globus pallidus, pars interna; MAO, monoamine oxidase; OH, orthostatic
hypotension; STN, subthalamic nucleus.
a
Anticholinergics (eg, trihexyphenidyl) are used only rarely and are contraindicated in patients older than 65 years owing to prominent autonomic and cognitive side
effects.
b
Carbidopa 25 mg, levodopa 100 mg.
c
Controlled release formulation: carbidopa 50 mg, levodopa 200 mg.
646 N E U R O L O GY
hallucinations. An important side effect of all these agents is levodopa, the presence of cerebellar or pyramidal signs, severe
the development of unpredictable episodes of daytime sleepi- orthostatic hypotension and urinary incontinence, sleep
ness. An important side effect of dopaminergic agonists is the apnea, and laryngeal stridor. The management of orthostatic
development of impulse dyscontrol, manifested as compul- hypotension includes eliminating potentially offending drugs
sive gambling, shopping, or hypersexuality. Patients and their (eg, vasodilators, diuretics, dopaminergic agonists, and cloza-
spouses should be counseled about these problems before ini- pine), increasing sodium and water intake, performing pos-
tiation of dopaminergic agonist therapy. tural maneuvers, elevating the head of the bed, and wearing
When given to a patient with newly diagnosed Parkinson support stockings. Drug treatment includes fludrocortisone
disease, selegiline or rasagiline (monoamine oxidase type B (0.11.0 mg daily) and vasoconstrictors such as midodrine
inhibitors) may give mild symptomatic relief and delay the (1040 mg daily). Pyridostigmine can also be used for ortho-
need to initiate levodopa therapy. Side effects include nau- static hypotension in dosages similar to those used in myasthe-
sea, hallucinations, confusion, dyskinesias, and orthostatic nia gravis (3060 mg 3 times daily).
hypotension. New-generation antipsychotic drugs, such as cloza-
Long-term high-dose levodopa monotherapy leads to pine, olanzapine, and quetiapine, can be used to manage
dyskinesias and motor fluctuations. Management strategies drug-induced psychosis because they have a lower risk of exac-
include the use of smaller and more frequent doses of levodopa, erbating parkinsonism in these patients.
long-acting levodopa preparations, dopaminergic agonists,
and inhibitors of catechol O-methyltransferase. Apomorphine
OT H E R MOVE M E N T D I S O R D E R S : B OT U L I NUM
can be administered subcutaneously for severe, hypomobile,
TOX I N T H E R A P Y
end-of-dose wearing-off times. A protein-restricted diet
may decrease unpredictable off times. Amantadine, a glu- Botulinum toxin, which blocks the neuromuscular junction,
tamate receptor antagonist, is used as adjuvant treatment in is effective therapy for cervical dystonia, blepharospasm,
patients with levodopa-induced dyskinesias. hemifacial spasm, spasmodic dysphonia, jaw-closing oroman-
A surgical approach, primarily DBS of the subthalamic dibular dystonia, and limb dystonia, including occupational
nucleus or globus pallidus, is an option to relieve motor symp- dystonias.
toms in eligible patients with levodopa-responsive Parkinson
disease and severe motor fluctuations. Patient selection is
critical to ensure maximal benefit of DBS. Patients who have I N F L A M M ATO RY A N D AU TO I M MU N E
cognitive or psychiatric disorders or who do not respond to DISORDER S
levodopa are not eligible. Manifestations such as dysphagia,
postural instability, and gait freezing do not respond to DBS.
MU LT I P L E S C L E RO S I S
DBS of the subthalamic nucleus may result in transient cogni-
tive or psychiatric manifestations: Suicide has been reported The most common inflammatory demyelinating disease of
among some patients. the CNS is multiple sclerosis, a disabling disorder that affects
predominantly young adults, with an onset between ages 20
Carbidopa-levodopa is the indicated treatment when and 50 years. It affects women twice as often as men. Multiple
patients have disabling motor symptoms or when the sclerosis has a complex immunopathogenesis, variable prog-
diagnosis of Parkinson disease is uncertain. nosis, and an unpredictable course. Polygenic and environ-
mental (possibly viral) factors probably have a substantial
Dopaminergic agonists are used as initial therapy in effect on susceptibility to multiple sclerosis. The disease
young patients to delay onset of levodopa-induced motor attacks white matter and (in both early and late stages) axons
fluctuations. of the cerebral hemispheres, brainstem, cerebellum, spinal
Before starting dopaminergic agonist therapy, patients and cord, and optic nerve. Most patients (80%-85%) present with
their spouses should be warned about the risk of falling relapsing-remitting symptoms. In about 15% of patients, the
asleep while driving and the possibility of compulsive disease is progressive from onset (primary progressive). Over
gambling, shopping, or hypersexuality. time, in 70% of patients with the relapsing-remitting form,
secondary progressive multiple sclerosis develops.
DBS may be helpful in relieving motor symptoms in Symptoms reflect multiple white matter lesions dissemi-
eligible patients with Parkinson disease, but patient nated in space and time. Typical syndromes include optic
selection is critical. neuritis, myelopathy, brainstem syndromes, and paroxysmal
attacks. Optic neuritis manifests with unilateral visual loss fre-
The management of nonmotor manifestations of Parkinson quently associated with eye pain with movement. Myelopathy
disease is summarized in Table 46.7. Orthostatic hypoten- manifests with sensory symptoms, including a bandlike sensa-
sion, constipation, bladder dysfunction, and other autonomic tion in the abdomen and chest, spastic weakness of the limbs,
manifestations develop in many patients with parkinsonism. and bladder and bowel dysfunction. Other typical symptoms
In these patients, Parkinson disease should be distinguished include diplopia (due to internuclear ophthalmoplegia) and
from multiple system atrophy. Findings suggestive of multi- ataxia. Paroxysmal symptoms, including trigeminal neural-
ple system atrophy include lack of a predictable response to gia and hemifacial spasm, in a young patient should increase
4 6. N E U R O L O G I C D I S O R D E R S C AT E G O R I Z E D BY M E C H A N I S M 647
Table 46.7 MANAGEMENT OF NONMOTOR MANIFESTATIONS OF PARKINSON DISEASE
Orthostatic hypotension Loss of sympathetic ganglion neurons & Increase sodium & water intake
effects of dopaminergic agonists Fludrocortisone, midodrine, pyridostigmine
Hallucinations Medication effect (exclude DLB) Discontinue use of anticholinergics, MAO-B inhibi-
tors, & amantadine
Reduce or discontinue use of dopamine agonists
Quetiapine or olanzapine
Abbreviations: DLB, dementia with Lewy bodies; MAO, monoamine oxidase; PLMS, periodic leg movement disorder; REM, rapid eye movement; SSRI, selective
serotonin reuptake inhibitor.
awareness of multiple sclerosis. Other important symptoms examples include vasculitis, infections (eg, human immunode-
are memory and cognitive dysfunction and depression. ficiency virus infection or Lyme disease), paraneoplastic disor-
Associated features that suggest multiple sclerosis include ders, neurosarcoidosis, systemic lupus erythematosus, Behet
excessive unexplained fatigue and exacerbation of symptoms disease, and lymphoma.
upon exposure to heat. Predictors associated with a more favorable long-term course
The diagnosis is primarily based on clinical and MRI of multiple sclerosis include age younger than 40 years at onset,
data that show lesions disseminated in space and time. female sex, optic neuritis or isolated sensory symptoms as the
Abnormalities on MRI are most helpful and include multi- first clinical manifestation, and relatively infrequent attacks.
focal lesions of various ages in the periventricular white mat- Prognostic factors associated with a poor outcome include age
ter, corpus callosum, brainstem, cerebellum, and spinal cord. older than 40 years at onset, male sex, cerebellar or pyramidal
Gadolinium-enhanced lesions are presumed to be active tract findings at initial presentation, relatively frequent attacks
lesions of inflammatory demyelination. In patients with clin- during the first 2 years, incomplete remissions, and a chroni-
ically isolated syndromes, such as optic neuritis, myelopathy, cally progressive course. However, no single clinical variable is
or brainstem syndrome, abnormal MRI findings are a strong sufficient to predict the course or outcome of this disease. There
predictor of the eventual clinical diagnosis of multiple sclero- is evidence that a subset of multiple sclerosis patients has very
sis in the next 5 years. CSF findings include oligoclonal bands, benign disease; hence, not every patient with multiple sclerosis
increased IgG synthesis, and moderate lymphocytic pleocy- must receive long-term treatment.
tosis (<50 mononuclear cells/L). Visual and somatosensory The recommended therapy for acute exacerbations of
evoked potential studies are less helpful. multiple sclerosis is a 3- to 5-day course of a high dose of intra-
Many other disorders mimic multiple sclerosis and should venous methylprednisolone (1.0 g daily). Severe or steroid-
be considered when patients have atypical findings. Important unresponsive exacerbations are treated with plasma exchange.
648 N E U R O L O GY
Interferon beta-1a, interferon beta-1b, and glatiramer (or both), cachexia, and panfascicular muscle necrosis.
acetate decrease the relapse rate and the intensity of relapse in Neurologic complications also occur in intensive care units
patients with the relapsing-remitting type of multiple sclerosis. for critical medical illness. These complications include met-
There is some evidence that these medications may also reduce abolic encephalopathy, seizures, hypoxic-ischemic encephal-
disability. They are expensive, however, and significant side opathy, and stroke.
effects, including depression, can occur. For patients receiving
interferon beta, periodic monitoring includes liver function
tests and complete blood cell counts. In 5% to 30% of patients S E P T I C E N C E P H A L O PAT H Y
receiving interferon beta, neutralizing antibodies develop and Septic encephalopathy is brain dysfunction in association
block the effects of interferon beta. with systemic infection without overt infection of the brain
Several drugs are used to treat specific symptoms of mul- or meninges. Early encephalopathy often begins before fail-
tiple sclerosis. Trigeminal neuralgia, flexor spasms, and other ure of other organs and is not due to single or multiple organ
paroxysmal symptoms respond to carbamazepine, and spastic- failure. Endotoxin does not cross the blood-brain barrier and
ity responds to baclofen and tizanidine. Fatigue, a disabling so probably does not directly affect adult brains. Cytokines,
symptom of multiple sclerosis, occasionally responds to aman- important components of sepsis syndrome, may contribute to
tadine, modafinil, or stimulants. encephalopathy. Gegenhalten or paratonic rigidity occurs in
more than 50% of patients, and tremor, asterixis, and multifo-
Typical clinical scenario for multiple sclerosis: A cal myoclonus occur in about 25%. Seizures and focal neuro-
35-year-old woman has a history of rapid loss of vision logic signs are rare.
in the right eye, with pain on eye movement. A similar Electroencephalography is a sensitive indicator of
episode occurred 2 years ago and involved the same eye; encephalopathy. The mildest abnormality is diffuse excessive
recovery was complete. She also has noticed weakness and low-voltage theta activity (47 Hz). The next level of severity
paresthesias of both legs in the past 6 months. CSF analysis is intermittent rhythmic delta activity (<4 Hz). As the condi-
shows increased protein levels and oligoclonal bands on tion worsens, delta activity becomes arrhythmic and continu-
electrophoresis. Multiple T2 hyperintense areas consistent ous. Typical triphasic waves occur in severe cases, especially in
with demyelination are seen on MRI. hepatic failure. In these cases, MRI and CT scans of the brain
may be normal.
N EU RO MY E L IT I S O P T I C A
Brain dysfunction is associated with systemic
Neuromyelitis optica (NMO) is a recurrent severe demyelinat- infection.
ing disease that may mimic multiple sclerosis. The diagnosis is
based on the following: a) presence of severe optic neuritis or Encephalopathy precedes failure of other organs.
transverse myelitis, or both; b) MRI evidence of contiguous Cytokines are an important part of sepsis syndrome.
spinal cord lesions spanning more than 3 vertebral segments;
c) absence of typical multiple sclerosis lesions on MRI of the More than 50% of patients have paratonic rigidity.
brain; and d) presence of NMO-IgG antibodies that react Tremor, asterixis, and multifocal myoclonus occur in 25%
against the water channel aquaporin 4. Unlike in multiple scle- of patients.
rosis, the CSF in NMO shows polynuclear pleocytosis (>50
cells/L) and an absence of oligoclonal bands. Exacerbations Electroencephalography is a sensitive indicator of
may respond to intravenous methylprednisolone or plasma encephalopathy.
exchange. The presence of NMO-IgG antibodies indicates
risk of recurrence and warrants long-term immunosuppres-
C R IT I C A L I L L N E S S P O LY N EU RO PAT H Y
sion with azathioprine, cyclophosphamide, or rituximab.
Critical illness polyneuropathy occurs in 70% of patients with
Not all acute demyelinating CNS disorders are multiple sepsis and multiple organ failure. There is often an unexplained
sclerosis. difficulty in weaning from mechanical ventilation. Nerve
The diagnosis of multiple sclerosis is primarily based on biopsy specimens show primary axonal degeneration of motor
clinical and MRI criteria showing dissemination in space and sensory fibers without inflammation. Most patients also
and time. have concomitant myopathy. Recovery from critical illness
polyneuropathy is satisfactory if the patient survives sepsis and
The presence of NMO-IgG is highly specific for NMO. multiple organ failure.
4 6. N E U R O L O G I C D I S O R D E R S C AT E G O R I Z E D BY M E C H A N I S M 649
S U M M A RY Cerebral metastasis is the most common neurologic
complication of systemic cancer.
Pathophysiologic mechanisms of ischemic
Tremor does not occur in 15% of patients with Parkinson
cerebrovascular disease include a cardiac source,
disease.
large-vessel disorders, small-vessel disorders, and
hematologic causes. The diagnosis of multiple sclerosis is primarily based on
clinical and MRI criteria showing dissemination in space
Atrial fibrillation is associated with 24% of ischemic
and time.
strokes and 50% of embolic strokes.
650 N E U R O L O GY
PA RT X I I I
D E R M ATO L O GY
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47.
DERMATOLOGY
Carilyn N. Wieland, MD, and Lisa A. Drage, MD
Discern the autoimmune bullous diseases. Basal cell carcinoma constitutes approximately 80% of all
skin cancers in the general population.
Recognize serious skin conditions such as erythema
multiforme and Stevens-Johnson syndrome. Basal cell carcinoma and squamous cell carcinoma occur on
sun-exposed skin.
Know the dermatologic manifestations of drug reactions.
The cure rate for nonmelanoma skin cancer is >90% with
Identify cutaneous signs of malignancy and common early detection and treatment.
medical conditions.
Organ transplant recipients have a high risk for squamous
cell carcinoma of the skin.
G E N E R A L D E R M ATO L O GY
M A L I G NA N T M E L A N O M A
In 2010, about 68,000 Americans received a diagnosis of cuta-
SKIN CANCER
neous melanoma, and 8,700 died of the disease. The estimated
Nonmelanoma skin cancers (basal cell carcinoma, squamous lifetime risk of invasive melanoma is about 2% for Americans
cell carcinoma) are the most common malignancies in the born in 2005.
United States. Skin cancers will be diagnosed in more than The strongest risk factors for melanoma are a family history
2 million people in the United States this year. The cure rate of melanoma, multiple benign or atypical nevi, and a previous
for nonmelanoma skin cancer is more than 90% with early melanoma. Additional risk factors include fair skin, blond or
detection and appropriate treatment. The incidence of non- red hair, sun sensitivity, freckling, intermittent sun exposure,
melanoma skin cancer is increasing because of a combina- blistering sunburns, immunosuppression, human immunode-
tion of increased exposure to ultraviolet light, changes in ficiency virus (HIV) infection, and tanning bed use. Inherited
clothing style, increased longevity, and atmospheric ozone mutations in CDKN2A and CDK4 genes, which have been
depletion. documented in some families with melanoma, are associated
Both basal cell and squamous cell carcinomas commonly with a 60% to 90% lifetime risk of melanoma. The famil-
occur on sun-exposed skin areas. The ratio of basal cell car- ial atypical mole-melanoma syndrome is transmitted by an
cinoma to squamous cell carcinoma is 4:1 in immunocompe- autosomal dominant gene. Patients with either familial or
tent people. Basal cell carcinomas are usually slow-growing nonfamilial atypical nevi have an increased risk for develop-
and locally invasive. They may invade vital structures and can ment of malignant melanoma. Other risk factors that have
cause considerable disfigurement. Basal cell carcinomas rarely been identified include a personal or family history of mela-
metastasize to regional lymph nodes. In contrast, the risk of noma or nonmelanoma skin cancer, a large number of benign
metastases of squamous cell carcinoma in the general popula- pigmented nevi, giant pigmented congenital nevus, and
tion is approximately 2%. immunosuppression.
653
Table 47.1 SURVIVAL IN MALIGNANT MELANOMA, BY Node status, determined by sentinel lymph node biopsy, is
TUMOR THICKNESS a the most powerful predictor of recurrence and survival.
TUMOR , MM 5-YEAR SURVIVAL, % New immune-based therapies show promise in select
patients with advanced disease.
<1.0 95.3
1.012.00 89.0
P R EV E N T I O N O F M E L A N O M A A N D
2.014.00 78.7 NONMELANOMA SKIN CANCER
>4.00 67.4 Dermatologists encourage regular use of sunscreens with a sun
protection factor (SPF) of at least 30 and sun-protective cloth-
a
No nodal or distant metastasis. ing. Sun exposure during the first 18 years of life accounts for
up to 80% of cumulative lifetime sun exposure. Persons with
light skin types and people who spend time outdoors need to
The key to improved survival with malignant melanoma be particularly vigilant with sun protection.
is early detection and diagnosis. A full skin examination is
recommended for persons at risk, including an evaluation for
CU TA N E O US T- C E L L LY M P H O M A
Asymmetry, Border irregularity, Color variation, a Diameter
more than 6 mm, and Evolution (an ABCDE evaluation). Cutaneous T-cell lymphoma is a non-Hodgkin lymphoma
Changing or symptomatic moles or moles that stand out characterized by expansion of malignant T cells within the
from other moles should be biopsied. Pathologic staging of skin. The most common clinical presentations are mycosis
the primary melanoma guides prognosis and further surgical fungoides and Szary syndrome. Mycosis fungoides generally
decisions. presents with discrete or coalescing patches, plaques, or nod-
Increase in thickness of a melanoma (Table 47.1), micro- ules on the skin. Mycosis fungoides may progress to involve
scopic ulceration, and mitotic rate are all inversely correlated lymph nodes and viscera. Once extracutaneous involvement is
with survival. However, micrometastasis to the first draining recognized, the median duration of survival is about 2.5 years.
lymph node is now the most powerful staging and prognostic The course of patients with patch- or plaque-stage cutaneous
tool. lesions, without extracutaneous disease, is less predictable,
but the median duration of survival is approximately 12 years.
The key to improved survival with malignant melanoma is Szary syndrome, the more aggressive leukemic form of cuta-
early diagnosis. neous T-cell lymphoma, is characterized by generalized eryth-
roderma, keratoderma of the palms and soles, and a Szary cell
Increased tumor thickness is associated with decreased count of more than 1,000/mm3 in the peripheral blood. Most
survival. patients have severe pruritus.
Micrometastasis to the first draining lymph node (sentinel
lymph node) is the most powerful staging and prognostic Mycosis fungoides and Szary syndrome are forms of
tool. cutaneous T-cell lymphoma.
Mycosis fungoides may progress to involve lymph nodes
Stages I and II malignant melanomas consist of the cuta- and viscera.
neous lesion without lymph node involvement. Stage III
consists of the primary skin lesion plus microscopic or mac- The median survival for patients with mycosis fungoides is
roscopic lymph node involvement, and stage IV represents 12 years, but it decreases to 2.5 years with extracutaneous
distant metastasis. Surgical management is recommended for involvement.
treatment of the primary melanoma and consists of excision
with tumor-free margins of 1 to 3 cm. Sentinel lymph node Both mycosis fungoides and Szary syndrome are char-
biopsy, whereby the first draining lymph node(s) is identified acterized by the presence of Szary cells (enlarged atypical
(with blue dye injection and lymphoscintigraphy) and sam- lymphocytes with convoluted nuclei) involving the epidermis
pled, improves prognostic accuracy in intermediate and thick (epidermotropism) and dermis. On immunohistochemical
melanomas and identifies candidates for systemic adjuvant stains of cutaneous lesions, these malignant T cells usually
treatment. Adjuvant high-dose interferon alfa-2b increases express CD3 and CD4 antigens (T-helper cell markers), and
relapse-free survival rates and may improve overall survival molecular genetic studies show clonal rearrangement of the
rates in select patients. New immune-based therapies have T-cell receptor gene in lymphocyte populations from skin
recently shown promise in select patients with advanced (dis- biopsy, lymph node, and peripheral blood specimens of
tant metastases) disease. Ongoing therapeutic studies focus on patients with cutaneous T-cell lymphoma.
vaccines, immunotherapy, and targeted chemotherapy.
Mycosis fungoides and Szary syndrome are T-cell
Surgical management of primary melanoma consists of lymphomas characterized by the presence of a clonal T-cell
excision with tumor-free margins of 13 cm. population in skin and peripheral blood.
654 D E R M ATO L O GY
Treatment of cutaneous T-cell lymphoma includes topical Phototherapy
corticosteroids, topical nitrogen mustard, psoralen and ultra-
violet A (PUVA), radiotherapy (electron beam, orthovoltage), Ultraviolet Light
and systemic chemotherapy. Interferons, retinoids, and mono- Natural sunlight contains ultraviolet B (UVB, 280320
clonal antibodies have also been used. Extracorporeal photo- nm), UVA (320400 nm), and visible light. The UVB radia-
pheresis has been used in the treatment of cutaneous T-cell tion causes sunburn reaction. It has been used in combina-
lymphoma. tion with tar for treating psoriasis. It also may benefit atopic
dermatitis, lichen planus, and certain other inflammatory
dermatoses.
PSORIASIS
Narrow-Band UVB
Psoriasis is a chronic, inflammatory, multisystem disease with The wavelength of UVB with therapeutic effect for pso-
considerable skin and joint signs that occurs in 2% of the US riasis has been identified in the 311-nm range. Light units pro-
population. Onset is most common in the third decade of life, ducing this wavelength have been developed (narrow-band
and about a third of patients have a family history of psoriasis. UVB) and have been shown to be more effective than tradi-
Psoriasis commonly presents with discrete red plaques cov- tional UVB for the treatment of psoriasis.
ered with a silvery scale. Patterns of psoriasis include psoriasis
vulgaris, which presents with plaques involving the elbows, Psoralen and Ultraviolet A
knees, and scalp. Guttate psoriasis is an acute form that often Therapy with PUVA consists of ingestion of psoralen fol-
follows streptococcal pharyngitis and presents with small, lowed by exposure of the skin to UVA light. It has been used
scaly papules of psoriasis on the trunk and limbs. Other, less most commonly for therapy of generalized psoriasis, but it
common, forms of psoriasis include pustular psoriasis, which is also effective for the treatment of lichen planus, mycosis
may be localized to the hands and feet or may be generalized. fungoides, urticaria pigmentosa, and vitiligo. This therapy is
Approximately 50% of patients with psoriasis have nail abnor- associated with minimal systemic adverse effects but is associ-
malities, most commonly onycholysis, pitting, and oil spots. ated with an increased risk of cutaneous squamous cell carci-
Lesions of psoriasis may occur at previous sites of trauma noma and melanoma in patients who have received long-term
(koebnerization). Medications such as lithium, -adrenergic therapy.
blockers, and antimalarials and discontinuation of the use of
systemic corticosteroids can precipitate or exacerbate psoria- Ultraviolet light is commonly used for therapy of
sis. Psoriatic arthritis occurs in 5% to 8% of patients with skin generalized psoriasis and other inflammatory dermatoses.
psoriasis.
PUVA, a form of phototherapy, consists of oral psoralen
The onset of psoriasis most often occurs in the third decade followed by UVA light exposure.
of life. Therapy with PUVA is associated with an increased risk of
One-third of patients have a family history of psoriasis. cutaneous squamous cell carcinoma and melanoma with
long-term use.
Psoriasis typically presents with red plaques with silver
scale on elbows, knees, and scalp.
ATO P I C D E R M AT I T I S
About 50% of patients have nail abnormalities.
Atopy is manifested by atopic dermatitis, asthma, and aller-
Psoriasis occurs at sites of trauma (koebnerization). gic rhinitis or conjunctivitis. Atopic dermatitis often presents
in the neonatal period with scaling and erythema of the scalp
The treatment of psoriasis includes topical corticoster- and face, later spreading to the trunk. The distribution is often
oids, topical tar preparations, and phototherapy. Newer extensor in the older infant, and by the age of approximately
treatments for localized psoriasis include a topical synthetic 3 years distribution is the more classic flexural. In adolescence,
vitamin D analogue, calcipotriene, and a topical retinoid, facial involvement (perioral, eyelid, and forehead) is common.
tazarotene. Generalized flares of eczema can occur at any age.
Systemic agents used in the treatment of resistant psoriasis Disturbances in cell-mediated immunity lead to an
include methotrexate, acitretin, and cyclosporine. increased incidence of bacterial and viral infections. Secondary
colonization with Staphylococcus aureus presents as a weeping,
crusting dermatitis (impetiginization). Eczema herpeticum is a
Targeted Therapy in Psoriasis secondary infection with the herpes simplex virus, which may
Research into the pathogenesis of psoriasis has shown that be generalized. In patients with atopic dermatitis, infections
the disease is T-cellmediated. This knowledge has led to with the human papillomavirus and molluscum contagiosum
the development of several antibody-based or fusion pro- are also common and the lesions are more numerous.
teinbased targeted therapies. Infliximab, etanercept, and
adalimumab (antitumor necrosis factor- agents) have been Eczema herpeticum, a generalized herpes simplex virus
effective in the treatment of psoriasis. infection, may occur in patients with atopic dermatitis.
Allergic contact dermatitis is a form of localized or general- Papular or pustular Same as above, plus topical or systemic
ized dermatitis that results from exposure to an antigen. This antibiotics
is a type 4 hypersensitivity reaction (delayed, cell-mediated). Cystic Systemic antibiotics; if severe, isotretinoin
Recognition of antigens by T lymphocytes requires participa-
tion of Langerhans cells, which are the antigen-presenting
cells of the epidermis. One must consider the anatomical loca- AC N E V U L G A R I S
tion of the cutaneous lesions and environmental exposure to
allergens, including occupational, household, and recreational Acne vulgaris is one of the most common problems addressed
contactants, to define the cause of the contact dermatitis. in clinical dermatology. Acne occurs physiologically at
puberty with varying degrees of severity but may persist into
Allergic contact dermatitis is a type 4 hypersensitivity the second and third decades of life. The pathogenesis of acne
reaction (delayed, cell-mediated). is multifactorial; inheritance, increase in sebaceous gland
activity, hormonal influences, disturbances of keratinization,
Langerhans cells are the antigen-presenting cells of the and bacterial infection have all been implicated. The primary
epidermis. lesions of acne are noninflammatory and include microcome-
dones, closed comedones (whiteheads), and open comedones
Patch testing is performed by applying substances to a (blackheads). The secondary or inflammatory lesions include
patients back; each substance is placed under a small alumi- papules and pustules, nodules, and cysts. Treatment options
num disk covered with adhesive tape. These are left on the for acne are given in Table 47.2.
patients back for 48 hours, and the results are interpreted
at 48 and 96 hours. Positive reactions occur most often to
the following antigens: nickel sulfate, potassium dichro- Systemic Retinoid Use in Acne Vulgaris
mate, thimerosal, paraphenylenediamine, ethylenediamine, Isotretinoin (13-cis-retinoic acid) is a synthetic vitamin A deriv-
neomycin sulfate, benzocaine, thiuram, formaldehyde, and ative used primarily for the treatment of severe nodulocystic
fragrance. acne vulgaris. The mechanism of action of 13-cis-retinoic acid
Nickel sulfate allergies are mainly associated with inex- in acne is probably multifactorial, including improvement in
pensive jewelry. Paraphenylenediamine is present in hair dyes keratinization, decrease in sebum production, and decrease in
and other cosmetics; para-aminobenzoic acid in sunscreens is inflammation. A 20-week course at a dosage of approximately
immunologically related to paraphenylenediamine. Potassium 1 mg/kg per day is the standard regimen.
dichromate sensitivity is one of the most common types of
occupational allergic contact dermatitis and occurs in con-
Isotretinoin is used for the treatment of severe acne
struction workers exposed to cement, leathers, and certain
vulgaris.
paints. Formaldehyde is a common preservative in cosmetics
and shampoos. Neomycin sulfate and benzocaine are com-
The greatest risk associated with use of systemic retinoids
ponents of many topical antimicrobial and analgesic prepara-
is teratogenicity. Before isotretinoin is prescribed, female
tions. Thimerosal is a commonly used preservative in contact
patients must be counseled on this adverse effect and use reli-
lens solutions and in some intramuscular injections. Thiuram
able contraception during therapy and for at least 1 month
is a rubber accelerator and fungicide and therefore may cor-
after use of the drug is discontinued.
relate with occupational dermatitis related to wearing shoes
containing rubber or rubber gloves. Allergic contact dermati-
The greatest risk with the use of systemic retinoids is
tis to thiuram and other rubber accelerators is associated with
teratogenicity.
rubber glove use in health care workers.
The systemic retinoids are associated with various adverse
Nickel sulfate allergies are associated with inexpensive
effects, including xerosis (dry skin), dermatitis, cheilitis,
jewelry.
sticky skin, peeling skin, epistaxis, conjunctivitis, hair loss,
Potassium dichromate sensitivity occurs in construction and nail dystrophy. Symptoms of arthralgias and myalgias
workers exposed to cement, leathers, and certain paints. also may occur. Hyperlipidemia, including both hypertri-
glyceridemia and hypercholesterolemia, develops in most
Formaldehyde is a common preservative in cosmetics and
patients. Other potential laboratory abnormalities include
shampoos.
increased liver enzyme values and leukopenia. Skeletal hyper-
Allergic contact dermatitis to thiuram and other rubber ostosis may occur, particularly in association with long-term
accelerators is associated with rubber glove use in health use. Concerns regarding depression and suicidal ideation are
care workers. being studied.
656 D E R M ATO L O GY
Almost all cases have deposition of C3 and IgG in a linear
pattern at the basement membrane zone.
BP230 and BP180 antibodies may be present in patients
with bullous pemphigoid.
Adverse effects of systemic retinoids include xerosis, On direct immunofluorescence testing, epidermolysis
dermatitis, cheilitis, sticky skin, peeling skin, epistaxis, bullosa acquisita has a pattern similar to that in bullous pem-
conjunctivitis, hair loss, and nail dystrophy. Concerns phigoid, namely, deposition of IgG and C3 in a linear pat-
regarding depression and suicidal ideation are being tern at the basement membrane zone. In contrast to bullous
studied. pemphigoid, C3 may be absent or IgG may be the dominant
immunoreactant. Indirect immunofluorescence testing of
serum shows IgG antibasement-membrane zone antibodies
AU TO I M MU N E BU L L O US D I S E A S E S in 25% to 50% of patients. Epidermolysis bullosa acquisita
tends to be resistant to immunosuppressive therapy.
Bullous pemphigoid (Figure 47.1) is the most common auto-
immune blistering disease. The disease predominantly occurs On direct immunofluorescence, epidermolysis bullosa
in elderly patients and usually presents with large, tense bul- acquisita shows deposition of IgG and C3 in a linear
lae on an erythematous base with a predilection for flexural pattern at the basement membrane zone.
areas.
Epidermolysis bullosa acquisita tends to be resistant to
Bullous pemphigoid is the most common autoimmune immunosuppressive therapy.
blistering disease.
Cicatricial pemphigoid is characterized by mucosal
It occurs predominantly in elderly patients. lesions, with limited or no cutaneous lesions. The disease pre-
It presents as large, tense bullae with a predilection for dominantly affects oral and ocular mucous membranes and,
flexural areas. less frequently, the genital, pharyngeal, or upper respiratory
mucosa. This disease is also known as benign mucous mem-
Autoantibodies induce disruption at the skins base- brane pemphigoid, which is a misnomer because untreated
ment membrane zone, leading to subepidermal blisters. ocular involvement may lead to blindness. Patients may pre-
Immunofluorescence testing of a skin sample is important sent with oral erosions or diffuse gingivitis.
for the diagnosis of bullous pemphigoid. Direct immuno-
fluorescence testing of perilesional skin shows deposition of Cicatricial pemphigoid affects oral and ocular mucous
C3 in a linear pattern at the basement membrane zone in membranes and, less frequently, genital, pharyngeal, or
almost all cases and of immunoglobulin (Ig) G in more than upper respiratory mucosa.
90%. Indirect immunofluorescence testing of serum shows
IgG antibasement-membrane zone antibodies in approxi- Treatment of cicatricial pemphigoid is similar to that of
mately 70% of cases. Targeted antigens in bullous pemphigoid bullous pemphigoid, namely, systemic corticosteroids, dap-
include bullous pemphigoid antigen 1 (BP230) and Bullous sone, azathioprine, cyclophosphamide, and mycophenolate.
Pemphigoid Antigen 2 (BP180). These bullous pemphigoid Cyclophosphamide has been used particularly in patients with
antibodies can be measured with enzyme-linked immunosor- ocular involvement.
bent assay. Herpes gestationis consists of intensely pruritic urticarial
papules, plaques, or blisters, usually occurring in the latter half
Immunofluorescence testing is important for the diagnosis of pregnancy. The lesions are histologically characterized by a
of bullous pemphigoid. subepidermal bulla with eosinophils.
658 D E R M ATO L O GY
High-dose corticosteroids generally are required to control
pemphigus, followed by institution of a steroid-sparing
agent.
E RY T H E M A MU LT I F O R M E
Erythema multiforme (Figure 47.4) is an acute, usually
self-limited eruption of maculopapular, urticarial, occasionally
bullous lesions characterized morphologically by iris or target
lesions. A subset of patients with erythema multiforme may
have recurrent lesions. When erythema multiforme presents
with extensive cutaneous and mucosal lesions, it is referred to
as Stevens-Johnson syndrome. Various etiologic factors have
been implicated in erythema multiforme. The most com-
Figure 47.3 Pemphigus Foliaceus.
monly cited precipitating factor is viral infection, particularly
herpes simplex virus. This is responsible for a considerable per-
centage of recurrent erythema multiforme. Other infectious
The clinical variants of pemphigus include pemphigus vul- agents that have been noted to cause erythema multiforme
garis and pemphigus foliaceus (with the subsets pemphigus include Mycoplasma pneumoniae and Yersinia enterocolitica.
erythematosus and fogo selvagem, the latter being an endemic Drugs have been reported to induce erythema multiforme,
form of pemphigus that occurs in South America). There is particularly sulfonamides, barbiturates, and anticonvulsants.
also a drug-induced variant of pemphigus, particularly associ- Erythema multiforme also may be associated with underly-
ated with D-penicillamine, captopril, or other thiol-containing ing connective tissue disease or malignancy. Erythema multi-
medications. forme tends to involve the lips, buccal mucosa, and tongue, in
More than 50% of patients with pemphigus vulgaris pre- contrast to pemphigus vulgaris, which typically involves the
sent with oral lesions, and more than 90% have oral mucosal pharynx, buccal mucosa, and tongue, and pemphigoid, which
involvement at some point in the course of the disease. most often involves gingivae. Neither pemphigus nor pemphi-
Pemphigus vulgaris is characterized by coalescing blisters and goid involves the lips.
erosions, often with generalized involvement. In contrast,
pemphigus foliaceus (Figure 47.3), considered to represent the The most commonly cited precipitating factor for erythema
superficial variant of pemphigus, may present with superficial multiforme is viral infection, particularly herpes simplex.
scaling-crusting lesions of the head and neck area (in a sebor-
rheic dermatitis-like pattern) or generalized distribution. Other infectious agents are Mycoplasma pneumoniae and
Yersinia enterocolitica.
Pemphigus vulgaris is characterized by coalescing blisters Drugs also induce erythema multiforme: sulfonamides,
and erosions. barbiturates, and anticonvulsants.
Pemphigus foliaceus may present with superficial
scaling-crusting lesions of the head and neck. E RY T H E M A N O D O S U M
All types of pemphigus are characterized by the deposi- Erythema nodosum (Figure 47.5) typically presents as ten-
tion of IgG and C3 at the intercellular space (epidermal cell der, erythematous, subcutaneous nodules localized to the
surface) on direct immunofluorescence testing (intercellular
substance [ICS] antibody). On indirect immunofluorescence
testing, IgG anti-ICS antibodies are found in approximately
90% of cases. The titer of IgG anti-ICS antibodies is useful for
both diagnosis and management of pemphigus.
Phototoxic Tetracyclines
Figure 47.5 Erythema Nodosum. About 2% of hospitalized patients have cutaneous drug
reactions.
pretibial areas. The nodules may be acute and self-limited or Penicillin, sulfonamides, and blood products are
chronic, lasting for months to years. The most common cause responsible for about two-thirds of drug reactions.
is streptococcal pharyngitis. Other infectious agents that have
been implicated in the development of erythema nodosum Urticarial drug reactions are most often related to aspirin,
include Yersinia enterocolitica, Coccidioides, and Histoplasma. penicillin, and blood products.
Drug-induced erythema nodosum most often is associated Photoallergic reactions are most often associated
with oral contraceptives and sulfonamides. Other associations with sulfonamides, thiazides, griseofulvin, and
with erythema nodosum include sarcoidosis, inflammatory phenothiazines.
bowel disease, and Behet syndrome.
Phototoxic reactions may be induced by tetracyclines.
The most common cause of erythema nodosum is
streptococcal pharyngitis. Exanthematous or morbilliform eruptions are the most
common type of cutaneous drug reaction. This type of
Drug-induced erythema nodosum most often is associated eruption usually begins within a week of onset of therapy,
with oral contraceptives and sulfonamides. but it may occur more than 2 weeks after initiation of the
Other associations of erythema nodosum are sarcoidosis, therapy or up to 2 weeks after use of the drug has been dis-
inflammatory bowel disease, and Behet syndrome. continued. Ampicillin, penicillin, and cephalosporins are
commonly associated with morbilliform eruptions. A fixed
drug eruption is one or several lesions that recur at the same
anatomical location on rechallenge with the medication. The
D RU G R E AC T I O NS
genital and facial areas are common sites of involvement.
The morphologic spectrum of reactions that may be induced Phenolphthalein, barbiturates, salicylates, and oral contra-
by medications is broad, and hundreds of drugs may produce a ceptives have been implicated in the cause of fixed drug erup-
given cutaneous reaction. Types of cutaneous lesions induced tions. Lichenoid drug eruptions are morphologically similar
by drugs include maculopapular eruptions, acne, folliculitis, to lichen planus (with violaceous papules of the skin) and
necrotizing vasculitis, vesiculobullous lesions, erythema mul- most often have been associated with gold and antimalarial
tiforme, erythema nodosum, fixed drug eruptions, lichenoid drugs, although various medications may induce this type of
reactions, photosensitivity reactions, pigmentary changes, and reaction.
hair loss.
Approximately 2% of hospitalized patients have cutane- Exanthematous or morbilliform eruptions are the most
ous drug reactions, and penicillin, sulfonamides, and blood common cutaneous drug reaction.
products are responsible for approximately two-thirds of such
A fixed drug eruption is one or several lesions that recur at
reactions. The most common types of clinical presentations
the same location on rechallenge.
(in descending order of frequency) are exanthematous or mor-
billiform eruptions, urticaria or angioedema, fixed drug erup- Phenolphthalein, barbiturates, salicylates, and oral
tions, and erythema multiforme. Stevens-Johnson syndrome, contraceptives are implicated in fixed drug eruptions.
660 D E R M ATO L O GY
C U TA N E O U S S I G N S O F U N D E R LY I N G
M ALIGNANCY
Acanthosis nigricans may be associated with Glucagonoma syndrome consists of erosions, crusting, and
adenocarcinoma of the gastrointestinal tract, particularly peeling involving the perineum and perioral areas.
the stomach. It is associated with an islet cell tumor of the pancreas.
Figure 47.6 Acanthosis Nigricans. Figure 47.8 Glucagonoma Syndrome (Necrolytic Migratory Erythema).
Acquired ichthyosis most often has been associated with Dermatomyositis is associated with an increased incidence of
Hodgkin disease, but it has been reported with other types of underlying malignancy.
lymphoma, multiple myeloma, and various carcinomas.
Dermatomyositis may involve the periorbital area
(heliotrope rash) or the dorsal aspect of the hands
Acquired ichthyosis is associated with Hodgkin disease.
(Gottron papules).
Hirsutism may reflect androgen excess due to an adrenal or The lesions are photosensitive and pruritic.
ovarian tumor, but hypertrichosis is an increase in hair unrelated Dermatomyositis is characterized by proximal myositis.
to androgen excess, such as hypertrichosis lanuginosa acquisita
(growth of soft downy hair). It has been associated with carci- Dermatomyositis is associated with an increased risk of
noid tumor, adenocarcinoma of the breast, lymphoma, gastro- internal malignancy.
intestinal malignancy, and other types of neoplasms.
Sweet syndrome (acute febrile neutrophilic dermatosis) Amyloidosis may present clinically as macroglossia
has skin lesions that consist of erythematous plaques and nod- (Figure 47.11), waxy papules on the eyelids or nasolabial folds,
ules, most commonly located on the proximal aspects of the pinch purpura, and postproctoscopic purpura (Figure 47.12).
extremities and face. The association is with leukemia, par- Amyloidosis may be associated with multiple myeloma.
ticularly acute myelocytic or acute myelomonocytic leukemia,
although many other diseases also have been associated. Amyloidosis may be associated with multiple myeloma.
Sweet syndrome is associated with leukemia (acute Tylosis is a rare disorder characterized by palmar-plantar
myelocytic or acute myelomonocytic). keratoderma associated with esophageal carcinoma. It has
autosomal dominant inheritance.
Generalized pruritus is the presentation for many cutane-
ous and systemic disorders. Pruritus may be the presenting Tylosis is associated with esophageal carcinoma.
symptom in lymphoma.
The autoimmune bullous diseases are a heterogeneous
Pruritus may be the presenting symptom in lymphoma. group of disorders characterized by antibody deposition at the
basement membrane zone or epidermis. An association with
In dermatomyositis, the pathognomonic skin lesions are malignancy has been found in several of these disorders.
Gottron papules (Figure 47.9) involving the skin over the
joints of the fingers, elbows, and knees. Poikilodermatous
lesions or erythematous maculopapular eruptions may dif-
fusely involve the face, particularly the periorbital area
(heliotrope rash [Figure 47.10]), and the trunk and extremi-
ties. The cutaneous lesions are photosensitive and pruritic.
The disease is characterized by proximal myositis. Although
creatine kinase and aldolase levels usually are increased in
patients with myositis, it is important to verify the diagnosis
by obtaining an electromyogram or a muscle biopsy specimen. Figure 47.10 Dermatomyositis: Heliotrope Discoloration.
662 D E R M ATO L O GY
Acute sarcoidosis may present with a combination of ery-
thema nodosum, bilateral hilar lymphadenopathy, fever, and
arthralgias (Lfgren syndrome). Erythema nodosum (Figure
47.5) is a reactive condition that may be associated with acute
sarcoidosis. Erythema nodosum typically presents as tender, ery-
thematous, subcutaneous nodules localized to pretibial areas.
C A R D I OVA S CU L A R
Pseudoxanthoma elasticum may be transmitted by autosomal
dominant or autosomal recessive inheritance. Yellow xanthoma-
like papules (plucked-chicken skin) occur on the neck, axillae,
groin, and abdomen. Angioid streaks may occur in the fundus
of the eye. Skin biopsy shows degeneration of elastic fibers.
Systemic associations include stroke, myocardial infarction,
Figure 47.12 Amyloidosis: Postproctoscopic Purpura. peripheral vascular disease, and gastrointestinal hemorrhage.
Acrodermatitis enteropathica is an inherited (autosomal Bowel bypass syndrome presents with a flu-like illness with
recessive) or acquired disease. fever, malaise, arthralgias, myalgias, and inflammatory papules
and pustules on the extremities and upper trunk. The disease
The disease is characterized by zinc deficiency (failure of is recurrent and episodic and occurs in up to 20% of patients
absorption or failure to supplement). after jejunoileal bypass. The condition responds to antibiotics
or to reversal of the bypass procedure.
Peutz-Jeghers syndrome is an inherited (autosomal domi-
nant) syndrome of intestinal polyposis. Patients have ham-
Bowel bypass syndrome presents with a flu-like illness and
artomas, mostly involving the small bowel, and a slightly
inflammatory papules and pustules.
increased risk for carcinoma. Cutaneous lesions include macu-
lar pigmentation (freckles) of the lips, periungual skin, fingers, Bowel bypass syndrome occurs in up to 20% of patients
and toes and pigmentation of the oral mucosa. after jejunoileal bypass.
664 D E R M ATO L O GY
Gardner syndrome and glucagonoma syndrome are
described earlier in this chapter.
N E P H RO L O G I C
Partial lipodystrophy is associated with C3 deficiency and
the nephrotic syndrome. Uremic pruritus is associated with
end-stage renal disease and responds to UVB therapy.
N EU RO C U TA N E O US
Fabry disease is an X-linked recessive disorder due to defi-
ciency of the enzyme -galactosidase A. The skin changes
consist of numerous vascular tumors (angiokeratomas) in a
bathing-suit distribution that develop during childhood
and adolescence. Corneal opacities are present in 90% of
patients. Systemic manifestations include paresthesias and
pain due to involved peripheral nerves, renal insufficiency,
and vascular insufficiency of the coronary and central ner-
vous system.
Associated features are intracranial calcification, mental In rheumatoid arthritis, rheumatoid nodules may occur
retardation, epilepsy, contralateral hemiparesis, and visual over the extensor surfaces of joints, most commonly on the
impairment. dorsal aspects of the hands and elbows. Rheumatoid vasculitis
with ulceration may occur in the setting of rheumatoid arthri-
R H EU M ATO L O G I C tis with a high circulating rheumatoid factor.
During the late stages of gout, tophi (urate deposits with
Psoriatic arthritis occurs in 5% to 8% of patients with cutane- surrounding inflammation) occur in the subcutaneous tissues.
ous psoriasis. Several different patterns of arthritis occur. An Improved methods of treatment account for the decrease in
asymmetric oligoarthritis occurs in 70% of patients. This group the incidence of tophaceous gout in recent years.
includes patients with sausage digits and monoarthritis. The
second most common presentation is asymmetric arthritis Gouty tophi may occur in subcutaneous tissues.
clinically similar to rheumatoid arthritis, which occurs in
15% of patients with psoriatic arthritis. Distal interphalangeal In lupus erythematosus (LE), cutaneous abnormalities
involvement, arthritis mutilans, and a spinal form of arthritis occur in approximately 80% of patients. The skin manifesta-
similar to ankylosing spondylitis each occurs in 5% of patients tions of lupus can be classified into acute cutaneous LE (malar
with psoriatic arthritis. rash, generalized photosensitive dermatitis, or bullous LE), sub-
acute cutaneous LE (annular or papulosquamous variants), and
Psoriatic arthritis occurs in 5%-8% of patients with chronic cutaneous LE (localized discoid LE, generalized discoid
psoriasis. LE, lupus panniculitis, tumid lupus, or chilblain lupus).
Asymmetric oligoarthritis is the most common pattern of
psoriatic arthritis. In LE, cutaneous abnormalities occur in 80% of patients.
666 D E R M ATO L O GY
of discoid LE at some point during the course of their illness.
Circulating antinuclear antibodies are demonstrable in most
patients with systemic LE and subacute cutaneous LE, but
they are present in only a small percentage of patients with
discoid LE.
Subacute cutaneous LE presents with annular plaques. Systemic scleroderma may include sclerodactyly, periungual
telangiectasia, telangiectatic mats, hyperpigmentation, and
Subacute cutaneous LE is characterized by the presence of cutaneous calcification.
anti-Ro (anti-SSA) antibodies and photosensitivity.
668 D E R M ATO L O GY
Figure 47.18 Necrobiosis Lipoidica Diabeticorum. Figure 47.19 Granuloma Annulare.
The stiff-hand syndrome has been reported in juvenile-onset Erythropoietic porphyria is a hereditary form (autosomal
insulin-dependent diabetes. Patients have limited joint mobil- recessive) characterized by marked photosensitivity, blisters,
ity and tight waxy skin on the hands. There is an increased risk scarring alopecia, hirsutism, red-stained teeth, hemolytic ane-
of subsequent renal and retinal microvascular disease. mia, and splenomegaly. The skin lesions are severely mutilat-
ing. Onset is in infancy or early childhood.
Stiff-hand syndrome is associated with an increased risk of
subsequent renal and retinal microvascular disease. Erythropoietic porphyria is autosomal recessive.
Skin lesions are severely mutilating.
In scleredema, there is an insidious onset of thickening and
stiffness of the skin on the upper part of the back and poste- Erythropoietic protoporphyria is an autosomal dominant
rior aspect of the neck. The diabetes is often long-standing and syndrome that usually begins during childhood. It is charac-
poorly controlled. terized by variable degrees of photosensitivity and a marked
itching, burning, or stinging sensation that occurs within
Scleredema is the onset of thickening of the skin on the minutes after sun exposure. It is associated with deficiency of
upper part of the back and posterior aspect of the neck. ferrochelatase.
In scleredema, diabetes is often long-standing and poorly
controlled. Erythropoietic protoporphyria is autosomal dominant.
It is associated with deficiency of ferrochelatase.
670 D E R M ATO L O GY
morbilliform, vesicular, or pityriasis rosea-like. Oral ulceration Epidemic Kaposi sarcoma usually presents as oval papules
and erosions, genital erosions, and erosive esophagitis also or plaques oriented along skin lines of the trunk, extremities,
may occur at this stage. The acute exanthem and enanthem are face, and mucosa. This presentation is in contrast to that of
self-limited and often go undiagnosed. classic Kaposi sarcoma in elderly patients, which occurs pre-
In the early stage of the disease, cutaneous manifestations dominantly on the distal lower extremities. Human herpesvi-
include genital warts, genital herpes, psoriasis, mild sebor- rus 8 (HHV-8) has been identified in tissue from patients with
rheic dermatitis, xerosis, and pruritic papular eruption. With both epidemic and classic Kaposi sarcoma.
symptomatic HIV infection (CD4 count of 200400/mcL),
both infections and inflammatory dermatoses occur more fre- Epidemic Kaposi sarcoma presents as oval papules or
quently. These include psoriasis, seborrheic dermatitis, oral plaques along skin lines of the trunk, extremities, face, and
hairy leukoplakia, candidiasis, herpes zoster, drug reactions, mucosa.
herpes simplex, tinea pedis, and onychomycosis. In patients
with a family history of atopy, atopic dermatitis may be a man- It is most commonly associated with HIV infection.
ifestation at this stage.
As the CD4 count decreases to less than 200/mcL, patients S U M M A RY
may present with a disseminated fungal infection, recur-
rent or severe herpes zoster, persistent herpes simplex, bac- Skin cancer is the most common cancer in the United
illary angiomatosis, and molluscum contagiosum. Bacillary States, accounting for almost half of all cancers.
angiomatosis consists of one or more vascular papules or
nodules caused by the gram-negative bacteria Bartonella Micrometastasis to the first draining lymph node (sentinel
quintana and Bartonella henselae. Eosinophilic folliculitis, a lymph node) is the most powerful staging and prognostic
pruritic eruption primarily involving the head, neck, trunk, tool for melanoma.
and proximal extremities, is characteristic of symptomatic Ultraviolet light is commonly used for therapy of
HIV infection. generalized psoriasis and other inflammatory dermatoses.
With advanced HIV infection (CD4 counts of <50/
mcL), overwhelming infection is characteristic. Infectious Immunofluorescence testing is important for the diagnosis
agents with skin manifestations include cytomegalovi- of bullous pemphigoid.
rus, Cryptococcus, Acanthamoeba, and extensive molluscum
Penicillin, sulfonamides, and blood products are
contagiosum.
responsible for about two-thirds of drug reactions.
Oral hairy leukoplakia is caused by Epstein-Barr virus
infection of the oral mucosa and usually occurs in patients Cutaneous metastasis occurs in 1%-5% of patients with
with advanced HIV infection. metastatic neoplasms.
Molluscum contagiosum, a common viral infection of oth-
In ANCA-associated granulomatous vasculitis, cutaneous
erwise healthy children, occurs in 10% to 20% of patients with
involvement occurs in >50% of patients.
HIV infection.
Pseudoxanthoma elasticum is associated with stroke,
Molluscum contagiosum occurs in 10%-20% of patients myocardial infarction, peripheral vascular disease, and
with HIV infection. gastrointestinal hemorrhage.
675
Table 48.1 GENETIC DISORDERS CAUSED BY CHROMOSOME ABNORMALITIES
Ehlers-Danlos syndrome Defect in gene coding for collagen. The Velvety textured, hyperextensible, & fragile skin
defect varies based on the subtype of Joints are hyperextensible & prone to dislocation
Ehlers-Danlos syndrome Mitral valve prolapse occurs in many patients
Most severe form results in tendency for arterial aneurysms &
visceral organ rupture
Hypertrophic cardiomyopathy Molecular defects in more than 20 dif- One of the most common causes of sudden death in adolescents
ferent genes can cause hypertrophic & young adults
cardiomyopathy All first-degree relatives should be evaluated
Course is variable
Marfan syndrome Defect in fibrillin-1 gene Involves musculoskeletal, ocular, & cardiovascular systems
Tall stature, scoliosis or kyphosis, & pectus deformities present
Dislocations of the lens occur in 50%-80%
All patients should have ophthalmologic evaluation
Cardiovascular manifestations include mitral valve prolapse &
dilatation of the ascending aorta
-Adrenergic blockers might delay progressive
aortic dilatation
Surgical treatment is often successful for mitral & aortic regurgi-
tation & aortic dissection
About 20% of cases arise by new mutation
Myotonic dystrophy Triplet repeat expansion in myotonin Most common form of muscular dystrophy in adults
protein kinase gene Diagnosis is based on clinical findings & a typical electro-
myographic pattern characterized by prolonged rhythmic
discharges
Genetic counseling is warranted for patients & family members
Age at onset is usually the second to third decade of life
Myotonia, muscle atrophy & weakness, ptosis of eyelids, expres-
sionless facies, & premature frontal baldness
(continued)
Neurofibromatosis 1 & 2 Multiple different mutations have been Neurofibromatosis 1 has markedly variable expression but very
identified high penetrance
Malignancy (often peripheral nerve sheath tumors) develops in
approximately 10% of patients
Characteristics of neurofibromatosis 2 are vestibular schwanno-
mas, nervous system gliomas, & subcapsular cataracts
Osler-Weber-Rendu disease Multiple genetic defects have been Characterized by abnormal blood vessel formation in the skin,
(hereditary hemorrhagic identified mucous membranes, lungs, liver, & brain
telangiectasia) Arteriovenous malformations occur in larger organs
Nosebleeds & gastrointestinal bleeding are common
Tuberous sclerosis complex One gene defect that causes tuberous About 50% of cases arise by new mutation
sclerosis is located on chromosome Characterized by nodules of the brain & retina, seizures, mental
9 (hamartin) & another is located on retardation in <50%, depigmented ash leaf or confetti
chromosome 16 (tuberin) macules, facial angiofibromas, dental pits, subungual fibro-
mas, & angiomyolipomas
Von Hippel-Lindau disease The gene that causes von Hippel-Lindau Typical case of von Hippel-Lindau disease: retinal, spinal cord,
disease (VHL) is localized to & cerebellar hemangioblastomas; cysts of kidneys, pancreas,
chromosome 3p2526. The normal gene & epididymis
has a key role in cellular response to Renal cysts, hemangiomas, & benign adenomas are usually
hypoxia & acts as a tumor suppressor asymptomatic
Retinal hemangioblastomas may be the earliest manifestation
Periodic magnetic resonance imaging with gadolinium is
recommended
Renal cancer is a major cause of death
Friedreich ataxia The gene involved, FXN, is localized to chromosome First sign of the disease is ataxic gait
9q13. The most frequent mechanism of mutation is Mean age at onset is approximately 12 years
expansion of a GAA trinucleotide repeat that results Dysarthria, hypotonic muscle weakness, loss of vibration & posi-
in abnormal accumulation of intramitochondrial tion senses, & loss of deep tendon reflexes develop subsequently
iron The major cause of death is cardiomyopathy
Gaucher disease Deficiency of the enzyme glucocerebrosidase, which Frequent in Ashkenazi Jews
results in lipid storage in the spleen, liver, bone May be asymptomatic or present in childhood or adulthood with
marrow, and other organs hepatosplenomegaly, thrombocytopenia, anemia, degenerative
bone disease, osteoporosis, or pulmonary disease
Enzyme replacement & substrate reduction therapies are effective
for nonneuronopathic Gaucher disease
Glucose-6-phosphate Abnormally low levels of G-6PD is important in red blood cell metabolism
dehydrogenase glucose-6-phosphate Most common human enzyme defect
deficiency (G-6PD) dehydrogenase Patients may experience hemolytic anemia due to infection, fava ingestion, medications
including antimalarials (primaquine & chloroquine), sulfa drugs, & isoniazid
Heinz bodies on peripheral smear
Coombs test negative
4 8. G E N ET I C S 677
M I TO C H O N D R I A L MU TAT I O N S Common diseases such as diabetes mellitus, asthma,
hypertension, and coronary artery atherosclerosis may have
Mitochondria contain several circular copies of their own genetic multifactorial causation.
material called mitochondrial DNA. Mitochondrial disorders
can arise as new mutations or be maternally inherited; in most
cases, only the egg contributes mitochondria that persist in the I M P O RTA N C E O F A N AC C U R AT E
zygote, and the sperm usually does not. Many mitochondrial C L I N I C A L D I AG N O S I S
enzymes, including most of the respiratory chain complex, are
encoded by nuclear DNA and transported into the mitochon- Molecular genetic testing can be used for diagnosing a disor-
dria. Mitochondrial DNA mutations cause Leber optic atrophy der in a patient who is suspected of having a specific disease.
and the multisystem syndromes of mitochondrial myopathy, It also can be used for testing relatives who are at risk. The
encephalopathy, episodes of lactic acidosis, and stroke (MELAS), importance of a correct diagnosis in the index patient when
myoclonic epilepsy with ragged red fibers (MERRF), and neu- diagnosis by DNA analysis for a relative is being contemplated
ropathy, ataxia, and retinitis pigmentosa (NARP). cannot be overemphasized.
Mitochondrial disorders are usually maternally inherited. Accurate clinical diagnosis is critical and supersedes
laboratory testing.
MU LT I FAC TO R I A L C AU S AT I O N
679
S U P P O RT Box 49.1 RISK FACTORS FOR FALLS
If an elderly patient has a compromised functional state, the Lower extremity weakness
degree of social support available for him or her should be History of falls
determined. The physician needs to ascertain who is available Gait deficit
to help with various tasks to keep the individual safe in an inde- Balance deficit
pendent environment. Support usually includes family (most Use of assistive device
often an adult daughter), friends, and community services. A Visual deficit
financial assessment should be made to determine whether the Arthritis
patient can afford treatments recommended by the physician Impaired activities of daily living
or whether he or she qualifies for financial assistance from the Depression
government. Cognitive impairment
Age >80 y
A referral to social services may be needed to determine Multiple medications
whether the patient meets the criteria for the benefits or
services available.
EVA LUAT I O N O F FA L L S
A thorough medical history is the most important compo-
A D VA N C E D I R E C T I VE S
nent of the assessment of a fall. The history should include the
patients perception of the cause of the fall, any warning symp-
Advance directives should be discussed early with each elderly
toms the patient experienced before the fall, and any associ-
patient. It is important for the caregiver to know the patients
ated symptoms that occurred with the fall. The patient also
designated decision-maker and health carerelated prefer-
should be questioned about how he or she felt immediately
ences should the patient become unable to make decisions.
after the fall. Loss of consciousness may suggest a cardiac or
Living wills and a durable power of attorney for health care
neurologic event.
should be discussed and the directives reviewed periodically to
The physical examination should include a neurologic
determine whether the patient thinks they continue to reflect
examination that tests gait, balance, reflexes, sensory impair-
his or her wishes.
ment, and extremity strength. Any sensory impairment
should be noted. Because falls may be associated with acute
FA L L S illnesses, patients should be assessed for infections, myocardial
infarction, and gastrointestinal tract hemorrhage. Orthostatic
Falls are a common cause of morbidity and an important con- hypotension, although common among the elderly, also may
tribution to mortality among the elderly. It is estimated that indicate a medication effect or hypovolemia from hemorrhage
three-fourths of all deaths related to falls occur in persons or dehydration.
older than 65 years. The increased frequency of falls among
the elderly reflects multiple age-related changes, including A thorough medical history is the most important
decreased strength from loss of muscle mass, decreased visual component of the assessment of a fall.
and hearing acuity, decreased proprioception, and slowed The physical examination should include a neurologic
reaction time. These changes can produce an alteration of gait examination that tests gait, balance, reflexes, sensory
and decreased balance in an elderly person. impairment, and extremity strength.
Most falls (70%) occur in the persons home. An accident,
usually related to hazards in the environment (throw rugs,
slippery floors, lack of grab bars in bathtubs, and inadequate
lighting), is the most common cause of falls among the elderly P R EV E N T I O N A N D T R E AT M E N T O F FA L L S
who live independently. Most accidental falls occur while
The goal of the assessment of a fall is to decrease the likelihood
the person is performing typical daily activities such as walk-
of subsequent falls. The treatment plan is based on the find-
ing or changing position (eg, sitting to standing). The com-
ings of the assessment. However, more than 1 factor is often
mon risk factors for injuries related to falls include weakness
identified as contributing to falls. Potential interventions for
of the legs (stroke or neuropathy), gait instability (Parkinson
the prevention of falls may include the following:
disease), balance disorder (vertigo or orthostatism), cognitive
impairment (dementia), and the use of multiple medications
1. Reduction in environmental hazards: provide adequate
(Box 49.1).
lighting, remove obstacles from floors, eliminate slippery
floors, and use appropriate footwear
Falls among the elderly usually reflect decreased strength
from loss of muscle mass, decreased visual and hearing 2. Physical therapy: improves gait, balance, and strength,
acuity, decreased proprioception, and slowed reaction time. especially in the lower extremities
Most falls (70%) occur in the persons home. 3. Assistive devices: improve gait and balance
A combination of anatomical and physiologic changes related The most common eye problem in the elderly is
to aging and various disease states common in the elderly presbyopia.
frequently cause decreased vision. Vision loss increases with
Cataracts are very common in the elderly. Surgery with
advancing age, and more than 25% of those older than 85
intraocular lens implantation can restore visual acuity.
years report marked visual impairment. More than 90% of the
elderly wear eyeglasses, and it is estimated that 25% of nursing Glaucoma is characterized by increased intraocular
home residents are legally blind. The most common eye prob- pressure and associated optic nerve damage.
lem in the elderly is presbyopia (difficulty with close focus).
Macular degeneration is associated with the gradual
Presbyopia is the result of decreased lens flexibility, which
and progressive loss of central vision and the sparing of
occurs with aging. Cataracts are also more common with
peripheral vision.
advancing age; they begin forming early in life, but the pro-
gression varies from person to person. Cataract surgery with
intraocular lens implantation is effective for restoring visual HEARING CHANGES
acuity.
Notable hearing loss in the elderly is common and usually due
G L AU C O M A to a central auditory processing disorder, which causes diffi-
culty with speech perception. The prevalence of hearing loss,
Glaucoma is characterized by increased intraocular pressure especially of high frequencies (presbycusis), increases mark-
and associated optic nerve damage. The 2 major types of glau- edly among persons older than 65 years and approaches 50%
coma are chronic open-angle and angle-closure. in those older than 80. Presbycusis is typically bilateral and
Open-angle glaucoma is more common and occurs in up to associated with a high-frequency hearing loss.
70% of adults with glaucoma. Chronic open-angle glaucoma Causes of conductive hearing loss include cerumen impac-
produces a slow, progressive loss of peripheral vision that often tion, perforation of the tympanic membrane, cholesteatoma,
is not appreciated by the patient until a considerable amount Paget disease, and otosclerosis. Hearing aids may be beneficial.
of vision is lost. Funduscopic examination shows atrophy and Hearing aids are most beneficial when used in an environment
cupping of the optic disk. Visual field testing documents typi- with minimal background noise, for example, a one-on-one
cal peripheral field defects. conversation in a quiet room.
Several options are available for the treatment of glau-
coma, including surgery and medication. Medications are
The prevalence of hearing loss, especially of high
effective for decreasing the production of aqueous humor or
frequencies (presbycusis), increases markedly in the elderly.
for increasing its outflow. The goal of surgical treatment is to
increase the flow of aqueous humor. Causes of conductive hearing loss include cerumen
Acute angle-closure glaucoma is much less common impaction, perforation of the tympanic membrane,
than chronic open-angle glaucoma. Patients with acute cholesteatoma, Paget disease, and otosclerosis.
angle-closure glaucoma present with symptoms of intense eye
pain, blurred vision with halos around lights, headache, and
nausea. Physical examination shows a slightly dilated pupil S E XUA L F U N C T I O N A N D S E XUA L I T Y
unresponsive to light. Urgent treatment is necessary to pre-
vent permanent loss of vision. Multiple physical and social changes occur with aging that
can result in changes in the desire and capacity of an older
person for sexual activity. Although there is evidence that
M AC U L A R D EG E N E R AT I O N
interest in sexuality is retained well into older age, for several
Macular degeneration is the leading cause of blindness in per- reasons the frequency of sexual activity tends to be reduced
sons older than 50 years. Macular degeneration is associated with aging. One of the most important factors that may deter-
with the gradual and progressive loss of central vision and mine whether a person is sexually active is the availability of
4 9. G E R I AT R I C S 681
a partner who is capable of sexual activity. Painful conditions new tasks and information. Loss of memory begins with
such as osteoarthritis also may contribute to diminishing recent events and eventually includes memory of distant
desire for sexual activity. events. Both receptive and expressive language difficulties
Evidence suggests that androgens will increase sexual inter- develop in which the patient has difficulty naming famil-
est. Lack of estrogen can produce reduced vaginal lubrication iar objects and understanding language. Patients may eas-
and mucosal atrophy, which can cause dyspareunia. ily become lost, even in familiar surroundings. Calculation
skills decline and patients may no longer be capable of
One of the most important factors that may determine such tasks as balancing a checkbook. Eventually behavioral
whether a person is sexually active is the availability of a problems develop in many patients, including the tendency
partner. to wander and to develop paranoia, agitation, delusions, or
hallucinations.
Typically, patients with Alzheimer disease have little
M E M O RY I M PA I R M E N T insight into the disease process. Driving safety is often
impaired in persons with dementia, and the physician should
play a prominent role in discussing this with the patient and
M I L D C O G N IT I VE I M PA I R M E N T
his or her family. At times the physician may need to take
Mild cognitive impairment is dysfunction in some cognitive steps to prevent the patient from driving if safety is an issue.
domains, but it is not severe enough to interfere with activi- Pathologically, the CNS findings include neuronal
ties of daily life. Mild cognitive impairment may be associated plaques, which represent extracellular deposits of protein
only with memory complaints or there may be impairments in containing amyloid and neurofibrillary tangles. Alzheimer
multiple cognitive areas. Mild cognitive impairment is a risk disease is associated with a decreased amount of CNS neu-
factor for conversion to dementia. Nursing home placement rotransmitters such as acetylcholine, norepinephrine, and
rates are 2 to 3 times higher for the elderly with mild cognitive serotonin. Acetylcholine deficiency is especially prominent, as
impairment. No medications have been shown to decrease the is a decrease in choline acetyltransferase activity.
rate of conversion to dementia. Screening mental status examinations (such as the
Mini-Mental State Examination, Mini-Cog test) often
Mild cognitive impairment is a risk factor for development identify patients who may not have obvious cognitive
of dementia. impairment. If cognitive impairment is suspected but the
mental status examination findings are normal, formal psy-
chometric studies should be conducted. Normal findings on
DEMENTIA mental status examinations do not rule out dementia. The
Dementia is an acquired cognitive impairment that affects all Mini-Mental State Examination is also used to follow future
spheres of the intellect. It is a gradually progressive disorder. deterioration.
Approximately 10% of the population older than 65 years has The medical evaluation consists of a medical history and
dementia. Cognitive functions that can be affected include physical examination and general laboratory tests. Accepted
judgment, abstract thinking, attention, ability to learn new laboratory tests include a complete blood count, electrolytes,
material, and the recognition and production of speech. liver transaminases, blood urea nitrogen, creatinine, calcium,
The most common form of irreversible dementia is glucose, vitamin B12, thyroid function, syphilis serology, chest
Alzheimer disease (50%-70%), followed by vascular dementia radiography, and electrocardiography. CNS imaging study
(15%-25%). The most common causes of potentially revers- may be performed to rule out potentially reversible CNS pro-
ible dementia include depression, drugs, metabolic disorders, cesses such as mass lesions, normal-pressure hydrocephalus, or
toxic agents, nutritional deficiencies, normal-pressure hydro- previous strokes. Electroencephalography, testing for human
cephalus, subdural hematoma, central nervous system (CNS) immunodeficiency virus, and lumbar puncture are performed
tumors, and CNS infections. only in specific clinical situations.
Until recently, the treatment of Alzheimer disease has been
The most common form of irreversible dementia is limited to controlling abnormal behavior with neuroleptic
Alzheimer disease (50%-70%), followed by vascular medications. However, none of the neuroleptic medications
dementia (15%-25%). improve cognitive function and may worsen memory and ori-
entation. Major tranquilizers may cause movement disorders
Only 1%-2% of dementias are due to reversible causes. (tardive dyskinesia) and can contribute to falls.
The recent availability of acetylcholinesterase inhibitors
(tacrine, donepezil, rivastigmine, and galantamine) has given
ALZHEIMER DISEASE
clinicians the first real options for treating Alzheimer disease.
The diagnosis of Alzheimer disease cannot be confirmed Although acetylcholinesterase inhibitors are not considered
until postmortem examination. The clinical diagnosis disease-modifying drugs, they may transiently delay cognitive
is made primarily on the basis of the history. The disease decline and should be considered for patients who have mild
is a gradually progressive impairment of cognition. It is to moderate dementia. The major benefit of these drugs is
characterized by gradually progressive difficulty learning their potential to delay institutionalization. There may also be
4 9. G E R I AT R I C S 683
Box 49.2 CAUSES OF DELIRIUM care units. The most important risk factor for the develop-
ment of a pressure ulcer is immobility. Nutritional deficien-
Drugs cies, age-related changes in the skin, and urinary incontinence
Sedative-hypnotics are also contributing risk factors. The common sites include
Anticholinergic agents the sacrum, greater trochanter, ischial tuberosity, calcaneus,
NSAIDs and lateral malleolus.
Antipsychotic agents Four factors are thought to be important in the develop-
Metabolic disturbances ment of pressure ulcers: pressure, shearing force, friction, and
Hyperglycemia moisture. When the persistent pressure of skin overlying a
Hypoglycemia bony prominence exceeds the capillary pressure, the blood
Hypercalcemia supply to the tissues is impaired. Tissue ischemia can occur
Hypoxia and result in skin ulceration.
Hypotension
Medical illness Risk factors for the development of pressure ulcers are
Urinary tract infection immobility, nutritional deficiencies, age-related changes in
Sepsis the skin, and urinary incontinence.
Pneumonia
Surgery Pressure ulcers can be classified into 1 of 4 stages (I-IV).
Hip fracture repair They tend to be understaged because often the underlying tis-
Coronary artery bypass grafting sue damage is not immediately apparent.
Trauma
Abbreviation: NSAID, nonsteroidal anti-inflammatory drug.
Stage I: Nonblanchable erythema of intact skin. There
may be associated edema.
cognitive impairment associated with delirium. Patients with Stage II: Partial-thickness skin loss involving the
delirium frequently have a preexisting mild (often unrecog- epidermis or dermis or both. The ulcer is superficial and
nized) dementia. may present as an abrasion, a blister, or a shallow crater.
Delirium is a medical emergency. It is important to find Stage III: Full-thickness skin loss with damage or necrosis
and treat the underlying cause, when possible. Work-up of subcutaneous tissue. The damage may extend to the
should be based on the history, often obtained from caregivers fascia. The ulcer is a deep crater.
and family, and the physical examination. Laboratory evalu-
ation should focus on fluid and electrolyte balance and signs Stage IV: Full-thickness skin loss with extensive
of underlying cardiac, pulmonary, renal, and liver disease. All destruction, tissue necrosis, or involvement of muscle,
medications should be reviewed. bone, or tendons. Sinus tracts may be present.
Treatment is largely supportive. The environment should
be simplified as much as possible. Frequent orientation, clocks, The most important component of pressure ulcer care is
and calendars are important. There are no drugs approved prevention. Preventive strategies include the following:
by the US Food and Drug Administration to treat delirium.
There is no difference between haloperidol and newer antipsy- 1. Repositioning patients at least every 2 hours
chotics for the treatment of delirium. 2. Use of pressure-reducing mattresses
Delirium is associated with increased risk of morbidity
and mortality. 3. Minimizing head elevation
4. Lifting instead of dragging the patient
Delirium is a reversible cause of cognitive impairment and
may be related to medications or acute medical conditions. 5. Keeping the patient as dry as possible when incontinent
Symptoms should be managed non-pharmacologically if 6. Keeping the skin moisturized to help maintain skin
possible. integrity
Haloperidol may be used for the treatment of symptoms. After a pressure ulcer has developed, the basic strategy for
its treatment includes the following:
4 9. G E R I AT R I C S 685
Table 49.1 TYPES OF ESTABLISHED URINARY INCONTINENCE
Urge incontinence Detrusor overactivity Urgency, frequency, nocturia. Loss Behavioral: urge suppression, elimination of
of small to moderate volumes of bladder irritants, timed voiding
urine Pharmacologic: antimuscarinic medications
Stress incontinence Urinary outlet incompetence Losses of small amounts of urine Behavioral: continence tampons, vaginal
from intrinsic urethral associated with transient increases cones, urethral plugs, continence
sphincter insufficiency or in intra-abdominal pressure pessaries, pelvic floor exercises
hypermobility of the bladder (eg, cough, sneeze, laugh) Surgical: urethral sling, tension-free vaginal
tape, bladder suspension, injection of
periurethral bulking agents, artificial
urinary sphincter
Overflow incontinence Urinary outlet obstruction or Difficulty emptying bladder, low Relief of bladder outlet obstruction
detrusor underactivity urine flow, straining to void, (TURP), -adrenergic antagonists,
urinary dribbling indwelling or intermittent bladder
catheterization
4 9. G E R I AT R I C S 687
50.
PREVENTIVE MEDICINE
Amy T. Wang , MD, and Karen F. Mauck, MD, MSc
Understand updated recommendations for adult 3. Tertiary prevention: improving outcomes (quality of
immunization. life, disease progression) in known disease (eg, use of
aspirin after myocardial infarction to decrease recurrence,
Identify appropriate preventive services and counseling in rehabilitation after a stroke).
the prevention of chronic disease.
Screening tests are considered secondary prevention.
688
Box 50.1 ROUTINE COUNSELING Box 50.2 ROUTINE SCREENING RECOMMENDATIONS
RECOMMENDATIONS FOR ASYMPTOMATIC DISEASE
c. Have a complementary, highly specific confirmatory Lung cancer is the second most common cancer and the leading
test. cause of cancer death among men and women. The mortality
d. Have an acceptable rate of false-positive results. Box 50.3 SCREENING INTERVENTIONS NOT
e. Be inexpensive. ROUTINELY RECOMMENDED FOR ASYMPTOMATIC,
AVERAGE-RISK PERSONS
3. Features of the patient:
a. Be at risk for the specific condition. Complete blood cell counts & routine urine tests
Thyroid disease testing
b. Have access to testing. CAD screening
c. Have adequate life expectancy and quality of life. Electrocardiography or cardiac stress testing
d. Be likely to follow through with additional testing and Nontraditional markers of CAD risk: high-sensitivity
treatment. C-reactive protein, ankle-brachial index, periodontal disease,
carotid intima-media thickness, coronary artery calcification
CANCER SCREENING score on electron-beam computed tomography, homocysteine,
and lipoprotein(a)
While prostate and breast cancers are the most common can-
Abbreviation: CAD, coronary artery disease.
cers in men and women, respectively, lung cancer continues
50. P R E VE N T I VE M E D I C I N E 689
rate from lung cancer increased steadily from the 1930s until BREAST CANCER
the 1980s, when it began to decrease in men. Incidence and
Breast cancer is the most commonly diagnosed cancer in
mortality rates of lung cancer in women increased substan-
women and the second leading cause of cancer death in
tially in the 1960s until levelling off in the late 1990s.
women. The lifetime risk is estimated at 1 in 8 women. Of the
women who receive a diagnosis of breast cancer, 10% to 15%
Screening Recommendations have a first-degree relative who has been affected by breast can-
For asymptomatic persons, numerous lung cancer screening cer. The estimated 5-year breast cancer survival rate from the
strategies, including chest radiography, sputum cytology, and time of diagnosis is 89%. If a woman is a BRCA1 or BRCA2
low-dose computed tomographic (CT) scan, have been stud- carrier, she has a 50% to 85% lifetime risk of breast cancer.
ied but have failed to consistently demonstrate a reduction in
mortality. This is reflected in the most recent guidelines. Screening Tests
Mammography with or without clinical breast examination is
1. US Preventive Services Task Force (USPSTF), 2004: the only recommended modality for breast cancer screening
a. States that there is insufficient evidence to recommend in average-risk, asymptomatic women. The American Cancer
for or against screening with any of the above modalities. Society (ACS) recommends magnetic resonance imaging of
the breast as an adjunct to screening mammography for women
2. American College of Chest Physicians, 2007: with a lifetime risk of breast cancer greater than 20% to 25%.
a. Does not recommend low-dose CT scan except in the
context of a well-designed clinical trial. Screening Recommendations
b. Recommends against chest radiography and sputum Timing of initiation and frequency of breast cancer screening
cytology. is a somewhat controversial topic. The USPSTF guidelines
(updated in late 2009) are summarized as follows:
Future Directions 1. For women aged 40 to 49, the age to start screening
The National Lung Screening Trial (NLST) was a well- mammography should be an individualized decision based
conducted randomized controlled trial (RCT) of low-dose on shared decision making.
CT scanning compared with chest radiography in current 2. For women aged 50 to 74, biennial screening
or former heavy smokers. In November 2010, the trial was mammography is recommended.
stopped early owing to findings of 20% fewer lung cancer
deaths in the low-dose CT group. Despite promising results, 3. For women aged 75 or older, there is insufficient
there are still many unanswered questions: Who should evidence to assess the benefits and harms of screening
undergo screening and how often? How should overdiagnosis mammography.
and high false-positive rates (>96%) be managed? What are 4. There is insufficient evidence to recommend clinical breast
the cost implications? Consequently, the findings are not yet examination.
reflected in clinical guidelines. However, the NLST and simi-
lar ongoing studies are likely to transform lung cancer screen- 5. The recommendation is against breast self-examination.
ing recommendations in the coming years.
The American College of Physicians, American Academy
of Family Physicians, and the Institute for Clinical Systems
Lung Cancer Prevention Improvement have adopted similar guidelines.
Smoking is the leading preventable cause of cancer in the Other organizations such as the ACS, the American College
United States and a leading cause of heart disease and stroke. of Radiology, and the American College of Obstetrians and
Smoking causes 85% of all lung cancers. Smoking cessation Gynecologists (ACOG) recommend that annual mammog-
decreases the risk of lung cancer in a former smoker by 20% raphy start at age 40. The National Cancer Institute recom-
to 90%. Physician advice to stop smoking, use of nicotine ces- mends screening mammography every 1 to 2 years starting at
sation aids and medications, and referral to smoking cessation age 40. Many of these organizations also recommend yearly
programs have been shown to be helpful in smoking cessation. clinical breast examinations and breast self-examinations.
Population-based strategies, such as cigarette taxes and smok-
ing restrictions in public places, have also been effective. Benefits of Screening Mammography
RCTs have shown a relative risk of 20% to 30% in breast
Currently, guidelines recommend against screening
cancer mortality attributed to screening mammography for
for lung cancer in asymptomatic persons (with chest
women aged 50 to 69. Data on the potential benefit of screen-
radiography, low-dose CT scan, or sputum cytology).
ing among women aged 40 to 49 have shown a decrease in
Smoking is the leading preventable cause of cancer in the breast cancer mortality of 15%. Data showing screening ben-
United States. efits for women older than 70 are limited.
50. P R E VE N T I VE M E D I C I N E 691
Men & women Symptomatic Diagnostic work-up
Asymptomatic
Figure 50.1 Algorithm for Colorectal Cancer Screening. See text for description of average-risk screening. Asterisk indicates either colorectal cancer
or adenomatous polyp. FAP indicates familial adenomatous polyposis; HNPCC, hereditary nonpolyposis colorectal cancer. (Adapted from Winawer
S, Fletcher R, Rex D, Bond J, Burt R, Ferrucci J, et al. Colorectal cancer screening and surveillance: clinical guidelines and rationaleupdate based on
new evidence. Gastroenterology. 2003 Feb;124[2]:54460. Used with permission.)
men, accounting for 10% of male cancer deaths annually in b. Conflicting RCT mortality data: The Prostate, Lung,
the United States. The mortality rate for prostate cancer has Colorectal, and Ovarian (PLCO) Cancer Screening
decreased, which may be attributable to earlier diagnosis Trial conducted in the United States did not show a
and improved treatment strategies. Risk of prostate cancer is mortality benefit; the European Randomized Study of
increased significantly for men with a family history of pros- Screening for Prostate Cancer (ERSPC) showed that
tate cancer and for African American men. PSA screening decreased the risk of death by 20%.
Reviews of autopsy series have identified prostate cancer in
c. PSA density, velocity, and doubling time and the ratio
46% of men in their 50s, 70% of men in their 60s, and 83% of
of free PSA to total PSA may improve sensitivity and
men in their 70s who died of other causes. This is reflected in
specificity, but more data are needed.
the high lifetime risk of prostate cancer, which is estimated at
1 in 6 men. More than 90% of prostate cancers are localized at d. PSA levels are often increased in benign conditions
the time of diagnosis, which corresponds to a 5-year survival such as prostatitis, urinary tract infection, and
rate approaching 100%. However, only 1 in 34 men die of instrumentation.
prostate cancer. Since prostate cancer has a high prevalence of
nonclinically relevant disease, screening and subsequent man- 3. Prostate imaging tests are not recommended for
agement of low-grade prostate cancer are difficult. screening.
50. P R E VE N T I VE M E D I C I N E 693
T Y P E S O F I M MU N IT Y Influenza Vaccination
1. Active immunity: Antigen is presented to the host, which Annual influenza vaccination is recommended for all adults:
produces an immune response that lasts for years.
2. Passive immunity: Large amounts of preformed antibodies 1. Intranasally administered live, attenuated influenza
prevent or diminish the effect of infection (eg, tetanus vaccine (FluMist) is an option only for healthy,
immune globulin [TIG] and hepatitis B immune globulin nonpregnant adults through age 49. Others should receive
[HBIG]); immune response lasts for months. the trivalent inactivated vaccine.
2. If a person has an egg allergy but the reaction has
been hives only, a provider familiar with egg allergy
manifestations may administer inactivated influenza
T Y P E S O F VAC C I N E S
vaccine with observation for at least 30 minutes after
Live virus vaccines are generally contraindicated in pregnant vaccination. For other reactions (respiratory distress,
women and in people who are severely immunocompromised angioedema, etc), patients should be referred to a
or who are receiving immunosuppressive therapy. Human physician with expertise in management of allergic
immunodeficiency virus (HIV)infected persons who are conditions.
immunocompetent and persons with leukemia in remission
for at least 3 months may be vaccinated with some live vaccines.
Examples of live virus vaccines include measles-mumps-rubella
Tetanus-Diphtheria (Td) and
(MMR), varicella virus, and smallpox.
Tetanus-Diphtheria-Acellular Pertussis (Tdap)
Inactivated vaccines are generally safe in pregnant women
Vaccination
in whom they are indicated and in immunocompromised per-
sons. The response may be decreased in immunocompromised 1. Adults who have completed the primary vaccination series
persons. should receive a tetanus booster every 10 years.
2. Primary vaccination series should be completed in early
A DV I S O RY C O M M IT T E E O N I M MU N I Z AT I O N childhood: the first tetanus-containing vaccine is given,
P R AC T I C E S (AC I P) R EC O M M E N DAT I O N S the second vaccination occurs 4 weeks later, and the
S U M M A RY third occurs 612 months after the second.
The schedule for recommended adult immunizations is sum- 3. Adults with an unknown or incomplete primary
marized in Figure 50.2. vaccination history should begin or complete the series.
Age Group
For all persons in this category who meet the age Recommended if some other risk factor is present No recommendation
requirements and who lack evidence of immunity (eg, on the basis of medical, occupational, lifestyle,
(eg, lack documentation of vaccination or have no or other indications)
evidence of prior infection)
Figure 50.2 Recommended Immunization Schedule for AdultsUnited States, 2011. Detailed footnotes accompanying this figure are published at
http://www.cdc.gov/vaccines/recs/schedules/adult-schedule.htm. Td indicates tetanus-diphtheria; Tdap, tetanus-diphtheria-acellular pertussis.
50. P R E VE N T I VE M E D I C I N E 695
Hepatitis B Vaccination working with rabies virus. Vaccination may be considered
for travellers to hyperendemic areas for at least 1 month and
Efforts are being directed toward universal infant vaccination for persons whose activities involve exposure to potentially
and catch-up vaccination for children and adolescents. Adult rabid animals. Postexposure prophylaxis requirements are as
vaccination (3-dose series: initial dose, second dose 1 month follows:
after initial, and third dose 2 months after second dose) is rec-
ommended for high-risk groups, including the following:
1. Persons with preexposure vaccination require 1 immediate
dose of rabies vaccine and a second dose 3 days later.
1. Adults with high-risk behavior (persons with multiple
sexual partners, persons with sexually transmitted diseases, 2. Unimmunized persons require rabies immune globulin
men who have sex with men, and injection drug users). and 4 doses of rabies vaccine.
2. Household and sexual contacts of persons with chronic
hepatitis B virus infection.
VAC C I N E S F O R P OT E N T I A L B I OT E R RO R I S M
3. Health care personnel with exposure to blood or body fluids. AG E N T S
4. Adults with chronic liver disease or HIV. Smallpox (Vaccinia Virus) Vaccination
5. Adults receiving hemodialysis. 1. Enough live smallpox vaccine has been stockpiled to
vaccinate everyone in the United States in an emergency.
6. Travelers planning extended stays in endemic areas.
2. Contraindications include pregnancy, atopic dermatitis
or eczema, immunocompromise, and immunosuppressant
Haemophilus Influenza Type b Vaccination therapy.
Persons with asplenia, leukemia, or HIV infection should
receive 1 dose.
Anthrax Vaccination
Polio Vaccination Preexposure prophylaxis with anthrax vaccine is recom-
mended only for certain military personnel and for laboratory
Vaccination is not recommended for adults unless they are personnel working directly with Bacillus anthracis.
traveling to an endemic area.
Know the mechanisms of and indications for medications Clinical BPH exists in most men aged 60 or older.
that are used to treat BPH.
Prostate size correlates poorly with symptoms of BPH.
Identify risk factors for erectile dysfunction (ED).
Complications of BPH include urinary tract
Discern the role of testosterone replacement therapy in infections, obstructive nephropathy, and recurrent
men with ED. hematuria.
697
Table 51.1 DIFFERENTIAL DIAGNOSIS FOR LOWER URINARY TRACT SYMPTOMS
Malignant Adenocarcinoma of the prostate Men should be offered PSA testing in conjunction with DRE
Transitional cell carcinoma of the bladder With microhematuria on urinalysis, consider urothelial
malignancies
Squamous cell carcinoma of the penis
Infectious Cystitis Urinalysis & urinary Gram stain are useful in evaluating for cystitis
Prostatitis Prostatic massage specimens (VB3) assist in diagnosis of prostatitis
Sexually transmitted diseases Sexually transmitted diseases may cause LUTS from urethral
(eg, chlamydial infection & gonorrhea) scarring & stricture
Neurologic Spinal cord injury Primary mechanisms for neurologic causes of LUTS are detrusor
Cauda equina syndrome weakness or uninhibited detrusor contractions (or both)
Stroke
Parkinsonism
Diabetic autonomic neuropathy
Multiple sclerosis
Alzheimer disease Alzheimer disease can cause functional urinary incontinence
Medical Poorly controlled diabetes mellitus Medical conditions associated with urinary frequency are often
Diabetes insipidus overlooked causes of LUTS
Congestive heart failure
Hypercalcemia
Obstructive sleep apnea
Abbreviations: BPH, benign prostatic hyperplasia; DRE, digital rectal examination; LUTS, lower urinary tract symptoms; PSA, prostate-specific antigen; UDS, urody-
namic studies; VB3, voiding bottle 3 (postprostatic massage) urine specimen.
Adapted from Beckman TJ, Mynderse LA. Evaluation and medical management of benign prostatic hyperplasia. Mayo Clin Proc. 2005 Oct;80(10):135662. Erratum
in: Mayo Clin Proc. 2005 Nov;80(11):1533. Used with permission of Mayo Foundation for Medical Education and Research.
and validity of the AUA/IPSS. The AUA/IPSS questionnaire Patients with LUTS should be evaluated for neurologic
asks 7 questions about the following symptoms: frequency, deficits, especially if the patients have a history or presenting
nocturia, weak stream, hesitancy, intermittency, incomplete symptoms that suggest a neurologic disorder. In such cases,
bladder emptying, and urgency. Each question is answered useful findings include saddle anesthesia, decreased rectal
on a 5-point scale. When the responses to the 7 questions are sphincter tone, absent cremasteric reflex, or lower extremity
summed, a score of 0 to 7 represents mild symptoms of BPH, neurologic abnormalities. On examination of the abdomen,
8 to 19 represents moderate symptoms, and 20 to 35 repre- masses resulting from a renal tumor, hydronephrosis, or blad-
sents severe symptoms. der distention may be detected. The penis should be examined
for pathologic changes. DRE findings most consistent with
Diuretics and sympathomimetic and anticholinergic
BPH are symmetrical enlargement and firm consistency, often
medications cause LUTS.
likened to the thenar muscle or the tip of the nose. In contrast,
Over-the-counter medications may cause LUTS. findings consistent with adenocarcinoma of the prostate are
The AUA/IPSS is a reliable and valid assessment of prostate asymmetry, induration, and nodularity, often likened
bothersome LUTS. to the consistency of a knuckle or the forehead.
Figure 51.1 A Treatment Algorithm for Benign Prostatic Hyperplasia (BPH). Treatment decisions are based partly on patient symptom severity as
determined with the American Urological Association International Prostate Symptom Score (AUA/IPSS). DRE indicates digital rectal examination;
PE, physical examination; PSA, prostate-specific antigen; PVR, postvoid residual urine; UTI, urinary tract infection.
a
In patients with clinically significant prostatic bleeding, a course of a 5-reductase inhibitor may be used. If bleeding persists, tissue ablative surgery is indicated.
b
Patients with at least a 10-year life expectancy for whom knowledge of the presence of prostate cancer would change management or patients for whom the PSA measurement may change the management of voiding
symptoms.
c
After exhausting other therapeutic options.
d
Some diagnostic tests are used in predicting response to therapy. Pressure-flow studies are most useful in men before surgery.
(Adapted from AUA Practice Guidelines Committee. AUA guideline on management of benign prostatic hyperplasia [2003]. Chapter 1. Diagnosis and treatment recommendations. J Urol. 2003 Aug;170[2 Pt 1]:53047.
Used with permission.)
Attempt to identify neurologic deficits on physical adenocarcinoma of the prostate. Nevertheless, because LUTS
examination. may indicate prostate cancer, it is appropriate to routinely offer
PSA testing. Although there is conflicting evidence regarding
The penis should be examined for pathologic changes.
the utility of screening for prostate cancer with PSA, screening
Prostate asymmetry, induration, and nodularity are for prostate cancer with DRE and PSA may be appropriate for
consistent with prostate adenocarcinoma. men aged 50 to 75 years, depending on the patients preference
after engaging in shared decision-making with his physician.
51. M E N S H E A LT H 699
transrectal ultrasonography without biopsy, cystoscopy, and also have abnormal results. Consequently, as with any test,
nontraumatic bladder catheterization. interpreting the results of uroflow studies depends on the pre-
test probability of disease. If the pretest probability of BPH
Other causes of increased PSA levels are prostate is high, an abnormal test result is useful for confirming the
carcinoma, bacterial prostatitis, acute urinary retention, diagnosis. But if the pretest probability is intermediate, an
instrumentation, prostate incision, and ejaculation. abnormal uroflow result is less useful. In such cases, patients
may need to undergo complete urodynamic studies to further
Conditions that generally do not increase serum PSA distinguish BPH from other causes of LUTS.
levels are routine DRE, transrectal ultrasonography
without biopsy, cystoscopy, and nontraumatic bladder
Different methods for assessing PSA include use of a cutoff
catheterization.
of 4 ng/mL, age-adjusted limits, the ratio of free PSA to
total PSA, and the PSA velocity.
There are different methods for interpreting serum PSA
levels: A uroflow study is an objective, noninvasive assessment of
LUTS.
1. Cutoff valuethe traditional cutoff is 4 ng/mL.
2. Age-adjusted valuesage-adjusted normal limits are M E D I C A L M A NAG E M E N T O F B P H
commonly used because prostate volume increases with age. Although this chapter focuses on the medical management
3. Ratio of free PSA to total PSAthe level of free of BPH, clinicians should recognize the indications for uro-
(unbound) PSA is lower in men with adenocarcinoma logic referral and consideration of invasive therapy. These
of the prostate; therefore, a low ratio of free PSA to total indications are moderate or severe symptoms, persistent gross
PSA is more consistent with prostate adenocarcinoma hematuria, urinary retention, renal insufficiency due to BPH,
than with BPH. recurrent urinary tract infections, and bladder calculi.
Expectant management is reasonable for patients with
4. PSA velocitya rapidly increasing PSA is more suggestive mild or moderate symptoms. These patients are monitored at
of carcinoma than BPH; in particular, an annual PSA least yearly or when new symptoms arise. In addition, these
velocity greater than 0.75 ng/mL is considered abnormal. patients may be advised to practice scheduled voiding (every 3
hours during the day), to avoid excess evening fluid intake, and
A uroflow study with ultrasonographic measurement of to be aware of potential adverse effects of over-the-counter
residual urine volume is an objective, noninvasive way to eval- decongestants.
uate men presenting with LUTS. An accurate study requires Nearly all patients presenting with BPH are candidates
urine volumes of at least 150 mL. Men with BPH often have for medical therapy. Moreover, medical therapy has replaced
peak flow rates less than 15 mL/s and increased residual urine interventional therapy as the most common treatment of
volume (Figure 51.2). Notably, men with detrusor dysfunction BPH. Prescription medications available for treating BPH are
1-adrenergic antagonists (eg, tamsulosin) and 5-reductase
inhibitors (eg, finasteride).
50
40 Expectant management is reasonable for patients with mild
30 or moderate BPH.
Urinary Flow Rate, mL/s
20
10 Available prescription medications are 1-adrenergic
0 antagonists and 5-reductase inhibitors.
50
40 The 1-adrenergic antagonist medications work on the
30
dynamic component of bladder outlet obstruction by decreas-
20
10 ing prostatic smooth muscle tone. They are the first line
0 of medical therapy for most men with BPH. Although all
0 10 20 30 40 50 60 70 80 90 100 1-adrenergic antagonist medications are equally efficacious
Seconds in treating BPH, terazosin and doxazosin are more likely
to cause side effects (mainly orthostatic hypotension) than
Figure 51.2 Uroflow Tracings. Top, Uroflow tracing from a young,
asymptomatic male. Note the parabolic flow curve and peak flow rate other medications in this class. Other common side effects
>15 mL/s. Bottom, Uroflow tracing from an elderly man with benign of 1-adrenergic antagonists include dizziness, hypotension,
prostatic hyperplasia. Note the prolonged voiding time and peak flow edema, palpitations, ED, and fatigue.
rate <10 mL/s. This patients ultrasonographically measured residual The second class of prescription medications for treat-
urine volume was 100 mL. (Adapted from Beckman TJ, Mynderse LA. ing BPH, the 5-reductase inhibitors, act on the static (ana-
Evaluation and medical management of benign prostatic hyperplasia.
Mayo Clin Proc. 2005 Oct;80[10]:135662. Erratum in: Mayo Clin tomical) component of bladder outlet obstruction. These
Proc. 2005 Nov;80[11]:1533. Used with permission of Mayo Foundation medications decrease the conversion of testosterone to dihy-
for Medical Education and Research.) drotestosterone in the prostate, thereby limiting prostate
E R E C T I L E DYS F U N C T I O N
GTP Erection
Male sexual dysfunction includes ED, decreased libido, ana- Guanylyl Smooth muscle
tomical abnormalities (eg, Peyronie disease), and ejaculatory cyclase relaxation
dysfunction. ED, defined as the inability to achieve erections
firm enough for vaginal penetration, affects millions of men in Nitric oxide
cGMP
the United States. The Massachusetts Male Aging Study showed
that the prevalence of ED increased by age: approximately 50% NANC nerve terminals
& endothelial cells PDE-5 PDE-5 inhibitors
of men experienced ED at age 50, and nearly 70% at age 70. (eg, sildenafil)
Erectile physiology includes hormonal, vascular, psychologic, Figure 51.3 Mechanism for Penile Erection and the Molecular
neurologic, and cellular components. Testosterone is primarily Activity of Phosphodiesterase Type 5 (PDE-5) Inhibitor Medications.
responsible for maintaining sexual desire (libido), and hypogo- cGMP indicates cyclic guanosine monophosphate; GMP, guanosine
nadism is sometimes associated with ED. Other hormonal monophosphate; GTP, guanosine triphosphate; NANC, nonadrenergic
noncholinergic. (Adapted from Beckman TJ, Abu-Lebdeh HS, Mynderse
causes of ED include hyperthyroidism and prolactinomas. The LA. Evaluation and medical management of erectile dysfunction. Mayo
penile blood supply begins at the internal pudendal artery, which Clin Proc. 2006 Mar;81[3]:38590. Used with permission of Mayo
branches into the penile artery, ultimately giving rise to the Foundation for Medical Education and Research.)
51. M E N S H E A LT H 701
Table 51.2 QUESTIONS TO ASK WHEN TAKING A HISTORY FROM PATIENTS WITH ERECTILE DYSFUNCTION
QUESTION COMMENT
Do you have difficulty achieving erections or difficulty with Sexual dysfunction includes various diagnoses, & it is important to deter-
orgasms & ejaculation? mine whether the patients primary complaint is ED
How often do you achieve erections? Often patients are not satisfied with the quality of their erections, yet if
Are your erections firm enough for vaginal penetration? patients can achieve erections adequately firm for vaginal penetration
most of the time, their complaints are not classically defined as ED
Did your ED occur suddenly? The sudden onset of ED & the persistence of nocturnal erections indicate
Do you have nocturnal erections? an inorganic (psychogenic) cause; in such cases, physicians should
Do you feel anxious or depressed? explore the psychosocial context of the patients sexual history, such as
Do you & your partner have a satisfactory relationship? whether the patient feels anxious or depressed or whether the patient is
experiencing interpersonal relationship difficulties
Do you have a desire to engage in sexual activity? Decreased sexual desire may indicate hypogonadism; if patients are
not interested in sexual activity, serum testosterone levels should be
assessed & mood disorders should be considered
Do you have penile curvature or pain with erections? A positive response to this question may indicate Peyronie disease, which
is sometimes detected on physical examination; identifying Peyronie
disease is important because it precludes intraurethral alprostadil &
penile injection therapy
Can you engage in vigorous physical activity without chest PDE-5 inhibitor medications will be considered in most patients, &
pain or unusual dyspnea? sexual activity is associated with cardiovascular stress; hence, a history
should be obtained to identify undiagnosed ischemic heart disease or
to assess the stability of known ischemic heart disease
What medications are you taking? Numerous medications are associated with ED, especially antihyperten-
sives & psychotropics; identify medications inhibiting cytochrome
P450 (eg, ritonavir) because these medications increase plasma levels
of PDE-5 inhibitor medications; an absolute contraindication to
PDE-5 inhibitor medications is the concurrent use of nitrates (eg,
isosorbide mononitrate); combining PDE-5 inhibitor medications with
1-adrenergic antagonist medications can cause hypotension
How much alcohol do you consume? Substance abuse, including alcoholism, is commonly overlooked as a cause
Do you use illegal drugs? of ED
Which ED treatments have you already tried? Knowing which medications patients have tried will help physicians
decide the next therapeutic plan
Do you have a history of diseases involving your heart, Identify common risk factors for ED
blood vessels, nervous system, or hormones?
risk of ED. Not surprisingly, randomized controlled trial data EVA LUAT I N G PAT I E N TS WH O H AVE E D
show that erectile function significantly improves in obese
History and Physical Examination
men who lose weight through diet and exercise.
Certain questions should be asked routinely when taking a
Nitric oxide increases cGMP levels; increased cGMP levels
history from patients who have ED (Table 51.2). Especially
cause cavernosal smooth muscle relaxation and erection.
important are questions about common ED risk factors such
ED is strongly associated with cardiovascular risk factors. as cardiovascular disease, smoking, diabetes mellitus, hyper-
Weight loss may lead to improved erectile function in tension, hyperlipidemia, prescription medications, alcohol
obese men. use, recreational drug use, and mood disorders. In addition,
51. M E N S H E A LT H 703
Treatment options for patients who have not had a response testosterone dependent, and for this reason it is necessary to
to PDE-5 inhibitors or who cannot take PDE-5 inhibitors screen for low serum testosterone levels in men who have no
include intraurethral alprostadil and penile injection therapy. response to medical therapy with sildenafil or whose presen-
These are generally more effective than PDE-5 inhibitors, but tation suggests hypogonadism. Hypogonadism is diagnosed
their obvious drawback is inconvenience. Contraindications by the presence of hypogonadal symptoms (such as decreased
for these treatments include blood cell dyscrasias (eg, sickle cell libido, cognitive decline, and generalized muscle weakness)
disease, leukemia, or multiple myeloma) and penile deformity, and by morning fasting total testosterone levels less than 200
especially Peyronie disease. Anticoagulation is an additional ng/dL on at least 2 separate occasions. In hypogonadal men,
contraindication to penile injection therapy. There is inade- PDE-5 inhibitor therapy in combination with testosterone
quate information on the safety of using PDE-5 inhibitors in is often effective. Moreover, testosterone replacement alone
combination with injection therapy, and hence, their coad- increases sexual interest, nocturnal erections, and frequency
ministration is not advised. of sexual intercourse. Nevertheless, testosterone replacement
has not been shown to improve erectile function in men with
normal serum testosterone levels.
Intraurethral Alprostadil
Intraurethral alprostadil (commercially available as MUSE Hypogonadism is diagnosed by the presence of
[Medicated Urethral System for Erection]) is effective in men hypogonadal symptoms and morning fasting total
of all ages who have ED from various causes. Intraurethral testosterone levels <200 ng/dL on at least 2 separate
alprostadil is inserted into the urethral meatus at the tip of occasions.
the penis with an applicator. Patients should be instructed on
Testosterone replacement has not been shown to improve
the application technique. Additionally, owing to the risk of
erectile function in men with normal serum testosterone
syncope, administration of the first dose should be supervised
levels.
by a health care provider. The most common side effect is ure-
thral and genital burning, and hypotension can occur. As for
Testosterone is available by injection, skin patch, topi-
all medical ED treatments, patients are educated about pria-
cal gel, or buccal oral tablets. Testosterone therapy is asso-
pism, and they are instructed to go to an emergency depart-
ciated with potential risks. For example, prolonged use of
ment if they have erections for more than 4 hours.
high-dose, orally active 17-alkyl androgens (eg, methyltes-
tosterone) is associated with hepatic neoplasms, fulminant
The most common side effect of intraurethral alprostadil is
hepatitis, and cholestatic jaundice. Other risks of exogenous
urethral and genital burning.
testosterone therapy include gynecomastia, alterations in
Hypotension and syncope may occur with alprostadil. the lipid profile (mainly decreased high-density lipopro-
tein cholesterol), erythropoietin-mediated polycythemia,
edema, sleep apnea, hypertension, infertility (through
Intracavernosal Penile Injections suppression of spermatogenesis), and BPH. Exogenous
Intracavernosal penile injection, an efficacious and gener- testosterone also increases the risk of prostate carcinoma.
ally safe therapy, is the most effective medical treatment of Although testosterone replacement may not cause prostate
ED. In practice, a triple-therapy combination of alprostadil, carcinoma, it may stimulate the growth of existing occult
papaverine, and phentolamine is usually used. These medica- prostate cancer. For this reason, all men should have screen-
tions increase penile blood flow. Specifically, alprostadil and ing for prostate cancer with DRE and serum PSA before
papaverine cause relaxation of cavernosal smooth muscle using exogenous testosterone.
and penile blood vessels, and phentolamine antagonizes
-adrenoreceptors. The use of intraurethral alprostadil requires Risks of testosterone therapy include hepatitis, cholestatic
patient instruction, and the initial dose is administered under jaundice, hepatic neoplasms, gynecomastia, polycythemia,
the supervision of a health care provider. Although many sleep apnea, and hypertension.
patients are hesitant to attempt penile injection, this method
Screening for prostate cancer is necessary before
is associated with minimal discomfort.
prescribing testosterone replacement.
Intracavernosal injections are the most effective medical
The goal of testosterone replacement is to increase serum
therapy for ED.
testosterone levels to the low or middle portion of the ref-
Initial doses of intraurethral and intracavernosal injections erence range. A recommended treatment is to apply topical
should be supervised by a health care provider. testosterone, 1% gel at a starting dose of 5 g daily, to the shoul-
ders, upper parts of the arms, or abdomen. A total testoste-
rone level may be reassessed as soon as 14 days after starting
treatment. The patients therapeutic response and testosterone
Testosterone
level are reassessed at 3 months, and decisions are then made
Various hormonal therapies, including testosterone, were once about whether to continue using testosterone and whether to
widely used to treat ED. The penile nitric oxide pathway is adjust the dose.
51. M E N S H E A LT H 705
52.
WOMENS HEALTH
Nicole P. Sandhu, MD, PhD, and Lynne T. Shuster, MD
706
the treatment of choice for emotional symptoms. They may The history directs evaluation and management and
be prescribed continuously or cyclically (luteal phase). Oral should include date of last period; timing, duration, and
contraceptives may improve physical symptoms of PMS, but amount of bleeding; bleeding pattern; associated pain; evi-
they do not seem to help mood. Dietary changes and cal- dence of ovulatory cycling (regular menses, cyclic symptoms);
cium carbonate seem to reduce the severity of premenstrual contraceptive history; medical conditions or history sugges-
symptoms. tive of a medical condition (eg, thyroid disease, celiac disease,
and blood dyscrasias); medications; and the impact of bleed-
Selective serotonin reuptake inhibitors are the treatment of ing on quality of life (which may help determine treatment
choice for severe PDD. options). The age and reproductive status of the patient assist
with differential diagnosis.
Oral contraceptives may improve physical symptoms, but Physical examination includes pelvic and breast examina-
they do not help mood. tions, assessing body habitus and hair distribution, and thy-
roid and skin examinations. Bleeding should be verified to
be coming from the cervical os whenever possible. Mucosal
A B N O R M A L U T E R I N E B L E E D I N G ( I N WO M E N lesions that may be the source of blood should be noted and
O F R E P RO D U C T I VE AG E) evaluated appropriately. Obese women can have irregular,
anovulatory bleeding due to increased circulating estro-
Bleeding that is excessive or outside the normal cyclic bleed- gen (androgen conversion in adipose tissue). Underweight
ing pattern is called abnormal uterine bleeding (Box 52.1). patients may have oligomenorrhea due to hypothalamic
The following are commonly used terms: amenorrhea, absence dysfunction. Hirsutism suggests polycystic ovary syndrome,
of bleeding for 3 usual cycles; oligomenorrhea, decreased a cause of infrequent and sometimes very heavy menstrual
frequency of menstrual periods; menorrhagia, excessive or periods associated with anovulation. Petechiae suggest
prolonged bleeding at regular intervals of menstruation; abnormal clotting disorders. Vaginal atrophy and cervical
metrorrhagia, light and irregular menstrual bleeding; and lesions can cause postcoital spotting or bleeding. Pregnancy
menometrorrhagia, heavy and irregular menstrual bleeding. must be considered first when evaluating abnormal uterine
Heavy menstrual bleeding that interferes with daily activities bleeding. Ectopic pregnancy must be considered if a woman
is the most common concern for women with abnormal uter- also has unilateral pelvic pain, particularly after an episode of
ine bleeding. Irregular bleeding is typically anovulatory and amenorrhea. In the nonpregnant patient, further evaluation
is most common at the extremes of reproductive age, whereas and management are guided by whether bleeding is irregu-
menorrhagia is typically ovulatory. lar or menorrhagia. Management depends on the underlying
cause, and medical causes should be considered (eg, thyroid
Excessive bleeding or bleeding outside the normal cyclic or other endocrine disease, polycystic ovary syndrome, bleed-
pattern is called abnormal uterine bleeding. ing dyscrasias, or medication use). Treatment should focus on
a defined medical or other underlying cause (eg, endocrine
abnormality and uterine structural abnormalities) and impact
on quality of life.
Box 52.1 POSSIBLE CAUSES OF ABNORMAL UTERINE
BLEEDING
The pattern of bleeding coupled with history and physical
examination findings direct further evaluation of abnormal
Pregnancy
uterine bleeding.
Anovulation or oligo-ovulation
Fibroids Medical problems (eg, thyroid and celiac disease) may
Polyps, endometrial or endocervical cause abnormal uterine bleeding.
Adenomyosis
Conservative management, including reassurance,
Endometriosis
monitoring, or hormonal agents, is often sufficient.
Infection, including pelvic inflammatory disease
Endometrial hyperplasia
For irregular bleeding in women 35 years or older or at
Endometrial carcinoma
high risk of endometrial cancer, consider transvaginal ultra-
Coagulation disorders
sonography or endometrial biopsy. If these tests are not indi-
Hyperprolactinemia
cated, therapy with oral contraceptives (or a progestin if oral
Liver disease
contraceptives are contraindicated) may be initiated. If the
Thyroid dysfunction
response is inadequate, increase the dose and consider trans-
Obesity
vaginal ultrasonography or biopsy. In the setting of menor-
Anorexia
rhagia, oral contraceptives (or a progestin or nonsteroidal
Rapid fluctuations in weight
anti-inflammatory drug) as first-line therapy is appropriate.
Corticosteroids
A levonorgestrel intrauterine device may be considered. If
Hormonal contraceptives
response is inadequate, transvaginal ultrasound or biopsy
Tamoxifen
should be considered.
52 . WO M E N S H E A LT H 707
Definitive management should be considered for endome- DYS F U N C T I O NA L U T E R I N E B L E E D I N G
trial polyps or submucosal fibroids and for persistent bleeding
Abnormal, excessive uterine bleeding not due to a specific,
inadequately responsive to medical therapy. Areas of hyper-
identifiable cause is called dysfunctional uterine bleeding. It
plasia should undergo biopsy. If there are no sonographic
is most commonly observed at the extremes of reproductive
abnormalities and childbearing is complete, definitive therapy
age. Dysfunctional uterine bleeding is a diagnosis of exclusion.
with endometrial ablation or hysterectomy or other appropri-
Useful therapies include hormonal contraception (usually
ate treatment (eg, myomectomy) can be considered. If child-
combination oral contraceptive pills), cyclic oral progestins
bearing is incomplete, follow the menstrual pattern, observe
(most commonly medroxyprogesterone acetate), and non-
the patient, and provide appropriate medical management. If
steroidal anti-inflammatory drugs (may reduce blood loss by
transvaginal ultrasonography is inconclusive, hysteroscopy for
up to 50%).
direct visualization of the endometrial cavity may be consid-
ered. Additional measures should be directed at medical issues
Dysfunctional uterine bleeding is a diagnosis of exclusion.
(eg, treatment of causative medical conditions, transfusion,
intravenous fluids, and complete blood count).
C O N T R AC E P T I O N A N D I N F E RT I L I T Y
First-line therapy for irregular bleeding is medical (usually
hormonal).
C O N T R AC E P T I O N
Nonsteroidal anti-inflammatory drugs may also be used
and help reduce blood flow. Contraceptive methods include hormonal (ie, oral, transder-
mal, vaginal, intrauterine, intradermal implant, and intramus-
Endometrial biopsy is often unnecessary but is
cular injection), barrier, chemical, and physiologic approaches.
recommended in women 35 years old or with a high risk
None are 100% effective, and all are associated with some
of endometrial cancer (eg, unopposed estrogen therapy).
degree of risk (Table 52.1).
With inadequate response to hormonal agents, Factors to consider in counseling women regarding con-
diagnostic testing (including hysteroscopy, transvaginal traceptive methods include efficacy, convenience, duration
ultrasonography, or endometrial biopsy) may be indicated. of action, reversibility and time to return of fertility, effect
Combined hormonal DVT, stroke, MI, HTN, Nausea, headaches, spotting, Reduced risk of dysmenorrhea; menor-
contraceptives depression, hepatic adenoma; weight gain, mastalgia, mood rhagia; anemia; ectopic pregnancy;
no STI prevention changes PID; ovarian, endometrial, &, pos-
sibly, colorectal cancer; acne
Progestin-only pill Less effective than combined Unpredictable spotting, Safer than combination OCs with regard
OC for preventing pregnancy bleeding to HTN, CV disease, breast cancer,
clotting. Does not interfere with
lactation
IUD STIs. Increased risk of Spotting, cramping, back pain; Levonorgestrel IUD reduces menorrhagia
ectopic pregnancy. longer, heavier periods
Insertion-associated risks of
infection & perforation
Depo-progestin Depression, weight gain, bone Menstrual changes, weight gain, Lactation not disturbed; convenience;
loss, dyslipidemia headache reduces seizures
Diaphragm UTIs, toxic shock syndrome Requires planning ahead; must Avoids hormone-related side effects
be left in place for 68 h after
sexual intercourse; vaginal
discharge if left in too long
Fertility awarenessbased Pregnancy risk estimated to be Takes time to learn; requires Learning biomarkers of fertility can help
methods 9% with perfect use, 19% with abstaining from sexual a committed couple plan pregnancy or
typical use intercourse or using barrier avoid pregnancy
method during fertile window
Abbreviations: CV, cardiovascular; DVT, deep vein thrombosis; HTN, hypertension; IUD, intrauterine device; MI, myocardial infarction; OC, oral contraceptive; PID,
pelvic inflammatory disease; STI, sexually transmitted infection; UTI, urinary tract infection.
52 . WO M E N S H E A LT H 709
contraceptives and a higher frequency of breakthrough bleed- and illicit drugs potentially harmful to the embryo should be
ing. Consider progestogen-only pills in women with migraine addressed. Additional recommendations include adequate
headaches, hypertension, diabetes mellitus, personal or fam- folic acid supplementation before conception (to decrease the
ily history of thromboembolism, cardiac or cerebrovascular risk of neural tube defect). Alcohol abuse during pregnancy is
disease, or hypertriglyceridemia and in women older than 35 the third leading cause of mental retardation. It is associated
years who are smokers. with early spontaneous abortion, placental abruption, and
fetal alcohol syndrome. The greatest negative impact is at the
Progestogen-only pills have adverse effects on total, time of conception through the first month of pregnancy.
high-density lipoprotein, and low-density lipoprotein Smoking is associated with low birth weight, perinatal
cholesterol levels, whereas the estrogen component in death, infertility, spontaneous abortion, ectopic pregnancy,
combination pills increases triglyceride levels. placenta previa and placental abruption, and subsequent sud-
den infant death syndrome. Caffeine intake of 1 to 2 cups of
Consider progestogen-only pills in women with migraines, coffee or other caffeinated beverage daily is not associated
cardiovascular or cerebrovascular disease, diabetes, or with miscarriage or birth defects.
history of blood clots and in women older >35 years who
are smokers.
Folic acid supplementation before conception reduces the
risk of neural tube defects.
Table 52.1 has additional information on contraceptive
methods. Alcohol abuse during pregnancy is the third leading
cause of mental retardation and is associated with early
spontaneous abortion and placental abruption.
I N FE RT I L IT Y
Smoking is associated with low birth weight, perinatal
Infertility is the inability to conceive after 1 year of intercourse
death, infertility, spontaneous abortion, ectopic pregnancy,
without contraception and may be due to male or female fac-
placenta previa and placental abruption, and sudden infant
tors or both. The cause may be difficult to identify. A womans
death syndrome.
age is the most important determinant of a couples fertil-
ity. Other common causes of female infertility are ovulatory
disorders (eg, polycystic ovary syndrome, hypothyroidism, I M MU N I Z AT I O N S A N D P R E G NA N C Y
hyperprolactinemia, eating disorders, or extreme stress),
Live vaccines should be avoided during pregnancy, but certain
endometriosis, pelvic adhesions, and tubal abnormalities.
inactivated vaccines should be routinely administered during
Declining oocyte quality with advanced age is a major cause
pregnancy, such as tetanus toxoid and the inactivated influ-
of infertility.
enza vaccine (Box 52.3).
Evaluation includes a careful history (duration of infer-
tility; prior evaluation or interventions; menstrual history;
sexual history; lifestyle factors including exercise, diet, stress, H Y P E RT E N S I O N A N D P R E G NA N C Y
smoking, and substance abuse; medical and surgical history), Hypertension complicates up to 10% of pregnancies and is an
partner semen analysis, documentation of ovulation through important cause of maternal and fetal morbidity and death.
history and midluteal serum progesterone level, assessment of Hypertension may precede pregnancy or develop during preg-
ovarian reserve (day 3 FSH and estradiol level measurements), nancy. The topics of hypertension during pregnancy and nurs-
assessment of fallopian tube patency with hysterosalpingogra- ing are covered in Chapter 8, Hypertension.
phy, and exclusion of endocrinologic causes by measurement
of prolactin and thyrotropin levels.
T H RO M B O E M B O L I C D I S E A S E A N D P R E G NA N C Y
Infertility may be due to female or male factors or both; Pregnancy creates a thrombogenic state, yet thromboembo-
the cause is often elusive. lism is uncommon during pregnancy. Women with hereditary
Components of the work-up of infertility include thrombophilias are at high risk for thrombosis during preg-
biochemical studies to evaluate ovulation, assessment of nancy, with potentially serious complications. Women with
fallopian tube patency with hysterosalpingography, and antiphospholipid antibodies are prone to arterial or venous
exclusion of endocrinologic causes through appropriate thromboembolism, placental infarction, recurrent pregnancy
testing. loss, preeclampsia, fetal growth retardation, or fetal death.
Low-molecular-weight heparin is the preferred treatment
for thromboembolism during pregnancy or for prevention in
MEDICAL ISSUES OF PREGNANCY high-risk women. Warfarin is teratogenic and increases the
risk for spontaneous abortion and should be avoided during
pregnancy. Aspirin is recommended before conception for
P R EC O N C E P T I O N C O U NS E L I N G
women with antiphospholipid antibodies. After conception,
Good prenatal care is associated with improved pregnancy additional treatment with heparin, glucocorticoids, or other
outcomes. A healthful diet, exercise, and avoidance of tobacco medications may be indicated.
Women with thrombophilias are at increased risk for Endometriosis is defined as the presence of endometrial glands
pregnancy-related thromboembolism. and stroma outside the endometrial cavity and uterine wall.
The most common sites (decreasing frequency) are the ovaries,
Low-molecular-weight heparin is the preferred treatment cul-de-sac, broad and uterosacral ligaments, uterus, fallopian
or prophylaxis for thromboembolism during pregnancy. tubes, sigmoid colon, appendix, and round ligaments. The
most common symptom is pain, which may manifest as pelvic
Warfarin should be avoided because of its teratogenicity
pain, chronic dyspareunia or dysmenorrhea, or cyclical bowel
and risk for spontaneous abortion.
symptoms. Endometriosis is found in 20% to 40% of women
with infertility and in up to 65% of women with chronic pelvic
pain. Physical examination findings may be normal; localized
T H Y RO I D D I S O R D E R S A N D P R EG NA N C Y
tenderness in the cul-de-sac or uterosacral ligaments suggests
Maternal hypothyroidism is associated with infertility, mis- endometriosis. Definitive diagnosis requires direct visualiza-
carriage, stillbirth, placental abruption, preeclampsia, and tion and biopsy of endometriotic implants, ideally through
motor and mental retardation in the infant. Thyrotropin laparoscopy. Imaging is rarely helpful for establishing the diag-
should be measured early in pregnancy, and women tak- nosis or determining the disease extent. Blood cancer antigen
ing thyroid hormone should be monitored regularly. About 125 (CA 125) levels are often increased, but they should not
20% require a dose increase. Thyrotropin levels are useful for be measured in this setting.
detecting hypothyroidism or for monitoring thyroid hor-
mone replacement. Endometriosis is the presence of endometrial glands and
Hyperthyroidism is the second most common endo- stroma in non-endometrial sites (eg, ovaries, cul-de-sac,
crine disorder during pregnancy (after diabetes mellitus), fallopian tubes, and colon).
but it occurs in only about 0.2% of pregnancies. Symptoms
Pain is the most common symptom.
and signs may overlap with normal findings in pregnancy,
and low weight gain may be the only clue. Poorly controlled Affected women may be infertile.
52 . WO M E N S H E A LT H 711
Table 52.2 TREATMENT OPTIONS FOR ENDOMETRIOSIS
IMPACT ON ENDOMETRIOTIC
SYMPTOM TREATMENT OPTIONS IMPLANTS ADVERSE EFFECTS
Mild pelvic pain Analgesics (eg, NSAIDs) Does not reduce endometriotic Minimal
implants
Oral contraceptives Evidence conflicts on whether Minimal
therapy reduces implant size
or inhibits progression of
disease
Moderate to severe pain GnRH agonist (eg, Reduces size of endometriotic Menopausal symptoms, bone loss
Pain that does not respond leuprolide, nafarelin, implants FDA approval for no more than 6 mo of
to analgesics or oral goserelin) continuous use
contraceptives Combination with progestins or low-dose
estrogen-progestin therapy minimizes adverse
effects & allows prolonged use
Progestins (oral or depot Evidence unclear as to effect on Weight gain, irregular uterine bleeding, mood
medroxyprogesterone implant size or inhibition of changes
acetate) disease progression
Danazol Reduces size of endometriotic Weight gain, muscle cramps, decreased breast
implants size, acne, hirsutism, lipid changes, hot flushes,
mood changes
Severe pain Surgery Reduces size of endometriotic May lead to development of postsurgical
Pain unresponsive to implants & adhesions adhesions
medical management
Advanced disease
Large or symptomatic
endometrioma
Abbreviations: FDA, US Food and Drug Administration; GnRH, gonadotropin-releasing hormone; NSAID, nonsteroidal anti-inflammatory drug.
Direct visualization and biopsy are required for definitive severity of symptoms, the age of the patient, and the desire for
diagnosis. fertility.
Imaging is rarely helpful, and the level of CA 125 should
Nonsteroidal anti-inflammatory drugs or oral
not be measured.
contraceptives are used first for treatment of endometriosis,
and progestins or danazol is used in more refractory cases.
Treatment is directed at symptom relief and may include
medical or surgical therapy, or both (Table 52.2). Treatment Conservative therapy is used first, moving to definitive
choice depends on symptom severity, disease extent and loca- surgery for the most severe, refractory cases.
tion, desire for pregnancy, age of the patient, and response to
prior therapies. A stepwise approach is usual. Empiric medi-
cal therapy with a nonsteroidal anti-inflammatory drug or
U T E R I N E F I B RO I D S
oral contraceptive is reasonable in patients suspected to have
endometriosis when other causes of pelvic pain have been Uterine leiomyomas (fibroids or myomas) are benign mono-
excluded. If this therapy fails, in severe cases a diagnostic lap- clonal tumors that arise from the smooth muscle of the myo-
aroscopy is often done. If endometriosis is confirmed, ablation metrium. There are 3 primary types: submucosal, intramural
and excision of endometriotic implants and adhesions can be (most common), and subserosal. They are the most common
performed. If pain persists, a trial of hormonal therapy with female pelvic tumors, occurring in 50% to 80% of women.
gonadotropin-releasing hormone agonists, danazol, or proges- They are most prevalent during the reproductive years and usu-
tins should be used. There is no definite evidence that any one ally regress after menopause. Approximately 25% of fibroids
medical agent is superior for pain control. Oral contraceptive are symptomatic. The degree and type of symptoms depend on
or other medical therapies may be used after surgery to main- the number, size, and location of the fibroids. Fibroid-related
tain remission or in unresectable disease. Surgical therapy is symptoms are grouped into 3 categories: menstrual symptoms
reserved for severe symptoms, lack of response to medical (eg, dysmenorrhea and menorrhagia), bulk-related symptoms
management, or advanced disease. Conservative surgical ther- (eg, pelvic pain, pelvic pressure, urinary frequency, constipa-
apy is usually attempted, with removal of the endometriotic tion, and dyspareunia), and reproductive dysfunction (eg,
implants and adhesions and preservation of the uterus and recurrent miscarriage and obstetric complications). Fibroids
ovaries. Definitive surgical therapy involves hysterectomy that distort the endometrial cavity (primarily submucosal)
and oophorectomy. The surgical approach depends on the increase infertility and risk for miscarriage. Large fibroids may
Fibroids are the most common female pelvic tumor and are Treatment of fibroids is reserved for those that are
benign; most are asymptomatic. symptomatic.
Fibroids are more common in black women than in white Medical therapy includes gonadotropin-releasing hormone
women and in women with early menarche and reduced agonists.
parity.
Surgical treatment of fibroids is indicated when symptoms
An enlarged, irregularly shaped, firm, nontender uterus on persist despite medical treatment, when infertility or recurrent
pelvic examination suggests fibroids. Fibroids are often inci- pregnancy loss is related to fibroids, or when malignancy is
dentally found on pelvic ultrasonography. Imaging should be suspected. Surgery should be considered in a postmenopausal
done if the diagnosis is uncertain, especially if the adnexa can- woman with a new or enlarging pelvic mass and pelvic pain
not be palpated separately from the suspected fibroid. The most and to exclude uterine sarcoma. Other risk factors for uter-
widely used imaging technique is transvaginal ultrasonogra- ine sarcoma include prior pelvic irradiation, tamoxifen use, or
phy, which has high sensitivity for fibroids. Sonographically, the rare syndrome of hereditary leiomyomatosis and renal cell
they are symmetric, well-defined, hypoechoic, heterogeneous carcinoma.
masses. Hysteroscopy may be used, particularly if myomec- Surgical options include myomectomy (if there is no suspi-
tomy is planned. Magnetic resonance imaging provides very cion of malignancy) or hysterectomy. Myomectomy involves
accurate imaging but is rarely used. It can be used to differ- removal of the myomas with uterine conservation and pre-
entiate fibroids from other conditions (eg, adenomyosis) serves childbearing potential. Disadvantages include high risk
and to predict the outcome of uterine artery embolization. for new fibroid formation (about 50% at 5 years) and increased
Annual pelvic examination should be done; further evalua- risk for uterine rupture in pregnancy. Less invasive options in
tion is warranted if symptoms change or uterine size increases. women who have completed childbearing and in whom there
Consider a complete blood cell count in patients with prior is no suspicion of malignancy include endometrial ablation,
anemia or menorrhagia. Routine surveillance imaging is not myolysis (laparoscopic thermal coagulation or cryoablation
recommended. of fibroids), uterine artery embolization, and magnetic reso-
nanceguided focused ultrasound ablation.
Clinically significant fibroids are identified on pelvic
examination by finding an enlarged, irregular, firm, Surgery is indicated in symptomatic cases of fibroids
nontender uterus. refractory to medical therapy.
Ultrasonographic features are well understood; magnetic Myomectomy preserves childbearing potential, whereas
resonance imaging is usually unnecessary, but it may be other less invasive options (eg, endometrial ablation,
helpful if other conditions are possible or uterine artery myolysis, uterine artery embolization, and magnetic
embolization is being planned. resonanceguided ultrasound ablation) do not; such
options are appropriate only when malignancy is not
Treatment of fibroids is necessary only if they are symptom- suspected.
atic. Abnormal uterine bleeding is the most common symp-
tom, typically causing prolonged or heavy menstruation but
not intermenstrual bleeding. The bleeding pattern is primarily
E N D O M ET R I A L C A N C E R
influenced by location of the fibroid; submucosal fibroids are
more likely to cause heavy bleeding. A trial of medical therapy Endometrial cancer is the most common gynecologic malig-
before surgical therapy is appropriate for symptomatic fibroids nancy in the United States. The incidence increases with age;
(anemia, heavy bleeding, or pain). Gonadotropin-releasing average age at diagnosis is 60 years. Most cases (75%) occur
hormone agonists (eg, leuprolide) cause amenorrhea and in postmenopausal women. Fewer than 5% of cases occur
reduce uterine size in most cases. They are used to reduce in women before age 40 years. Most cases are due to excess
blood loss before definitive surgery, to reduce uterine size to estrogen stimulation without adequate progestin exposure.
allow less invasive surgical approach (vaginal or laparoscopic Box 52.4 lists other risk factors for endometrial cancer, includ-
vs laparotomy), or as therapy for women approaching meno- ing increasing age, nulliparity, chronic anovulation, late meno-
pause who are expected to require no more than 6 months of pause, obesity, diabetes mellitus, and tamoxifen therapy.
treatment. Adverse effects, including reduced bone density, The main genetic association is hereditary nonpolyposis
preclude long-term use. Pretreatment bleeding patterns and colorectal cancer (Lynch syndrome II). Women with Lynch
uterine size usually return rapidly after cessation of treat- syndrome II have a lifetime risk for endometrial cancer of 27%
ment. The role of oral contraceptives and progestins in the to 71% and should undergo surveillance for this cancer and
52 . WO M E N S H E A LT H 713
Box 52.4 FACTORS THAT AFFECT THE RISK OF The initial diagnostic test to exclude endometrial cancer
ENDOMETRIAL CANCER is endometrial biopsy. Alternatives include hysteroscopy with
dilation and curettage or hysteroscopy with directed biopsy
Risk factors and curettage. Transvaginal ultrasonography is an acceptable
Increasing age initial step for postmenopausal women with uterine bleed-
Obesity ing who cannot tolerate an endometrial biopsy or women for
Unopposed estrogen therapy whom imaging of the adnexa is needed. In postmenopausal
Nulliparity women, an endometrial thickness of less than 4 to 5 mm is
Chronic anovulation (including polycystic ovary syndrome) associated with a low risk of endometrial disease; a thicker
Early menarche lining should prompt endometrial biopsy or hysteroscopy
Late menopause with dilation and curettage. Diffuse or focal increased echo-
Obesity texture or inadequate visualization of the endometrium on
Diabetes mellitus ultrasonography or persistent unexplained bleeding should
Hypertension also prompt hysteroscopy or endometrial biopsy. Transvaginal
Tamoxifen use ultrasonography alone cannot exclude endometrial cancer in
First-degree relative with endometrial cancer premenopausal women with abnormal uterine bleeding, given
Hereditary nonpolyposis colorectal cancer (Lynch syndrome II) the cyclic variability in the thickness of the endometrium.
Protective factors
Combination oral contraceptive therapy Endometrial biopsy is used to exclude endometrial cancer.
Smoking
ADNEXAL MASSES
for colorectal cancer or consider preventive surgery. In other
populations, screening for uterine cancer in asymptomatic The adnexa are the ovaries and fallopian tubes (the term also
women is not warranted. includes the uterine ligaments). Most adnexal masses are
benign and can occur at any age. Differential diagnosis and
Endometrial cancer is the most common gynecologic management depend on the patients age and menstrual status.
malignancy, and the majority of cases occur in The differential diagnosis of an adnexal mass includes ovarian
postmenopausal women. and extraovarian masses; see Box 52.5 for examples.
A physiologic ovarian cyst is the most common adnexal
Hereditary nonpolyposis colorectal cancer (Lynch mass in a premenopausal woman. In this population, less than
syndrome II) is associated with a considerable lifetime 20% of adnexal masses are malignant. Ectopic pregnancy must
risk of endometrial cancer, and affected women should
undergo surveillance ultrasonography or preventive surgery
once childbearing is complete. Box 52.5 DIFFERENTIAL DIAGNOSIS OF
ADNEXAL MASS
The most common endometrial cancer is endometrioid
adenocarcinoma. Clear cell and serous carcinomas are rarer Ovarian mass
and more aggressive. The classic symptom is abnormal Physiologic cyst, simple or hemorrhagic
uterine bleeding, occurring in 90% of cases. Endometrial Follicular
cancer must be excluded in any postmenopausal woman Corpus luteum
with uterine bleeding (with the exception of predictable Polycystic ovary syndrome
bleeding related to hormone therapy). Although atypical Benign ovarian neoplasm
glandular cells on Papanicolaou smear are often due to Leiomyoma (fibroid)
benign conditions, underlying neoplasia in 9% to 38% of Endometrioma
such women (including adenocarcinoma of the endome- Dermoid cyst (cystic teratoma); most common ovarian tumor
trium, cervix, ovary, and fallopian tube) may be identified, in women in their second & third decades
and evaluation should include colposcopy, endocervical Cystadenoma
sampling, testing for human papillomavirus, and endome- Metatstatic carcinoma (ie, colon, endometrium, breast);
trial assessment. non-Hodgkin lymphoma
Ovarian carcinoma
Any postmenopausal woman with uterine bleeding not Extraovarian mass
associated with hormone therapy should be evaluated for Ectopic pregnancy
endometrial cancer. Tubo-ovarian abscess
Paraovarian cyst
Although atypical glandular cells on Papanicolaou
Peritoneal inclusion cyst
smear are usually due to benign conditions, underlying
Diverticular abscess
neoplasia and endometrial evaluation must be
Cancer of the fallopian tube
considered.
52 . WO M E N S H E A LT H 715
A suspicious result on pelvic ultrasonography and an follow-up and unnecessary treatment. Although cervical dys-
increased CA 125 level are highly specific and sensitive for plasia is common in women younger than 21 years, it rarely
ovarian carcinoma in postmenopausal women. progresses to invasive cancer, and excisional treatment is
associated with more subsequent premature births. The opti-
The only populations in whom CA 125 screening should
mal frequency of cervical cytologic testing is every 2 years for
be routinely undertaken are in women with known BRCA
women aged 21 to 29 years. Women aged 30 years or older
mutations or women with an established diagnosis of
with 3 prior normal cytologic results should undergo testing
ovarian cancer.
every 3 years. The rate of dysplasia decreases with increasing
sequential negative testing. In the absence of high-risk fac-
tors, testing can be discontinued at age 65 to 70 years. Peak
C E RVI C A L C A N C E R S C R E E N I N G incidence of cervical cancer is during the fifth decade of life
in white women, in the early 70s in Hispanic women, and in
Cervical cytologic screening has resulted in a decline of the late 70s in Asian-Pacific Islander women. The incidence
more than 50% in the incidence of cervical cancer in the past increases during the lifespan of African American women.
3 decades. Approximately half of women in whom cervical After total hysterectomy for benign indications and no prior
cancer is diagnosed annually have not previously undergone high-risk cytologic findings, cervical cytologic testing can be
cervical cytologic testing. High-risk human papillomavirus discontinued (Obstet Gynecol. 2009 Dec;114[6]:140920).
(HPV) subtype infection is necessary, but not sufficient,
for development of squamous cervical neoplasia, including Begin cervical cytologic testing at age 21 years.
malignancy. In most HPV-infected women, cervical abnor-
malities of clinical significance will not develop. Although Women 30 years or older without high-risk factors and
the virus is easily sexually transmitted, the immune response with 3 consecutive normal test results should be tested
usually clears the infection or reduces viral load to unde- every 3 years.
tectable levels 8 to 24 months after exposure. Infection and In the absence of high-risk factors and with 3 consecutive
HPV-related cervical dysplasia are most common in young normal results, discontinue testing at age 6570 years.
women (teens and early 20s), but they typically resolve spon-
taneously. Older women are more likely to have persistent The incidence of cervical cancer varies among different
infection, which correlates with increasing high-risk dyspla- ethnic populations.
sia with increasing age. Cervical cytologic testing is not indicated after
hysterectomy for benign indications in women without
High-risk HPV subtype infection is necessary, but prior high-risk cytologic findings.
insufficient, for cervical neoplasia.
The immune system usually clears or sufficiently reduces High-risk groups may require more frequent screening.
the viral load within 2 years of exposure. These groups include women with human immunodeficiency
virus (HIV) infection, women who are immunosuppressed
HPV is sexually transmitted. (eg, transplant patients), women with in utero exposure to
Young women are most commonly infected, but infection diethylstilbestrol, and women who have had treatment for
and cervical dysplasia usually clear spontaneously in this high-grade intraepithelial lesions ( J Low Genit Tract Dis.
group. 2007 Oct;11[4]:22339).
Liquid-based and conventional cervical cytologic meth- High-risk groups may require testing more often than every
ods are acceptable for screening, but conventional methods 3 years.
require avoidance of blood, discharge, and lubricant for accu-
rate test results. The liquid-based method is more convenient, Additional evaluation and treatment based on cervical
and gonorrhea and Chlamydia testing can be performed using cytologic findings depend on the abnormality (Table 52.3).
the same preparation. However, it is more expensive and has As severity of dysplasia increases, likelihood of progression to
decreased cytologic specificity. cancer increases and time of progression decreases.
High-risk subtype HPV testing stratifies risk in women 21
Both liquid-based and conventional cytologic methods are years or older with atypical squamous cells of undetermined
acceptable. significance and postmenopausal women with a low-grade
squamous intraepithelial lesion and is an adjunct to cervi-
Conventional methods have greater specificity. cal cytologic testing in women 30 years or older. However,
in premenopausal women with low-grade squamous intra-
In average-risk women, cervical cancer screening should epithelial neoplasia, HPV testing has very low specificity and
begin at age 21 years (regardless of age of first sexual inter- should not be used to triage women to colposcopy. HPV test-
course). Invasive cervical cancer is rare in women younger ing is not recommended in women younger than 21 years; if
than 21 years (0.1% of cases). Screening at ages younger done, results should not influence management. HPV test-
than 21 years is associated with more adverse effects from ing has little utility when cytologic results show high-grade
CERVICAL
CYTOLOGIC
FINDING SIGNIFICANCE MANAGEMENT
ASC-US Insufficient atypia to warrant squamous intraepi- If HPV-negative, follow-up cytology in 12 mo or repeat cytology in 6 & 12
thelial lesion designation mo or colposcopy (not best first step)
If HPV-positive, management is same as LSIL and consider colposcopy
ASC-H Cytologic changes suggest but are Colposcopy; if no CIN 2, 3, then repeat cytology at 6 & 12 mo or HPV
insufficient to identify HSIL testing at 12 mo. If CIN 2, 3, see HSIL
LSIL Indicator of probable HPV infection Colposcopy; if no lesion or unsatisfactory, endocervical biopsy is
Prevalence of CIN 2 or higher >10% preferred; with satisfactory colposcopy and lesion identified, biopsy is
preferred. If no CIN 2 or 3, repeat cytology at 6 & 12 mo or HPV
testing at 12 mo; if ASC or higher or HPV-positive, perform
colposcopy; if normal, resume routine screening; if CIN 2 or 3, see HSIL
HSIL High risk for significant cervical disease. High Loop electrosurgical excision or colposcopy with endocervical biopsy. If
incidence of HPV positivity; therefore, cannot no CIN 2, 3, then colposcopy & cytology at 6 & 12 mo or diagnostic
triage with HPV testing or cytology. Failure to excision
detect CIN 2, 3 at colposcopy does not exclude
the possibility
AGC Uncommon and usually benign; may be associ- Colposcopy with endocervical biopsy. HPV testing or repeat cervical
ated with adenocarcinoma of the cervix, endo- cytology every 6 mo until 4 consecutive normal results. If HPV-negative,
metrium, ovary, or fallopian tube repeat cytology at 12 mo; if HPV-positive, repeat cytology at 6 mo
CIN 1 Low risk for progression; usually Repeat cytology at 6 & 12 mo or HPV testing. If cytology or HPV test
spontaneously regresses negative, resume screening. If findings are greater than ASC or are
HPV-positive, perform colposcopy
CIN 2, 3 CIN 2 has a higher likelihood to progress to Colposcopy with excision or ablation then follow-up with cytology or cytol-
CIN 3 but often regresses; CIN 3 is a cancer ogy & colposcopy or HPV testing. If initial colposcopy is unsatisfactory
precursor or if recurrent CIN 2, 3, then diagnostic excision & follow-up with HPV
or cytology with or without colposcopy
Abbreviations: AGC, atypical glandular cells (more likely associated with squamous and glandular abnormalities than ASC-US); ASC-H, atypical squamous cells,
cannot exclude HSIL; ASC-US, atypical squamous cells, undetermined significance; CIN, cervical intraepithelial neoplasia (CIN 2 more likely to progress to CIN 3
and cancer than CIN 1, but often regresses spontaneously); HPV, human papillomavirus; HSIL, high-risk squamous intraepithelial lesion (includes moderate-severe
dysplasia, CIN 2 & 3, & carcinoma in situ); LSIL, low-risk squamous intraepithelial lesion (includes low-grade dysplasia, HPV, & CIN 1).
intraepithelial lesion because results are expected to be posi- Women previously treated for high-grade squamous intra-
tive in this group. epithelial lesion (cervical intraepithelial neoplasia 2 or 3) or
The combination of negative results of high-risk HPV cervical cancer remain at increased risk for at least 20 years after
testing and normal cervical cytologic results in women older treatment, and initial posttreatment surveillance and annual
than 30 years indicates a very low risk for development of a cytologic screening should be done for at least 20 years.
high-grade squamous intraepithelial lesion in the next 4 to
6 years; thus, cervical cytologic testing should not be done Women at high risk after treatment (high-grade squamous
sooner than 3 years. Combination testing increases sensitivity intraepithelial lesion or cervical cancer) remain at high risk
but also decreases specificity and increases cost. of recurrence or residual disease for at least 20 years and
should be followed annually.
Use of HPV results to triage to colposcopy depends on the
population.
HPV testing should not be done in women <21 years old. V U LVA R S K I N D I S O R D E R S
HPV test results are not useful when high-grade
Vulvar itching, burning, and pain are common genital symp-
squamous intraepithelial lesion is the cervical cytologic
toms. Symptoms may be acute or chronic, and skin changes
result.
may be visible; these features guide differential diagnosis
Negative HPV test results and normal cytologic results in (Box 52.6). Common causes of acute vulvar pruritus are
women >30 years old indicate low risk for development vulvovaginal candidiasis and contact dermatitis. Causes of
of a high-grade squamous intraepithelial lesion; repeat chronic vulvar pruritus include lichen sclerosus, lichen simplex
cytologic testing no sooner than 3 years. chronicus, neoplastic conditions such as vulvar intraepithelial
52 . WO M E N S H E A LT H 717
Box 52.6 CONDITIONS COMMONLY ASSOCIATED done to confirm the diagnosis before initiation of topical cor-
WITH VULVAR ITCHING ticosteroids (typically clobetasol).
52 . WO M E N S H E A LT H 719
In women presenting with hot flushes and a clinical Box 52.8 BENEFITS AND RISKS OF HORMONE
scenario atypical for menopause, serum FSH and estradiol THERAPY
levels should be evaluated; in premenopausal women,
consider nonmenopause-related causes of hot flushes. Benefits
Reduces hot flushes & night sweats
Reduces vaginal dryness & dyspareunia
P O S T M E N O PAU S A L B L E E D I N G Reduces postmenopausal osteoporotic fractures
Reduces new onset of diabetes
In postmenopausal women with bleeding not caused by vagi- Associated with decreased risk of colon cancer (estrogen plus
nal or endometrial atrophy or cervical lesions, endometrial progestogen therapy, not estrogen therapy alone)
cancer must be ruled out, unless the patient is using cycling Risks
hormonal therapy. Endometrial cancer must be considered in Increases risk of venous thromboembolism
the setting of any uterine bleeding in postmenopausal women Increases risk of coronary heart diseasea
(unless cyclic hormonal therapy is being used). Transvaginal Increases risk of ischemic stroke
ultrasonography or endometrial biopsy should be considered. Increases risk of breast cancerb
If endometrial thickness is more than 4 mm on ultrasonog- Increases risk of dementia when started in women >65 yc
raphy, there are other endometrial abnormalities (eg, a focal
lesion), or bleeding is persistent, biopsy is indicated. Once a
Hormone therapy may reduce coronary heart disease risk when initiated in
malignancy is excluded, reassurance is usually sufficient. younger & more recently postmenopausal women. Longer-duration hormone
therapy is associated with reduced coronary heart disease risk & death & has
been found to be associated with less accumulation of coronary artery calcium.
Postmenopausal bleeding requires evaluation to exclude Hormone therapy is not recommended as the sole or primary indication for
coronary protection in women of any age.
malignancy.
b
Transvaginal ultrasonography or endometrial biopsy Breast cancer risk increases with estrogen plus progestogen therapy beyond
3-5 years. The increased events are rare: 4 to 6 additional cases per 10,000
should be considered for evaluation. women per year of estrogen plus progestogen therapy use beyond 5 years. No
increased risk for women taking estrogen therapy alone, based on Womens
Biopsy is indicated if transvaginal ultrasonography shows Health Initiative data. Estrogen plus progestogen therapy reduces diagnostic
any abnormalities or if bleeding is persistent after normal interpretation of mammograms.
findings on ultrasonography. c
Observational data report benefit of hormone therapy for reducing dementia
when started in younger women & early in menopause. Hormone therapy is not
recommended for cognitive protection in women of any age.
HORMONE THERAPY
Estrogen is the most effective treatment of hot flushes and guidelines should be considered: 1) estrogen therapy alone
other menopausal symptoms, but it is associated with poten- is used when a woman has undergone hysterectomy; 2) com-
tial risks (Box 52.8). Postmenopausal hormone therapy is bination estrogen-progestogen therapy is used in the setting
appropriate only for women with moderate to severe symp- of an intact uterus; 3) transdermal estrogen is associated with
toms of menopause interfering with quality of life or activi- less risk for venous thromboembolism (in observational stud-
ties of daily living. It should be prescribed at the lowest dose ies; no randomized controlled trials); 4) transdermal estrogen
that relieves symptoms and for the shortest duration needed is preferred over oral in the clinical setting of hypertriglyc-
for treatment goals. It is not indicated to treat osteopenia eridemia, headaches, liver or gallbladder disease, or history
or osteoporosis in most women. In women with an intact of phlebitis; 5) topical, localized vaginal estrogen therapy is
uterus, unopposed estrogen increases the risk of uterine dys- preferred over systemic estrogen for treatment of urogenital
plasia and malignancy, and thus a cyclic progestogen must be atrophy; and 6) extended-use hormone therapy should not
used; women must be made aware that cyclic bleeding will be used to prevent bone loss or reduce fracture risk in women
occur in this setting. with osteopenia or osteoporosis unless alternative therapy is
not possible, causes adverse effects, or its risk-benefit ratio is
Systemic estrogen is the most effective therapy for unfavorable.
menopausal symptoms but is associated with potential
risks and is primarily indicated when symptoms are Combination estrogen-progestogen is indicated in the
moderate to severe. setting of an intact uterus, whereas estrogen alone can be
used in women who have undergone hysterectomy.
The lowest dose of estrogen for the shortest duration to
achieve symptom management is recommended. When vaginal symptoms prevail, vaginal estrogen (rather
than systemic) is recommended.
Systemic estrogen therapy is not indicated for management
of osteopenia or osteoporosis in most women. Transdermal estrogen is preferable in the setting of
hypertriglyceridemia, liver or gallbladder disease, and
When estrogen therapy is indicated in the absence of sig- history of phlebitis or headaches, and it seems to be
nificant contraindications (Box 52.2), the following general associated with a reduced thromboembolic risk.
52 . WO M E N S H E A LT H 721
reassurance and pain management, depending on severity, is Nipple discharge is usually benign.
usually sufficient.
Discharge may be due to ductal lesions or galactorrhea.
Breast pain may be cyclic, noncyclic, or extramammary. In the setting of galactorrhea and a normal serum prolactin
level, further evaluation is usually unnecessary.
In the setting of a history consistent with cyclic pain
and negative results on physical examination, additional
Nipple discharge not due to galactorrhea may be benign
evaluation is not warranted; reassurance and pain
or caused by ductal lesions, including malignancy. Benign
management are adequate.
nipple discharge typically is bilateral, nonbloody, and multi-
Breast pain as the sole finding is very rarely related to breast ductal, but it may be unilateral. Green, gray, or blue is typical
cancer. of fibrocystic breast change. Brown or yellow discharge is also
usually benign. Clear (watery) discharge is usually benign,
After appropriate evaluation, reassurance is often the only but malignancy must be excluded. Check thyrotropin and
necessary treatment. For persistent or moderate to severe prolactin levels to exclude hypothyroidism and hyperpro-
pain, initial treatment strategies for cyclic and noncyclic lactinemia if the discharge is milky. Pathologic discharge
breast pain overlap: a well-fitted support brassiere (including (which may be due to malignancy) is typically unilateral,
nighttime use), heat or cold packs, gentle massage, dietary uniductal, and spontaneous. It is typically bloody, serosan-
changes (eg, caffeine, sodium, and dietary fat), relaxation guineous, or, sometimes, watery or clear. The most common
techniques, and exercise. Over-the-counter analgesics may cause of bloody nipple discharge is a benign intraductal pap-
be effective. Eliminating or adjusting exogenous estrogen illoma, followed by ductal ectasia (ductal dilatation with or
doses may alleviate breast pain. Other hormonal agents may without inflammation) and carcinoma. Ductal carcinoma
be effective in patients with severe cyclic breast pain unre- in situ and papillary carcinoma are the most common types
sponsive to conservative measures. Danazol is the only medi- of breast cancer associated with bloody nipple discharge.
cation approved by the US Food and Drug Administration Factors associated with a higher likelihood of cancer are
for mastalgia; adverse androgenic effects limit its utility. For detailed in Box 52.9.
noncyclic pain related to a nonmalignant breast cause, the
above-listed methods and management of the underlying Nipple discharge features that are concerning for
problem, if possible, are recommended (eg, treatment of an malignancy or other abnormality include it being
abscess and cyst aspiration). unilateral, uniductal, spontaneous, and bloody,
serosanguineous, or watery or clear.
Conservative methods are usually sufficient to manage
Green, gray, or blue nipple discharge is characteristic of
cyclic and noncyclic breast pain.
fibrocystic change and requires no evaluation.
Although danazol may be used for refractory cyclic
mastalgia, adverse effects limit its utility. Mammography and ultrasonography should be done for
all nonlactating women with nipple discharge who are older
than 30 years unless it is clearly due to fibrocystic change.
N I P P L E D I S C H A RG E Ultrasonography alone should be done in women younger
Nipple discharge is common in reproductive-aged women than 30 years. Galactography and ductoscopy are not rou-
and is usually benign. Evaluation to exclude breast can- tinely used in the evaluation of nipple discharge and should
cer, a pituitary tumor, or infection should be considered not be performed.
on the basis of clinical presentation. Nipple discharge Patients with nipple discharge that is neither pathologic
can be classified into 2 categories: due to ductal lesions nor galactorrhea and with normal diagnostic breast imaging
or due to galactorrhea, defined as the discharge of milk results can be reassured and observed. Patients with pathologic
or milk-like secretions 6 months or more postpartum in discharge that can be clinically localized to one duct should
a non-breastfeeding woman. Galactorrhea presents as
spontaneous, milky discharge from multiple ducts of both Box 52.9 FACTORS THAT INCREASE THE LIKELIHOOD
breasts as a result of increased serum prolactin. Evaluation OF CANCER ASSOCIATED WITH NIPPLE DISCHARGE
and treatment of galactorrhea due to hyperprolactinemia
are discussed in the Endocrinology section of this book.
Associated palpable mass
The patient with galactorrhea and a normal serum pro-
Age >40 y
lactin level does not require either visual field evaluation
Grossly bloody, guaiac-positive, serosanguineous, or watery or
or brain imaging. Hypothyroidism should be considered.
clear discharge
Treatment is offered only if the patient is bothered by the
Unilateral
discharge, is unable to conceive, or has evidence of hypo-
Spontaneous
gonadism or low bone density. Prolactin levels should be
Persistent
monitored periodically in patients with persistent galac-
Single duct
torrhea and previously normal prolactin levels.
Yes No
No Yes
? Potential
pathologic diagnosis
No Yes
Figure 52.1 Algorithm for Evaluation of
Spontaneous Nipple Discharge. CBE indicates
clinical breast examination; F-U, follow-up;
R/O endocrinologic cause
R/O endocrinologic cause Surgical duct excision MMG, mammography; R/O, rule out; US,
Close interval F-U
ultrasonography.
be considered for surgical duct excision, even when imaging varies depending on the histologic classification; the overall
results are negative. Patients who report bloody or watery average relative risk is 1.56. The classification is detailed in
nipple discharge with clinically nonreproducible discharge Box 52.10.
and normal results on imaging studies require close interval
follow-up. Surgical duct excision should be performed if the In premenopausal women, a simple cyst is the most
involved duct subsequently can be identified. Subareolar duct common discrete breast lump and a fibroadenoma is the
excision can be considered if the discharge is persistent and most common benign solid mass.
bothersome to the patient, but it is not required. Figure 52.1
is a suggested algorithm for the evaluation of spontaneous Benign breast disease should be considered in the
nipple discharge. context of risk conferred for screening and counselling
recommendations.
Galactography and ductoscopy should not be performed in
the evaluation of nipple discharge.
Box 52.10 CATEGORIES OF BENIGN BREAST DISEASE
Reassurance is appropriate in the absence of galactorrhea or
pathologic discharge with normal results of breast imaging Nonproliferative breast lesions (RR 1.27)
(when appropriate to perform). Duct ectasia
Fibroadenoma without proliferative epithelial changes
Surgical duct excision should be performed if uniductal
Fibrosis
discharge and the duct can be clinically identified and
Mastitis
in the setting of potentially pathologic discharge with
Mild hyperplasia without atypia
negative imaging results as a means to exclude malignancy.
Cysts
Simple apocrine metaplasia
Squamous metaplasia
BENIGN BREAST DISEASE
Proliferative breast lesions without atypia (RR 1.88)
Simple cysts are the most common cause of discrete benign Fibroadenoma with proliferative epithelial changes
breast lumps and occur most often between ages 35 and 50 Moderate or florid hyperplasia without atypia
years. Fibroadenomas are the most common solid, benign Sclerosing adenosis
masses; the median age at diagnosis of fibroadenomas is 30 Papilloma
years, but they may also occur in postmenopausal women. Radial scar
There are many other histologic classifications of benign Atypia (RR 4.24)
breast disease. The main significance lies in whether they Atypical ductal hyperplasia
confer an increased risk of breast cancer. Patients at signifi- Atypical lobular hyperplasia
cantly increased risk should be counselled about appropriate
Abbreviation: RR, relative risk.
screening and risk reduction options. The magnitude of risk
52 . WO M E N S H E A LT H 723
BREAST CANCER RISK ASSESSMENT AND Women with a family history worrisome for a mutation
P R EVE N T I O N should see a genetics counselor and consider gene mutation
testing.
Women at increased risk for breast cancer should be coun-
selled about recommendations and options for screening and Lifetime risk of breast (and ovarian) cancer is significant in
risk reduction. The most widely used risk assessment model BRCA mutation carriers.
for use in women older than 35 years without a history of
breast cancer is the National Cancer Institute Risk Assessment
Tool (Gail model). The tool cannot be applied to women 35 M A NAG E M E N T O P T I O N S F O R WO M E N AT
years or younger with a history of breast cancer (including INCREASED RISK OF BREAST CANCER
ductal carcinoma in situ). It overestimates risk in women with
Options for surveillance and risk reduction should be dis-
numerous prior biopsies for nonproliferative (overall low risk)
cussed, depending on the womans preferences and risk level.
disease and women with high-risk lesions (eg, atypical hyper-
plasia) and a family history of breast cancer, and it underes-
timates risk in generations or cases of suspected inherited Lifestyle Modifications
susceptibility. Alternative models are used in women whose
Factors associated with an increased risk include postmeno-
predominant risk factor is family history. Current models do
pausal weight gain, alcohol intake in excess of 2 drinks per
not account for breast density, an independent risk factor for
day, and physical inactivity. Corresponding lifestyle modi-
breast cancer.
fications in combination with healthy dietary choices may
reduce risk. In general, it is prudent to try to avoid systemic
The Gail model may underestimate or overestimate breast hormone therapy in women at significant risk for breast
cancer risk. cancer.
Only 5% to 10% of all breast cancers are due to an inher-
ited gene mutation. Both BRCA1 and BRCA2 mutations Careful Screening
have autosomal dominant inheritance. Deleterious mutations Guidelines recommend that women with a known or sus-
confer a 55% to 80% lifetime risk of breast cancer and a 15% pected BRCA mutation begin monthly breast self-examination
to 40% lifetime risk of ovarian cancer. Maternal and paternal by age 18 to 21 years, annual or semiannual clinical breast
family histories must be considered. Family history patterns examinations by age 25 to 35 years, and annual mammogra-
concerning for a BRCA mutation include the following: phy beginning at age 25 to 35 years. Mutation carriers should
begin annual or semiannual ovarian cancer screening with
1. 2 first-degree relatives with breast cancer, one of whom transvaginal ultrasonography and measurement of the CA
received the diagnosis at age 50 years or younger 125 serum level at age 30 to 35 years. Women with a family
2. 3 first- or second-degree relatives with breast cancer history of breast cancer not consistent with a BRCA muta-
regardless of age at diagnosis tion should begin annual screening mammography 10 years
before the age at diagnosis of the youngest affected relative
3. Both breast and ovarian cancer among first- and but no later than age 40 years.
second-degree relatives The American Cancer Society recommends consid-
4. A first-degree relative with bilateral breast cancer eration of annual breast magnetic resonance imaging (in
addition to annual mammography) for women with any of
5. 2 first- or second-degree relatives with ovarian cancer the following characteristics: 1) known BRCA mutation,
regardless of age at diagnosis 2) unknown BRCA status and a first-degree relative with a
6. A first- or second-degree relative with both breast and known mutation, 3) lifetime risk of breast cancer of 20%
ovarian cancer at any age to 25% (using an accepted breast cancer risk assessment
model), or 4) chest irradiation between ages 10 and 30 years
7. Breast cancer in a male relative (eg, mantle radiation for lymphoma). Evidence was insuffi-
cient to recommend magnetic resonance imaging screening
For women of Ashkenazi Jewish descent, a worrisome fam- for women with 1) a prior history of breast cancer, 2) dense
ily history includes any first-degree relative (or 2 second-degree breast tissue, or 3) a history of atypical hyperplasia or lobu-
relatives on the same side of the family) with breast or ovarian lar carcinoma in situ.
cancer. Specific founder mutations exist in this and other pop-
ulations. Several statistical models are available to estimate the Screening guidelines for breast cancer are affected by
probability of BRCA1 or BRCA2 mutation. Women with fam- degree of risk.
ily histories suggestive of an inherited mutation should undergo
genetic counseling and consideration of BRCA testing. Magnetic resonance imaging as an adjunct to
mammography can be considered in certain populations.
Ashkenazi Jewish women are at increased risk of a Chest irradiation at a young age confers significant lifetime
mutation due to founder mutations. risk of breast cancer.
AGENT
Risk
Deep vein thrombosis and pulmonary embolus Increased risk (R<T)a Increased risk (R<T)
Stroke Increased risk (R=T)b Increased risk (R=T)
Ischemic heart disease events No change No change
Uterine cancer No change or decreased risk Increased risk
Cataracts Increased risk (R<T) Increased risk (R<T)
Benefit
Invasive breast cancer Decreased risk (R=T) Decreased risk (R=T)
Noninvasive breast cancer No change Decreased risk
Fractures Decreased risk Decreased risk
Adverse effects
Hot flushes Increased risk (R<T) Increased risk (R<T)
Weight gain Increased risk (R>T)c Increased risk (R>T)
Leg cramps Increased risk (R<T) Increased risk (R<T)
Cognition No change May worsen cognition
52 . WO M E N S H E A LT H 725
Table 52.5 DIFFERENCES IN CARDIOVASCULAR DISEASE BY SEX
Risk factors Before menopause, risk profile more favorable (lower blood pressure, lower LDL-C level, higher HDL-C level)
After menopause, similar risk profiles
Higher systolic blood pressure after age 45 y; more isolated systolic hypertension
Higher fibrinogen, CRP levels
Lower smoking rates
Greater attributable risk for hypertension, diabetes mellitus, smoking
Clinical More likely to delay seeking evaluation & treatment after onset of symptoms
presentation More likely to present without chest pain
More likely to present with unstable angina or nonST-segment elevation MI
Less likely to present with STsegment-elevation MI
Less likely to present with MI or sudden cardiac death as initial manifestation
More likely to have hypertension & diabetes mellitus as comorbidities
Treatment After MI, less likely to be admitted to monitored intensive care settings & to receive specialty care
Less likely to receive early aspirin, -blocker therapy, reperfusion therapy, & timely reperfusion
Less likely to receive percutaneous coronary intervention or CABG after MI
Lower utilization of cardiac rehabilitation
Prognosis Higher short-term mortality rate from MI (in part due to older age at presentation & greater burden of comorbid disease)
Women <50 y have twice the mortality rate due to MI compared with same-age men; narrowing mortality gap with
advancing age
Higher adjusted mortality rates after ST-elevation MI
Higher short-term, but better long-term, mortality rate after CABG
Increased complication rates after percutaneous coronary intervention
Abbreviations: CABG, coronary artery bypass grafting; CRP, C-reactive protein; ECG, electrocardiogram; HDL-C, high-density lipoprotein cholesterol; LDL-C, low-
density lipoprotein cholesterol; MI, myocardial infarction.
low-density lipoprotein cholesterol and triglyceride lev- Serum C-reactive protein is an independent risk factor for
els and higher high-density lipoprotein cholesterol levels. cardiovascular disease in women.
However, these differences do not persist after menopause.
Women with diabetes mellitus have a higher relative risk of
Low levels of high-density lipoprotein cholesterol are more
death from coronary heart disease than men.
predictive of risk in women than high levels of low-density
lipoprotein cholesterol. The total ratio of cholesterol to Smoking confers greater risk in women than men.
high-density lipoprotein cholesterol is most highly pre-
dictive of cardiovascular events among women. Serum
C-reactive protein is a strong independent risk factor in PAT H O G E N E S I S O F C O RO NA RY H E A RT D I S E A S E
women that adds to the predictive value of traditional risk
factors. The relative risk of death from coronary heart dis- Women presenting with an acute coronary syndrome are less
ease is greater in females with diabetes mellitus than males. likely than age-matched men to have obstructive coronary artery
Smoking seems to confer a higher risk of coronary heart dis- disease, particularly triple-vessel or left main disease. Women
ease in women than men. Among patients with a first myo- referred for angiographic evaluation of presumed angina are
cardial infarction, women are more likely to be older and to more likely than men to have normal coronary arteries. Coronary
have a history of diabetes mellitus, hypertension, hyperlipi- microvascular dysfunction or myocardial infarction, or both,
demia, or heart failure. occurs in up to half of women with chest pain and normal coro-
nary arteries. Proposed mechanisms for the absence of detectable
coronary artery disease on angiography include diffuse athero-
Men and women share similar risk factors for coronary
sclerosis not detectable by angiography, rapid clot lysis, coronary
heart disease, but the magnitude of risk differs.
vasospasm, coronary microvascular dysfunction, or reduced
After menopause, lipid abnormalities accumulate in myocardial perfusion due to high left ventricular filling pressures
women. related to hypertension or diastolic dysfunction.
Women having a myocardial infarction often present with Women are less likely to receive standard of care medical
symptoms different from the typical ones observed in men; therapy or early revascularization after a myocardial infarction.
hence, a high degree of clinical suspicion is necessary.
Women appear to have better long-term outcomes after
CABG, but the in-hospital survival rate after surgery is higher.
52 . WO M E N S H E A LT H 727
but it was associated with a significant reduction in stroke AT R I A L FI B R I L L AT I O N I N WO M E N
incidence in women 65 years or older. Aspirin is effective for
Although atrial fibrillation is less common in women than
acute treatment of myocardial infarction and for secondary
men, women are at higher risk for stroke. This difference may
prevention of cardiovascular disease in both men and women.
be due to women being less likely to receive treatment with
Bleeding risk is similar for women and men.
anticoagulation (see the Cardiology section of this book).
Statins appear to be equally effective in women and men
for primary prevention. For secondary prevention, statin
therapy is at least equally effective in women as in men.
Postmenopausal hormone therapy should not be used for D E P R E S S I O N A N D A N X I ET Y I N WO M E N
primary or secondary prevention of coronary artery disease.
Hormone therapy should be discontinued if a cardiovascu- The lifetime prevalence of depression is higher in women than
lar disease event occurs. Lipid alterations associated with men, and the peak age at onset is 33 to 45 years in women
hormone therapy include both favorable and unfavorable and older than 55 years in men. Women are less likely to com-
changes (see Hormone Therapy section, this chapter). mit suicide but twice as likely to make an attempt, and white
Oral, but not transdermal, estrogen increases C-reactive women are twice as likely as African American women to com-
protein levels. mit suicide. The lifetime prevalence of dysthymia is slightly
higher in women than in men. There is no sex difference for
Hormone therapy should not be used for the purpose bipolar disorder.
of primary or secondary prevention of cardiovascular
disease. Women are more likely to have depression, and it occurs at
a younger age than in men.
H E A RT FA I LU R E I N WO M E N Men are more likely to commit suicide, but women are
twice as likely to make an attempt.
Women account for nearly 50% of hospital admissions for
heart failure, which usually develops at an older age in women African American women are at lower risk of suicide.
than in men. During the past 50 years, the incidence of heart
failure has declined among women but not among men. The risk of depressive symptoms and clinical depres-
Women with heart failure are more likely to have hyperten- sion increases during perimenopause. There is no association
sion, diabetes mellitus, obesity, tobacco use, or atrial fibril- between natural or surgical menopause and rate of depres-
lation, whereas men are more likely to have coronary artery sion. Hormone therapy leads to improved Beck Depression
disease and left ventricular systolic dysfunction. Women are Inventory scores in nondepressed women but not in clinically
more likely to have diastolic heart failure with preserved sys- depressed women. Postmenopausal estrogen may improve
tolic function. Women with heart failure usually survive lon- mild depressive symptoms, but it is not sufficient for treat-
ger than men with heart failure, but they have more dyspnea ment of clinical depression.
on exertion and functional impairment. Depression, often
associated with heart failure, is more common in women than Depression increases during perimenopause.
in men.
Postmenopausal estrogen helps mild symptoms but not
clinical depression.
Nearly 50% of heart failure-related hospital admissions
occur in women.
Postpartum depression affects 10% to 15% of women and
Women more commonly have hypertension, diabetes, develops in the first month after childbirth. It is often unrec-
obesity, tobacco use, or atrial fibrillation than men, whereas ognized. Risk factors include prior major or postpartum
men are more likely to have coronary artery disease and left depression, depression during pregnancy, unmarried status,
ventricular systolic dysfunction. or unplanned pregnancy. It is essential to evaluate thyroid
function in postpartum women with depressive symptoms
Women are more likely to have diastolic dysfunction with
because of overlap in presentation. Psychosis develops in few
preserved systolic function.
women with postpartum depression; it usually requires acute
hospitalization.
Peripartum cardiomyopathy, in which left ventricu-
lar systolic dysfunction and heart failure symptoms occur
Postpartum depression is not uncommon and is often
between the last month of pregnancy and the first 5 months
unrecognized.
postpartum, has unknown cause. It is a diagnosis of exclu-
sion. Medical management is similar to that of other forms Evaluate thyroid function in postpartum women with
of dilated cardiomyopathy (see the Cardiology section of depression symptoms.
this book).
Anxiety disorders that are more prevalent in women include
Peripartum cardiomyopathy is a diagnosis of exclusion and panic disorder, agoraphobia, social phobia, generalized anxi-
is managed like other forms of dilated cardiomyopathy. ety disorder, and posttraumatic stress disorder. Women with
52 . WO M E N S H E A LT H 729
53.
GENERAL INTERNAL MEDICINE: PREOPERATIVE
EVALUATIONa
Karen F. Mauck, MD, MSc, and Margaret Beliveau, MD
730
Box 53.1 CLINICAL PREDICTORS OF INCREASED Table 53.1 ESTIMATED REQUIREMENTS FOR VARIOUS
PERIOPERATIVE CARDIOVASCULAR RISK ACTIVITIES
(MYOCARDIAL INFARCTION, HEART FAILURE, AND
REQUIREMENT ACTIVITY
DEATH)
1 MET Can you take care of yourself ?
Active Cardiac Conditions Eat, dress, or use the toilet?
Unstable coronary syndromes Walk indoors around the house?
Walk a block or 2 on level ground at 23 mph
Acute or recent MI with evidence of important ischemic risk by (3.24.8 kph)?
clinical symptoms or noninvasive studya Do light work around the house like dusting or
Unstable or severe anginab (CCS class III or IV)c washing dishes?
Significant arrhythmias
4 METs Climb a flight of stairs or walk up a hill?
High-grade atrioventricular block Walk on level ground at 4 mph (6.4 kph)?
Symptomatic ventricular arrhythmias in the presence of under- Run a short distance?
lying heart disease Do heavy work around the house like scrubbing
Supraventricular arrhythmias with uncontrolled ventricular rate floors or lifting or moving heavy furniture?
Severe valvular disease Participate in moderate recreational activities such
as golf, bowling, dancing, doubles tennis, or
Decompensated heart failure throwing a baseball or football?
Clinical Risk Factorsd
History of ischemic heart disease (including patients with patho- >10 METs Participate in strenuous sports such as swimming,
singles tennis, football, basketball, or skiing?
logic Q waves on ECG)
History of compensated or prior heart failure (systolic or diastolic)
History of cerebrovascular disease (TIA or stroke) Abbreviations: kph, kilometers per hour; MET, metabolic equivalent task; mph,
miles per hour.
Diabetes mellitus requiring insulin
Adapted from Eagle KA, Brundage BH, Chaitman BR, Ewy GA, Fleisher
Renal insufficiency (preoperative serum creatinine >2 mg/dL) LA, Hertzer NR, et al. Guidelines for perioperative cardiovascular evalua-
tion for noncardiac surgery. Report of the American College of Cardiology/
Abbreviations: CCS, Canadian Cardiovascular Society; ECG, electrocardio- American Heart Association Task Force on Practice Guidelines (Committee on
gram; MI, myocardial infarction; TIA, transient ischemic attack. Perioperative Cardiovascular Evaluation for Noncardiac Surgery). Circulation.
a
Recent MI means that MI occurred more than 7 days previously but within 1996 Mar 15;93(6):1278317 and Eagle KA, Brundage BH, Chaitman BR, Ewy
30 days; acute MI, within 7 days. GA, Fleisher LA, Hertzer NR, et al. Guidelines for perioperative cardiovascular
b
evaluation for noncardiac surgery. Report of the American College of Cardiology/
May include stable angina in patients who are unusually sedentary. American Heart Association Task Force on Practice Guidelines (Committee on
c
Campeau L. Grading of angina pectoris. Circulation. 1976 Sep;54(3):5223. Perioperative Cardiovascular Evaluation for Noncardiac Surgery). J Am Coll
d
Cardiol. 1996 Mar 15;27(4):91048. Used with permission.
From the revised cardiac risk index: Lee TH, Marcantonio ER, Mangione
CM, Thomas EJ, Polanczyk CA, Cook EF, et al. Derivation and prospective
validation of a simple index for prediction of cardiac risk of major noncardiac
surgery. Circulation. 1999 Sep 7;100(10):10439. gallops, rales, rhonchi, and wheezes. Perform a brief abdom-
Adapted from Fleisher LA, Beckman JA, Brown KA, Calkins H, Chaikof inal examination for features such as organomegaly and
E, Fleischmann KE, et al. ACC/AHA 2007 guidelines on perioperative scars. Examine the extremities for palpable distal pulses and
cardiovascular evaluation and care for noncardiac surgery: a report of the evidence of peripheral edema. Perform a limited neurologic
American College of Cardiology/American Heart Association Task Force
on Practice Guidelines (Writing Committee to Revise the 2002 Guidelines examination that includes mental status and a gross sensory
on Perioperative Cardiovascular Evaluation for Noncardiac Surgery). J Am and motor evaluation (ie, identify baseline cognitive or neu-
Coll Cardiol. 2007 Oct 23;50(17):e159242 and Fleisher LA, Beckman rologic problems).
JA, Brown KA, Calkins H, Chaikof E, Fleischmann KE, et al. ACC/AHA
2007 guidelines on perioperative cardiovascular evaluation and care for non-
cardiac surgery: a report of the American College of Cardiology/American
Heart Association Task Force on Practice Guidelines (Writing Committee IMPRESSION AND PLAN
to Revise the 2002 Guidelines on Perioperative Cardiovascular Evaluation
for Noncardiac Surgery): developed in collaboration with the American Summarize your assessment of perioperative risk and any
Society of Echocardiography, American Society of Nuclear Cardiology, additional testing and management recommendations based
Heart Rhythm Society, Society of Cardiovascular Anesthesiologists, Society
for Cardiovascular Angiography and Interventions, Society for Vascular
on this risk. This usually includes the following statement:
Medicine and Biology, and Society for Vascular Surgery. Circulation. 2007 The patient is medically optimized for the planned surgical
Oct 23;116(17):e41899. Epub 2007 Sep 27. Errata in: Circulation. 2008 procedure. Avoid using the expression cleared for surgery,
Aug 26;118(9): e1434. Circulation. 2008 Feb 5;117(5):e154. Used with
permission.
which implies a guarantee of no problems and can be easily
misinterpreted. For completeness, it is often helpful to divide
this section into the following categories:
P H Y S I C A L E X A M I NAT I O N
1. Cardiac risk: Include important factors that led to your
Include blood pressure, temperature, and pulse and respira- recommendations, such as active cardiac conditions,
tory rates. The head and neck examination should include clinical risk factors, functional capacity, and the urgency
neck range of motion, evaluation of the airway (Figure 53.1), and type of operation planned. Include your rationale
carotid auscultation, and assessment of the jugular veins. The and plan for additional testing if indicated and a plan for
cardiopulmonary examination should focus on murmurs, perioperative management and surveillance.
2. Pulmonary risk: Include risk factors for perioperative The type of operation performed is also an important
pulmonary complications, the rationale for additional determinant of cardiovascular morbidity and mortality
testing if indicated, and a plan for perioperative (Table 53.3). However, the importance of comorbid disease in
management for risk reduction. determining surgical risk may outweigh the nature of the pro-
cedure or the type of anesthesia used in predicting outcome.
3. DVT risk: Include risk factors for DVT risk and the
The following sections discuss 1) cardiac and pulmonary risk
rationale for a perioperative prophylaxis regimen.
assessment and management strategies and 2) prophylaxis of
4. Perioperative management of medical comorbidities: List thromboembolism and management of anticoagulants in the
other medical comorbidities that will affect perioperative perioperative period.
care, and comment on management recommendations
(for diabetes mellitus, seizure disorder, renal insufficiency,
corticosteroid dependence, sleep apnea, hypertension, C A R D I AC R I S K A S S E S S M E N T A N D R I S K
etc). R E D U C T I O N S T R AT E G I E S
5. Perioperative management of medications: Include a plan Coronary artery disease (CAD) is a frequent cause of peri-
for continuing or discontinuing use of medications and a operative cardiac mortality and morbidity after noncardiac
recommendation for the timing of the administration of surgery. Perioperative myocardial infarction (MI) occurs in
the medications. approximately 1% of general surgical procedures and in up
6. Perioperative alerts: Include alerts for allergies, personal to 3.2% of vascular surgical procedures. Among patients who
or family history of serious anesthetic complications, have a perioperative MI, the hospital mortality rate is 15% to
concern for difficult intubation, pacemaker dependence, 25%, and those who survive to dismissal from the hospital
defibrillator, known aortic stenosis, concern for neck have an increased risk of another MI and cardiovascular death
instability in rheumatoid arthritis or Down syndrome during the ensuing 6 months postoperatively. Perioperative
patients, etc.
Table 53.2 AMERICAN SOCIETY OF
ANESTHESIOLOGISTS CLASSIFICATION OF
R I S K S O F A N E S T H E S I A A N D S U R G E RY ANESTHETIC MORTALITY WITHIN 48 HOURS
POSTOPERATIVELY
Mortality associated with anesthesia and surgery has decreased
markedly in the past several decades. Today the overall mor- MORTALITY
CLASS PHYSICAL STATUS AT 48 H
tality is 1:250,000 even though more complex surgical proce-
dures are performed on sicker patients. The American Society I Healthy person younger than 80 y 0.07%
of Anesthesiologists (ASA) classification, with broadly defined
categories, is used to estimate overall risk of mortality within II Mild systemic disease 0.24%
48 hours postoperatively (Table 53.2). Although this classifi- III Severe but not incapacitating systemic 1.4%
cation system is quite subjective, it has stood the test of time disease
and reproducibility in broadly estimating overall risk.
Neuraxial anesthesia and general anesthesia are not associ- IV Incapacitating systemic disease that is a 7.5%
constant threat to life
ated with significantly different outcomes for mortality and
cardiac events. Many anesthesiologists recommend one type V Moribund patient not expected to survive 8.1%
of anesthetic technique over another, depending on the surgi- 24 h, regardless of surgery
cal procedure performed and the comorbidities of the patient, E Suffix added to any class to indicate emer- Doubles risk
but even though spinal, regional, and general anesthesia have gency procedure
different risks and benefits, the internist should not recom-
mend a particular anesthetic technique or agent. This decision Adapted from Pinnock C, Lin T, Smith T, Jones R. Fundamentals of anaesthesia.
is best left to the anesthesia team at the time of surgery. 2nd ed. London (UK): Greenwich Medical Media; c2003. Used with permission.
C A R D I AC R I S K A S S E S S M E N T A S T E PWI S E A P P ROAC H
A stepwise approach is used for perioperative cardiac assess- With the above information, use the ACC/AHA guidelines
ment as outlined in the ACC/AHA 2007 Guidelines in your decision process (Figure 53.2).
on Perioperative Cardiovascular Evaluation and Care for
Step 1. Does the patient need emergency noncardiac sur-
Noncardiac Surgery (Figure 53.2). These guidelines pres-
gery? If the answer is yes, the patient should be taken to the
ent a framework for determining which patients are candi-
operating room without delay, and risk stratification and sur-
dates for further testing on the basis of patient-related and
veillance should be done postoperatively.
surgery-related risk factors.
Step 2. Does the patient have an active cardiac condition
(Box 53.1)? If an active cardiac condition exists, the patient
1. Surgical or percutaneous intervention is rarely
should be evaluated according to ACC/AHA guidelines. If
necessary simply to lower the risk of surgery unless the
there are no active cardiac conditions, proceed to step 3.
intervention is indicated irrespective of the preoperative
Step 3. Is the patient undergoing low-risk surgery (ie, a
context.
skin, eye, or breast procedure)? If so, the patient can proceed
2. No testing should be performed unless the results will to the operating room without further cardiac evaluation. If
influence patient treatment. not, proceed to step 4.
No
No
Step 5 No or unknown
Consider testing if it
will change management;
consider perioperative Proceed with planned surgery with HR control (Class IIa, LOE B) or Proceed with
-blockadec consider noninvasive testing (Class IIb, LOE B) if it will change management planned surgery
Figure 53.2 Stepwise Approach to Perioperative Cardiac Assessment. This cardiac evaluation and care algorithm for noncardiac surgery is based
on active clinical conditions, known cardiovascular disease, and cardiac risk factors for patients 50 years or older as outlined in ACC/AHA 2007
Guidelines on Perioperative Cardiovascular Evaluation and Care for Noncardiac Surgery. Clinical risk factors include ischemic heart disease,
compensated or prior heart failure, diabetes mellitus, renal insufficiency, and cerebrovascular disease. Superscript letters indicate the following: a, see
Box 53.1; b, see Table 53.1; c, see Table 53.4. HR indicates heart rate; LOE, level of evidence; MET, metabolic equivalent task. (Adapted from Fleisher
LA, Beckman JA, Brown KA, Calkins H, Chaikof E, Fleischmann KE, et al. ACC/AHA 2007 guidelines on perioperative cardiovascular evaluation
and care for noncardiac surgery: a report of the American College of Cardiology/American Heart Association Task Force on Practice Guidelines
[Writing Committee to Revise the 2002 Guidelines on Perioperative Cardiovascular Evaluation for Noncardiac Surgery]. J Am Coll Cardiol. 2007
Oct 23;50[17]:e159242 and Fleisher LA, Beckman JA, Brown KA, Calkins H, Chaikof E, Fleischmann KE, et al. ACC/AHA 2007 guidelines on
perioperative cardiovascular evaluation and care for noncardiac surgery: a report of the American College of Cardiology/American Heart Association
Task Force on Practice Guidelines [Writing Committee to Revise the 2002 Guidelines on Perioperative Cardiovascular Evaluation for Noncardiac
Surgery]: developed in collaboration with the American Society of Echocardiography, American Society of Nuclear Cardiology, Heart Rhythm
Society, Society of Cardiovascular Anesthesiologists, Society for Cardiovascular Angiography and Interventions, Society for Vascular Medicine and
Biology, and Society for Vascular Surgery. Circulation. 2007 Oct 23;116[17]:e41899. Epub 2007 Sep 27. Errata in: Circulation. 2008 Aug 26;118[9]:
e1434. Circulation. 2008 Feb 5;117[5]:e154. Used with permission.)
Step 4. Does the patient have a good functional capac- that controls the heart rate at less than 65 beats
ity (4 METs) without symptoms? If yes, the patient should per minute. Noninvasive testing should be
proceed to surgery without further evaluation. If the func- performed only if the results will change
tional capacity is unknown or less than 4 METs, proceed to management.
step 5.
Step 5. Does the patient have any clinical risk factors 3. With 3 or more risk factors, the type of surgery needs to
(Box 53.1)? be considered.
1. With no clinical risk factors, the patient should proceed a. For an intermediate-risk procedure, the patient should
to surgery. proceed to surgery with a -blocker dosage that
controls the heart rate at less than 65 beats per minute.
2. With 1 or 2 clinical risk factors, the patient Noninvasive testing should be performed only if the
should proceed to surgery with a -blocker dosage results will change management.
General anesthesia 2.4 (1.83.1) All patients who are identified as having an increased risk of
postoperative pulmonary complications should receive both
Transfusion >4 units 1.5 (1.31.7) of the following interventions postoperatively:
Abbreviation: ASA, American Society of Anesthesiologists. 1. Deep breathing exercises or incentive spirometry (positive
Adapted from Smetana GW, Lawrence VA, Cornell JE; American College of airway pressure for patients unable to perform these).
Physicians. Preoperative pulmonary risk stratification for noncardiothoracic sur-
gery: systematic review for the American College of Physicians. Ann Intern Med. 2. Selective use of a nasogastric tube (as needed for
2006 Apr 18;144(8):58195. Used with permission. postoperative nausea and vomiting, inability to tolerate
oral intake, or symptomatic abdominal distention).
intensive care unit transfers, serious complications, and length The following procedures should not be used for the pur-
of hospital stay in the postoperative period. pose of reducing postoperative pulmonary complications:
Significant patient-related risk factors include COPD, age 1. Right heart catheterization.
older than 60 years, ASA class II, functional dependence,
congestive heart failure, and serum albumin <35 g/L. 2. Total parenteral or enteral nutrition (for patients who are
malnourished or have low serum albumin levels).
Obesity, mild or moderate asthma, and restrictive lung
disease are not significant risk factors for postoperative
pulmonary complications.
VE N O U S T H R O M B O E M B O L I C
Procedure-related risk factors include prolonged surgery P R O P H Y L AX I S
(>3 hours), open aortic aneurysm repair, abdominal
surgery, thoracic surgery, head and neck surgery, vascular Although all surgical patients are at increased risk of venous
surgery, emergency surgery, and general anesthesia. thromboembolic (VTE) disease, certain patients form a
Low
Minor surgery in mobile patients <10 No specific thromboprophylaxis
Medical patients who are fully mobile Early and aggressive ambulation
Moderate
Most general, open gynecologic or urologic 1040 LMWH (at recommended doses), LDUH 2 or
surgery patients 3 times daily, fondaparinux
Medical patients (bed rest or sick)
Moderate VTE risk plus high bleeding risk Mechanical thromboprophylaxisc
High
Hip or knee arthroplasty, hip fracture 4080 LMWH (at recommended doses), fonda-
surgery parinux, oral vitamin K antagonist (INR
Major trauma, spinal cord injury 23)
High VTE risk plus high bleeding risk Mechanical thromboprophylaxisc
Abbreviations: DVT, deep vein thrombosis; INR, international normalized ratio; LDUH, low-dose unfractionated heparin; LMWH, low-molecular-weight heparin;
VTE, venous thromboembolic.
a
The descriptive terms are purposely left undefined to allow individual clinician interpretation.
b
Rates are based on objective diagnostic screening for asymptomatic DVT in patients not receiving thromboprophylaxis.
c
Mechanical thromboprophylaxis includes intermittent pneumatic compression or venous foot pump, with or without graduated compression stockings; consider
switching to anticoagulant thromboprophylaxis when high bleeding risk decreases.
Adapted from Geerts WH, Bergqvist D, Pineo GF, Heit JA, Samama CM, Lassen MR, et al. Prevention of venous thromboembolism: American College of Chest
Physicians Evidence-Based Clinical Practice Guidelines (8th Edition). Chest. 2008 Jun;133(Pt 6 Suppl):381S453S. Used with permission.
high-risk subset, including those who are elderly and those for DVT prophylaxisit may be best to wait until the
who have prolonged anesthesia, previous VTE, hereditary catheter is removed.
disorders of thrombosis, prolonged immobilization or paraly-
5. Some patients should continue a prolonged course of
sis, malignancy, obesity, varicosities, or pharmacologic estro-
DVT prophylaxis well after hospital dismissal. Patients
gen use. The American College of Chest Physicians released
undergoing major surgery for malignancy, hip or knee
the eighth edition of its antithrombotic and thrombolytic
replacement, or hip fracture repair require 2 to 6 weeks
therapy guidelines, which includes a section on prevention
of DVT prophylaxis postoperatively. Details on specific
of venous thromboembolism. This guideline is lengthy and
duration and recommended methods are described in the
provides group-specific recommendations for patients under-
American College of Chest Physicians guidelines.
going surgery. A simplified classification system is outlined in
Table 53.6.
General principles to keep in mind include the following:
P R E O P E R AT I VE T E S T I N G GU I D E L I N E S
1. Aspirin alone is not recommended as prophylaxis against
Results of routine laboratory and diagnostic tests, while often
VTE for any patient group.
obtained, usually have little effect on perioperative manage-
2. Patients undergoing an operation for hip or knee ment. Therefore, routine tests are often not necessary before
replacement, hip fracture, or malignancy are at particularly many surgical procedures unless a specific indication is
high risk. In these patient populations, prophylaxis is present.
more aggressive and data suggest that prophylaxis should
continue after hospital dismissal (from 10 days to 1
C OAGU L AT I O N S T U D I E S
month).
Prothrombin time and international normalized ratio are
3. Consider renal impairment when deciding on doses of
recommended for patients who have a known coagulation
low-molecular-weight heparin, fondaparinux, and other
abnormality or a history suggestive of coagulation problems
antithrombotic drugs that are renally excreted, particularly
(chronic liver disease, malnutrition, excessive bleeding with
for elderly patients and those who are at high risk of
past procedures, etc). Additionally, patients who are taking
bleeding. Many of these drugs are contraindicated in
anticoagulants or who will receive full doses of anticoagu-
dialysis patients.
lants postoperatively should have coagulation studies preop-
4. In all patients undergoing neuraxial anesthesia or eratively. Partial thromboplastin time and bleeding time are
analgesia, use special caution when using anticoagulants rarely indicated for these patients preoperatively.
E L E C T RO LY T E S
An ECG is recommended before intermediate- or high-risk
surgery for men older than 40 years, or women older than
Measurement of the potassium level should be considered for 50. Additionally, an ECG is recommended for any patient
patients who are taking digoxin, diuretics, angiotensin-converting (regardless of age) with known CAD or for those who are
enzyme inhibitors, angiotensin receptor blockers, or other med- at increased risk of CAD because they have a history of dia-
ications known to alter electrolytes. It is recommended for any betes mellitus, cerebrovascular disease, hypertension, chest
patient with a history of renal insufficiency or renal failure. pain, congestive heart failure, smoking, peripheral vascular
Measurement of the sodium level should be considered for disease, inability to exercise, or morbid obesity. An ECG is
patients who are undergoing urologic procedures that involve recommended for any patient with any new cardiovascular
bladder irrigation or patients who have conditions associated symptoms or with signs and symptoms of new or unstable
with hyponatremia or hypernatremia (congestive heart failure, cardiac disease. An ECG performed within 6 months preop-
liver failure, syndrome of inappropriate secretion of antidi- eratively is adequate if clinical symptoms have not changed in
uretic hormone, etc). the interim.
C R E AT I N I N E CHEST RADIOGRAPHY
Measurement of the creatinine level is recommended for Chest radiography is recommended for patients older than
patients with any of the following: renal insufficiency, age 50 years, patients who have known cardiac or pulmonary dis-
older than 50 years, diabetes mellitus, hypertension, cardio- ease, and patients who have symptoms or physical examina-
vascular disease, plans to undergo major surgery, or use of tion findings suggestive of new or unstable cardiopulmonary
medications that may affect renal function. disease.
741
T R E AT M E N T O F A L C O H O L WI T H D R AWA L Delirium tremens occurs in up to 20% of untreated
patients with alcohol withdrawal.
Alcohol abuse in hospitalized patients is underrecognized.
Patients with alcohol withdrawal are best treated as inpa- Wernicke encephalopathy, seen in thiamine-deficient
tients, especially if they have a history of seizures, delirium tre- patients, is characterized by palsy of the abducens
mens, psychiatric disease, or multiple medical comorbidities. nerve (cranial nerve VI), nystagmus, ataxia, and
Delirium tremens occurs in up to 20% of untreated patients disorientation.
with alcohol withdrawal.
Patients in early withdrawal, within 48 hours of the last
drink, may have mild hypertension and tachycardia, mild M E D I C AT I O N R E C O N C I L I AT I O N
hyperthermia, fine tremors, agitation, slightly impaired orien- Medication reconciliation involves comparing a patients
tation, and early visual and auditory hallucinations. Seizures medication orders or prescriptions with the list of medica-
may occur during early withdrawal and may be the presenting tions that the patient has actually been taking. This process
complaint for admission. Seizures can occur in up to one-third must occur with each transition of care to decrease the risk of
of the patients and should be considered in patients who have duplications, incorrect dose or frequency, omissions, and drug
had withdrawal seizures previously. Other causes or cofactors interactionserrors that occur too easily during transitions
to exclude are hyponatremia, hypoglycemia, central nervous of care and lead to considerable morbidity and mortality. All
system trauma, and infection. Alcohol withdrawal seizures are medications should be reviewed for ongoing indications. For
best treated with benzodiazepines. example, proton pump inhibitors, which are often prescribed
It is hard to predict which patients will progress to late for prophylaxis at admission are commonly continued after-
withdrawal (ie, delirium tremens). Risk factors include older ward without an indication.
age, concomitant medical disease, prior delirium tremens, and Polypharmacy is common among geriatric patients and
abnormal liver function test results. This condition is charac- patients receiving treatment for psychiatric conditions. Each
terized by tachycardia, hyperthermia, gross tremors, delirium, year, patients older than 65 years fill an average of 12 prescrip-
disorientation, and hallucinations. Nausea and vomiting may tions in addition to buying over-the-counter and herbal medi-
lead to aspiration. Fluctuations in blood pressure may predis- cations. Medication reconciliation becomes even more crucial
pose the patient to cardiac and cerebrovascular events. Patients for these patients since the risk of adverse events increases with
with arrhythmias need to be monitored, and often a bed in the the number of medications.
intensive care unit is required if the patient is severely affected The use of electronic health records (EHRs) does not
and may need intubation. Severe withdrawal carries a signifi- eliminate the need for careful medication reconciliation;
cant risk of death. an outdated EHR itself can be the source of serious medi-
Patients with alcohol withdrawal are evaluated with the cation errors and provide a false sense of security. Arguably,
revised Clinical Institute Withdrawal Assessment (CIWA), the most important innovation for applying EHRs to The
a symptom-based nurse-administered scale for assessing nau- Joint Commissions National Patient Safety Goal is improved
sea and vomiting, tremulousness, diaphoresis, anxiety, agita- interoperability of medication lists across organizations and
tion, paresthesias, auditory and visual disturbances, headache, EHRs.
and disorientation. The results are used for determining the
benzodiazepine dosage. Patients who have had severe with-
drawal previously should receive a loading dose of benzo- NU T R IT I O NA L A S S E S S M E N T A N D P ROVI S I O N
diazepines, preferably one with a longer half-life, such as I N T H E H O S P I TA L
chlordiazepoxide. Phenobarbital can be used if withdrawal
is refractory to benzodiazepines; however, patients receiving Up to 40% of patients admitted to the hospital may be mal-
both of these agents may not be able to protect their airway. nourished. While hospitalization offers opportunities to
Alcoholic patients should routinely receive chemical depen- correct this condition, a patients nutritional status can also
dency counseling and psychiatric evaluation. Notably, these worsen malnutrition since the acute illness that led to hospi-
patients are at risk of Wernicke encephalopathy, which is seen talization may trigger a hypermetabolic state. If the digestive
in thiamine-deficient patients and is characterized by palsy of tract is functioning properly, and the person can eat, mal-
the abducens nerve (cranial nerve VI), nystagmus, ataxia, and nourishment may be the consequence of impaired access to
disorientation. The usual replacement dosage of thiamine is adequate food. Patients most at risk of malnutrition include
100 mg daily. Hypomagnesemia should be treated since a low those with gastrointestinal tract dysfunction (eg, xerostomia,
magnesium level may decrease the seizure threshold. dysphagia, malabsorption, pancreatitis, and diarrhea), malig-
nancy, infection, chronic lung disease, alcoholism, and depres-
sion. Micronutrient deficiencies are often associated with
Alcohol abuse in hospitalized patients is often
specific signs and symptoms (Table 54.1).
underrecognized.
Patients who cannot eat enough to satisfy metabolic
The revised CIWA is a symptom-based scale for assessing demand should be evaluated for a mechanical feeding prob-
nausea and vomiting, tremulousness, diaphoresis, anxiety, lem, malabsorption, or causes of increased metabolic require-
agitation, paresthesias, auditory and visual disturbances, ments. Mechanical feeding problems may require altering the
headache, and disorientation. consistency of food and nutritional supplements.
Vitamin C Petechial & gingival hemorrhage, corkscrew hair, spongy gums with tooth loss, poor wound healing
Cobalt Anemia
Vitamin B12 (cobalamin) Macrocytic anemia, smooth tongue, subacute combined degeneration of the spinal cord, bilateral paresthe-
sias, impaired proprioception & vibrational sense, spastic ataxia, central scotomata, dementia, weakness,
hyperreflexia, bilateral extensor plantar responses
a
Many complications are frequently attributed to micronutrient deficiencies that are still controversial, especially when complications occur without classic features and
with measured nutrient levels near or within the reference range (eg, putative associations of vitamin D deficiency).
54 . H O S P I TA L M E D I C I N E 743
Box 54.1 ACTIVITIES OF DAILY LIVING (ADL) AND C O M P L I C AT I O N S O F H O S P I TA L I Z AT I O N
INSTRUMENTAL ACTIVITIES OF DAILY LIVING (IADL)
Complications of hospitalization may be iatrogenic (caused by
ADL medical examination or treatment) or nosocomial (originating in
Bathing the hospital). Some adverse outcomes are predictable, and others
Dressing are not. Adverse events related to the hospital environment itself
Using toilet include falls, thrombosis, debility, pressure ulcers, sleep depriva-
Mobility tion, and aspiration pneumonia. Infections related to the hospi-
Continence tal include health careassociated pneumonia, catheter-related
Feeding self bloodstream infections, Clostridium difficile colitis, and the
IADL development of resistant organisms. Discontinuity of patient
Using telephone care caused by poor communication during patient handoffs
Shopping and dismissals can lead to preventable injury and error. In addi-
Preparing meals tion, health care workers are exposed to risks of occupational
Housekeeping injury while taking care of hospitalized patients.
Laundry
Transportation PRESSURE ULCERS
Taking medicine
Managing money Pressure ulcers result from soft tissue being compressed
between bone and an external surface, leading to tissue necro-
sis. Ulcers are staged according to their degree of penetration.
older, which translated into 832.6 reports for every 100,000 Several factors may contribute to the formation of pressure
people over the age of 60 in 2006. ulcers. Patient-specific risk factors include immobility, malnu-
Mobility and fall risk assessment should include evaluating trition, impaired cognition, circulatory dysfunction, immuno-
the need for assistive devices such as walkers, toilet seats with suppression (eg, diabetes mellitus), and sensory impairment.
arms, and appropriate footwear. The history of recent falls and External factors include pressure, shearing forces (such as
the circumstances associated with them should be obtained. when a patient slides in a bed or chair, leading to stretching and
Physical therapy and occupational therapy guidance should be angulation of the underlying subcutaneous tissue and impaired
sought if needed. Several simple mobility scales are available. lymphatic and capillary flow), friction, and moisture.
Neuropsychiatric evaluation should include screening for Prevention of ulcers is of utmost importance. The first step
depression, delirium, and dementia. Depression is a common in management is to identify patients at risk and modify their
problem that can be assessed with the Geriatric Depression risk factors. Sites most at risk are the heels and the sacrum.
Scale. Delirium is common in hospitalized patients and results Frequent turning, maintaining skin hygiene, and maintaining
from various causes, including medication, infections, and opi- nutritional integrity are essential. Underlying pressure must be
ates. Patients can be assessed with the Confusion Assessment relieved, and various pressure-relieving devices, including heel
Method (Box 54.2). The Mini-Cog assessment, the Folstein boots and specialty mattresses, are available.
Mini-Mental State Examination, and other tests are available The wound should be dbrided by surgical, chemical,
to screen for dementia. Screening for alcoholism also is essen- mechanical, or biotherapeutic means. Superficial wounds are
tial. Visual and auditory deficits may exacerbate cognitive treated with semipermeable membranes; deeper wounds may
problems, depression, and barriers to education. require either hydrocolloids or hydrogels. Deep wounds may
Assessment for urinary incontinence, urinary retention, be treated surgically with skin grafts or flaps. The cornerstone of
and problems with bowel function should occur at admission ulcer treatment is to keep the wound moist and the surround-
and before discharge. ing skin dry. Adjunctive therapy may include vacuum-assisted
Nutritional issues specific to geriatric patients include closure, larval therapy, or growth factors. Routine antibiotics
problems related to dentition, dentures, the risk of dysphagia are not indicated unless the ulcer is complicated by soft tissue
and aspiration, reduced appetite, and recent weight changes. infection or osteomyelitis.
1. Acute onset with fluctuating course Falls among hospitalized patients are common and may lead
2. Inattention to serious injury or death. The outcome of a fall can vary with
3. Disorganized thinking patient-specific and environmental factors. For example, it is
4. Altered level of consciousness important to recognize that the outcome of an otherwise sim-
ple fall may be worse for a patient receiving anticoagulation.
a
Diagnosis of delirium requires the presence of 1 and 2, along with either 3 or 4. Risk factors for in-hospital falls include debility, toileting,
Data from Inouye SK, van Dyck CH, Alessi CA, Balkin S, Siegal AP, Horwitz RI, orthostatic hypotension, altered mental status, sedation, his-
et al. Clarifying confusion: the confusion assessment method. A new method tory of previous falls, recent environmental changes, binders
for detection of delirium. Ann Intern Med. 1990 Dec 15;113(12):9418.
(such as urinary catheters), restraints, poor communication
Binders Routinely assess need for urinary catheter, oxygen, & Remove unneeded binders; avoid physical restraints
intravenous lines
Delirium Determine CAM score for admitted patients (Box 54.2) Identify & address risk factors (electrolytes, medications, etc)
Medications Review medication list for medications with Avoid tricyclic antidepressants & other drugs that increase
anticholinergic properties fall risk
Insufficient education Assess patients knowledge of call lights & assistive Education of patients & families
devices
Inadequate staff Monitor ratio of number of staff to number of falls Provide adequate staff for high-risk patients
between providers, depression, sensory impairment, and the rates of use vary by center. Other anticoagulants continue
incontinence. Falls tend to occur in periods of lower staff- to be studied and compared with these more established ones.
ing (eg, nights and weekends). Interventions to prevent falls Ximelagatran, a direct thrombin inhibitor, has been shown to
include identifying at-risk patients, avoiding excess binders, have an efficacy and side-effect profile comparable to those of
encouraging early mobilization, and providing physical ther- warfarin.
apy (Table 54.2).
H O S P I TA L-AC Q U I R E D I N F E C T I O N S
V E N O US T H RO M B O E M B O L I S M
Since Semmelweis understood the cause of puerperal fever
Venous thromboembolism (VTE) is a common complication in the hospital, hand washing has been encouraged to reduce
of hospitalization. Even among patients receiving standard-of- hospital-acquired infection. Although hand hygiene is a sim-
care pharmacologic prophylaxis, the risk of VTE in some pop- ple, readily available intervention, it still fails to reach 100%
ulations may be as high as 7% to 10%. That risk may be 15% or adherence. There has been extensive debate about factors that
higher (much higher after knee, hip, pelvic, and other ortho- contribute to deficient hand hygiene and options to improve
pedic operations) among patients who do not receive appro- compliance. These include the health beliefs of health care
priate prophylactic care. Unsuspected pulmonary embolism workers (eg, the providers belief about the potential risk
may be associated with 5% to 10% of hospital deaths. of infection, relating to both the body site and the patients
Medical conditions that predispose a patient to VTE assumed cleanliness), time constraints, established care prac-
include acute infectious disease, congestive heart failure, acute tices, and demonstration by example of senior staff.
myocardial infarction, cerebrovascular accident, rheumatic
disease, and inflammatory bowel disease. Specific risk factors
C AT H ET E R-R E L AT E D B L O O D S T R E A M
include age older than 75 years, previous VTE, immobility,
INFECTIONS
recent trauma or surgery, estrogen use, obesity, and hypercoag-
ulable states. Patients with malignancyparticularly pancre- Each year, 150 million central or peripheral intravenous cath-
atic cancer and other mucin-positive adenocarcinomasare eters are placed (an average of 5 per patient). They result in
at especially high risk. Patients with a cerebrovascular acci- around 850,000 infections (<0.6%), including about 250,000
dent are also at higher risk but carry a putative increased risk catheter-related bloodstream infections (CRBIs) that result in
of intracranial hemorrhage. septic thrombophlebitis, bacteremia, and endocarditis. CRBIs
Among nonpharmacologic means of VTE prophylaxis, lead to increased morbidity, mortality, and health care costs
ambulation is the most easily accomplished. In postoperative and to longer hospitalizations.
nonambulatory patients, graduated compression stockings The risk of CRBI is related to the type of catheter, the loca-
have been shown to decrease the rate of VTE by 50%. Isolated tion, placement (who places the catheter and the technique
ankle exercises are also helpful in increasing lower extremity used) and the length of time the catheter remains in place.
venous blood flow. These nonpharmacologic approaches are The highest risk is with peripheral catheters placed by surgi-
especially important in patients for whom anticoagulation is cal cutdown. The next highest risks are with peripheral steel
contraindicated. needles, intra-aortic balloon pumps, and short-term hemodi-
Pharmacologic prevention with heparin, low-molecular- alysis catheters. Nasal carriers of Staphylococcus aureus have a
weight heparin, or fondaparinux (a factor Xa inhibitor) higher risk of CRBI than noncarriers. Use of simple infection
appears to be effective, although the rates of risk reduction and control procedures can decrease the risk of infection by 65%.
54 . H O S P I TA L M E D I C I N E 745
Box 54.3 CONTROL AND PREVENTION GUIDELINES H O S P I TA L-AC Q U I R E D D I A R R H E A
RECOMMENDED BY THE CENTERS FOR DISEASE One of the most common hospital-acquired infections and the
CONTROL AND PREVENTION most common cause of diarrhea among hospitalized patients
is C difficile. It is a frequent cause of morbidity and mortality
Hand washing among elderly hospitalized patients. The spectrum of disease
Full barrier precautions when inserting central venous lines includes asymptomatic carrier, mild to moderate diarrhea,
Chlorhexidine for skin disinfection pseudomembranous colitis, and toxic megacolon. Symptoms
Avoidance of a femoral insertion site usually occur after 5 to 10 days of antibiotic treatment, but
Timely removal of catheters they may develop as early as 1 day into treatment or as late
Data from Boyce JM, Pittet D; Healthcare Infection Control Practices
as 10 weeks after its cessation. Presenting manifestations may
Advisory Committee; HICPAC/SHEA/APIC/IDSA Hand Hygiene Task include fever, abdominal pain, and a prominent leukocytosis.
Force. Guideline for hand hygiene in health-care settings: recommendations Diagnosis is made by demonstrating C difficile toxin in the
of the Healthcare Infection Control Practices Advisory Committee and the
HICPAC/SHEA/APIC/IDSA Hand Hygiene Task Force. MMWR Recomm
stool, although patients may need to have direct colon imag-
Rep. 2002 Oct 25;51(RR-16):145. ing in unclear cases.
Nonpharmacologic treatment of C difficile infection
includes correcting fluid losses and electrolyte imbalances and
Safety checklists and specialized teams that use a standard- avoiding the use of antiperistaltic agents. Strict observation of
ized approach have been shown to significantly decrease rates. contact isolation precautions and hand washing with soap and
Specific measures include changing peripheral catheter sites water are essential.
every 72 to 96 hours to reduce the risk of infection and patient Pharmacologic treatment of C difficile infection includes
discomfort associated with superficial phlebitis. Control and use of the following:
prevention guidelines from the Centers for Disease Control
and Prevention (CDC) are given in Box 54.3. 1. Metronidazolefirst-line antibiotic for mild infection
2. Oral vancomycinfor severe resistant infections and
during pregnancy
H E A LT H C A R E A S S O C I AT E D P N EU MO N I A
3. Rifaximin, intravenous immune globulin, and fecal
Health careassociated pneumonia (HCAP) is defined as transplantpossible adjuncts in refractory infection
pneumonia in a patient who has been hospitalized in an
acute care facility for 2 or more days within the past 90 days, 4. Probiotics (eg, Lactobacillus species and Saccharomyces
has resided in a nursing home or long-term care facility, has boulardii)useful for decreasing the incidence of
received recent intravenous antibiotic therapy or chemother- antibiotic-associated diarrhea but not reliably useful for
apy or wound care within 30 days of the current infection, or preventing C difficile infection
is receiving hemodialysis.
Bacteria frequently involved in HCAP include Indications for surgical intervention include poor clinical
Streptococcus pneumoniae, methicillin-sensitive S aureus, and response to antibiotics, progressive fever, rigors, peritoneal
methicillin-resistant S aureus (MRSA); antibiotic-sensitive signs, bacteremia, persistent leukocytosis, or computed tomo-
gram-negative bacilli such as Escherichia coli, Klebsiella graphic (CT) evidence of significant pericolonic inflamma-
pneumoniae, Enterobacter species, Proteus species, and tion with increasing bowel wall edema. The recommended
Serratia marcescens; and multidrug-resistant (MDR) enteric surgical procedure is subtotal colectomy with ileostomy, which
gram-negative bacilli such as Pseudomonas aeruginosa and may be converted to ileorectal anastomosis later.
Acinetobacter. Fungal pathogens such as Candida and
Aspergillus may need to be considered in immunosuppressed
C AT H ET E R-A S S O C I AT E D U R I NA RY T R AC T
patients. Although a viral pathogen is less frequent, the most
INFECTIONS
common virus is Influenzavirus A. Risk factors for infection
with MDR pathogens include the following: recent antibi- Catheter-associated urinary tract infections (CAUTIs) are
otic therapy, current hospitalization of more than 5 days, high the most common type of health careassociated infection
local resistance rates, and an immunosuppressed state. MDR (Box 54.4). Approximately 900,000 CAUTIs are reported
pathogens are most frequent in intensive care units and trans- each year. They are responsible for an estimated $500 mil-
plant patients. lion in additional expense annually, and they increase the
Treatment of HCAP should include early recognition, ini- patient length of stay by 2 to 4 days. Over 10,000 deaths
tial broad-spectrum coverage with subsequent de-escalation are attributable to CAUTIs annually; CAUTIs are the
based on culture results, attempts at bacteriologic diagnosis, leading cause of secondary bloodstream infections, with
avoidance of the overuse of antibiotics, and application of pre- approximately 10% mortality. Other negative repercussions
vention strategies. Hospitalized patients, especially those with of CAUTIs are the additional antibiotic use and the associ-
impaired mentation or neuromotor deficits, may be at risk of ated risks of resistance. The CDC recommends the follow-
aspiration. These patients should be kept in a semirecumbent ing evidence-based measures for reducing the incidence of
position (30 45), especially when receiving enteral feeding. CAUTIs:
C O M P L I C AT I O N S O F S U R G E RY
Box 54.5 RISK FACTORS FOR POSTOPERATIVE
DELIRIUM
The following section deals with some of the common medi-
cal issues in postoperative patients, including ileus; delirium;
alterations in pulmonary, renal, and cardiac function; and the Uncontrolled pain
complications of bariatric surgery. Geriatric patient
Preexisting cognitive impairment
Cerebrovascular & neurodegenerative disease
I L EUS History of delirium
Alcohol abuse & withdrawal
Postoperative ileus is a nonmechanical disruption of nor-
Narcotic or benzodiazepine dependence
mal gastrointestinal tract motility. Physiologically, gastric
Anticholinergic medications
motility and small-bowel motility normalize several hours
Hypoxia
postoperatively; colon motility normalizes at 24 to 48 hours.
Anemia
Postoperative ileus can cause discomfort, adversely affect nutri-
Hyperglycemia & hypoglycemia
tion, increase the risk of infection, compromise wound healing,
Electrolyte abnormalities
increase catabolism, and increase the risk of need for parenteral
Infection & sepsis
nutrition by delaying oral feeding. Signs include abdominal dis-
Myocardial ischemia
tention, diffuse abdominal pain, nausea and vomiting, absence
54 . H O S P I TA L M E D I C I N E 747
even higher rates associated with vascular and orthopedic sur- 1. Upper airway obstruction, manifested as stridor, is a
gery (around 60%). medical emergency. Causes include laryngeal edema, vocal
Initial management is nonpharmacologic and involves cord injury, and obstruction by the tongue.
identifying and eliminating the likely cause along with provid-
2. Atelectasis is best managed with incentive spirometry,
ing supportive measures such as frequent orientation, a quiet
which is relevant to both prevention and treatment. It is
environment (especially at night), and adequate hydration.
dependent on user compliance, though.
Restraints and binders should be avoided if possible.
Antipsychotic drugs (eg, haloperidol, olanzapine, quetia- 3. Bronchospasm can be caused by aspiration, drug reactions,
pine) may be used, but caution should be taken with patients or activation of an underlying pulmonary disease.
who have long QT intervals and a risk of torsades de pointes. Treatment is similar to nonpostoperative management.
Benzodiazepines exacerbate delirium in the elderly and should
not be used. 4. Pleural effusions, common in patients who have had
abdominal surgery, usually resolve spontaneously. An
effusion in combination with fever or leukocytosis,
S T R E S S G A S T RO I N T E S T I NA L T R AC T U L C E R S especially after abdominal surgery, raises the possibility of
a subphrenic abscess.
Routine stress gastrointestinal tract ulcer prophylaxis is not
indicated. Certain conditions in critically ill patients carry a 5. Chemical pneumonitis results from aspiration of gastric
higher risk of upper gastrointestinal tract ulcers. These include contents (exacerbated by diminished upper airway
thrombocytopenia, respiratory failure, liver failure, multisys- reflexes perioperatively in combination with anesthetic
tem organ failure, and a previous history of ulcer and recent medications) and is usually manifested as infiltrates on
corticosteroid use. Proton pump inhibitor use should be dis- chest imaging.
continued at hospital discharge if the need for prophylaxis no
longer exists. 6. Postoperative pneumonia, which is nosocomial by
definition and should be treated as an HCAP, is caused
by either S pneumoniae or Haemophilus influenzae in 20%
O L I GU R I A to 30% of the patients. The risk of S aureus, which may be
Postoperative acute kidney injury with acute oliguria (urine MRSA, is increased in neurosurgical patients, in patients
output <400 mL daily) is a common surgical complication who have chronic renal failure or diabetes mellitus, and in
that may be caused by several factors (Box 54.6). intravenous drug abusers. Pseudomonas is more common
in late infections after prolonged intubation. Other
organisms to consider are Acinetobacter and anaerobes.
P U L MO NA RY C O M P L I C AT I O N S
7. Pulmonary edema can result from excessive fluid
Pulmonary complications of surgery are as common as cardiac administration in the perioperative setting.
complications and as important clinically for mortality, mor-
bidity, and length of hospital stay. Pulmonary complications
include the following:
P O S TO P E R AT I V E F EV E R
Most fever in the first days after surgery is related to inflam-
Box 54.6 FACTORS CAUSING ACUTE OLIGURIA mation. If the fever is persistent, a search is indicated for
POSTOPERATIVELY surgical site infections or other common hospital-related
infections such as urinary tract infection, aspiration pneu-
Prerenal causes monia, ventilator-related pneumonia, or line infection.
Decreased cardiac preload from blood loss, extravasation of Noninfectious causes include drug fever and, less commonly,
fluid, & inadequate hydration deep vein thrombosis, malignant hyperthermia, gout, transfu-
Cardiac events (eg, myocardial infarction) that may cause hypo- sion reactions, thyroid storm, and atelectasis. The type of fever
tension & decrease perfusion pressure and the timing may aid in the diagnosis. Neurosurgical proce-
Vasodilation due to sepsis, drugs, or anaphylaxis dures may cause meningitis. Abdominal surgery may result in
Arterial obstruction with thrombosis or embolism secondary to deep abdominal abscess formation, and fever after transplant
the procedure should lead to a search for unusual causes in a newly immuno-
Acute tubular necrosis due to perioperative ischemia suppressed patient.
Intravenous radiologic contrast-induced nephropathy
Transfusion-related myoglobinuria Persistent postoperative fever may be from surgical
Rhabdomyolysis site infection, urinary tract infection, aspiration or
Postrenal causes ventilator-related pneumonia, or line infection.
Opioid-related urinary retention
Noninfectious causes of fever include drug fever and, less
Ureteral obstruction
commonly, deep vein thrombosis, malignant hyperthermia,
Urethral obstruction or blocked urinary catheter
gout, transfusion reactions, thyroid storm, and atelectasis.
54 . H O S P I TA L M E D I C I N E 749
Box 54.8 METHODS FOR IMPROVING are required to report, identify, and respond to these events.
PHYSICIAN-RELATED ELEMENTS OF HOSPITAL CARE Not all sentinel events are caused by medical error, and not all
errors are sentinel events. Errors of commission are the result
Educationboard recertification, guideline dissemination of an action taken (committed), such as a patient being given
Feedbackbenchmarks & peer comparison the wrong drug, a drug by the wrong route, or a drug with the
Regulationrequired length of stay for childbirth wrong timing; surgical procedures performed on the wrong
Financialpay for performance patient or at the wrong site; and blood crossmatch errors.
Provider-led initiativecontinuous quality improvement Errors of omission result from an action not taken (omitted),
Informaticscomputer-generated support such as a delay in an indicated procedure, a missed or delayed
medication dose, a suicide due to a lapse in a procedure, or a
lack of provision of an interpreter.
PAT I E N T S AT I S FAC T I O N
Patient satisfaction is a vital measure of the quality of health A sentinel event is any unanticipated event in a health care
care and correlates with a physicians communication skills. setting resulting in death or serious physical or mental
Patients satisfaction with their care may have both financial injury and not related to the natural course of the patients
and legal implications. disease.
Inpatient physicians should be aware of the patient satis-
Common sentinel events include suicide, wrong-site
faction indexes that increasingly are being assessed by over-
surgery, medication errors, and delay in treatment.
sight organizations. These indexes cover patients perceptions
of the frequency with which physicians and nurses treat them Errors can be of commission (eg, wrong site surgery) or
with courtesy and respect, listen carefully, respond promptly omission (eg, delay in treatment).
to a call light (particularly for assistance with bed pans and
other toileting needs), explain things clearly (including infor- A common method for identifying the source of an error
mation about side effects and indications before administra- is root cause analysis (RCA), a collection of problem-solving
tion of medications), clarify details of postdismissal follow-up, methods designed to isolate the root causes of untoward events.
and provide adequate pain control. The focus is on systems and procedures as opposed to individ-
During end-of-life care, communication is especially ual error. The goal is to learn from errors and avoid repeating
important. Frequent updates, culturally competent educa- them. RCA is an important tool of CQI. Multidisciplinary
tion, and empathy are essential to patients and families as they teams review the causes and suggest ways to prevent events.
deal with impending death. The most important elements of With the use of a plan-do-study-act (PDSA) cycle, the effect
end-of-life care from a patient satisfaction viewpoint include of these changes can be monitored and modified.
control of pain, dyspnea, secretions, toileting, and anxiety.
RCA is a common approach to identifying the source of
PAT I E N T S A FET Y
error.
Patient safety refers to freedom from accidental or preventable A PDSA cycle is a method for responding to a sentinel
injury. A report in 1999 from the Institute of Medicine high- event.
lighted the issue of patient safety in the hospital. Awareness
of this issue has been raised by the often-quoted estimate of Several major national safety initiatives target certain
44,000 to 98,000 deaths annually related to medical errors in harmful events and call for increased efforts to eliminate them
US hospitals. Among hospitalized patients, 1% to 5% sustain (Box 54.9). Never events are particular medical errors that
a major injury related to their medical care. should never occur. Hospital payment and reporting have
Errors in the hospital may result from failure to complete been linked to these events. Those most applicable to intern-
a planned action or, alternatively, from the wrong approach to ists are listed in Box 54.10.
achieve an aim. Adverse events are untoward incidents, thera-
peutic misadventures, iatrogenic injuries, or other adverse
M E D I C AT I O N S A F ET Y
occurrences that result directly from care or services pro-
vided and not from the underlying disease or condition of the Initiation of medication therapy and withdrawal can lead to
patient. A near miss (or close call) is an event or situation that drug errors, drug-drug and drug-disease interactions, and side
could have resulted in an accident, injury, or illness but did not effects. Adverse drug events (ADEs) are common, expensive,
happen because of chance or a timely intervention. dangerous, and frequently preventable. They affect an esti-
A sentinel event, as defined by The Joint Commission, is any mated 5% to 7% of hospitalized patients. Medication-related
unanticipated event in a health care setting resulting in death errors for hospitalized patients cost roughly $2 billion annu-
or serious physical or mental injury and not related to the ally. As many as 40% of serious ADEs are preventable. About
natural course of the patients disease. The term sentinel event one-half of all medication errors occur during ordering, and
is not synonymous with error. The goal is to focus attention one-third during administration.
on potentially deleterious factors that lead to the event and Errors may involve the incorrect choice of medication for a
induce change in systems, procedures, and culture. Hospitals condition: either the drug is prescribed inappropriately or the
54 . H O S P I TA L M E D I C I N E 751
Table 54.4 ELECTROLYTE IMBALANCES RESULTING FROM DRUG-INDUCED PATHOPHYSIOLOGIC CHANGES
Abbreviations: ACE, angiotensin-converting enzyme; ADH, antidiuretic hormone; CMV, cytomegalovirus; HIV, human immunodeficiency virus; HSV, herpes simplex
virus; NSAID, nonsteroidal anti-inflammatory drug; PTH, parathyroid hormone; SIADH, syndrome of inappropriate secretion of antidiuretic hormone; SSRI, selective
serotonin reuptake inhibitor.
The syringe is the most frequent cause of NSIs. Hepatitis B exposure from NSI or mucous membrane
contact involving a patient with known or suspected
Nurses have the highest rate among HCWs (approximately
HBsAg-positive status requires evaluation for postexposure
35%), and residents and fellows have almost the same rate
prophylaxis.
as attending physicians (10%).
For an unvaccinated HCW, treatment with HBIG and
Before the use of hepatitis B virus (HBV) vaccine, the rate HBV vaccine is indicated.
of HBV infection was more than 10,000 per year. The rate of
An HCW who is a nonresponder (ie, received treatment
infection in unvaccinated HCWs is 10% to 30%. Postexposure
but did not mount an antibody response) should receive
prophylaxis is required after HBV exposure from NSI or
HBIG or HBIG and another vaccination.
mucous membrane contact involving a patient with known
or suspected positive status for hepatitis B surface antigen
(HBsAg). For an unvaccinated HCW, treatment with hepati- Hepatitis C virus (HCV) seroconversion after an NSI
tis B immune globulin (HBIG) and HBV vaccine is indicated. from an infected person is approximately 0% to 5%. No cases
An HCW who is a known responder to vaccine does not need have been reported from blood exposure to intact skin, but
treatment. An HCW who is a nonresponder (ie, received treat- cases have been reported from conjunctival exposure. Routine
ment but did not mount an antibody response) should receive testing recommended after exposure includes the following:
HBIG or HBIG and another vaccination. For the HCW who
has been vaccinated but has an unknown antibody response, 1. Baseline testing for anti-HCV, HCV RNA, and alanine
test the status immediately and proceed accordingly. aminotransferase
EFFECT ON METABOLISM
CYTOCHROME P450
ISOZYME DRUG Increased Decreased
Abbreviations: ARB, angiotensin receptor blocker; HIV, human immunodeficiency virus; NSAID, nonsteroidal anti-inflammatory drug.
54 . H O S P I TA L M E D I C I N E 753
2. Follow-up testing for HCV RNA at 4 to 6 weeks after into account possible barriers to learning such as health illiter-
exposure acy and dementia. Key elements of this education may include
indications for medications, the natural course of a disease,
3. Follow-up testing for anti-HCV, HCV RNA, and ALT at
and the signs of disease progression. For example, the patient
4 to 6 months after exposure
with congestive heart failure who recognizes the early warning
signs of exacerbation can seek care before reaching extremis.
Treatment with immune globulin after exposure is not An accurate and clear discharge summary can be useful for the
recommended; however, effective treatment is available for patient and for outpatient health care providers. Written or
HCWs who have an acute HCV infection (pegylated inter- oral interprofessional communication of key details may also
feron with an antiviral such as ribavirin). be helpful; these include the patients condition at discharge,
recent or expected changes, and plans for follow-up. Provision
HCV seroconversion after an NSI from an infected person of discharge instructions is a Joint Commission core perfor-
is approximately 0%-5%. mance measure.
Human immunodeficiency virus transmission is even less As part of any handoff, accurate information should be
likely with exposure (0.3%); however, postexposure prophy- provided about a patients care, treatment and services,
laxis with a combination regimen of antiretroviral therapy is present condition, and any recent or expected changes.
indicated.
Provision of discharge instructions is a Joint Commission
core performance measure.
D I S C H A R G E F R O M T H E H O S P I TA L
From the hospital, all patients should return to a safe envi-
Each year, 35 million patients are discharged from US hos- ronment. Patients who have had long hospitalizations almost
pitals. The majority of these patients are older than 75 years; invariably are debilitated and may require short-term rehabil-
of those older than 85, one-third transition from hospitals itation. A predischarge evaluation should include assessment
to long-term care facilities. A premature dismissal may lead for risk of falling, particularly for older patients. Before dis-
to ADEs or to other safety issues, decreased satisfaction, and charge, arrangements should be made for home health care,
an increased risk of readmission. For approximately 20% of home infusion therapy, or physical therapy when indicated.
patients, adverse events occur after dismissal from the hospital; Other predischarge considerations include the patients
at least one-third of these events are preventable, and another functional status (ADL), cognitive status, caregiver capacity,
third can be made less severe by timely intervention. Of these, knowledge deficits, and environmental factors. Preserving
ADEs are the most common. independence and continuing to live at home safely are
Discharge from the hospital is a critical period of transition. important goals.
As the health care setting changes from the hospital to a home, Some disease-specific guidelines recommend initiating
assisted living center, nursing home, hospice facility, or reha- certain interventions before discharge (eg, medications for
bilitation center, care providers change, as may the patients myocardial infarction, counseling for tobacco dependence).
diet, level of activity, and routes of medication administration. Such changes in management may require close follow-up
This culmination of the hospital stay has the potential to affect after discharge.
patient satisfaction, safety, medical outcome, and cost of care. Many medications carry a high risk of adverse events
Patients at highest risk are the elderly and those with multiple after hospital discharge (Box 54.11). Appropriate warfarin
medical conditions. dosing, for example, depends on drug interactions, diet, and
The discharge process should begin at admission. In an era a patients sensitivities. Corticosteroid use is accompanied
of increasing costs and pressures to limit the use of resources, by short-term risks (eg, hypertension, delirium, hypergly-
a successful hospital discharge must be planned in detail. cemia) and long-term effects (eg, osteoporosis, immuno-
Prolonged or unnecessary hospitalization may increase the suppression). Medication reconciliation before discharge is
risk of hospital-associated adverse outcomes such as infections, essential.
falls, debility, loss of independence, and overall dissatisfaction.
Discharge from the hospital is a critical transition in care. Box 54.11 HIGH-RISK DRUGS AT HOSPITAL
DISCHARGE
The discharge process should begin at admission.
Elderly patients and those with complex medical issues are Antiarrhythmics
at highest risk. Antihypertensives
Corticosteroids
After discharge, 20% of patients have adverse events; many
Diuretics
of these are preventable.
Narcotics
Oral hypoglycemic agents & insulin
A safe discharge from the hospital depends on excellent
Warfarin
communication. Patient and family education should take
54 . H O S P I TA L M E D I C I N E 755
55.
GENERAL INTERNAL MEDICINE AND QUALIT Y
IMPROVEMENT
Christopher M. Wittich, MD, and Thomas J. Beckman, MD
756
acute bacterial rhinosinusitis if the patient is afebrile and has pharyngitis and to treat them to prevent rheumatic fever.
only mild pain. If antibiotics are chosen, the first-line agent With the Centor clinical prediction criteria for the diagnosis
is amoxicillin. If there is no response within 10 days, therapy of GABHS, 1 point is assigned for each of the following:
with an alternative antibiotic should be initiated.
Patients who have chronic rhinosinusitis have had symp- 1. Fever
toms for more than 12 weeks. In these patients, sinus imaging
with computed tomography may be indicated. Allergy testing 2. Anterior cervical lymphadenopathy
and immune function testing may also be appropriate. 3. Tonsillar exudates
55. G E N E R A L I N T E R N A L M E D I C I N E A N D Q UA L I T Y I M P R O VE M E N T 757
may be present. Viral conjunctivitis is usually caused by an Scleritis
adenovirus and is highly contagious. It is a self-limited condi-
tion, and no antimicrobials are warranted. Scleritis manifests as an intense, deep pain in the eye caused
Patients with bacterial conjunctivitis usually present with by scleral inflammation. The pain worsens with movement
acute unilateral redness, irritation, and discharge. The infec- of the eye and may be referred to the ipsilateral temple. On
tion warrants topical antibacterial therapy. Failure to resolve examination, the scleral vessels are dilated and the eye appears
within 7 to 10 days should prompt consultation with an red. Many patients with scleritis have an associated systemic
ophthalmologist. Chlamydial and gonorrheal conjunctivitis disorder, such as polyarteritis nodosa, systemic lupus erythe-
should be suspected in high-risk patients. matosus, Wegener granulomatosis, seronegative spondyloar-
thropathies (eg, ankylosing spondylitis), and rheumatoid
arthritis. Successful therapy requires treatment with topical
Blepharitis corticosteroids, cycloplegics, and systemic therapy for any
underlying disease.
A hordeolum, or stye, is an infectious, painful, erythematous,
localized nodule of the eyelid. An external hordeolum is caused
by a blockage and subsequent infection of the glands of the Iritis
eyelid. An internal hordeolum is caused by infection of the
meibomian glands. Staphylococcus aureus is responsible for Iritis, also called acute anterior uveitis, is inflammation of
the majority of these infections. Although most of the lesions the iris and ciliary body. Patients typically present with ery-
drain spontaneously, some require incision and drainage by thema, photophobia, pain, and blurred vision. Disorders
an ophthalmologist. Application of warm compresses may associated with iritis include autoimmune diseases. Patients
assist in spontaneous drainage. Antibiotics are not generally with HLA-B27 are at an increased risk of iritis. The diagnosis
required unless the infection has spread beyond the nodule. requires a slit-lamp examination, and immediate referral to an
A chalazion is a more chronic, rarely painful, and always ophthalmologist is necessary.
internal noninfectious eyelid disorder. It is caused by granu-
lomatous inflammation in the meibomian glands. It may be Angle-closure Glaucoma
removed if bothersome or large.
The development of acute angle-closure glaucoma is a medi-
cal emergency. Patients with angle-closure glaucoma present
Episcleritis with abrupt ocular pain, headache, visual blurring, and often
Patients with episcleritis (Figure 55.1) present with sectorial nausea. Frequently, there is diffuse redness of the eye, and the
injection of the episcleral vessels. Most cases are idiopathic, cornea is hazy. It is more common in the elderly. Patients with
but sometimes there is an associated disease. Typically, the dis- angle-closure glaucoma should be immediately referred to an
eases are the same disorders that are associated with scleritis. ophthalmologist.
The condition is usually self-limited and an oral nonsteroidal
anti-inflammatory medication is usually sufficient to relieve Although the majority of causes of red eye are benign, the
symptoms. clinician should be able to recognize the syndromes on
examination to determine when an emergent referral to an
ophthalmologist is indicated.
G L AU C O M A
Glaucoma is a form of optic neuropathy caused by elevated
intraocular pressure. Risk factors for open-angle glaucoma
include age, being African American, and having diabetes
mellitus. The majority of patients with glaucoma are treated
with ocular hypotensive drops. Patients who cannot toler-
ate topical medications or those who progress despite treat-
ment are candidates for surgical therapies, such as laser
trabeculectomy.
AG E -R E L AT E D M ACU L A R D EG E N E R AT I O N
Age-related macular degeneration (ARMD) is a common
cause of visual impairment in older adults. Women and ciga-
Figure 55.1 Episcleritis. (Adapted from McDonald FS. Mayo Clinic rette smokers are at higher risk for ARMD. There are 2 forms
images in internal medicine: self-assessment for board exam review.
Rochester [MN]: Mayo Clinic Scientific Press and Boca Raton [FL]: of the disease: dry ARMD is characterized by soft drusen and
CRC Press; c2004. p. 123. Used with permission of Mayo Foundation for pigmentary changes, whereas wet ARMD is characterized by
Medical Education and Research.) exudative and choroidal neovascular changes. Patients with
55. G E N E R A L I N T E R N A L M E D I C I N E A N D Q UA L I T Y I M P R O VE M E N T 759
Patient Factors Clinic/System Factors
Lack of time
No interest/motivation
No educational materials/counselors
Comorbidities
Too much paperwork (no check Figure 55.2 Cause-and-Effect (Fish
Lack of resources box; cumbersome referral forms)
High cost of good food Bone) Diagram. (Adapted from Fluker
Promoting Diet SA, Whalen U, Schneider J, Cantey
P, Bussey-Jones J, Brady D, et al.
Lack knowledge or skill Incorporating performance improvement
Have other priorities for the visit
Do not eat right: feel hypocritical methods into a needs assessment:
Easier to use medications experience with a nutrition and exercise
Apathy curriculum. J Gen Intern Med. 2010
Sep;25[Suppl 4]:S62733. Used with
Doctor Factors permission.)
and equipment, and defects. In health care, the most common Pareto Chart
type of waste is patient waiting time. The goal of LEAN is to
eliminate waste and make the system lean. Pareto charts (Figure 55.5) are used to graphically display
Six Sigma (invented by Motorola Inc) is a quality improve- sources of a problem in order of frequency. The objective is to
ment methodology designed to remove defects and variation identify and fix the most common causes of the problem. The
from a system. The name Six Sigma refers to 6 standard devia- 8020 rule states that 80% of the problem is attributable to
tions from the mean, which represents 3.4 defects per 1 mil- 20% of the root causes.
lion opportunities. Six Sigma uses a stepwise approach called
DMAIC (Define, Measure, Analyze, Improve, and Control). Quality improvement tools include cause-and-effect
diagrams, control charts, value stream maps, and Pareto
LEAN is a quality improvement methodology designed to charts.
eliminate waste.
PAT I E N T S A F ET Y
Six Sigma is a quality improvement methodology that
seeks to decrease defects and variation. Medical errors occur. Patient safety principles state that the
system should be examined to determine ways to prevent
future errors. In medicine in general, procedures are a com-
mon source of error. In internal medicine, medication errors,
Q UA L I T Y I M P RO VE M E N T TO O L S
infections, and falls are a frequent threat to patient safety.
Root Cause Analysis Computerized physician order entry systems have helped
to decrease medication errors. Medications that commonly
Root cause analysis is a process to identify the nature of a
interact with other medications include warfarin, cimeti-
problem or error. A cause-and-effect diagram (Figure 55.2)
dine, antibiotics, phenytoin, HMG-CoA reductase inhibi-
is a quality improvement tool that organizes root causes of a
tors, lithium, and antifungals. Medications with common
problem. These diagrams are also known as fish bone diagrams
adverse events include those that can prolong the QT
because of their visual appearance. The backbone of the dia-
gram is the problem being studied. Root causes are grouped
together and displayed as the ribs.
Performance of the variable over time
Average
Control Chart Upper control limit
A control chart (Figure 55.3) plots variation in a process over
time. The chart includes a line representing the mean in the
Variable
DB shows
when labs &
DB tells other reqs
RN patient are complete
has arrived DB notifies MD Labs collected
of patients are shown
arrival on DB
C/T = 4 min C/T = 3 min C/T = 5 min C/T = 8 min C/T = 4 min C/T = 10 min C/T = 12 min
Waste = 2 min Waste = 4 min Waste = 28 min Waste = 15 min Waste = 10 min Waste = 20 min Waste = 40 min
2 min 4 min 28 min 15 min 10 min 20 min 40 min Lead time = 165 min
4 min 3 min 5 min 8 min 4 min 10 min 12 min Value-added time = 46 min
Figure 55.4 Value Stream Map. C/T indicates cycle time; DB, dashboard; info, information; lab, laboratory test result; MD, physician; reqs,
requisitions; RN, registered nurse. (Adapted from Dickson EW, Singh S, Cheung DS, Wyatt CC, Nugent AS. Application of lean manufacturing
techniques in the Emergency Department. J Emerg Med. 2009 Aug;37[2]:17782. Epub 2008 Aug 23. Used with permission.)
interval (eg, amiodarone, methadone, quinolones), war- Infections, including central lineassociated bloodstream
farin, heparin, insulin, antibiotics, and narcotics and those infections and catheter-associated urinary tract infections
with a low therapeutic index (eg, digoxin, lithium). When have been a major focus of quality improvement in hospitals.
any of these medications are prescribed, special care should Hand washing initiatives and standardized orders have been
be taken to prevent errors. instituted at many hospitals to prevent these infections.
100 100
90 90
80 80
Frequency of Barrier Documentation
70 70
Cumulative Percentage
60 60
50 50
40 40
30 30
20 20
10 10
0 0
Patient Patient Lack Patient lack Poor Lack of Poor Physician Other visit
comorbidities apathy of time of resources physician educational physician apathy priorities
knowledge materials diet
Barriers to Nutrition Counseling
Figure 55.5 Pareto Chart. (Adapted from Fluker SA, Whalen U, Schneider J, Cantey P, Bussey-Jones J, Brady D, et al. Incorporating performance
improvement methods into a needs assessment: experience with a nutrition and exercise curriculum. J Gen Intern Med. 2010 Sep;25[Suppl
4]:S62733. Used with permission.)
55. G E N E R A L I N T E R N A L M E D I C I N E A N D Q UA L I T Y I M P R O VE M E N T 761
Falls are another focus of patient safety endeavors. To computerized systems, medication reconciliation, and patient
improve patient care, patients at risk of falling have been iden- education.
tified and prevention strategies have been instituted. Medical errors should be examined from a systems
Human factors include how people interact with their perspective.
environment. Eliminating human factor errors through engi-
neering is an approach to improve patient safety. Techniques Medication errors, infections, and falls are common
to eliminate human factor errors include memory aids, sources of patient safety issues.
checklists, standardization, mistake proofing, redundancy, Human factors should be considered to improve patient safety.
G OA L S d. Rules to remember:
Describe the diagnostic test characteristics of sensitivity 1) SN outif a test has 100% sensitivity, a negative
and specificity. test rules out the disorder
Demonstrate the influence of disease prevalence on 2) Screening tests are used to maximize sensitivity
positive and negative predictive values. and avoid missing a person who has the disease
Illustrate how clinicians may use likelihood ratios to 3) Characteristic of testnot affected by the
analyze the results of a diagnostic test. prevalence of disease in the population
763
Table 56.1 FOUR OUTCOMES OF A DIAGNOSTIC TEST NPV is the proportion of patients who do not have
the disease of interest among all the patients who test
OUTCOME DISEASE STATUS TEST RESULT
negative for the disease.
True positive Present Abnormal NPV is affected by the prevalence of disease in the
False positive Absent Abnormal population.
False negative Present Normal
TN
The 22 table definition: NPV =
FN + TN
True negative Absent Normal = d/(c + d).
5. Prevalence
are of primary interest. Among all patients with a positive
diagnostic test result (TP+FP), in what proportion, Prevalence is defined as the proportion of persons with the
disease in the population to whom the test has been applied.
TP
, has the diagnosis been predicted correctly or In terms of the 22 table, prevalence is written as follows:
TP + FP
ruled in? This proportion is the positive predictive value TP + FN a +c
= .
(PPV). TP + FP + FN + TN a +b+c+d
PPV is the proportion of patients who have the disease
among all the patients who test positive for the disease. H OW TO C ONST RUCT A 2 2 TA B L E
PPV provides information most useful in clinical The sensitivity, specificity, and predictive values of normal and
practice. abnormal test results can be calculated with even a limited
amount of information. For example, assume that a new diag-
PPV is affected by the prevalence of the disease in the
nostic test is positive in 90% of patients who have the disease
population.
and is negative in 95% of patients who are disease-free. The
TP prevalence of the disease in the population to which the test is
The 22 table definition: PPV = = a/(a + b).
TP + FP applied is 10%. This provides the following information:
Positive 90 45 135
Diagnostic a b a+b
Test Result c d c+d
Negative
10 855 865
Clinicians should be able to perform these simple cal- The formula for a likelihood ratio for a positive test result
culations. Clinical decision making by internists is more (LR+) is
likely to depend on the PPV and NPV of test results for Positive Test in Disease Sensitivity .
a given population than on the sensitivity or specificity of LR+ = =
the test. Positive Test in No Disease 1 Specificity
For example, if the prevalence of the disease in the clini- The formula for a likelihood ratio for a negative test result
cians population is 2% instead of 10%, the PPV and NPV can (LR) is
be recalculated. The PPV of abnormal test results decreases to Negative Test in Disease 1 Sensitivity
26.9%, which is quite different from 66.7% (based on a preva- LR = = .
Negative Test in No Disease Specificity
lence of 10%), although the tests sensitivity (90%) and speci-
ficity (95%) have not changed (Table 56.4). For example, if test A has a sensitivity of 95% and a specificity
of 90%,
An important factor in interpreting a patients test result Sensitivity
is knowledge of the prevalence of the disease in the 95
LR+ = = = 9.5 and
population being tested. 1 Specificity 10
High-risk populations (high prevalence of disease) tend to 1 Sensitivity 5
improve the PPV of an abnormal test result. LR = = = 0.06.
Specificity 90
Low-risk populations (screening tests) make the NPV of a However, if test B has a sensitivity of 20% and a specificity of
normal test result look impressive. 80%, then
Sensitivity 20
LR+ = = = 1 and
US E O F O D D S A N D L I K E L I H O O D R AT I O S 1 Specificity 20
Some physicians prefer interpreting diagnostic test results 1 Sensitivity 80
by using the likelihood ratio. This ratio takes properties of a LR = = = 1.
Specificity 80
diagnostic test (sensitivity and specificity) and makes them
more helpful in clinical decision making. It helps the clinician As a general rule, diagnostic tests with an LR+ greater than 10
determine the probability of disease in a specific patient after a or an LR less than 0.1 have a greater influence on the posttest
diagnostic test has been performed. probability of disease (ie, they are better tests) than diagnostic
5 6. G E N E R A L I N T E R N A L M E D I C I N E : C L I N I C A L E P I D E M I O L O GY 765
Table 56.4 2 2 TABLE FOR TEST WITH 90% SENSITIVITY, 95%
SPECIFICITY, AND 2% PREVALENCE
Positive 18 49 67
Diagnostic a b a+b
Test Result
c d c+d
Negative
2 931 933
a+c b+d
a+b+c+d
20 980 1,000
tests with likelihood ratios between 10 and 0.1. In the 2 exam- responses are positive for all 4 questions. The LR+ for 3 or
ples above, test A is more likely to rule in or rule out disease more CAGE questions is 250.
than test B. At this point, you have 2 choices. The first is to use a nomo-
Sample likelihood ratios are provided in the example below gram (Figure 56.1) and, with a straightedge, connect the pre-
and in Table 56.5. test probability of 20% and the LR+ of 250 to the posttest
probability. This shows that the posttest probability for a diag-
nosis of alcoholism is 99%.
Example The second option should be used when there is no nomo-
gram for performing this simple calculation. Without a nomo-
A 40-year-old man is admitted to the hospital for pneumo- gram, the following steps must be done:
nia. He says that he consumes 2 six-packs of beer each week.
On the basis of this history and your clinical judgment, you 1. Convert the pretest probability to pretest odds.
assume that he has a pretest probability of 20% for a diag-
nosis of alcoholism. You ask him questions from the CAGE 2. Multiply the pretest odds by the likelihood ratio to obtain
(cut down, annoyed, guilty, eye opener) questionnaire, and his the posttest odds.
Table 56.5 EXAMPLES OF SYMPTOMS, SIGNS, AND TESTS AND THE CORRESPONDING LIKELIHOOD RATIO (LR)
Alcohol abuse or Patients admitted to orthope- US teaching Yes to 3 questions on CAGE 250
dependency dic or medical services over hospital questionnaire
a 6-mo period
Sinusitis (by further Patients with nasal complaints US teaching Maxillary toothache, purulent nasal 4 6.4
investigation) hospital secretion, poor response to nasal 3 2.6
decongestants, abnormal 2 1.1
transillumination, or history of 1 0.5
colored nasal discharge 0 0.1
Ascites Male veteran patients US veterans Presence of fluid wave (done by 9.6
hospital internal medicine residents)
Abbreviation: CAGE, cut down, annoyed, guilty, eye opener (screening questionnaire for potential alcoholism).
Data from Bush B, Shaw S, Cleary P, Delbanco TL, Aronson MD. Screening for alcohol abuse using the CAGE questionnaire. Am J Med. 1987 Feb;82(2):2315; Williams
JW Jr, Simel DL. Does this patient have sinusitis? Diagnosing acute sinusitis by history and physical examination. JAMA. 1993 Sep 8;270(10):12426; Williams JW Jr,
Simel DL, Roberts L, Samsa GP. Clinical evaluation for sinusitis: making the diagnosis by history and physical examination. Ann Intern Med. 1992 Nov 1;117(9):70510;
Williams JW Jr, Simel DL. The rational clinical examination: does this patient have ascites? How to divine fluid in the abdomen. JAMA. 1992 May 20;267(19):26458;
and Simel DL, Halvorsen RA Jr, Feussner JR. Quantitating bedside diagnosis: clinical evaluation of ascites. J Gen Intern Med. 1988 SepOct;3(5):4238.
95 0.5
0.001 R E L AT I VE R I S K R E D U C T I O N
5 6. G E N E R A L I N T E R N A L M E D I C I N E : C L I N I C A L E P I D E M I O L O GY 767
CER EER 33 patients; that is, 33 patients would need to be treated
RRR = .
CER with warfarin (INR, 2.03.0) for 1 year to prevent 1 addi-
Often RRR is not clinically useful because it does not tional stroke.
provide information about the baseline risk rate.
NNT identifies the number of patients who need to be
treated with a therapy to prevent 1 additional bad outcome.
1
A B S O LU T E R I S K R E D U C T I O N
NNT = .
ARR
In the example above, it would be useful for the physician
and patient to know the absolute difference in rates of stroke N U M B E R N E E D E D TO H A R M
between the control group and the atrial fibrillation group Conversely, if the rate of adverse events caused by the experi-
given anticoagulants (CEREER). This measure is called mental therapy is known and compared with the rate of adverse
the absolute risk reduction (ARR). In the combined Stroke events in the placebo group, the number needed to harm
Prevention in Atrial Fibrillation (SPAF) trials, the ARR or (NNH) can be calculated. This useful number tells the physi-
(CEREER) = (5%2%) = 3% per year. cian how many treated patients it takes to produce 1 additional
harmful event. In the SPAF trials, the average risk of intracra-
ARR = (CEREER). nial hemorrhage for the group given warfarin was 0.3% per year,
ARR is clinically more useful for interpreting therapeutic compared with 0.1% per year for the placebo group. Therefore,
results. the NNH can be calculated as the reciprocal of the absolute risk
increase (ARI). The ARI is calculated by subtracting the harm
CER from the harm EER or, in this case, 0.3%0.1% = 0.2%. In
1 1
N U M B E R N E E D E D TO T R E AT this example, NNH = = = 500. Therefore, 500
0.2% 0.002
The physician and patient often want to know the number patients would need to be treated with anticoagulant for 1
of patients needed to treat (NNT) with a therapy to pre- year to cause 1 additional intracranial hemorrhage, compared
vent 1 additional bad outcome. That number can be calcu- with the control group.
1
lated as . The NNT to prevent 1 stroke by using the NNH identifies how many treated patients are needed to
ARR
adjusted dose of warfarin in patients with atrial fibrillation produce 1 additional harmful event.
1 1 1
would be = = 33. Therefore, the NNT would be NNH = .
0.03 3% Harm EER Harm CER
G OA L S ET H I C A L D I L E M M A S
Identify the 4 prima facie principles of medical ethics. An ethical dilemma is a predicament caused by conflict-
Relate the tension among the 4 principles to common ing moral principles in which there is no clear course to
ethical dilemmas in clinical medical practice. resolve a problem (ie, credible evidence exists both for and
against a certain action). Advances in medical science and
Investigate the intersection of medical ethics and the law the ever-changing social and legal milieu are responsible for
by examining major cases. dynamic changes, challenges, and ethical dilemmas in medi-
cal practice. Even when ethically challenging situations and
Examine ethical principles governing medical care at the
dilemmas are resolved, physicians may still experience distress
end of life.
due to conflicting values and personal conscience.
Medicine is first and foremost a relationshipa coming
An ethical dilemma is a predicament caused by conflicting
together of a patient, who is ill or has specific needs, and a phy-
moral principles in which there is no clear course to resolve
sician, whose goal is to help the patient. The physician-patient
a problem.
relationship is a fiduciary relationship; physicians have
knowledge, skills, and privileges that patients do not have. In Advances in medical science and the ever-changing
turn, patients trust that physicians act in their patients best social and legal milieu are responsible for dynamic
interests. changes, challenges, and ethical dilemmas in medical
Medical ethics consists of a set of principles and systematic practice.
methods that guide physicians on how they ought to act in
their relationships with patients and others and how to resolve
moral problems that arise in the care of patients. These prin- P R I N C I P L E S O F M E D I C A L ET H I C S
ciples and methods are based on moral values shared by both
the lay society (which may vary from culture to culture) and A widely used framework for medical ethics is principal-
the medical profession. ism, which delineates 4 prima facie principles that encom-
pass most clinical ethical concerns. These principles are
The physician-patient relationship is a fiduciary 1) beneficence, 2) nonmaleficence, 3) respect for patient
relationship; physicians have knowledge, skills, autonomy, and 4) justice. Beneficience refers to the duty to
and privileges that patients do not have. As a result, do good, nonmaleficence refers to the duty to prevent or do
patients trust that physicians act in their patients best no harm, respect for patient autonomy refers to the duty to
interests. respect persons and their rights of self-determination, and
justice refers to the duty to treat patients fairly (free of bias
Medical ethics consists of a set of principles and systematic
and based on medical need). No principle has ethical prior-
methods that guide physicians on how they ought to act in
ity over another. Although beneficence is a primary motivat-
their relationships with patients and others.
ing ethical principle for most physicians, the other principles
contextualize and inform our orientation to accomplish the
good (Figure 57.1). In clinical practice, these principles can
be at odds with each other. For example, a beneficent physi-
a
Portions previously published in Mueller PS, Hook CC, Fleming KC. cian may recommend an intervention with minimal risks of
Ethical issues in geriatrics: a guide for clinicians. Mayo Clin Proc. 2004
Apr;79(4):55462. Used with permission of Mayo Foundation for Medical harm. However, the patient may exert his or her autonomy
Education and Research. and decline the intervention.
769
Nonabandonment is an ethical obligation to provide
Justice
ongoing care once the patient and physician mutually
c t fo
r patient aut
on
concur to enter into an alliance.
e o
esp a le fi
m
m c e
R
o n nce
y
N
Conflict of Interest
Beneficence Physicians should refrain from activities that are not in
patients best interests. Nevertheless, physicians may have
conflicts of interest. Such conflicts may unduly influence phy-
sicians practices (eg, prescribing, ordering of tests, or thera-
peutic recommendations). For example, accepting a gift from
a representative of a pharmaceutical company constitutes a
conflict of interest if the physician accepting the gift writes
prescriptions for drugs manufactured by that company.
Figure 57.1 The 4 Principles of Medical Ethics.
Conflict of interest is contrary to the principles of
beneficence and nonmaleficence.
B E N E FI C E N C E
Beneficence is acting to benefit patients by preserving life, The Impaired Physician
restoring health, relieving suffering, and restoring or maintain-
ing function. The physician is obligated to help patients attain According to the Americal Medical Association, the impaired
their own interests and goals as determined by the patient, not physician is one who is unable to practice medicine with
the physician. This principle may be viewed on several levels reasonable skill and safety to patients because of physical or
of benefit, including how an intervention may 1) biomedically mental illness, including deteriorations through the aging pro-
or physiologically benefit a patient, 2) personally benefit the cess, or loss of motor skill, or excessive use or abuse of drugs
patient (ie, waiting for family to arrive before withdrawing a including alcohol. Impairment is distinct from competence,
ventilator), or 3) ultimately benefit the patient (ie, in respect which specifically concerns the physicians knowledge and
to a patients belief system or world view). skills to adequately perform his or her duties as a physician.
Impairment and incompetence both may compromise patient
care and safety. Physicians have a moral, professional, and legal
N O N M A L E F I C E N C E A N D P R AC T I C A L
obligation to report impaired and incompetent colleagues to
A P P L I C AT I O NS I N C L I N I C A L P R AC T I C E
the appropriate authority. Specifics of reporting vary by state,
Nonmaleficence closely couples with beneficence and but all states have a reporting requirement. Typical authorities
requires that physicians should not harm (or should pre- to contact include the institutional chief of staff or impairment
vent harm to) patients. This principle has roots in the program, local or state medical society impairment programs,
Hippocratic corpus, as to diseases, help, but at least do no or the state licensing body. It is important that reporting the
harm. This principle also addresses unprofessional behav- behavior of a colleague be based on objective evidence rather
ior, such as verbal, physical, and sexual abuse of patients or than supposition.
uninformed and undisclosed interventions or experimenta-
tion on patients. Physicians have an obligation to report impaired
colleagues.
Nonabandonment
The Rule of Double Effect (Beneficence vs
Abandonment is the act of leaving the patient (for whom the Nonmaleficence)
physician has provided health care in the past) without pro-
viding for immediate or future medical care. Abandonment In managing patients, pursuing beneficence may lead to
of patients is contrary to the fiduciary nature of the injury or death. Classic examples of such include 1) a ter-
physician-patient relationship and is a legally punishable act. minally ill patient who may require high doses of opioids
In contrast, nonabandonment denotes an ethical obligation to for adequate analgesia yet such doses risk the potential for
provide ongoing medical care once the patient and physician respiratory depression and earlier death, 2) taking patients
mutually concur to enter into an alliance. Nonabandonment is to surgery with the risk of anesthetic or surgical complica-
closely related to the principles of beneficence and nonmalefi- tions and death, or 3) giving chemotherapy for malignant
cence and is fundamental to the long-term physician-patient disease with the risk of possible treatment-related mortal-
relationship. Patient noncompliance, in terms of taking medi- ity. The rule of double effect attempts to resolve the con-
cations or following a physicians instructions, is not grounds flict. The rule of double effect states that 1) the act itself
for abandonment. Physicians should strive to respond to a must be good or morally neutral, 2) the act or agent intends
patients needs over time, but they should not trespass their only the good effect, 3) the bad effect must not be a means
own values in the process. to the good effect (eg, death is the only way to achieve the
OPTION
Life-Sustaining Treatment
Palliative Sedation and Physician-
Withhold Withdraw Analgesia Assisted Death Euthanasia
Cause of death Underlying disease Underlying disease Underlying diseasea Intervention prescribed by Intervention used
physician & used by patient by physician
Intent/goal of Avoid burdensome Remove burdensome Relieve symptoms Termination of patients life Termination of
intervention intervention intervention patients life
Legal? Yesb Yesb Yes Noc No
a
Palliative sedation & analgesia may hasten death (double effect).
b
Several states limit the power of surrogate decision makers regarding life-sustaining treatment.
c
Legal only in Oregon, Washington, & Montana.
desired outcome), and 4) the good effect must outweigh the Capacity is the physicians clinical determination of the
bad effect. By the reasoning of double effect and the benefi- patients ability to understand his or her situation and
cent goal of mitigating patient suffering, adequate analge- make appropriate decisions for treatment.
sia to relieve suffering should always be given even if death
Competence is the legal determination and status that an
is hastened. Analgesics should be dosed and administered
individual has the right to make life-affecting decisions.
with the primary intent of relieving pain and not hastening
death. If death occurs after analgesia is given in this care-
ful fashion, it is not equivalent to euthanasia, in which the In clinical practice, the lack of decisional capability should
central intent is termination of a patients life (Table 57.1). be proved, not presumed. Confusion, disorientation, psychosis,
Adequate analgesia, particularly in patients at lifes end, is and other cognitive changes caused by diseases, metabolic dis-
the responsibility of the physician. turbances, and medical interventions can affect decision-making
ability. Decisionally capable patients have the right to refuse all
medical interventions, even at the risk of death.
Analgesics should be dosed and administered to patients
with the primary intent of relieving pain and not hastening
patient death. Furthermore, if dosed and administered The lack of decisional capability should be proved, not
appropriately, opioids are rarely associated with hastening presumed.
death by respiratory depression.
Several clinical standards are used to assess decision-making
capacity: 1) the patient can make and communicate a choice;
R E S P EC T F O R PAT I E N T AU TO N O MY 2) the patient understands the medical situation and progno-
The word autonomy derives from the Greek words auto sis, the nature of the recommended care, available alternative
(self ) and nomos (rule). The principle of respect for options, and the risks, benefits, and consequences of each; 3)
patient autonomy is the concept that persons have the right the patients decisions are stable over time; 4) the decision is
to establish, pursue, and maintain their values and goals (the consistent with the patients values and goals; and 5) the deci-
right to self-determination). For patients to be fully autono- sion is not due to delusions.
mous, they must be informed (see below), have liberty (free The ethical principle of respect for patient autonomy
from coercion and duress), and have decision-making capac- and numerous court decisions, from the Quinlan (1976) and
ity. Notably, decision-making capacity is not the same as the Cruzan (1990) cases to the Schiavo (2005) case (Table 57.2),
legal term competence. Capacity is a physicians clinical deter- establish a patients right to refuse medical treatment, even if
mination of a patients ability to understand his or her situa- death inevitably follows such refusals.
tion and make appropriate decisions for treatment, whereas Liberty allows a patient the freedom and opportunity to
competence is the legal determination and status that an influence the course of ones life and medical treatments.
individual has the right to make life-affecting decisions (not
only health-related decisions but also, for example, financial The principle of respect for patient autonomy, particularly
decisions). as it affects an individuals right to refuse life-sustaining
treatments, has been affirmed by ethicists and the courts.
Respect for autonomy is the concept that persons have the
right to establish, pursue, and maintain their values and Promoting and Preserving Patient Autonomy
goals (the right to self-determination).
Physicians commonly care for patients who lack or lose
Autonomy requires decision-making capacity. decision-making capacity. To preserve their autonomy,
57. M E D I C A L ET H I C S 771
Table 57.2 PERTINENT LEGAL RULINGS
Salgo, 1957 Informed consent California Court of Appeals First used term informed consent
Brooks, 1965 Jehovahs Witness refusal of blood Illinois District Court Patients have right to personal treatment on religious grounds
Canterbury, 1972 Degree of disclosure required for adequate informed consent US District Court Established prudent patient test
Quinlan, 1976 PVSdiscontinuation of mechanical ventilation, previously New Jersey Supreme Court Discontinuation (based on right to privacy)
articulated directive
Brophy, 1986 PVSdiscontinuation of gastrostomy feedings, previously Massachusetts Supreme Court Discontinue feedings (based on autonomy)
articulated directive
Bouvia, 1986 Severely impaired, refusal of nasogastric tube feedings by a California Court of Appeals Removal of nasogastric tube (based on autonomy)
decisionally capable patient
Corbett, 1986 PVSdiscontinuation of nasogastric tube feedings, no Florida Court of Appeals Discontinue feedings (based on right to privacy)
predefined directive(s)
Cruzan, 1990 PVSstate of Missouri required clear & convincing US Supreme Court States have right to restrict exercise of right to refuse treatment by
evidence of individuals wishes before allowing surrogates; decisionally capable patients may refuse life-sustaining
withdrawal of life support therapy, including hydration, nutrition, & mechanical ventilation
Wanglie, 1991 PVSfamily wished continued Minnesota District Court Continuation (based on autonomy, substituted judgment)
support despite objections to continue life-sustaining
therapy by physicians & institution
Quill, Lee, 1997 Assisted suicide US Supreme Court States have the right to make laws prohibiting or allowing
physician-assisted suicide & euthanasia
Schiavo, 2005 PVSfamily conflict over withdrawal of feeding tube Florida District Court of Appeals, Upheld the right of surrogates to withdraw a feeding tube if acting in
Florida Supreme Court, US accord with patients wishes
Supreme Court
Gonzales, 2006 Assisted suicide US Supreme Court Upheld the Constitutional legitimacy of the Oregon assisted suicide law
57. M E D I C A L ET H I C S 773
loved one could wake up for 15 minutes, understand his or her voluntary acceptance (or refusal) of physician recommenda-
situation, and then had to return to it, what would he or she tions by decisionally capable patients, or their surrogates,
choose? (N Engl J Med. 2005 Apr 21;352[16]:16303. Epub who have been provided sufficient information regarding the
2005 Mar 22). In some circumstances the surrogate may not risks, benefits, and alternatives of the proposed interventions.
have engaged in adequate communication with the patient There are 3 required elements of informed consent: 1) patient
to be able to project how the patient would decide. In these decision-making capacity, 2) patient voluntariness, and 3)
circumstances, the surrogates and clinicians obligations are to accurate and sufficient information. The amount of informa-
try to decide in the patients best interests. tion shared with the patient should be guided not only by
Advance directives are often lacking, and jurisdictions what the physician believes is adequate (professional practice
vary regarding which individuals may serve as surrogate if one standard) but also by that which the average, prudent person
has not been appointed. Physicians should be aware, in the would need in order to make an appropriate decision (reason-
absence of an advance directive, of which individuals should able person standard). Discussion of available alternatives to
be approached about the surrogate role. Indeed, this vari- the proposed treatment, including doing nothing, should be
ability underscores the value and importance of encouraging included.
patients to formally designate a surrogate through an advance
directive. Informed consent (and refusal) requires patient
decision-making capacity and voluntariness and accurate
In the absence of explicit directives (written or oral), and sufficient information.
surrogates should use substituted judgment (what the
The amount of information shared with a patient should
choices would be if the patient were able to speak for
be guided by the reasonable person standard: what an
himself or herself ).
average prudent person would need to make an informed
If substituted judgment is not possible, the surrogate decision.
should make choices in the patients best interest.
In shared decision making, the physician should present
Patients may also delegate decision making to a surrogate, the patient with recommendations that the patient can accept
even while still possessing decisional capacity. This situation or reject. Simply laying out a menu of choices before the
arises in certain cultural contexts in which decision-making patient may lead to confusion or the perception by the patient
authority is given to a certain member of the family or to a that the physician is unconcerned with his or her welfare. If the
community leader. It is respectful of the patients autonomy to patient refuses the recommended treatment and chooses one
accept his or her delegation of decision making to another. of the alternatives, the physician should respect the patients
choice. The final plan should reflect an agreement between a
A patient may delegate decision-making authority to a well-informed patient and a well-informed, sympathetic, and
surrogate, even while still possessing decision-making unbiased physician.
capacity himself or herself.
The physician should provide all alternatives, followed by
Situations may arise in which a surrogates decisions or specific recommendations.
instructions to physicians conflict with a patients previously If the patient refuses the recommended treatment, the
expressed directive or with those of other family members. physician should respect the patients choice.
Because the physicians primary responsibility is to the patient,
the physician should determine as best as possible what the In rare exceptions, the physician can treat a patient
patient would choose for himself or herself. When the phy- without informed consent (eg, in an emotionally unstable
sician is unable to resolve the conflict, it may be helpful to patient who requires urgent treatment, when informing
involve an independent third-party arbitrator, such as an eth- the patient of the details may produce further problems).
ics consultant or committee or legal counsel. Once it has been The principle of implied consent is invoked when true
established what the patient would want, it is the obligation of informed consent is not possible because the patient (or
the treating physician(s) to comply with those wishes, even in surrogate) is unable to express a decision regarding treat-
the face of disagreement with surrogates. Only if clear evidence ment. This situation often occurs in emergencies in which
can be provided that the advance directive does not reflect physicians are compelled to provide medically necessary
what the patient really desired can the directive be overruled. therapy, without which harm would result. Implied con-
sent and duty to assist a person in urgent need of care have
The primary responsibility of the physician is to serve the been legally accepted (eg, Good Samaritan laws) and pro-
patients interest. vide the physician a legal defense against battery (although
not negligence).
Informed Consent and Exceptions Informed consent from surrogates is necessary to perform
an autopsy (except in certain instances such as coroners cases)
A derivative of the principle of respect for patient autonomy or to practice intubation, placement of intravascular lines, or
(and nonmaleficence) is informed consent (and refusal): the other procedures on the newly dead.
57. M E D I C A L ET H I C S 775
undertaken. This approach often takes the form of ongoing, The physician and medical institutions should provide
regular assessment of goals of care, exploring where fundamen- alternative means for patients to secure legally sanctioned
tal disagreements regarding care are occurring, and involving interventions if requested.
external experts (eg, palliative medicine consultants and eth-
ics consultants) when appropriate. If differences cannot be
resolved, efforts at intra-institutional or inter-institutional J US T I C E
transfer may need to be arranged. The principle of justice expresses that every patient
deserves and must be fairly provided optimal care as war-
A futile intervention is one that cannot achieve the goals of ranted by the underlying medical condition and within
intervention no matter how many times it is repeated. the constraints of available resources. The identification of
As much as possible, resolution of futility conflicts should optimal medical care should be based on the patients med-
be attempted by using a due-process approach. ical need and the perceived medical benefit to the patient.
The patients social status, ability to pay, or perceived social
worth should not dictate the quality or quantity of medi-
Conscientious Objection cal care. The physicians clear-cut responsibility is to the
patients well-being (beneficence). Physicians should not
Another conflict between patient and physician (and other make decisions about individual patient care based on larger
health care providers) occurs when the patient requests an societal needs, because the bedside is not the place for gen-
intervention that may be legally sanctioned but is morally eral policy decisions. Nevertheless, physicians should be
unacceptable to the physician. In this situation, the ethical conscious of larger societal needs and should be leaders in
issue centers on moral acceptability of the intervention and developing fair policies to regulate the allocation of scarce
not on efficacy. An objector may believe so strongly against or costly resources, but these endeavors should take place
the intervention that he or she considers the intervention as away from the bedside and an individual physician-patient
commission of evil. relationship.
Historically, dating back to the Hippocratic Oath, medical
ethics has recognized that physicians, in their obligations to Justice is allocation of medical resources fairly and
protect life, may conscientiously object to acts involving the according to medical need.
deliberate taking of human life. Many states have conscience
laws protecting health care providers from being forced to be Physicians should be conscious of larger societal needs and
complicit in acts that would violate their conscience. should be leaders in developing fair policies to regulate
What constitutes an issue of conscience? In medicine, the allocation of scarce or costly resources, but these
the issue of objection must regard a specific act. Claims of involvements must take place away from the bedside and
conscience regard acts, not persons. Claims of conscience the individual physician-patient relationship.
that intrinsically involve discrimination against a given indi-
vidual (eg, race, color, sexual preference, nationality, reli-
gion) are not legitimate and violate the principle of justice ET H I C A L C O N S I D E R AT I O N S AT T H E E N D
(see Justice below). Furthermore, the conscientious objec- OF LIFE
tor is restricted to forgoing participation only in the specific
objectionable act, not in the rest of the patients care as such.
I N C U R A B L E D I S E A S E A N D D E AT H
To do otherwise would be an act of abandonment. For exam-
ple, a physician may refuse to participate in performing an Transitioning from full therapeutic efforts against illness to
abortion (including providing anesthesia and those actions comfort care for patients inevitably approaching death can
directly and immediately involved in the act), but a physician be difficult. Nevertheless, compassionate, ongoing care for
may not decline postoperative care of a patient who might patients at the end of life is critical. The patient and family (if
experience complications of the procedure. Although the the patient so desires) should be provided ample opportunity
conscientious objector has the right to decline participation to talk with the physician and ask questions. An unhurried
in the requested intervention, he or she should not berate or openness and willing-to-listen attitude on the part of the phy-
obstruct the patient in receiving that intervention from oth- sician are critical for a positive outcome.
ers. Health care organizations may legitimately expect the The physician should assume responsibility for furnish-
physician to refer the patient to another provider, or at least ing and arranging for physical, emotional, and spiritual sup-
to institutional resources that can assist the patient in secur- port. Adequate pain control, respect for human dignity, and
ing legally sanctioned interventions, such as a patient affairs ongoing contact with the patient and family are crucial. The
office or an administrator. emotional and spiritual support available through hospital
chaplains or local clergy (as appropriate, given the patients
Health care professionals have a right of conscience and to personal beliefs) and efforts to avoid dehumanization of the
decline from participation in acts that violate deeply held patient are important. These nonpharmacologic interventions
religious and philosophical principles, but they do not have often are invaluable for alleviating patient suffering as opposed
a right to discriminate against persons. to a firm reliance on sedation.
57. M E D I C A L ET H I C S 777
College of Physicians, and other large professional medical D E F I N I T I O N O F D E AT H
groups have maintained a stance against physician-assisted
Death is the irreversible cessation of circulatory and respira-
suicide and euthanasia.
tory function or the irreversible cessation of all functions of
In 1997, the US Supreme Court ruled that states may main-
the entire brain, including the brainstem. Clinical criteria (at
tain laws prohibiting euthanasia and assisted suicide but may
times supported by electroencephalographic testing or assess-
also pass laws allowing these practices. Although the Court
ment of cerebral perfusion) permit the reliable diagnosis of
did not find a right to physician-assisted death, it emphasized
brain death.
the patients right to adequate, aggressive pain control, even if
The family should be informed of brain death but should
it might shorten the patients life. In 1997, the people of the
not be asked to decide whether further medical therapy
state of Oregon reiterated their support for physician-assisted
should be continued. One exception is when the patients
suicide by reapproving a referendum first passed in 1994 legal-
surrogate (or the patient, via an advance directive) permits
izing assisted suicide but prohibiting euthanasia. The Oregon
certain decisions, such as organ donation, in the case of brain
law requires that the patient 1) have a terminal condition, 2)
death.
be decisionally capable, 3) has initiated 2 verbal requests and
Once it is ascertained that the patient is brain dead and
1 written request for a prescription for a lethal overdose, 4)
that no further therapy can be offered, the primary physician,
undergo a second-opinion consultation, 5) receive appropri-
preferably after consultation with another physician involved
ate psychiatric intervention if perceived to be depressed, and
in the patients care, may withdraw supportive measures. This
6) undergo a 15-day waiting period after the request has been
approach is accepted throughout the United States, with the
made to allow the patient to change his or her mind. Similar
exception of the states of New Jersey and New York, which
decisions have been made in Washington and Montana. At the
have modified their definition-of-death statutes to allow a reli-
time of publication, assisted suicide is illegal in the 47 other
gious exemption for groups (such as Orthodox Jews) that do
states and euthanasia is illegal throughout the United States.
not accept brain death as a valid criterion for death. In these
Regardless of ones position on physician-assisted suicide
states, continued care may be requested of the caregivers until
and euthanasia, physicians are obligated to address the under-
circulatory and respiratory function collapses.
lying concerns that lead patients and physicians to believe that
assisted suicide and euthanasia are necessary. Physicians should
Death is defined as the irreversible cessation of circulatory
be acquainted with appropriate means of pain management
and respiratory function or the irreversible cessation of all
and palliative care and treat patients distressing symptoms.
functions of the entire brain, including the brainstem.
Euthanasia is legally prohibited in the United States.
Physician-assisted suicide is permitted only in the states of
AU T H O R S N OT E
Oregon, Washington, and Montana.
Physicians should strive to provide optimal symptom This review is meant as a guide; individual practitioners are
management and to promote dignity in dying patients in referred to their state medical societies for further information
all locations. regarding state-specific mandates and laws.
ERRNVPHGLFRVRUJ
Note: Page numbers followed by b, f, or t indicate a box, figure, table, respectively
A acute cutaneous lupus erythematosus, 666 in pregnancy, 295 agoraphobia, 601602, 627b, 728729
abdominal aortic aneurysm (AAA), 98, acute eosinophilic pneumonia, 211 for meningoencephalitis, 338 AIDS (acquired immunodeficiency
100 acute febrile neutrophilic dermatosis for varicella-zoster virus, 267 syndrome)
male vs female incidence data, 100 (sweet syndrome), 662 for viral pneumonia, 272 adenovirus in, 129
medical management, 101 acute gouty arthritis, 388389 adalimumab, 128, 251, 392, 655 associated malignancies
risk factors, 100 acute hemolytic transfusion reactions, 509 Addison disease (primary adrenocortical Kaposi sarcoma, 291, 308, 311b,
symptoms, 101 acute inflammatory demyelinating failure), 452453 312, 319
abdominal compartment syndrome, 203 polyradiculoneuropathy, 632 adenomas non-Hodgkin lymphoma, 312,
abdominal tuberculosis, 283 acute intermittent porphyria, 511t in adrenal incidentaloma, 459 319320
abnormal uterine bleeding, 707708, acute interstitial nephritis, 554555, 555b aldosterone-producing, 457 primary CNS lymphoma, 320
707b, 713, 714 acute interstitial pancreatitis, 139 in colorectal cancer, 136, 137 bacterial pathogens in
acanthosis nigricans, 446, 464, 488t, acute interstitial pneumonia, 211 fibroadenomas, in breast pain, 721 Campylobacter jejuni, 129
661, 661f acute kidney injury (AKI) hepatic adenomas, 183 Mycobacterium avium-intracellulare,
achondrogenesis type II, 383t classification, staging system, 552f, 552t pituitary adenomas, 442443, 446, 455 129
achondroplasia (autosomal dominant), defi nition, diagnosis, 551 toxic thyroid adenoma, 414 Salmonella ser Enteritidis, 129
383t diagnostic approach to, 556557 in Zollinger-Ellison syndrome, 153 Salmonella ser Typhimurium, 129
acidbase disorders. See also metabolic intrinsic renal AKI, 553556 adenosine, 1314, 27 Shigella fl exneri, 129
acidosis management of, 557558 adenosine-sensitive ventricular CMV pneumonia in, 272
acidbase determination example, 546b postrenal AKI, 556 tachycardia, 13 Cryptosporidium parvum in, 306
acidbase status determination, 546b, prerenal AKI, 552553 adenovirus effects on the heart, 60
547 Acute Kidney Injury Network (AKIN), in AIDS, 129, 130 fungal pathogens in, 129
anion gap metabolic acidosis, 548549 551 bronchiectasis and, 240 gastrointestinal manifestations
non-anion gap acidosis, 546, 547 acute lymphocytic leukemia, 536 viral arthritis and, 353, 405 bacterial pathogens, 129
renal tubular acidoses, 547t acute mesenteric ischemia, 131 viral conjunctivitis and, 758 diarrhea, diagnostic evaluation, 130
respiratory acidbase alterations, acute monarticular arthritis, 403 viral pneumonia and, 272 fungal pathogens, 129
549550 acute muscle weakness, 635636, 636b adrenal crisis, 453 protozoan pathogens, 129130
acne vulgaris, 653, 656657 acute myelogenous leukemia, 507 adrenal gland disorders viral pathogens, 128129
acquired bacterial meningitis, 276t277t, acute myeloid leukemia, 507, 535536 adrenal incidentaloma, 459 noninfectious pulmonary complications,
331, 332f, 333t acute myocardial infarction adrenocortical failure, 452454 291292
acquired bleeding disorders -blockers for, 28 Cushing syndrome, 454456 protozoan pathogens in, 130
acquired hemophilia, 518 role of pacing in, 29 pheochromocytoma, paraganglioma, pulmonary hypertension in, 291
acquired von Willebrand syndrome, 518 acute necrotizing pancreatitis, 139 457459 viral pathogens in, 128129
causes of deficiencies, 517t acute otitis externa, 757 primary aldosteronism, 456457 airway management, 191192
disseminated intravascular coagulation, acute pancreatitis adrenal incidentaloma, 459 endotracheal intubation, 193b
517518 clinical presentation, 140 adrenalitis, 266 intubation difficulties, 192b
liver disease, 516517 complications, 141142 adrenocortical failure, 452454 Mallampati classification, 192f
acquired ichthyosis, 662 diagnosis, 140141 clinical features, 452453 mask ventilation difficulties, 192b
acquired von Willebrand syndrome, 518 etiological factors, 139140 endocrine diagnosis, 453 mask ventilation, intubation, 192b
acrodermatitis enteropathica, 664 severity assessment, 142 etiologic diagnosis, 453 AKI. See acute kidney injury
acromegaly and gigantism treatment, 141 primary adrenocortical failure, 452 albendazole, for helminths, 270
clinical features, 446 acute phosphate nephropathy, 555 secondary adrenocortical failure, 452 alcohol abuse
etiology, 445446 Acute Physiology and Chronic Health therapy, 453454 bupropion contraindication in, 756
therapy, 446447 Evaluation (APACHE) criteria, adult-onset still disease, 380 chronic pulmonary disease and, 287
Actinobacillus actinomycetemcomitans, 345 142 Advisory Committee on Immunization differential diagnosis, 499
Actinomyces israelii, 254 acute respiratory distress syndrome Practices (ACIP) recommendations lung abscesses and, 281
acute adrenocortical failure, 453 (ARDS), 141, 194195 hepatitis A vaccine, 695 metformin contraindication in, 426
acute alcoholic myopathy, 635 associated conditions, 194t hepatitis B vaccine, 696 peripheral neuropathy and, 286
acute arterial occlusion, 107108 description, 194 HPV vaccine, 695 postoperative delirium and, 747b
acute aseptic meningitis, 337t hypercapnic respiratory failure and, 193 influenza vaccine, 694 during pregnancy, 710
acute chest syndrome, 502 pathophysiology, 194 meningococcal vaccine, 695 withdrawal treatment, 605, 742
acute chronic gastritis, 151 treatment, 194195 MMR vaccine, 695 alcoholic liver disease
acute confusional states, 604, 614, 617, acute/subacute inflammatory pericarditis, pneumococcal polysaccharide vaccine, alcoholic cirrhosis, 178179
622, 683 62 695 alcoholic hepatitis, 178
acute coronary syndromes acute tubular necrosis, 553554, 553f polio vaccine, 696 aldosterone antagonists
causes of, 82 acute uric acid nephropathy, 555 rabies vaccine, 696 for adrenal hyperplasia, 457
management of, 9091 acyclovir Td, Tdap vaccines, 694695 for dilated cardiomyopathy, 73
nonST-segment elevation MI, 8991 for encephalitis, 338 varicella vaccine, 695 for heart failure, 66f, 69t
ST-segment elevation MI, 9197 for esophageal infections, 149 Aeromonas hydrophila, 165, 350 for hypertension, 118
therapeutic pathways for, 92f for herpes simplex virus, 128129, 251, age-related macular degeneration aldosteronism. See primary aldosteronism
U.S. hospital admittance data, 92 265, 294 (ARMD), 758759 alemtuzumab, 250
779
allergic bronchopulmonary aspergillosis, for drug-resistant tuberculosis, 283 amyloidosis in, 56 for thoracic aortic atherosclerosis, 105
262, 595596 for febrile neutropenia, 249 in aortic stenosis, 39 for thyrotoxicosis-associated atrial
causes, 595 for HAP, VAP, HCAP, 328 intestinal angina, 131132 fibrillation, 55
chest radiograph, 596f for infective endocarditis, 345 angina, unstable, nonST-segment for venous thromboembolism, 527
diagnostic features, 596b for Legionella, 278 elevation MI, 8991 anticonvulsant therapy, for seizure
allergic contact dermatitis, 656 nephrotoxicity of, 554 biomarkers, 90 disorders
allergic eosinophilia, 58 for Yersinia enterocolitica, 164 conservative vs. invasive strategy, 9091 antiepileptic drugs, 619621, 620t
allergic transfusion reactions, 509510 amiodarone, 13, 13t, 14t, 419 management, 90 blood levels, 621
allergies amiodarone-induced ILDs, 209 pathophysiology, 8990 starting and stopping, 621
anaphylaxis, 583 amlodipine, 74, 86, 400 angiomyolipomas, 213, 665, 677t systemic side effects, 620t
chronic rhinitis, 578579, 578b amoxicillin angiotensin-converting enzyme (ACE) antidepressants. See also tricyclic
common variable immunodeficiency, for community-acquired pneumonia, inhibitors antidepressants
588 274 for acute MI, 94 for fibromyalgia, 360
drug allergies, 585587 for dental procedures, 351 for angina, 86 general principles, 606
involving IGE or immediate-type for febrile neutropenia, 490 contraindication in pregnancy, 56 for panic disorder, agoraphobia, 602
reactions, 587 for Helicobacter pylori, 153 for diabetes mellitus in heart patients, for postpartum depression, 599
not involving IGE or immediate-type for infectious mononucleosis, 265 56 antihypertensive agents. See angiotensin-
reactions, 585586 for Leptospirosis, 257 for dilated cardiomyopathy, 7273 converting enzyme (ACE)
environmental modifications, 580 liver injury from, 182 hyperkalemia from, 571 inhibitors; angiotensin II receptor
eosinophilia, 587588 for Lyme disease, 258 for hypertension, 39 blockers; -blockers
food allergies, 583584 for Salmonella in AIDS, 129 for kidney patients, 570571 antimicrobial therapy
mastocytosis, 587 for sinusitis, 581 mechanics of action of, 72f for febrile neutropenia, 249
nonallergenic rhinitis, 578 amphotericin, 129, 262 angiotensin II receptor blockers (ARBs) for HAP, VAP, HCAP, 275, 328
sinusitis, 580581, 581b, 581f amphotericin B for CKD complications, 571 for intra-abdominal abscesses, 306
stinging insects, 584585 for blastomycosis, 261 for diabetic nephropathy, 562 antineutrophil cytoplasmic autoantibody
terminal complement component for candidiasis, 264 for dilated cardiomyopathy, 73 (ANCA)-associated
deficiencies, 588 for coccidioidomycosis, 260 for focal segmental glomerulosclerosis, granulomatous vasculitis, 663
testing methods, 577578 for cryptococcal infections, 263 561 antiphospholipid antibody syndrome, 372
urticaria, 581583 for histoplasmosis, 261 for heart failure, 66f characteristics, 399
allogenic hematopoietic stem cell for leishmaniasis, 271 hyperkalemia from, 571 clinical features, 399400
transplant, 501 ampicillin, 129, 265 for hypertension, 118f treatment, 400
-glucosidase inhibitors, 426 ampicillin-mononucleosis rash, 586 for kidney patients, 570571 antiplatelet therapy. See also aspirin
-thalassemias, 498 amylin analogue, 427 for lupus nephritis, 563 therapy
Alport syndrome, 558, 564 amyloidosis, 534535 risk factors, 553, 555, 557 for chronic unstable angina
aluminum phosphate crystals, 390 characteristics of, 166167 anion gap metabolic acidosis, 548549 with coronary stents, 87t
alveolar hemorrhage syndromes, 218 effects on the heart, 5657 ankylosing spondylitis, 39, 391392 for ischemic cerebrovascular disease, 639
Alzheimer disease macroglossia and, 663 effects on the heart, 59 for peripheral artery disease, 107
dementia and, 613, 617, 682 multiple myeloma and, 662 psoriatic arthritis and, 666 for ST-segment elevation MI, 90
dementia with Lewy bodies and, 683 oropharyngeal dysphagia from, 146b thoracic aortic aneurysm and, 98 for thoracic aortic atherosclerosis, 105
Down syndrome and, 676t senile amyloidosis, 5657, 534 in valvular aortic regurgitation, 39 antipsychotic agents
EEG evaluation, 614 amyotrophic lateral sclerosis, 4t, 146b, anorexia nervosa benzodiazepines, 605, 607
frontotemporal dementia and, 683 237, 629 in ACTH deficiency, 440 lithium, 607
geriatric assessment for, 682 analgesic-overuse headaches, 625 in acute hepatitis, 170 for mania, bipolar disorders, 601
intellectual disability (ID) and, 741 anaphylaxis in adrenal crisis, 453 side effects, 606607
mood disorders and, 601 in allergies, 579, 583584 in alcoholic hepatitis, 178 antiretroviral agents, for HIV infection
patient presentation, 617618, 682 in food allergies, 584 in bronchiectasis, 240 chemokine coreceptor antagonists,
pharmacologic therapy, 618b, 682683 hallmarks of, 583 in Cryptosporidium, 129, 319 323, 325
urinary incontinence and, 698t IgA-related, 509t in diabetic ketoacidosis, 427 fusion inhibitors, 323
vascular dementia and, 683 in stinging insect allergies, 584585 in gastroparesis, 155 guidelines for use of, 325326
amantadine anaplastic carcinoma, 418 in hypercalcemia, 488 HIV replication cycle, 320
for influenza A, 273 anatomically involved neurological in intra-abdominal abscesses, 306 integrase inhibitors, 323
for influenza A viruses, 273274 disorders. See neurological in pancreatic carcinoma, 143 nonnucleoside analogue reverse
for levodopa-induced dyskinesias, 647 disorders, anatomical involvement in polymyalgia rheumatica, 362 transcriptase inhibitors, 322323,
for lower UTIs, 698t ANCA (antineutrophil cytoplasmic in secondary hyperlipidemia, 422b 322t
for Parkinson disease, 646t, 648t autoantibody)-associated in uremia, 570 nucleoside, nucleotide analogue reverse
Amaurosis fugax, 638 granulomatous vasculitis, 663 anthrax (Bacillus anthracis), 251, 254 transcriptase inhibitors, 320322
ambulatory ECG (Holter) monitoring, 11 ANCA vasculitides, 560 anthrax vaccination, 696 postexposure prophylaxis
amebic colitis, 132 anemia of chronic disease (ACD), 501 antiarrhythmic drugs, 1214, 13t, 14t, 15f, recommendations, 326327
amenorrhea, 461463 anemias 23, 27, 289 protease inhibitors, 323, 324t
clinical features, 463 evaluation, 497 antibiotic colitis, 130 recommendations, treatment-nave
diagnosis, 463 hemolytic anemias, 503508 anticholinergic agents. See also ipratropium patient with no resistance, 326t
estrogen replacement therapy, 463 macrocytic anemias, 499501 for allergies, 577 viral load, resistance testing, 327
ovulation induction therapy, 463 microcytic anemias, 497498 for asthma, 592 antithrombotic therapy, 50t, 347t
primary amenorrhea, 461462 normocytic anemias, 501 for carotid sinus hypersensitivity antituberculosis drug toxicity
secondary amenorrhea, 462463 sickle cell anemia, 304, 384, 387, 404, syndrome, 21 ethambutol, 289290
American College of Cardiology/ 502, 637, 675 for COPD, 240, 592 isoniazid, 289
American Heart Association sideroblastic anemias, 498499, 503 for Parkinsonian symptoms, 606, 644t, pyrazinamide, 289
heart failure stages, 65, 66f aneurysmal disease, 98101 646 rifampin, 289
American College of Rheumatology, 359 abdominal aortic aneurysm, 100 for systemic mastocytosis, 166 streptomycin, 290
American Joint Committee on Cancer, axillary-subclavian artery aneurysm, 110 anticoagulant system defects, 523527. See anxiety disorders
staging system, 476, 477b iliac artery aneurysms, 105 also venous thromboembolism agoraphobia, 601602, 627b, 728729
American Urological Association peripheral artery aneurysms, 105 anticoagulation therapy generalized anxiety disorder, 602, 606,
International Prostate Symptom popliteal artery aneurysms, 98, 105, 375 for atrial septal defect, 54 728729
Score (AUA/IPSS), 697698 pulmonary artery aneurysm, 214 for dilated cardiomyopathy, 74 obsessive-compulsive disorder,
amikacin, 257, 280, 315, 328 subclavian vein aneurysms, 110 for Ebstein anomaly, 54 602603, 606
aminoglycoside thoracic aortic aneurysm, 98100 for mitral valve prolapse, 49t panic disorder, 244, 601602, 606,
for bacterial meningitis, 331, 335t angina. See also chronic stable angina for ST-segment elevation MI, 90, 94 728729
780 INDEX
posttraumatic stress disorder, 602, 606, thoracic outlet compression syndrome, glucocorticoids, 593b warm agglutinins, 506
728729 109110 glucocorticoids with 2-agonists, 593b autoimmune hepatitis, 177178
women and, 728729 thromboangiitis obliterans, 108109, topical, 593b autoimmune thrombocytopenic purpura,
aorta, diseases of 369 methacholine bronchial challenge, 592, 522
aneurysmal disease, 98101 arteritis 592b characteristics, 518
thoracic aortic atherosclerosis, 105 classic polyarteritis nodosa, 366368, occupational asthma, 590 clinical manifestations, 519
thoracic aortic dissection, 101105 367, 368t pathology of, 589 diagnosis, 519
aortic regurgitation giant cell arteritis, 216, 363365 pathophysiology of, 589 laboratory fi ndings, 519
aortic root dilatation, 39, 60, 383t Takayasu arteritis, 217218, 365366 severity assessment, 591592 treatment, 519520
diagnosis, 40 thoracic aortic aneurysm and, 98 asymmetric oligoarthritis, 666 autoimmune vascular disease, 62
natural history, severe patients, 42t arthritis. See also osteoarthritis; atazanavir (ATZ), 324 autosomal aneuploidy syndrome, 675
physical examination, 40 rheumatoid arthritis atenolol autosomal dominant polycystic kidney
symptoms, 3940, 42t acute bacterial arthritis, 353 for atrial fibrillation, 22, 22t disease (ADPKD), 566
treatment, 4042 acute gouty arthritis, 388389 IV, for thoracic aortic dissection, avascular necrosis, 384385
valvular, 39 acute monarticular arthritis, 403 104b avian influenza A (H5N1) virus, 272
aortic root dilatation, 39, 60, 383t asymmetric oligoarthritis, 666 contraindication, in asthma, 590591 axillary-subclavian artery aneurysm, 110
aortic stenosis, 32, 33 bacterial arthritis, 403 for migraine, tension headaches, 624 azathioprine
acquired von Willebrand syndrome bypass arthritis, 393 atheroembolic disease, 554 for classic polyarteritis nodosa, 367
and, 515 chronic monoarticular arthritis, 353 atherosclerosis for microscopic polyangiitis, 367
angiodysplasia and, 135 in chronic renal failure, 386 abdominal aortic aneurysm and, 100 pancreatitis caused by, 139
diagnosis, 39 gonococcal arthritis, 404 acute arterial occlusion and, 108 T-cellmediated infections from, 250
dilated cardiomyopathy and, 71, 75 immune complex-mediated arthritis, atheroembolic disease and, 554 azithromycin
physical examination, 3839 406 Carotid Atherosclerosis Study, 638 for Babesia, 271
pregnancy/cardiac disease and, 60 infectious arthritis, 403, 407 chronic mesenteric ischemia and, 131 for CAP, 274
severe patients, 41f, 60 inflammatory bowel disease and, 392 diabetes mellitus and, 56 for cat-scratch disease, 255
severity quantitation, 40t juvenile idiopathic arthritis, 393 diagnosis, 37 for chancroid, 294
symptoms, 38 nongonococcal bacterial arthritis, 404 hypertension and, 114 for cystic fibrosis, 240
treatment, 39, 40t poststreptococcal reactive arthritis, 405 hypothyroidism and, 5556 for dental procedures, 351t
types, 38 psoriatic arthritis, 392393 ischemic cerebrovascular disease and, for gonorrhea, 296, 298
aortoenteric fistula, 167 reactive arthritis, 392 657 for HIV-associated toxoplasmosis, 317b
APACHE (Acute Physiology and Chronic septic arthritis, 261, 403404 mechanism of, 82 for Lyme disease, 258
Health Evaluation), 200 spinal septic arthritis, 405 response-to-injury hypothesis, 82 for MAC disease, 312t, 315
apathetic thyrotoxicosis, 413 viral arthritis, 353, 405406 risk factors, 81
apatite microcrystals, 384 asbestos-related pneumoconioses, 210 secondary Raynaud phenomenon and, B
apical impulse, 3233 ascites, 183184 400 Babesia microti (tick-borne illness), 271
aplastic anemia, 501 aseptic bursitis, 361 sleep-related breathing disorders and, Bacillus anthracis (anthrax) infection,
aplastic crisis, 502 aseptic necrosis of bone 244b 251, 254
ARDS. See acute respiratory distress mnemonic device for causes of, 384b thoracic aortic aneurysm and, 98 Bacillus cereus, 163, 302t
syndrome aspergillosis, 262 thoracic aortic atherosclerosis, 105 bacterial arthritis, 403
arginine vasopressin-mediated renal water Aspergillus species, 249250, 262 thoracic aortic dissection and, 101 bacterial infections, causative agents
retention, 541 aspiration pneumonia, 280281 treatment, 80 Actinomyces israelii, 254
arrhythmias aspirin therapy atopic dermatitis, 588b, 655656, 671, Bartonella species, 255
bradycardias for antiphospholipid antibody 696, 718 Brucella, 255
carotid sinus hypersensitivity syndrome, 400 Atopobium vaginae, 300 Clostridium botulinum, 163, 252t, 255
syndrome, 2021 for hypertension, 56 atrial fibrillation Clostridium tetani, 255256
conduction system disorders, for ischemic heart disease, 8081 nonrheumatic atrial fibrillation, 23t Corynebacterium diphtheria, 256
1820 for mitral valve prolapse, 49t stroke risks/prevention, 2324 Corynebacterium jeikeium, 249
described, 17 for peripheral artery disease, 107 treatment Legionella, 251t
sinus node dysfunction, 1718 for ST-segment elevation MI, 90, 93 AV node catheter ablation, 23 Listeria, 251t
Eisenmenger syndrome in, 52 asthma -blockers, 22, 22t Mycobacterium species, 251t
evaluation of acute bronchopulmonary aspergillosis, calcium channel blockers, 2223, 22t Nocardia, 251t, 256257
ambulatory ECG monitoring, 11 595596, 596f CHADS2 risk scoring system, 22 Salmonella species, 251t
electrocardiography, 11 assessment of contributors, 591 class IA, IC, III antiarrhythmics, 22t Streptococcus mitis, 249250
electrophysiologic testing, 12 asthma-provoking drugs, 590591 digoxin, 22, 22t bacterial meningitis, 269, 276t277t,
event recording, 1112 causative industrial agents, 590b in Wolff-Parkinson-White syndrome, 331, 332f
mechanisms of, 11 cigarette smoking and, 591 2627 bacterial pathogens, in AIDS
in pregnancy, 61 contributors assessment, 591 in women, 728 Campylobacter jejuni, 129
tachycardias diagnosis algorithm, 594f atrial flutter, 21, 21f Mycobacterium avium-intracellulare,
atrial fibrillation, 2124 differential diagnosis, 592, 592b atrial septal defect 129
atrial flutter, 21 exhaled nitric oxide measure, 592 ostium primum, 50t Salmonella ser Enteritidis, 129
differentiating SVT with aberrancy genetics of, 589590 ostium secundum, 50t Salmonella ser Typhimurium, 129
from VT, 2425 GERD with, 149, 590 primary (partial av canal), 5051 Shigella fl exneri, 129
paroxysmal SV tachycardia, 24 hypercapnic respiratory failure and, 193 secundum, 49, 50t bacterial vaginosis, 300
tachycardia-mediated management sinus venosus, 4950, 50t balloon angioplasty, 53, 736
cardiomyopathy, 28 acute asthma, 594595, 595f atrioventricular (AV) nodal reentrant balloon atrial septostomy, 221222
torsades de pointes, 28 chronic asthma, 594 tachycardia, 12f bariatric surgery, for obesity, 179
ventricular ectopy, nonsustained goals of, 594b atrophic gastritis, 154 complications of, 434435, 749, 749b
VT, 27 steps (diagram), 594f atypical hypertrophic cardiomyopathy, 77f death from, 437
ventricular tachycardia, fibrillation, medical history, 591 atypical lymphocytosis, 265 indications for, 433434
2728 medications autoimmune bullous diseases, 657659, oxalate stones from, 759
Wolff-Parkinson-White syndrome, anti-allergic compounds, 593b 662 post-surgery nutrition, 434435
2527 anti-IgE treatment, 594 autoimmune gastritis (type A gastritis), 154 Barrett esophagus, 148150, 149150
treatment anti-inflammatory compounds, 593 autoimmune hemolytic anemia Bartonella bacilliformis, 255
antiarrhythmic drugs, 1214 antileukotrienes, 593b cold agglutinin syndrome, 505506 Bartonella henselae, 255
device therapy, 1617 bronchodilator compounds, 592593, differential diagnosis, 506f Bartonella quintana, 255
transcatheter RFA, 1416 593b mechanisms of, 505 basal cell carcinoma, 653
arterial occlusive disease corticosteroids, 593594 paroxysmal cold-hemoglobinuria, 506 basic calcium phosphate disease, 390
INDEX 781
beer potomania, 541 tularemia, 252t, 254 BPAP (bilevel positive airway pressures) C
bees and vespids allergies, 584 viral hemorrhagic fevers, 252t devices, 245 C1 esterase inhibitor deficiency, 582
Behet disease, 217, 372 bipolar disorder and mania bradycardias CABG. See coronary artery bypass grafting
erythema nodosum and, 660 gender-neutrality of lithium treatment, carotid sinus hypersensitivity syndrome, caf au lait spots, 665
thoracic aortic aneurysm and, 98 728 2021 calcium and bone metabolism disorders,
uveitis from, 393 lithium treatment, 606 characteristics, 17 465471
benign hematology manic episode features, 600601, conduction system disorders, 1820 hypercalcemia
anemias 600b fi rst-degree AV block, 18 management, 467
evaluation, 497 bisphosphonates second-degree AV block, 1819, PTH-dependent, 465466
macrocytic anemias, 499501 for hypercalcemia of malignancy, 489 18f, 19f PTH-independent, 466467
microcytic anemias, 497498 for multiple myeloma, 534 third-degree AV block, 1920, 19f hypoparathyroidism, 467468
normocytic anemias, 501 for osteoporosis, 469 sinus node dysfunction, 1718 osteomalacia, 469470
sideroblastic anemias, 498499 for Paget disease, 470 brain abscess osteoporosis, 468469
hemolytic anemias, 503508 Blastocystis hominis, 130 Aspergillosis and, 262 Paget disease, 470
porphyria, 510511 Blastomycosis dermatitidis, 261 Nocardia infection and, 257, 280 calcium channel blockers
sickle cell disorders, 501503 bleeding disorders pulmonary arteriovenous malformation for acute MI, 94
transfusion reactions, 508510 acquired bleeding disorders, 517518 and, 214 for angina, 86
benign prostatic hyperplasia congenital plasmatic bleeding disorders, untreated sinusitis and, 580 for atrial fibrillation, 22
differentiation difficulty, 484 513516 brain death, 614, 616, 778 contraindications
evaluation, 699700 laboratory evaluation brain metastasis, 642 in dilated cardiomyopathy, 74
history/physical examination, 697699 aPTT, 512 brainstem lesions, 626 for coronary artery spasm, 89
medical management, 700701 bleeding time, 513 breast cancer for hypertension in pregnancy, 6162
overactive bladder and, 685 not detected with PT, aPTT, 513 ductal/lobular carcinomas, 476, 476f for mitral stenosis, 44
overflow incontinence and, 686 prolonged PT/aPTT approach, 513 follow-up after curative therapy, for mitral valve prolapse, 47
urinary tract infection and, 302 PT assessment, 512 479480 for ventricular ectopy, nonsustained
benzodiazepines, 605, 607 platelet disorders, 518522 inflammatory bowel disease and, 136 VT, 27
for alcohol withdrawal seizures, 742 bleomycin lung toxicity, 209 natural history, prognostic factors in Wolff-Parkinson-White syndrome,
dialysis for removal of, 573b blood pressure. See also hypertension grade, 478 with atrial fibrillation, 27
EEG influences of, 614 abdominal aortic aneurysm and, 101 HER2/neu, 477478 calcium oxalate arthropathy, 390
mood disturbance caused by, 601 acute aortic dissection, 104t hormone receptor status, 477 calcium oxalate stones, 759
for panic disorder, agoraphobia, 602 acute cerebral infarction and, 639 nodal status, 477, 477f calcium phosphate disease, basic
side effects, 620t acute pancreatitis and, 141 triple-negative breast cancer, 478 diagnosis, treatment, 390
for time-limited anxiety treatment, 607 alcohol withdrawal and, 742 tumor size, 477 differential diagnosis, 390
withdrawal issues, 617, 619 blood loss and, 202t pathology, 476 presentation, 390
Bernard-Soulier syndrome, 521 carotid sinus hypersensitivity syndrome plain chest radiography evaluation, 223 calcium phosphate stones, 759
-agonists, 73, 594. See also dobutamine and, 2021 problem magnitude, 475 calcium pyrophosphate deposition disease
-blockers. See also atenolol; carvedilol; chronic headaches and, 622 recurrence patterns, 480 (CPPD), 389390
metoprolol; propranolol CKD complications and, 570 risk assessment, factors, 463, 465, 475, Campylobacter jejuni, 129, 164165, 302
for abdominal aortic aneurysm, 101 classification in adults, 115t 476t CA-MRSA. See community-acquired
for acute myocardial infarction, 28 diabetes mellitus and, 56 screening, 223, 475476, 690691, 724 methicillin-resistant S aureus
for angina, 86 diabetic nephropathy and, 562 staging, 476, 477b cancer. See oncology
for atrial fibrillation, 22 erectile dysfunction and, 703 treatment, 478479 cancer antigen 125 (CA 125), 483484
for cardiac issues in pregnancy, 61 febrile neutropenia and, 490t adjuvant, 478 cancer pain, 491493
for dilated cardiomyopathy, 7273 gender considerations, 726t advanced disease, 478479 cancer screening
hyperkalemia from, 571 giant cell arteritis and, 363 chemoprevention, 725 breast cancer, 223, 475476, 690691
for hypertension in pregnancy, 62 glomerular disease and, 558 chemotherapy, 479 cervical cancer, 693
for hyperthyroidism, 415 health risk assessment of, 432 Herceptin, 479 colorectal cancer, 137138, 137t, 138t,
for hypertrophic cardiomyopathy, 78 hypokalemia and, 457, 545f hormonal therapy, 479 691, 692f
limited benefit, for syncope, 30 hypoparathyroidism and, 467 lapatinib, 479 lung cancer, 482, 689690
for mitral stenosis, 44 ischemic heart disease and, 80 lifestyle modifications, 724 ovarian cancer, 484, 693
for mitral valve prolapse, 47 murmurs and, 34 pamidronate, 479 prostate cancer, 691693
for myocardial infarction, 94 myocardial infarction and, 94 primary/local-regional, 478 Candida endocarditis, 264
for TAA with Marfan syndrome, 99 neuroleptic malignant syndrome and, surgical, 477t, 725 Candida esophagitis, 148, 264265
for thyroid storm, 415 606 trastuzumab, 479 Candida glabrata, 301
for ventricular ectopy, nonsustained oral contraceptives and, 709 zoledronic acid, 479 Candida osteomyelitis, 264
VT, 27 screening in adults, 115t bronchiectasis candidiasis, 249250, 263264
in Wolff-Parkinson-White syndrome, severe aortic stenosis and, 41f causes, associations, 240241 Capnocytophaga canimorsus, 353
with atrial fibrillation, 27 smoking risk factors, 80 complications, 241 carcinoembryonic antigen (CEA),
-lactam antibiotics, 274, 328. See also sodium balance and, 541 treatment, 241 481482
amoxicillin Takayasu arteritis and, 366b bronchodilator therapy carcinoid heart disease, 58, 487
-thalassemias, 498 tamponade and, 62 for asthma, 592, 593b, 594595 carcinoid syndrome
bilateral hilar lymphadenopathy, 663 thoracic aortic rupture and, 104 for Bordetella pertussis, 279 carcinoid heart disease and, 58
bilateral synchronous pneumothorax, 291 bone and joint infections for bronchiectasis, 242 description, 487
bile duct stones, 187 acute bacterial arthritis, 353 for COPD, 239, 241 differential diagnosis, 592b
bilevel positive airway pressures (BPAP) chronic monoarticular arthritis, 353 for hypercapnic respiratory failure, 193 menopause and, 719
devices, 245 diskitis and vertebral infections, for hypersensitivity pneumonitis, 212 secondary diarrhea and, 160161
biliary tract disease 354 for intrinsic PEEP, 196 tricuspid regurgitation and, 48
bile duct stones, 187 osteomyelitis, 264, 330, 349b, 353354, Brucella, 255, 338, 341b, 354, 595b tricuspid stenosis and, 48
gallbladder carcinoma, 187 353355, 384 brucellosis, 255 carcinoma of unknown primary origin,
gallstones, cholecystitis, 186187 viral arthritis, 353, 405406 Buerger disease (thromboangiitis 487
malignant biliary obstruction, 187 bone marrow failure syndromes, 501 obliterans), 108109, 369 cardiac coarctation of the aorta, 115t
bioterrorism infections, recognition and Bordetella pertussis infection, 279 bulimia, 604, 606 cardiac myxomas, 6364
management Borrelia burgdorferi infection, 259, 666. bullous pemphigoid, 657 cardiac pacemaker, permanent
anthrax, 251, 252t, 254 See also Lyme disease bupropion, 753t, 756 implantation, 1617, 17t
botulism toxin, 252t botulism toxin (Clostridium botulinum), Burkitt lymphoma, 266, 532b, 533 cardiac physical examination, 3137
plague, 252t, 254 252t bursitis, 361362 additional palpation, 33
smallpox, 254 bowel bypass syndrome, 664 bypass arthritis, 393 apical impulse, 3233
782 INDEX
arterial pulses, 32, 38 primary/secondary prevention, 727728 cerebrovascular disease chronic lymphocytic leukemia, 388b,
cardiac cycle, normal, 33f risk factors, 725726 carotid sinus hypersensitivity syndrome 505506, 528529
heart sounds stress testing, 727 and, 20 chronic meningitis syndrome, 338,
fi rst heart sound, 32f, 33 cardiovascular implantable electronic diabetes/insulin goals and, 425 618b
fourth heart sound, 34 devices infections, 346, 349b, 350f exam question likely diagnosis, 4t chronic mesenteric ischemia (intestinal
opening snap, 34 cardioverter-defibrillators, implantable, 17 focal occlusive cerebrovascular disease, angina), 131132
second heart sound, 32f, 34 Carney complex, 63, 64 627 chronic monoarticular arthritis, 353
third heart sound, 34 carotid artery disease, 108 hemorrhagic cerebrovascular disease, chronic myeloid disorders, 536538
imaging hypertension and, 116 640 characteristic features, 537t
coronary angiography, 36 peripheral artery aneurysms and, 105 ischemic cerebrovascular disease, chronic myeloid leukemia, 536537
echocardiography, 3637 peripheral artery disease and, 106 637640 myeloplastic syndromes, 536
electron beam computed tomography, thoracic aortic aneurysm and, 99 peripheral artery disease and, 107 Philadelphia chromosome-negative
37 Carotid Atherosclerosis Study (CAS), 638 cervical cancer myeloproliferative neoplasms,
magnetic resonance imaging, 37 carotid sinus hypersensitivity syndrome, background, 480 537538
radionuclide imaging, 37 2021 invasive, in HIV infection, 312 chronic myeloid leukemia, 536537
jugular venous pressure, 31, 32f carpal tunnel syndrome prevention, 480 chronic obstructive pulmonary disease
murmurs, 3435, 35f amyloidosis and, 57, 535 screening for, 693 (COPD)
thrills, 33 amyotrophic lateral sclerosis and, 629 treatment, 480 differential diagnosis, 68
cardiac risk assessment, preoperative arthritis in chronic renal failure and, cervical osteophytes, 146b, 392 exacerbations, complications and causes,
evaluation 386 Charcot joint (neuropathy arthropathy), 241
coronary stent patients, 737 CKD and, 572 384 hypercapnic respiratory failure and, 193
noncardiac surgery, 733t eosinophilic fasciitis and, 402 chemokine coreceptor (CCR5) management approaches, 239b
patient-specific, 733 mononeuropathy and, 632 antagonists, 323, 325, 326t. See also treatment, 239241
perioperative ischemia monitoring, rheumatoid arthritis and, 376 maraviroc adjuvant therapy, 241
736737 carvedilol, 22t, 69t, 73, 753t chest radiograph fi ndings anticholinergic agents, 239
resting echocardiography, 735 caspofungin, 262, 264 for aortic regurgitation, 40, 42t bronchodilators, 239
risk reduction strategies, 735736 catheter ablation for aortic root dilatation, 39 corticosteroids, 240
stepwise approach, 733735 for atrial fibrillation, 15, 23 for atrial septal defect, 49, 5051, 51f long-acting -selective agonists, 240
stress test choice, 735 for atrial flutter, 21 for Ebstein anomaly, 5354 oxygen, 241
surgery-specific, 733 heart rhythms amenable to, 16t for heart murmur evaluation, 35f phosphodiesterase inhibitors, 240
cardiac tamponade, 199t, 377 for symptomatic PSVT, 24 for mitral regurgitation, 45 reducing risk factors, 239
cardiac tumors, 6364 transcatheter RFA, 1416 for mitral stenosis, 43, 44f short-acting -selective agonists, 239240
Cardiobacterium hominis, 340, 341b, 344t, for Wolff-Parkinson-White syndrome, for pulmonary stenosis, 52, 52f surgery, 241
345, 346t 26 childhood-type myopathies, 403 chronic pancreatitis
cardiogenic shock, 73, 9496, 96t catheter-associated urinary tract infections Chlamydia, 81 laboratory diagnosis, 142143
cardiogenic syncope, 12, 29, 30 (CAUTIs), 746747 Chlamydia trachomatis cervicitis, 299 malabsorption in, 143
cardiomyopathy(ies), 6874. See also catheter-related bloodstream infections Chlamydia trachomatis genital infection, pain in, 143
dilated cardiomyopathy; (CR-BSIs), 200, 329, 744 299 triad of, 142
hypertrophic cardiomyopathy; cavernous hemangioma, 183 Chlamydophila (Chlamydia) pneumoniae, chronic pernio, 112
restrictive cardiomyopathy cavernous sinus thrombosis, 580 274 chronic stable angina
amyloidosis and, 56 cefepime, 249, 276t, 279, 328, 330, 335t chloramphenicol, 163, 164, 252t, 276t, CABG treatment, 8788
anatomical, pathophysiologic processes, celiac disease (CD), 165 299, 333t, 501 clinical presentation, 83
70t cellulitis, 349 cholangiocarcinoma, 183 silent ischemia, 83
with atrial fibrillation, 21 central nervous system infections, 250, 331, cholesterol crystals, 390 symptomatic stable CAD, 83
divisions of, 6869 335339 chorioretinitis, 266, 294, 316 invasive coronary angiography, 85
hypothyroidism-related, 56 aseptic meningitis syndrome, 337338 chronic cholestatic liver disease medical therapy, 8586
restrictive, 63 bacterial meningitis, 269, 276t277t, primary biliary cirrhosis, 179 catheter-based vs surgical vs, 8889
symptomatic dilated, pregnancy 331, 332f primary sclerosing cholangitis, noninvasive testing for ischemia
contraindication, 60 chronic meningitis syndrome, 338 179180 coronary angiography, 8485
cardiorenal syndrome, 552 encephalitis, 258, 265, 337338 chronic cutaneous lupus erythematosus, left ventricular function, 83
cardiovascular disease. See also meningococcal meningitis, 277t, 331, 666 stress testing, 8384
cardiovascular disease, in women 335336 chronic disseminated candidiasis, 264 pathophysiology, 8283
CKD and, 572573 pneumococcal meningitis, 331, 336 chronic gastritis, 151152, 155 percutaneous coronary intervention,
community-acquired pneumonia and, poliovirus, 338 chronic idiopathic urticaria, 581 8687
275 rabies, 338 chronic intestinal pseudo-obstruction, postcardiotomy syndrome, 88
endocarditis and, 351 slow viruses, prion-associated diseases, 167168 surgical treatment, 8788
end stage renal disease and, 572 338339 chronic kidney disease (CKD). See also TIMI risk score for, 89b
erectile dysfunction and, 701, 702703 central sleep apnea, 244245 kidney function, evaluation Churg-Strauss syndrome (eosinophilic
estrogen replacement therapy and, 469 cephalosporin, 404 cardiovascular disease and, 572573 granulomatosis with polyangiitis),
hyperlipidemia and, 423 cerebellar degenerative dementia, 488t causes, 570t 59, 216, 663
hyperparathyroidism and, 572 cerebellar hemorrhage, 640 dietary recommendations, 570 clinical features, 368369
hypertension and, 114, 116117 cerebellar lesions, 626 progression prevention, 570572 treatment and outcome, 369
hypertriglyceridemia and, 572 cerebrospinal fluid analysis stages of, 570t cicatricial pemphigoid, 657
ischemic heart disease and, 8081, 428 in acute inflammatory demyelinating treatment, complications, 570572 ciliary dyskinesia, 580
nutritional support for, 435b polyradiculoneuropathy, 632 anemia of CKD, 572 cilostazol, 107
oral contraceptive contraindication, 709 in brain metastasis, 642 arthritis, 572 ciprofloxacin, 129, 328
phosphorous retention and, 570 in community-acquired bacterial 2-microglobulin deposition, 572 for Campylobacter jejuni, 129
rheumatoid arthritis and, 373 meningitis, 332f carpal tunnel syndrome, 572 for HAP, VAP, HCAP, 328
SLE and, 397 in cryptococcus infections, 263f end stage renal disease, 571, 573 for Salmonella in AIDS, 129
syncope and, 29b in hemorrhagic cerebrovascular disease, GI tract disorders, 572 for Shigella fl exneri, 129
syphilis and, 296 640 hyperkalemia, 571 Citrobacter, 328
cardiovascular disease, in women in hydrocephalus, 626 hyperphosphatemia, 571 CKD. See chronic kidney disease
atrial fibrillation, 728 in multiple sclerosis, 648649 metabolic acidosis, 572 clarithromycin, 274
clinical presentation, 727 in neurological disorders, 614615 neurologic complications, 572 classic polyarteritis nodosa, 217, 366368,
gender-based differences, 726t, 727 in neuromyelitis optica, 649 osteomalacia, 571 368t
heart failure, 728 in seizure disorders, 619 secondary hyperthyroidism, 571 clindamycin, 254, 270271, 297t, 300,
pathogenesis, 726727 cerebrospinal fluid pleocytosis, 338 U.S. data, 569570 313t, 351, 352
INDEX 783
clinical epidemiology toxic megacolon, 126 factor VII deficiency, 516 conversion disorder, 603
diagnostic test interpretation tuberculosis and diarrhea, 132 factor XI deficiency, 516 Coombs-negative hemolytic anemias, 506
negative predictive value, 764 ulcerative colitis, treatment, 126127 factor XIII deficiency, 516 COPD. See chronic obstructive pulmonary
positive predictive value, 763764 colonic polyps, 134135 hemophilia A and B, 515516 disease
sensitivity, 763 colon polyposis, 662 von Willebrand disease, 513515 coronary artery bypass grafting (CABG)
specificity, 763 colorectal cancer congenital platelet disorders in chronic stable angina, 8788
odds and likelihood ratios, 765767 diagnosis, 136137 Bernard-Soulier syndrome, 521 medical vs catheter-based therapy vs,
examples, 766767, 766t epidemiology, etiology, 135 Glanzmann thrombasthenia, 522 8889
therapeutic results interpretation fecal occult blood testing for, 480 Wiskott-Aldrich syndrome, 522 post-CABG mortality rates, 88
absolute risk reduction, 768 genetic factors, 135136 congestive heart failure (CHF) coronary artery spasm, 89
number needed to harm, 768 pathology, prognostic indicators, 136 amiodarone for, 13 cortical lesions, 626
number needed to treat, 768 postoperative management, no amyloidosis and, 56, 535 corticosteroid crystals, 390
relative risk reduction, 767768 metastases, 137 antiarrhythmic drug toxicity, 14t corticosteroids
2x2 table construction, 764765, 765t prevention strategy in aortic stenosis, 39 for allergic bronchopulmonary
clopidogrel, 87, 90, 92, 93, 107, 615, primary, secondary, 137 apathetic thyrotoxicosis and, 413 aspergillosis, 262
638639 screening, 137138, 137t, 138t, 692f assessment for, 31 for ARDS, 195
Clostridium botulinum (botulism toxin), risk factors, 136, 480481 cardiac amyloidosis and, 5657 for asthma, 593594, 595
163, 252t, 255 screening for, 691 causes of, 102, 256 for avian influenza A virus, 272
Clostridium difficile, 130, 162, 305, 318, staging and survival, 481t deep vein thrombosis and, 219 for Behet disease, 216, 393
392 treatment, 137, 481482 diabetes mellitus and, 56 for bullous pemphigoid, 657
Clostridium perfr ingens, 162163, 252t, carcinoembryonic antigen, 481482 diagnostic criteria, 67t for chronic rhinitis, 578579
302t, 303 metastatic disease, 481 eosinophilia and, 587 for Churg-Strauss syndrome, 369
Clostridium tetani, 255256 surgery, 481 Framingham diagnostic criteria, 67, 67b for COPD, 240
CMV retinitis, 250, 266267, 311b, 316 common variable immunodeficiency hemochromatosis and, 58 for cutaneous T-cell lymphoma, 655
CMV syndrome, 266267 (CVID), 588 hyperthyroidism in pregnancy and, 711 for Felty syndrome, 380
coagulase-negative staphylococci, 249, 301, communicating hydrocephalus, 626, 640 hyponatremia and, 541 for giant cell arteritis, 364365
330, 335t, 340341, 346t community-acquired methicillin-resistant pleural eff usion and, 242b for hemolytic anemia, 265
coagulation system. See bleeding disorders S aureus (CA-MRSA), 352 postcardiotomy syndrome and, 88 for nasal polyposis, 579
Coccidioides immitis, 259260 community-acquired pneumonia (CAP), prerenal AKI and, 552 for pemphigus vulgaris, 659
Coccidioides meningitis, 260 274275 pulmonary embolism and, 218 for restrictive cardiomyopathy, 79
coccidioidomycosis, 239, 242, 250, antimicrobial therapy, 276t277t risk factors, 14t, 22, 23, 131, 165, 433b, for small cell vasculitis, 371
259260, 311b, 337t Bordetella pertussis, 279 604, 738t for Taenia solium, 270
cold agglutinin syndrome (primary cold Burkholderia pseudomallei, 280 valve replacement surgery and, 340, for Takayasu arteritis, 217
agglutinin disease), 505506 causes, 274 345b T-cellmediated infections from, 250
colitis chlamydia, 278 venous thromboembolism and, 524 for varicella pneumonia, 272
amebic colitis, 132 Enterobacter, 279 connective tissue for viral arthritis, 405
antibiotic colitis, 130 Francisella tularensis, 279280 inherited disorders, 383t for Wegener granulomatosis, 370
ischemic colitis, 131 Klebsiella pneumoniae, 279 mixed connective tissue disease, 399 Corynebacterium diphtheriae, 256
radiation colitis, 131 Legionella, 278 overlap connective tissues disease, 403 Corynebacterium jeikeium, 249
ulcerative colitis, 126127 Moraxella, 278 related interstitial lung diseases, 208 Coxiella burnetii, 259, 279, 340, 341b
collagenopathies, Type II, 383t Mycoplasma pneumoniae, 278 undifferentiated connective tissue CPAP (continuous positive airway
collagen vascular disease, 44, 62, 206b, Serratia, 279 disease, 399 pressures) devices, 245
508, 587, 634 treatments, 274275 constrictive pericarditis, 31, 6263 CPPD. See calcium pyrophosphate
colon, 125138. See also colorectal cancer Yersinia pestis, 280 contact dermatitis, 586 deposition disease
AIDS, gastrointestinal manifestations computed tomography (CT) continuous positive airway pressures CR-BSIs. See catheter-related bloodstream
bacterial pathogens, 129 for cavernous hemangioma, 183 (CPAP) devices, 197t, 198, 245 infections
diarrhea, diagnostic evaluation, 130 for dementia, 613, 618 contraceptives, hormonal CREST syndrome, 147, 209, 401402,
fungal pathogens, 129 for disk evaluation, 613614 abnormal uterine bleeding and, 707b 667, 667f
protozoan pathogens, 129130 for hepatocellular carcinoma, 183 dysfunctional uterine bleeding and, 708 Creutzfeldt-Jakob disease, 339
viral pathogens, 128129 for intracranial tumors, 613 oral contraceptive comparison, 719 cricopharyngeal dysfunction, 146b
amebic colitis, 132 for meningeal metastases, 642 types of, 709 critical care medicine, 191204
angiodysplasia, 133 for normal pressure hydrocephalus, 618 contraceptives, oral endocrinology, 201
antibiotic colitis, 130 for spinal cord lesions, 613 acne vulgaris and, 656 gastroenterology
congenital megacolon, 132133 for trauma, 612 acute ischemia and, 116t abdominal compartment syndrome,
Crohn disease, treatment, 127128 for vascular diseases, 612 adenomas and, 183 203
diverticular disease for white matter lesions, 613 anticonvulsant therapy and, 620 fulminant hepatic failure, 202203
defi nitions, 133 conduction system disorders, 1820 antiepileptic drugs and, 620t GI hemorrhage, 201202, 202t
diagnosis, management, 134t fi rst-degree AV block, 18 antiphospholipid antibody syndrome hematologic disorders, 203204
diverticulitis, 133134 second-degree AV block, 1819, 18f, 19f and, 399 ICU-related bleeding disorders,
hereditary polyposis syndromes third-degree AV block, 1920, 19f drug-induced erythema nodosum and, 203204
no risk of cancer, 135 congenital bicuspid valvular aortic stenosis, 660 hemodynamic status assessment,
with risk of cancer, 134135 38 estrogen-containing, 399, 523, 709, 199200, 199f
inflammatory bowel disease congenital bone marrow failure syndromes, 709b respiratory critical care
extraintestinal manifestations, 501 hemolytic uremic syndrome and, 563 airway management, 191192
125126 congenital heart disease, 4954 hyperlipoproteinemia and, 140 mechanical ventilation, 195198
indications for colonoscopy, 126 atrial septal defect mechanisms, 116t respiratory failure, 192195
irritable bowel syndrome, 132133 primary (partial atrioventricular oral contraception comparison, 719 sepsis, 200201
ischemia canal), 5051 ovarian cancer and, 693 shock, 198, 199t
acute ischemia, 131 secundum, 49 rifampin and, 289 critical illness polyneuropathy, 649
anatomical review, 131 sinus venosus, 4950 secondary hypercoagulable states and, Crohn disease
chronic mesenteric ischemia, 131132 coarctation of the aorta, 5253 219b aphthous ulceration and, 664
lower GI tract bleeding, 133 Ebstein anomaly, 5354 theophylline clearance and, 242b colon cancer and, 136
nontoxic megacolon, 133 Eisenmenger syndrome, 5152 thrombophilia and, 523, 524b common variable immunodeficiency
polyps, 134 patent ductus arteriosus, 51 types of, 709 and, 588
pseudomembranous enterocolitis, 130 pulmonary stenosis, 52 vitamin B12 levels and, 500 diarrhea and, 161
radiation colitis, 131 ventricular septal defect, 51 vulvovaginal candidiasis and, 263264 intestinal fistulas in, 125
Streptococcus bovis endocarditis, 132 congenital plasmatic bleeding disorders contrast-induced nephropathy, 553554 intestinal lymphangiectasia and, 166
784 INDEX
peptic ulcer disease and, 151 hypertension and, 115t, 120 cerebellar degenerative dementia, 488t hematologic, 668
primary sclerosing cholangitis and, 126 identification, 455 Creutzfeldt-Jakob disease and, 339 metabolic, 669670
pyostomatitis vegetans and, 664 therapy, 456 delirium comparison, 604, 683684 nephrologic, 665
renal lithiasis and, 126 cutaneous Crohn disease, 664 diagnosis of, 613, 618619 neurocutaneous, 665666
treatment of, 126, 127128, 251 cutaneous leishmaniasis, 271 differential diagnosis, 618b pulmonary, 663
vitamin B12 deficiency and, 499500 cutaneous T-cell lymphoma, 587, 654655 EEG evaluation, 617 rheumatologic, 666668
vulvar itching and, 718 cutaneous vasculitis, 370371 frontotemporal dementia, 4t, 617, 618, nail clues, to systemic disease, 670
cryoglobulin crystals, 390 clinical features, 370371 683 underlying malignancy, cutaneous signs,
cryoglobulinemia, 371372 diagnosis, 371 geriatric assessment for, 682 661663
laboratory studies, 372 histopathology, 371 hypertensive target organ injury and, dermatomyositis, 403, 488
outcome, 372 treatment and outcome, 371 116t heliotrope discoloration in, 662f
types I and II, 371372 CVID. See common variable Lewy body dementia, 646t, 683 oropharyngeal dysphagia from, 146b
cryoglobulinemic GN associated with immunodeficiency lumbar puncture and, 618 desmopressin acetate (DDAVP) treatment,
hepatitis infection, 563 cyclophosphamide Lyme disease and, 258 515
cryptococcosis, 250, 263 for cicatricial pemphigoid, 657 normal-pressure hydrocephalus and, desquamative interstitial pneumonia
Cryptococcus neoformans disease, 263, for classic polyarteritis nodosa, 367 618, 682 (DIP), 207t, 211
315316 for microscopic polyangiitis, 367 progress multifocal device therapy, for suspected rhythm
cryptogenic organizing pneumonia, 211 for Wegener granulomatosis, 370 leukoencephalopathy and, 318 disorders
Cryptosporidia belli, 129 Cyclospora cayetanensis, 306 syphilis and, 295 implantable cardioverter-defibrillator,
Cryptosporidium, 129 cyclosporin, 250 vascular dementia, 613, 618b, 682, 683 17
Cryptosporidium parvum, 306 cystic fibrosis, 143144, 223, 231f, Whipple disease and, 166 indications for implantable pacemaker,
crystal deposition due to medication or 241242, 287 dementia with Lewy bodies, 4t, 618, 646t, 16b
toxins, 555 cystic fundic gland polyps, 155 683 permanent cardiac pacemaker, 1617
crystalline arthropathies cystic renal disease, 566 Demerol (meperidine), 141 diabetes insipidus (DI), 544
aluminum phosphate crystals, 390 cytomegalovirus (CMV), 81, 250 dental procedure regimens, for clinical features, 449
basic calcium phosphate disease, 390 in AIDS, 128 endocarditis prevention, 351b, 351t diagnosis, 544
calcium oxalate arthropathy, 390 aplastic anemia and, 501 depressive disorders. See also endocrine diagnosis, 449
calcium pyrophosphate deposition hepatitis and, 177 antidepressants etiologic diagnosis, 449
disease, 389390 HIV association, 316 adjustment disorder etiology, 448
cholesterol crystals, 390 infections caused by, 266267 with anxious mood, 602 nephrogenic DI, 446
corticosteroid crystals, 390 treatment, 316t with depressed mood, 600 pituitary tumors and, 442
cryoglobulin crystals, 390 cytomegalovirus (CMV) pneumonia, 272 Cushing syndrome and, 455 primary aldosteronism and, 456
hyperuricemia and gout, 387388 cytoplasmic ANCA (c-ANCA), 207, dysthymia, 600, 607, 728 pulmonary Langerhans cell histiocytosis
CT computed tomography (CT) scan 215216, 369 fibromyalgia and, 359 and, 213
in abdominal aortic aneurysm, 101 hypothyroidism and, 55 secondary hyperuricemia and, 388b
in acute pancreatitis, 140, 141 D ischemic heart disease and, 80 shock in, 199t
in adrenal gland disorders, 453, 455, dactylitis (sausage fi nger or toe), 393, major depression therapy, 449, 544
457, 458 406, 502 episode criteria, 600b diabetes mellitus (DM). See also diabetes
in brain trauma, 612 darunavir (DRV), 324t postpartum depression, 599600, mellitus (DM), type 1; diabetes
in cavernous hemangioma, 183 deep vein thrombosis (DVT) 728 mellitus (DM), type 2
in chronic pancreatitis, 142 AIDP and, 632 with psychotic features, 599 characteristics, 424
in colorectal cancer, 137 anticoagulation and, 94 seasonal affective disorder, 599 chronic mesenteric ischemia and, 131
in conjugated hyperbilirubinemia, 172f in Behet disease, 217 as medication side effect, 322t, 492 clinical features, 424
in dementia, 613 chemoprevention risk factors, 725 perimenopause and, 728 dermatologic disorders in, 668669
for focal cerebral, cerebellar processes, 614 coagulation disorders leading to, 219b, polymyalgia-like syndrome and, 362b diabetic ketoacidosis and, 424, 430
in gastric cancer, 154 517 sleep-disordered breathing and, 244b diagnosis, 424
in gonadotropin-producing tumors, 447 congestive heart failure and, 219 treatment principles, 600 effects on the heart, 56, 64
in hepatocellular carcinoma, 183 estrogen-containing oral contraceptives women and, 728729 etiology and classification, 423424
in hypopituitarism, 441 and, 708b de Quervain thyroiditis (subacute painful gestational diabetes, 424, 429
in intestinal angina, 131 incidence in various clinical thyroiditis), 414 ischemic heart disease and, 80
in intracranial tumors, 613 circumstances, 219t dermatitis herpetiformis, 658, 664 kidney treatment and, 570
in lumbar spinal stenosis, 106 preoperative surgical evaluation, 730 dermatology therapy, 425427
in myasthenia gravis, 634 in pulmonary embolism, 218 general dermatology diabetes mellitus (DM), type 1
in neurogenic thoracic outlet syndrome, ventilator-induced pneumonia and, 196 acne vulgaris, 656657 characteristics, 424
110 VTE and, 524, 525t allergic contact dermatitis, 656 clinical features, 424
in normal-pressure hydrocephalus, 618 Wells model for predicting, 525t atopic dermatitis, 588b, 655656, therapy
in obstructive lymphedema, 112 degenerative aortic valve disease, 38, 39 696, 718 amylin analogue, 425
in pancreatic carcinoma, 143 delayed hemolytic transfusion reactions, 510 autoimmune bullous diseases, glycemic goals, 425
in pancreatic endocrine tumors, 144 delirium, 604 657659, 662 insulin replacement, 424425
in peripheral artery disease, 107 in acute confusional states, 617 cutaneous T-cell lymphoma, 587, nutrition, 425
in pituitary incidentalomas, 447 in alcohol withdrawal, 605 654655 pramlintide, 425
in pulmonary embolism, 220 in botulism, 634 drug reactions, 660, 660t diabetes mellitus (DM), type 2
in pulmonary vascular disease, 214 causes of, 684b erythema multiforme, 164, 278, 294, characteristics, 424
in rhinitis, 578, 581 dementia comparison, 604, 683684 659, 659f, 660, 663 clinical features, 424
in thoracic aortic aneurysm, 99 geriatric assessment for, 683684 erythema nodosum, 4t, 125, 164, 260, drug therapy
in thoracic aortic dissection, 103, 104f in geriatric patients, 679 305, 366, 659660 -glucosidase inhibitors, 426
in thyrotropin-producing tumors, 447 in lithium toxicity, 607 malignant melanoma, 63, 653654 amylin analogue, 427
in vascular diseases, 612 in Parkinson disease, 646 nonmelanoma skin cancer, 653, 654 dipeptidyl-peptidase-4 inhibitors, 426
culture-negative pulmonary tuberculosis, postoperative delirium, 747748, 747b psoriasis, 4t, 310b, 368b, 655, 666, glucagon-like peptide-1 analogues,
288f in refeeding syndrome, 437 670, 718, 757 426
Cushing syndrome, 454456 in thrombocytopenia, 508 skin cancer, 529, 653 insulin, 426427
clinical features, 455 in thyroid storm, 415, 419 HIV-infection, cutaneous metformin, 426
etiologic diagnosis, 455456 dementia manifestations, 670671 nateglinide, 426
etiology Alzheimer disease and, 613, 617618, internists perspective repaglinide, 426
ACTH-dependent, 454 682 cardiovascular, 663664 sulfonylureas, 426
endogenous, 454 antiphospholipid antibody syndrome endocrinologic, 668669 thiazolidinediones, 426
exogenous, 454 and, 399400 gastrointestinal, 664665 nutrition therapy, 425
INDEX 785
diabetic ketoacidosis for cardiac issues in pregnancy, 61 for mitral stenosis, 44 prevalence data, 728
diabetes mellitus and, 424, 430 for dilated cardiomyopathy, 73 for nephrotic syndrome, 558 treatment principles, 600
G6PD deficiency and, 507 for PAH, 221 for PAH, 221
mucormycosis and, 264 toxicity, 11 for pulmonary arterial hypertension, E
nonpancreatic hyperamylasemia and, in Wolff-Parkinson-White syndrome, 221 eating disorders. See also anorexia nervosa
140 with atrial fibrillation, 27 for restrictive cardiomyopathy, 79 bulimia, 604, 606
secondary hyperuricemia and, 387, 388b dihydropyridines (calcium channel DMARD (disease-modifying bupropion, contraindication in, 756
treatment, 427428 blockers), 2223, 86, 111, 119. antirheumatic drug) treatments. infertility and, 710
diabetic nephropathy (DN), 557t, 558, See also amlodipine; felodipine; See also methotrexate Ebstein anomaly, 5354
562. See also diabetes mellitus nifedipine for rheumatoid arthritis, 379 Echinococcus granulosus (echinococcosis or
diabetic peripheral neuropathy, 384 dilated cardiomyopathy DNR. See do-not-resuscitate (DNR) orders hydatid disease), 290
diabetic retinopathy, 424, 428429, 562 AIDS and, 60 dobutamine echocardiography
diarrhea. See also diarrhea, bacterial and anatomical processes, 70t for cardiogenic shock, 96 in acute aortic regurgitation, 40
toxigenic cardiac replacement therapy, 74 for dilated cardiomyopathy, 73 in amyloidosis, 57
acute diarrhea, 159 clinical presentation, 70 in pharmacologic stress tests, 84 in atrial fibrillation, 22
in AIDS, 130 etiology, pathology, 6970 for regional wall motion abnormalities, in atrial septal defect, 5051
bile acid malabsorption, causes, 162 evaluation, 71 36 in cardiac examination, 3637, 39
chronic diarrhea, 159 Friedreich ataxia and, 59 for right ventricular infarction, 96 in cardiac tumor diagnosis, 64
clinical approach to, 158 ischemic cerebrovascular disease and, dofetilide in cardiogenic shock, 96t
invasive bacterial diarrhea, causes, 637 adverse effects of, 14t in cerebral infarction, 638b, 639
163165, 303t Lyme disease and, 258 properties of, 13t in constrictive pericarditis, 63
mechanisms of, 157158 mitral regurgitation and, 44t relative effectiveness of, 13t in coronary heart disease, 727
noninvasive bacterial diarrhea, causes, pathophysiology, 70t, 71 do-not-resuscitate (DNR) orders, 777 in dilated cardiomyopathy, 71
162163 in pregnancy, 6061 Doppler echocardiography, 3839, 41f, 43, in eosinophilia, 587588
nutrient absorption physiology, treatment 49, 52, 63, 220 in heart failure, 68
159160, 160t cardiac replacement therapy, 74 doripenem, 328, 330 in heart murmurs, 34, 35f
organic vs. functional, 159t device therapy, 74 Down syndrome, 50t in infective endocarditis, 339, 340b,
osmotic diarrhea, causes, 160 nonpharmacologic, 72 acute myeloid leukemia and, 535 341f
parasitic diarrhea, 306 pharmacologic treatment, 7274 atrioventricular canal defects and, 51 in ischemia, 83
secretory diarrhea, causes diltiazem autosomal aneuploidy syndrome and, in left ventricular hypertrophy, 76
carcinoid syndrome, 160161 for acute gouty arthritis, 389 675 in mitral valve prolapse, 47
laxative abuse, 161162 for atrial fibrillation, 22t, 23 congenital megacolon and, 132 in pericardial eff usion, 62
surreptitious laxative ingestion, for dilated cardiomyopathy, 74 diabetes and, 424 in perioperative cardiac assessment, 734f
161162 for ST-segment elevation MI, 94 secondary hyperuricemia and, 388b in preoperative LV assessment, 735
VIPoma, 160 DIP. See desquamative interstitial trisomy 21 abnormality in, 676t in pulmonary hypertension, 221
in tuberculosis, 132 pneumonia drug allergies in pulmonary vascular disease, 214
viral diarrhea, 305306 dipeptidyl-peptidase-4 inhibitors, 426 involving IgE or immediate-type in restrictive cardiomyopathy, 79
diarrhea-associated hemolytic uremic Dirofilaria immitis (dirofi lariasis), 290 reactions risk factors in stroke, 24
syndrome (D+HUS), 563564 discoid lupus erythematosus, 667 penicillin allergy, 586587 in scleroderma, 401
diarrhea, bacterial and toxigenic disease-modifying antirheumatic drug radiographic contrast media in secundum atrial septal defect, 49
Campylobacter jejuni, 129, 164165, 302 (DMARD) treatments, 379 reactions, 587 in ST-segment elevation MI, 96
causes of, 302t diskitis and vertebral infections, 354 not involving IgE or immediate-type in syncope evaluation, 30f
Clostridium perfr ingens, 303 disopyramide reactions in transient ischemic attack, 638b
Escherichia coli, 303304 adverse effects of, 14t, 28 ampicillin-mononucleosis rash, 586 in valvular diseases, 3637
Salmonella infection, 304 heart failure and, 69t, 78 contact dermatitis, 586 eczema herpeticum, 655
Shigella species, 304 narrow complex tachycardia and, 27 erythema nodosum, 586 Ehlers-Danlos syndrome
staphylococcal enterotoxin, 302303 properties of, 13t fi xed drug eruptions, 586 abdominal aortic aneurysm and, 100
didanosine, 139, 321, 321t, 322 relative effectiveness of, 13t morbilliform skin reaction, 586 bullous lung disease and, 239
pancreatitis caused by, 139 torsades de pointes and, 28 Stevens-Johnson syndrome, 585 gene defect in, 383t, 676
dietary (nutritional) support disseminated gonococcal arthritis toxic epidermal necrolysis, 585 subgroups of, 664
for ascites, 184 syndrome, 404 drug-eluting stents thoracic aortic aneurysm and, 98
for aspiration pneumonia, 403 disseminated intravascular coagulation for chronic stable angina, 87, 87t Ehrlichia species, 259
for Crohn disease, 128 (DIC), 517518 perioperative patient studies, 737 ehrlichiosis, 259, 271
for cystic fibrosis, 241 ancillary therapies for, 518 drug-induced erythema nodosum, 660 Eikenella corrodens, 345, 350
for diverticular disease, 134t blood component replacement therapy, drug-induced myopathies, 403 Eisenmenger syndrome, 5152, 6061, 64
for GERD, 150 517518 drug-induced SLE electroconvulsive therapy (ECT), 599, 607
for hypertension, 117t clinical features, 517 clinical features, 398 electroencephalography (EEG)
for irritable bowel syndrome, 132 laboratory testing, 517 implicated agents, 398b in brain death, 616
for ischemic heart disease, 81, 97 management, 517 laboratory abnormalities, 398 in dementia, 617
for obesity, 436437 pathophysiology, 517 metabolism, 398 for neurological disorders, 614
enteral support, 436 distal tubular acidosis, 547 treatment, 398399 in seizure disorders, 619, 621
micronutrient deficiencies, 436 diuretics. See also loop diuretics; drug-induced thrombocytopenia, 520 in status epilepticus, 622
micronutrient supplements, 435436 potassium-sparing diuretics; dual-chamber pacemakers (DDD in stupor and coma, 617
parenteral support, 437 thiazide diuretics pacemaking), 17 electromyography (EMG) studies
for Peutz-Jeghers syndrome, 135 for AKI, 557 ductal carcinoma (breast cancer), 476, 476f for acute inflammatory demyelinating
for portal systemic encephalopathy, 185 for angina, 86 dumping syndrome, 155 polyradiculoneuropathy, 632
for premenstrual syndrome, 706707 for ascites, 184 duodenal ulcer, 151152, 154 for electrolyte imbalance, 635
for scleroderma, 401 for circulatory overload, 510 dysfunctional uterine bleeding, 708 for external sphincter of the bladder, 685
for types 1, 2 diabetes mellitus, 425 for CKD complications, 578579 dysphagia for inflammatory myopathy, 403, 634
differentiating supraventricular for dilated cardiomyopathy, 7273 causes of, 145 for low back pain, 361
tachycardia with aberrancy from for heart failure, 66t, 67b, 69 diagnostic scheme for, 146f for multifocal motor neuropathy, 629
VT, 2425 for hypertension, 39, 62, 117, 118f GERD with, 149 for myotonic dystrophy, 676t
diff use idiopathic skeletal hyperostosis in pregnancy, 62 mechanical, 145, 147148 for neurological disorders, 614
(DISH), 382, 392 for idiopathic restrictive motor, 145, 146147 for peripheral arterial conditions, 106
diff use scleroderma, 402t cardiomyopathy, 79 oropharyngeal, 145, 146, 148 for peripheral neuropathy, 631b
digoxin for lower urinary tract infections, 698 dysthymia for thoracic outlet compression
for atrial fibrillation, 22 for LV dysfunction, 76, 86 characteristics, 607 syndrome, 109
786 INDEX
electron beam computed tomography, 36t, Enterococcus faecium, 345 erythropoietic protoporphyria, 669 febrile neutropenia, 489490
37, 689 Enterocytozoon bieneusi (Microsporidia), Escherichia coli, 163164, 301, 302t, 328 aminoglycoside for, 249
electrophysiologic (EP) testing, 12, 1718, 129 esophageal carcinoma, 662 amoxicillin for, 490
26, 2830 enteroviruses, 251t, 337, 405 esophageal eosinophilia, 148 antimicrobial therapy for, 249
Enbrel (etanercept), 251 eosinophilia esophageal webs, 146b, 148 complications, emergencies, 489490
encephalitis adrenal crisis and, 453 esophagitis hyponatremia and, 490t
acyclovir treatment, 338 allergic eosinophilia, 58 Candida esophagitis, 148, 264265, infections associated with, 249250
Behet disease and, 216, 393 Aspergillus and, 262 312f, 318 febrile transfusion reactions, 510
from CMV, 266 causes of, 587588, 588b dysphagia and, 146f felodipine, 22, 22t, 74
cytomegalovirus and, 266 esophageal eosinophilia, 148 eosinophilic esophagitis, 148 Felty syndrome, 241, 380, 380b, 530
Epstein-Barr virus and, 265 idiopathic hypereosinophilia, 58 erosive esophagitis, 671 femoral aneurysm, 98
HSV encephalitis, 265, 337, 614 idiopathic pulmonary hemosiderosis HSV and, 128 fibromuscular dysplasia, 115t
inclusion body encephalitis, 339 and, 218 medication-induced, 149 fibromyalgia
Japanese encephalitis virus, 337t nasal eosinophilia, 579 medication-induced esophagitis, 149 diagnosis, 359360
meningoencephalitis, 216, 337, 666 neoplastic eosinophilia, 58 reflux esophagitis, 149 in HIV infection, 406b, 407
mumps meningoencephalitis, 269 peripheral blood eosinophilia, 560, Zollinger-Ellison syndrome and, natural history, 360
paraneoplastic limbic encephalitis, 641 596b, 668 153154 1990 classification criteria, 360b
progressive multifocal leukoencephalitis, peripheral eosinophilia, 166, 211, 290, esophagus. See also gastroesophageal reflux symptoms, 359
317 368, 402, 554, 663 disease treatment, 360
simplex encephalitis, 265 pleural fluid eosinophilia, 243 abnormalities in scleroderma, 59 fi rst-degree AV block, 18
subacute sclerosing panencephalitis, pulmonary eosinophilia, 211 Candida albicans and, 129 fi rst heart sound, 32f, 33
339, 614 tropical eosinophilia, 592 Crohn disease involvement, 125 Fitz-Hugh-Curtis syndrome, 299
Toxoplasma gondii encephalitis, 312t, eosinophilic endocarditis, 79 cytomegalovirus and, 128 fi xed drug eruptions, 586
317 eosinophilic esophagitis, 148 dysphagia flecainide
West Nile virus encephalitis, 4t eosinophilic fasciitis, 668 diagnostic scheme for, 146f adverse effects of, 14t
endocarditis. See also infective endocarditis eosinophilic gastroenteritis, 161, 166 mechanical, 145, 147148 properties of, 13t
dental prophylaxis recommendations, eosinophilic granulomatosis with motor, 145, 146147 relative effectiveness of, 13t
351b, 351t polyangiitis (Churg-Strauss oropharyngeal, 145, 146, 148 fluconazole
eosinophilic endocarditis, 79 syndrome), 59, 216, 663 esophageal perforation, 151 for Candida albicans, 129
Libman-Sacks endocarditis, 59 eosinophilic leukemia, 588 function, 145 for candidiasis, 264
Lffler endocarditis, 58 epidemic Kaposi sarcoma, 671 herpes simplex virus and, 128 for coccidioidomycosis, 260
nonbacterial marantic endocarditis, 143 epidermolysis bullosa acquisita, 657, 663 Mallory-Weiss tear, 151 for vulvovaginal candidiasis, 301
prosthetic valve endocarditis, 346t epididymitis, 296, 298t, 299, 302 noncardiac chest pain, 150151 fluoroquinolones
from Q fever, 259 epilepsy. See also seizure disorders nonpancreatic hyperamylasemia and, complications of, 751
in valvular aortic regurgitation, 39 antiphospholipid antibody syndrome 140 for gonococcal infections, 297
endocrine pheochromocytoma, 115t and, 399400 normal motility, 145 for HAP, VAP, HCAP, 328
endocrinology. See also diabetes mellitus; causes, 619 odynophagia for Mycoplasma pneumoniae, 278
lipid disorders; obesity childhood neurologic disorders and, 602 esophageal infections, 148149 for pneumococci, 275
adrenal gland disorders, 452459 ECT and, 607 medication-induced esophagitis, 149 focal nodular hyperplasia, 183
calcium and bone metabolism disorders, EEG evaluation, 614 tumors of, 63 focal segmental glomerulosclerosis, 215,
465471 idiopathic generalized epilepsy, 620 ESRD. See end-stage renal disease 369, 371, 561
and critical illness management considerations, 621 essential thrombocythemia, 538 focal segmental glomerulosclerosis (FSGS),
abdominal compartment syndrome, mitochondrial mutations and, 678 estrogen-containing oral contraceptives, 561
203 neurologic differential diagnosis, 613t 399, 523, 709, 709b follicular carcinoma, 418
fulminant hepatic failure, 202203 pseudoseizures, 619 estrogen replacement therapy food allergies
GI hemorrhage, 201202 status epilepticus, 595, 614, 622 complications of, 463 allergy testing, 584
glucose management, 201 Sturge-Weber-Dimitri syndrome and, contraindications, 81 in chronic urticaria, 582
ovarian disorders, 461464 666 goals in secondary amenorrhea, 463 clinical history, 583
pituitary disorders, 439451 tuberous sclerosis and, 665 LDL-C/HDL-C and, 423 common causes, 583, 583b
testicular disorders, 459461 epoprostenol, 221 for osteoporosis in postmenopausal food-related anaphylaxis, 583584
thyroid gland disorders, 411419 Epstein-Barr virus women, 469 fosamprenavir (FPV), 324t
end-of-life considerations aplastic anemia and, 501 etanercept (Enbrel), 251 fosfomycin, 301
defi nition of death, 778 hepatitis and, 177 ethambutol, 289290 fourth heart sound (S 4), 34
do-not-resuscitate orders, 777 infections caused by, 265266 ethics. See medical ethics fragile X-linked mental retardation
incurable disease, death, 776777 X-linked lymphoproliferative syndrome euthanasia (physician-assisted death), 771, syndrome, 676t
persistent vegetative state, 777 and, 266 771t, 772t, 777778 Framingham criteria for CHF diagnosis,
physician-assisted death, 771, 771t, erectile dysfunction (ED) exogenous hyperthyroidism, 414 67, 67b
772t, 777778 evaluation questions, 702t Extensively drug-resistant tuberculosis Framingham risk score for ischemic heart
withholding/withdrawing treatments, history/physical examination, 702703 (XDR-TB), 283284 disease, 80
777 medical management extramammary Paget disease, 661 Francisella tularensis (tularemia) infection,
end-stage liver disease, complications intracavernosal penile injections, 704 254
ascites, 183184 intraurethral alprostadil, 704 F Friedreich ataxia, 59, 677t
hepatorenal syndrome, 185 PDE-5 inhibitors, 703704 Fabry disease, 558, 631t, 665 frontotemporal dementia, 4t, 617,
portal systemic encephalopathy, testosterone, 704705 factitious disorders, 599, 603 618, 683
185186 nonmedical treatment, 705 factor VII deficiency, 516 FSGS. See focal segmental
spontaneous bacterial peritonitis, physiology, 701702, 701f factor V Leiden, 218, 219b, 523524, glomerulosclerosis
184185 erysipelas, 349 526527, 637 fulminant hepatic failure, 202203
end-stage renal disease (ESRD) erythema marginatum, 664 factor XI deficiency (hemophilia C), 516 fungal pathogens, in AIDS, 129
cardiovascular disease and, 572 erythema migrans, 666 factor XIII deficiency, 513, 516, 517 fungi
long-term dialysis erythema multiforme, 164, 278, 294, 659, famciclovir aspergillosis, 262
complications of, 573 659f, 660, 663 for herpes simplex virus, 265, 294 blastomycosis, 261
overdoses and, 573b erythema nodosum, 4t, 125, 164, 260, 305, for varicella-zoster virus, 267 candidiasis, 263264
statin therapy for slowing, 571 366, 586, 659660, 659f familial adenomatous polyposis, 134135 coccidioidomycosis, 259260
enfuvirtide (T-20), 325 erythematous plaques of the penis, 666 familial hypocalciuric hypercalcemia cryptococcosis, 263
Entamoeba histolytica, 130, 270, 290, 306 erythromelalgia, 112 (FHH), 465466 histoplasmosis, 260261
Enterobacter, 328 erythropoiesis-stimulating agents, 572 familial paraganglioma syndrome, 119 mucormycosis, 250, 264, 428, 580, 581f
Enterococcus faecalis, 345 erythropoietic porphyria, 510, 669 familial precocious osteoarthropathy, 383t sporotrichosis, 261262
INDEX 787
furosemide genetics glucagonoma, 144 hantavirus pulmonary syndrome and,
for acute hemolytic transfusion chromosome abnormalities, 675 glucagonoma syndrome (necrolytic 273
reactions, 509 mitochondrial mutations, 678 migratory erythema), 661, 661f hypersensitivity pneumonitis and, 212
acute interstitial nephritis and, 555b molecular genetic testing, 678 glucocorticoid therapy leptospirosis and, 257
for ascites, 184 multifactorial causation, 678 for low back pain, 361 lumbar puncture and, 614615
causative for secondary hyperuricemia, single gene defects for primary adrenocortical failure, migraine/tension headaches, 623624
388b autosomal dominant, 675, 676t677t 453454 obstructive sleep apnea and, 115t, 120,
for hypercalcemia, 489 autosomal recessive, 675, 677t glucose-6-phosphate dehydrogenase 244b
pancreatitis caused by, 139 X-linked recessive, 675, 677t deficiency (G-6PD), 677t pheochromocytoma and, 115t, 119, 458
for SIADH, 450 genital ulcers and lesions glycoprotein IIb/IIIa inhibitors, 94 pituitary tumors and, 442443
theophylline clearance and, 242 chancroid, 294 goiter, multinodular, 414 potential serious causes, 623b
fusion inhibitors, 323. See also enfuvirtide HSV, 294 gonococcal arthritis, 404 pregnancy and, 120
(T-20) HSV in pregnancy, 294295 gonococcal infections rickettsial infections and, 259
syphilis, 295296 disseminated gonococcal infection, SLE and, 397t
G genitourinary tuberculosis, 283 298299 systemic mastocytosis and, 166
G6PD deficiency, 507 gentamicin gonococcal pharyngitis, 296 thrombocytopenia and, 508
gallbladder carcinoma, 187 for bioterrorism-related infections, 252t treatment regimens, 297t298t toxoplasmosis and, 317
Gardnerella, 300 for gonococcal infections, 297t gonococcal pharyngitis, 296 trigeminal neuralgia, 4t, 625, 647649
Gardner syndrome, 135, 662, 665 for HAP, VAP, HCAP, 328 gonorrhea vasculitis and, 363
gastric cancer, 145, 152, 154156 for tularemia, 254, 280 cervicitis, 294, 296, 299 head and neck malignancy, 486487
gastric carcinoids, types 1, 2, 3, 155 for Yersinia pestis, 280 epididymitis, 296, 298t, 299, 302 health careassociated infections
gastric polyps, 155 GERD. See gastroesophageal reflux disease gonococcal pharyngitis, 296 catheter-related bloodstream infection,
gastric tumors, 152 geriatric assessments, 679687 nongonococcal urethritis, 296, 299 200, 329, 744
gastric ulcers, 151154 advance directives, 680 Goodpasture disease, 218, 560561, 564 common nosocomial pathogens,
gastroduodenal dysmotility syndromes, depression, 679 gout. See hyperuricemia and gout 329330
155 falls, 680681 graft-versus-host disease (GVHD), 668 group B -hemolytic streptococci, 337
gastroenterology. See also colorectal cancer functional status, 679 granulocyte colony-stimulating factor, 380 health careassociated pneumonia, 7,
colonic polyps, 134135 hearing changes, 681 granuloma annulare, 668, 669f 328329, 744
critical illness and medications, 687 granulomatosis with polyangiitis (GPA) hospital-acquired pneumonia, 328329
abdominal compartment syndrome, memory impairment, 682683 (Wegener granulomatosis), ventilator-associated pneumonia, 196,
203 nutrition, 679 215216, 369370 328329, 330
fulminant hepatic failure, 202203 pressure ulcers, 684685 clinical features, 369 health careassociated pneumonia
GI hemorrhage, 201202, 202t sexual function, sexuality, 681682 pathologic diagnosis, 369370 (HCAP), 7, 328329
diverticular disease of the colon, support, 680 treatment and outcome, 370 heart and systemic disease. See also
133134 urinary incontinence, 685686 granulomatous cheilitis, 664 individual diseases
inflammatory bowel disease, 125126, urinary tract infections, 687 granulomatous ILDs AIDS, 60
136, 392 vision changes, 681 hypersensitivity pneumonitis, 212 amyloidosis, 5657
signs/symptoms, exam questions, 4t gestational diabetes, 424, 429 other diseases, 212 ankylosing spondylitis, 59
ulcerative colitis, 126127 gestational hypertension, 120 sarcoidosis, 211212 carcinoid heart disease, 58
gastroesophageal reflux disease (GERD), gestational thrombocytopenia, 522 Graves disease, 413, 414 cardiac trauma, 60
145 giant cell arteritis (temporal arteritis), 216, Group A -hemolytic S pyogenes, 293294 diabetes mellitus, 56, 64
Barrett esophagus, 148150 363365 Group B -hemolytic streptococci, 337 Friedreich ataxia, 59
chronic cough from, 223 classic clinical features, 364b growth hormone (GH) tumors. See hemochromatosis, 58
complications of, 149 clinical features, 364 acromegaly and gigantism hypereosinophilic syndrome, 5859
reflux, 149 diagnosis, 364 gummatous osteomyelitis, 295 hyperthyroidism, 55
testing for, treatment of, 150 outcome, 364365 guttate psoriasis, 655 hypothyroidism, 5556
sleep-related breathing disorder from, pathology, 364 GVHD. See graft-versus-host disease Lyme disease, 60
244b treatment, 364365 gynecomastia Marfan syndrome, 59
gastrointestinal infections Giardia lamblia, 130, 270 causes/diagnosis of, 461 osteogenesis imperfecta, 60
bacterial and toxigenic diarrhea gigantism. See acromegaly and gigantism in elderly/younger men, 413 rheumatoid arthritis, 59
Campylobacter jejuni, 129, 164165, Glanzmann thrombasthenia, 522 etiology, 461 scleroderma, 59
302 glaucoma, 758 gonadotropin deficiency and, 440 systemic lupus erythematosus, 59
causes of, 302t angle-closure glaucoma, 758 male hypogonadism and, 460 heartburn. See gastroesophageal reflux
Clostridium perfr ingens, 303 asthma and, 591 disease
Escherichia coli, 303304 characteristics, 681 H heart disease and pregnancy. See pregnancy
Salmonella infection, 304 diabetes mellitus and, 428 H5N1 (avian influenza A) virus, 272 heart failure, 6568. See also congestive
Shigella species, 304 narrow-angle glaucoma, 236 HACEK endocarditis, 345 heart failure
staphylococcal enterotoxin, 302303 perioperative evaluation for, 730 Haemophilus aphrophilus, 345 developmental stages, 66f
Yersinia enterocolitica, 264, 305 transient ischemic attacks and, 638 Haemophilus ducreyi, 294 diagnosis, 6768
Clostridium difficile, 305 glomerular disease, manifesting with Haemophilus influenzae, 241, 268, 274, differential diagnosis, 68
intra-abdominal abscesses, 306307 nephritic syndrome, 558. See also 276t, 331, 336 Framingham diagnostic criteria, 67b
Listeria monocytogenes, 251t, 304305 polyarteritis nodosa Haemophilus parainfluenzae, 345 in hemochromatosis, 58
parasitic diarrhea, 306 ANCA vasculitides, 560 Haemophilus paraphrophilus, 345 management
Vibrio species, 305 Goodpasture disease, 561, 564 hairy cell leukemia, 529530 outpatient, 67
viral diarrhea, 305306 Henoch-Schnlein purpura, 559 half-and-half nails, 670 pharmacological, 22, 22t, 49t, 68
gastrointestinal ulcerations, 266 IgA nephropathy, 559 Hantavirus, 273 mechanisms, 68
gastroparesis, 155 membranoproliferative GN, 559 hantavirus pulmonary syndrome, 273 myocardial infarction and, 29
gated sestamibi imaging, 37 postinfectious GN, 559 headaches precipitating factors, 68
Gaucher disease, 677t rapidly progressive GN, 560 acute HIV-infection and, 310t presentation, 65, 6667
GBM (glomerular basement membrane) glomerular disease, usually manifesting as acute myeloid leukemia and, 535 right-sided, 49, 58, 63
abnormality-related diseases nephrotic syndrome analgesic-overuse headaches, 625 symptoms prompting hospitalization,
Alport syndrome, 558, 564 focal segmental glomerulosclerosis, 215, clinical scenarios, 624625 67b
thin basement membrane nephropathy, 369, 371, 561 cluster headaches, 624 tachycardia in, 28
564 membranous nephropathy, 562 cryptococcal infections and, 263, 315 in women, 728
generalized anxiety disorder (GAD), 602, minimal change nephropathy, 559, 561 diabetic hypoglycemia and, 427 heart failure with preserved ejection
606, 728729 glomerulonephritis, 217 fibromyalgia and, 359 fraction, 7475
genetic hemochromatosis, 180, 181f glucagon-like peptide-1 analogues, 426 giant cell arteritis and, 364b heart sounds. See also murmurs
788 INDEX
fi rst heart sound, 32f, 33 polyarteritis nodosa and, 560561 Peutz-Jeghers syndrome, 135 cholangiopathy, 179
fourth heart sound, 34 secondary urticaria and, 581 with risk of cancer Coccidioidomycosis infections, 259
opening snap, 34 serologic markers, 174t familial adenomatous polyposis, colonic manifestations, 129
second heart sound, 32f, 34 time after HBV infection, 174f 134135 Cryptococcus neoformans disease, 263,
systolic clicks, 98 vasculitis and, 406 Gardner syndrome, 135 315316
third heart sound, 34, 60 viral arthritis and, 405 Turcot syndrome, 135 cryptosporidiosis, 319
Helicobacter pylori infection, 81, 145, 151 hepatitis C virus (HCV), 176177 hereditary spherocytosis, 507 Cyclospora infection, 319
associated diseases, 151152 anti-HCV results interpretation, 176t herpes gestationis, 657658 cytomegalovirus, 316, 316t
diagnostic tests for, 152153, 152t blood transfusion complications and, herpes hepatitis, 177 enteric disease, 318
epidemiology of, 151 500t herpes simplex encephalitis, 265, 337, 614 interstitial lung disease, 207
the organism, 151 chronic hepatitis and, 171t herpes simplex virus (HSV), 250, 265 isosporiasis, 319
treatment of, 153 mimicking of autoimmune diseases AIDS and, 128129 lung abscess, 281
HELLP (hemolysis elevated liver enzymes by, 406 Candida esophagitis with, 264 microsporidiosis, 319
and low platelet count) syndrome, mixed essential cryoglobulins in, 563 description, 294 mucocutaneous candidiasis, 318
120121, 522 MPGN and, 559 odynophagia and, 249 Mycobacterium avium complex
helminths, 269270 natural history, 177f oral ulcerations in, 249 infection, 314315
hematology. See benign hematology; hepatitis E virus (HEV), 177 organ transplant infections and, 250t Nocardia infections, 256
bleeding disorders; malignant hepatocellular carcinoma, 183 in pneumonia, 272 Pneumocystis pneumonia, 313314
hematology; platelet disorders; hepatology, 169187. See also hepatology, in pregnancy, 294295 progressive multifocal
thrombophilia specific diseases psoriasis and, 655 leukoencephalopathy, 318
hematopoietic stem cell transplants, 503 abnormal liver tests interpretation, 169 treatment for, 128129, 251, 265, 294 pulmonary hypertension, 179
hemochromatosis, 58, 383384 algorithms, 172 herpes viruses. See cytomegalovirus; respiratory disease, 275
hemodynamic status assessment commonly used tests Epstein-Barr virus; herpes simplex rheumatologic manifestations, 406407
(performance), 199200, 199f alkaline phosphatase, 169 virus; human herpesvirus 6; human Salmonella infection, 318319
hemoglobin H disease, 498 aminotransferases, 169 herpesvirus 8; varicella-zoster syphilis, 316317
hemolytic anemias, 502, 503508 bilirubin, 169170 hirsutism toxoplasmosis, 317318, 317b
autoimmune hemolytic anemia, prothrombin time, albumin, 170 causes of, 662 tuberculosis, 283, 314
505506 hepatology, specific diseases Cushing syndrome and, 454 viral arthritis, 405
causes, 503 acute liver failure, 182 endometriosis and, 712t vulvovaginal candidiasis, 264, 301
Coombs-negative hemolytic anemias, alcoholic liver disease erythropoietic porphyria and, 669 Hodgkin disease
506 alcoholic cirrhosis, 178179 hyperprolactinemia and, 444 acquired ichthyosis and, 622
diagnosis, 503504 alcoholic hepatitis, 178 polycystic ovary syndrome and, 464, 707 bleomycin lung toxicity and, 209
G6PD deficiency, 507 autoimmune hepatitis, 177178 His-Purkinje system, 15f, 1819, 2526, breast cancer and, 476t
hereditary spherocytosis, 507 biliary tract disease 27f complications, 530
intravascular hemolysis vs extravascular bile duct stones, 187 Histoplasma capsulatum, 260261 Cotswolds staging classification, 531t
hemolysis, 505 gallbladder carcinoma, 187 histoplasmosis, 250, 260261 Cryptococcus neoformans and, 263
paroxysmal nocturnal hemoglobinuria, gallstones, cholecystitis, 186187 HIV-associated nephropathy (HIV-AN), diagnosis, 530
507 malignant biliary obstruction, 187 563 differential diagnosis, 714
thrombotic microangiopathies, cholestatic disorders, 171, 172f HIV infection, 308327. See also HIV eosinophilia and, 587
507508 chronic cholestatic liver disease infection, antiretroviral agents; immunodeficiency and, 251t
hemolytic uremic syndrome (HUS), 508, primary biliary cirrhosis, 179 HIV infection, associated inflammatory pericarditis and, 62
563564 primary sclerosing cholangitis, infections and conditions microcytic anemias and, 497
hemophilia A and B, 515516 179180 adult AIDS-defi ning conditions, 311b pericarditis and, 62
classification, 515 drug-induced liver injury, 182183 AIDS-associated malignancies, 319320 screening, 475
clinical features, 515516 end-stage liver disease complications aplastic anemia and, 501 treatment, 530
complications of treatment, 516 ascites, 183184 clinical clues, 255, 310b WHO classification, 532b
inheritance, 516 hepatorenal syndrome, 185 cutaneous manifestations of, 670671 honey-bee stings, 584
management, 516 portal systemic encephalopathy, epidemiology of, 308 hookworm (Necator americanus), 270
hemophilia C (Factor XI deficiency), 516 185186 fibromyalgia in, 406b, 407 hormone replacement therapy. See also
hemorrhagic cerebrovascular disease spontaneous bacterial peritonitis, gestational thrombocytopenia and, 522 estrogen replacement therapy
cerebellar hemorrhage, 640 184185 laboratory diagnosis, 309 for ACTH deficiency, 440
intracerebral hemorrhage, 612, 640 fulminant hepatic failure, 202203 malignant melanoma and, 653 for hypothyroidism, 416, 417
subarachnoid hemorrhage, 614, 638, hepatocellular disorders, 170171 natural history, 310 hornet stings, 584
640641 hereditary liver diseases primary care, 311313 hospital-acquired pneumonia (HAP),
Henoch-Schnlein purpura, 559 genetic hemochromatosis, 180, 181f psoriasis and, 310b, 671 328329
heparin-induced thrombocytopenia (HIT) Wilson disease, 180182 risk of acquiring, by exposure type, 309t hospital medicine
anticoagulant management, 521 jaundice, 171172 symptom frequency, associated fi ndings, admission considerations
clinical presentation, 520521 liver tumors, 183 310t alcohol withdrawal treatment, 742
dos and dont of, 521b nonalcoholic fatty liver disease, 179 transmission of, 308309 cross-cultural awareness, 741
laboratory testing, 521 viral hepatitis HIV infection, antiretroviral agents geriatric assessment, 743744
pathophysiology, 521 other causes, 177 chemokine coreceptor antagonists, intellectual disabilities, 741
rare presentations, complications, 521 type A, 173 323, 325 medication reconciliation, 742
type I and II, 520 type B, 173176, 174f, 175f, 175t fusion inhibitors, 323 nutritional assessment, 742743
hepatitis A vaccine, 695 type C, 176177 guidelines for use of, 325326 complications
hepatitis A virus (HAV), 170t, 171t, 173, type D, 176 HIV replication cycle, 320 catheter-associated UTIs, 746747
501, 695 type E, 177 integrase inhibitors, 323 catheter-related bloodstream
hepatitis B vaccine, 175, 696 hepatopulmonary syndrome (HPS), 214 nonnucleoside analogue reverse infections, 745746
hepatitis B virus (HBV), 173176 hepatorenal syndrome (HRS), 185, 553 transcriptase inhibitors, 322323 falls, 744745
agents for treatment, 175t hepatosplenic candidiasis, 264 nucleoside, nucleotide analogue reverse health careassociated pneumonia,
blood transfusion complications and, hereditary angioneurotic edema (HANE), transcriptase inhibitors, 320322 746
509t 582 postexposure prophylaxis hospital-acquired diarrhea, 746
cryoglobulinemia and, 406 hereditary hemorrhagic telangiectasia recommendations, 326327 hospital-acquired infections, 745
HIV infection and, 325 (Osler-Weber-Rendu syndrome), protease inhibitors, 323 pressure ulcers, 744
immune complex-mediated arthritis 214, 664, 677t viral load, resistance testing, 327 venous thromboembolism, 745
and, 406 hereditary pancreatitis, 142, 143 HIV infection, associated infections and continuous quality improvement
MPGN and, 559 hereditary polyposis syndromes conditions medication safety, 750751
phases of, 175f with no risk of cancer B henselae infections, 255 patient safety, 750
INDEX 789
hospital medicine (Cont.) ACTH deficiency and, 440 secondary hypertension, 115t, 117118 diagnosis, 430
patient satisfaction, 750 aldosterone deficiency and, 453 special cases etiology, 429
cytochrome P450 interactions, 753t diagnosis, 545, 546f breastfeeding, 121 insulinoma, 430
discharge considerations GH deficiency and, 440 hypertensive crisis, 121 pancreatic endocrine tumors and, 144
departure against medical advice, 755 medication causes of, 571 pregnancy, 6062, 64 postprandial hypoglycemia, 430
disease/medication-specific, 754755 renal parenchymal disease, 119 in thoracic aortic aneurysm, 98 in pregnancy, 61
health care worker risks, 751752, 754 risk factors, 192 in thoracic aortic atherosclerosis, 105 hypokalemia
surgical complications treatment, 94, 108, 545547 in thoracic aortic dissection, 104b diagnosis, 544, 545f
of bariatric surgery, 749 hyperlipidemias. See also treatment gastroparesis and, 155
ileus, 747 hypercholesterolemia goals, 116 hyperglycemic hyperosmolar nonketotic
oliguria, 748, 748b carotid artery disease and, 108 lifestyle modifications, 117, 117t coma and, 428
postoperative delirium, 747748, chronic hepatitis and, 171t pharmacological, 56, 117 hypertension and, 115
747b chronic pancreatitis and, 142 hyperthyroidism, 412415. See also nephrogenic DI and, 446
postoperative fever, 748 clinical features, 420 hyperparathyroidism primary aldosteronism and, 119,
postoperative MI, 749 in diabetes mellitus, 56, 429 causes, specific 456457
pulmonary, 748 diagnosis, 420 exogenous hyperthyroidism, 414 secretory diarrhea and, 160
stress GI tract ulcers, 748 DVT/pulmonary embolism and, 219 Graves disease, 413 torsades de pointes and, 28
hot tub folliculitis, 349 giant cell arteritis and, 365f multinodular goiter, 414 toxic megacolon and, 126
house dust mite sensitivity, 578, 580 heart transplant and, 74 painless lymphocytic thyroiditis, treatment, 73, 544
Howell-Jolly bodies, 502 ischemic heart disease and, 81 413414 Y enterocolitica and, 164
HPV vaccine, 695 nonalcoholic fatty liver disease and, 179 subacute painful thyroiditis, 414 hyponatremia (water excess), 541542
HTLV-I and II. See human T-cell primary hyperlipidemias, 421t toxic thyroid adenoma, 414 ACTH deficiency and, 440
lymphotropic virus (HTLV)-I secondary hyperlipidemias, 422b clinical features, 413 cortisone deficiency and, 453
and -II SLE and, 395 diagnosis, 413 Coxiella burnetii and, 279
human herpesvirus 6 (HHV-6), 268 therapy for, 422423, 423t effects on the heart, 55 diabetic ketoacidosis and, 427
human herpesvirus 8 (HHV-8), 268, 671 hypernatremia (water deficiency), 542 etiology, 412 diagnosis, 542, 542t
human parvovirus B19, 501 congestive heart failure and, 740 oropharyngeal dysphagia from, 146b febrile neutropenia and, 490t
human T-cell leukemia, 269 diabetes insipidus and, 544 secondary hyperparathyroidism, 571 myxedema coma and, 417
human T-cell lymphotropic virus diagnosis, 543, 543f treatment SIADH and, 416, 450451, 542
(HTLV)-I and -II, 269 drug-induced causes of, 752t radioactive iodine, 414415 therapy, 542, 542t
Humira (adalimumab), 251 liver failure and, 740 supportive therapy, 415 vWD and, 515
hydralazine osmotic diuresis and, 543 thionamides, 414 hypoparathyroidism, 115t
for dilated cardiomyopathy, 7374 seizure disorders and, 619 hypertriglyceridemia clinical features, 467
for hypertension in pregnancy, 61, 62 SIADH and, 740 acute pancreatitis and, 140 diagnostic approach, 468
hydrocephalus hyperparathyroidism bariatric surgery and, 434 differential diagnosis, 468
cerebellar hemorrhage and, 640 apatite microcrystals and, 384 cardiovascular disease and, 572 etiology
communicating hydrocephalus, 626, CPPD and, 389 hyperlipidemia and, 420, 422b pseudohypoparathyroidism, 467
640 familial hyperparathyroidism, 465 obesity and, 433, 433b, 437 pseudopseudohypoparathyroidism,
dementia and, 613, 617 hypercalcemia and, 488 treatment, 423 467
dysequilibrium and, 628 hypertension and, 120 hypertrophic cardiomyopathy, 17, 32, 676t therapy, 468
normal-pressure hydrocephalus, 618, pituitary tumors and, 443 anatomical, pathophysiologic processes, hypopituitarism
682 primary hyperparathyroidism, 465 70t critical features
obstructive hydrocephalus, 442, 448, surgical intervention for, 466t diagnostic testing, 76, 77f, 78 acute illness, 440
626 secondary hyperparathyroidism, 115t, differential diagnosis, 39 chronic illness, 440
Paget disease and, 470 434, 436, 470, 572 dynamic LV outflow tract obstruction, diagnosis
hyperaldosteronism, 452 Zollinger-Ellison syndrome and, 153 76b ACTH axis, 441
hyperamylasemia, 140 hyperphosphatemia, 571 pathophysiology, 75 documentation, 440441
hypercalcemia, 488489, 556 hyperplastic polyps, 155 physical examination, 7576 gonadotropin axis, 441
management, 467 hyperprolactinemic syndrome. symptoms, 75 growth hormone, 441
PTH-dependent, 465466 See prolactinoma and treatment, 78, 78f prolactin, 441
PTH-independent, 466467 hyperprolactinemic syndrome hypertrophic obstructive cardiomyopathy, radiologic evaluation, 441
hypercapnic respiratory failure, 193 hypertension 32 TSH axis, 441
hypercholesterolemia in aortic root dilatation, 39 hypertrophic osteoarthropathy, 385 etiology, 439
atherosclerosis and, 82, 637 in atrial fibrillation, 21 hyperuricemia and gout, 387388 therapy
autosomal dominant defects and, 675 causes clinical manifestations, acute gout, ACTH deficiency, 442
diagnosis, 420, 422 drugs, 116t 387388 GH deficiency, 442
evaluation recommendations, 420 secondary, 115t points of importance, 389 gonadotropin deficiency, 442
familial hypercholesterolemia, 421t chronic mesenteric ischemia and, 131 predisposing factors, 387 TSH deficiency, 442
hypothyroidism and, 55 classification, 18+ years old, 115t secondary hyperuricemia, causes, 387 hyporeninemic hypoaldosteronism, 545,
nephritic syndrome and, 558 in coarctation of the aorta, 53 treatment 547
nephrotic syndrome and, 558 initial evaluation for acute gouty arthritis, 388389 hypothyroidism, 415417
hypereosinophilia syndrome, 5859, 587 lifestyle, CV risk factors, 114115 during intercritical period, 389 apatite microcrystals and, 384
hyperglycemia target organ damage, 115116, 116t uric acid pathway enzyme abnormalities, clinical features, 415416
gastroparesis and, 155 kidney treatment and, 570 387 cystic fibrosis and, 241
hyperglycemic hyperosmolar nonketotic measurement, classification, 114 hypervolemic hyponatremia, 541 diagnosis, 71, 411413, 416
coma and, 428 renovascular hypertension, 118119 hypoalbuminemia, 291 etiology, 415
hypertension and, 115t S2 influenced by, 33 hypochondriasis, 603 heart-related influences
microcirculation damages from, 428 secondary causes hypochondrogenesis, 383t effects on the heart, 55
nonalcoholic fatty liver disease and, 179 coarctation of the aorta, 115t, 120 hypocomplementemic vasculitis, 372 heart failure, 70
obesity and, 437 Cushing syndrome, 115t, 120 hypogammaglobulinemia, 580 hypertension, 115t, 120
primary aldosteronism and, 119 fibromuscular dysplasia, 115t hypoglycemia physical examination, 56
protease inhibitors and, 323, 324t hyper-/hypoparathyroidism, 115t in diabetes, 424427 symptoms, 55
type 1 diabetes and, 424 obstructive sleep apnea, 115t, 120 dumping syndrome and, 155 treatment, 57
type 2 diabetes and, 425 pheochromocytoma, 115t, 119120 glucose management, 201 miscellaneous circumstances
hyperglycemic hyperosmolar nonketotic primary aldosteronism, 115t, 119 myxedema coma and, 417 myxedema coma, 417
coma, 428 renal parenchymal disease, 115t, 119 in nondiabetic patients subclinical hypothyroidism, 417
hyperkalemia renovascular hypertension, 118 clinical features, 429430 T4 replacement in cardiac disease, 417
790 INDEX
T4 replacement in elderly patients, 417 radionuclide imaging, 37 HACEK endocarditis, 345 pulmonary fibrosis, 210
T4 replacement in pregnancy, 416 gated sestamibi imaging, 37 mitral valve prolapse and, 46 of known cause
oropharyngeal dysphagia from, 146b myocardial perfusion imaging, 37 modified Duke criteria diagnosis, 340b connective tissue disease related, 208
polymyalgia-like syndrome and, 362 radionuclide angiography, 37 native valve endocarditis, 342t344t inflammatory myopathies, 208
secondary hyperuricemia and, 388b imipenem, 328 prosthetic valve endocarditis, 340341, rheumatoid arthritis, 208
symptoms and signs, 416b immune complex-mediated arthritis, 406 346t, 347t348t scleroderma, 209
treatment, 416 immune reconstitution inflammatory subacute bacterial endocarditis, 47, 51, systemic lupus erythematosus, 208
hypotonic beer ingestion, 541 syndrome, 314 345, 378 lymphangioleiomyomatosis, 213
hypoxemic respiratory failure, 193 immunosuppressive medications, infection inferior vena cava interruption, 220 pneumoconioses
hysterectomy associations, 250251, 251t infertility (female) asbestos-related, 210
for abnormal uterine bleeding, 708 implantable devices chlamydia and, 299 silicosis, 210
for cervical cancer, 480 cardiac pacemaker, implantation, cystic fibrosis and, 241 pulmonary alveolar proteinosis, 213
for endometriosis, 712 1617, 17t endometriosis and, 711 pulmonary Langerhans cell
post-surgery estrogen therapy, 720 cardiovascular device infections, 346, gonadotropin deficiency and, 439 histiocytosis, 212213
for uterine fibroids, 713 349b, 350f gonorrhea and, 296 interstitial pancreatitis, 139
implantable cardioverter-defibrillator, Hodgkin lymphoma and, 530 intestinal lymphangiectasia, 166
I 17 hyperprolactinemia and, 444, 449, 463 intestinal pseudo-obstruction (nontoxic
ibutilide, 13t, 14t implantable loop event recording, 12 maternal hypothyroidism and, 711 megacolon), 133
ichthyosis, acquired, 662 inclusion body encephalitis (subacute pelvic inflammatory disease and, 299 intimate partner violence, 729
ICU-related bleeding disorders, 203204 sclerosing panencephalitis), 339 polycystic ovary syndrome and, 464 intra-abdominal abscesses, 306307
idiopathic acute interstitial nephritis, 554 indinavir (IDV), 324t smoking and, 710 intracerebral hemorrhage, 612, 640
idiopathic AIDS enteropathy, 128 infectious arthritis, 403, 407 uterine fibroids and, 712713 intracranial aneurysm, 566
idiopathic ARDS, 21 infectious syndromes, from specific infertility (male) intracranial lesions
idiopathic autoimmune microorganisms cystic fibrosis and, 241, 245 cortical lesions, 626
thrombocytopenia, 522 bacteria hypogonadism and, 460 leptomeningeal lesions, 625
idiopathic avascular necrosis of the femoral Actinomyces israelii, 254 testosterone and, 704 parasagittal lesions, 626
head, 383 Actinomyces species, 254 inflammatory bowel arthritis syndrome, intrinsic renal AKI
idiopathic bilateral hyperplasia, 456 Bartonella species, 255 372, 392 acute interstitial nephritis, 554555
idiopathic bronchiolitis obliterans, 211 Brucella, 255 inflammatory bowel disease acute phosphate nephropathy, 555
idiopathic calcium urolithiasis, 759 Clostridium botulinum, 163, 252t, arthritis associated with, 372, 392 acute tubular necrosis, 553554
idiopathic chronic pancreatitis, 143 255 breast cancer and, 136 acute uric acid nephropathy, 555
idiopathic crescentic glomerulonephritis, Clostridium tetani, 255256 extraintestinal manifestations, 125126 atheroembolic disease, 554
370 Corynebacterium diphtheria, 256 indications for colonoscopy, 126 contrast-induced nephropathy, 553554
idiopathic dilated cardiomyopathy, 6970 Corynebacterium jeikeium, 249 inflammatory myopathies, 403, 634635 crystal deposition due to medication or
idiopathic eosinophilic disorder, 587 Legionella, 251t acute alcoholic myopathy, 635 toxins, 555
idiopathic generalized epilepsy, 620 Listeria, 251t childhood type, 403 hypercalcemia, 556
idiopathic hypereosinophilic syndrome, Mycobacterium species, 251t dermatomyositis, 403 pigment nephropathy, 554
588 Nocardia, 251t, 256257 electrolyte imbalance, 635 iodoquinol, 270
idiopathic hyperprolactinemia, 445 Streptococcus mitis, 249250 endocrine diseases, 635 ipratropium, 239
idiopathic hypothalamic diabetes fungi malignancy-related myositis, 403 iron deficiency anemia, 497498
insipidus, 448 aspergillosis, 262 overlap connective tissues disease, 403 irritable bowel syndrome, 132133
idiopathic interstitial lung diseases blastomycosis, 261 polymyositis, 403 ischemia (of the colon)
acute eosinophilic pneumonia, 211 candidiasis, 263264 statin-induced myopathy, 635 acute ischemia, 131
acute interstitial pneumonia, 211 coccidioidomycosis, 259260 infl iximab (Remicade), 251 anatomical review, 131
cryptogenic organizing pneumonia, 211 cryptococcosis, 263 influenza A strains, 273 chronic mesenteric ischemia, 131132
DIP/RB-ILD, 211 histoplasmosis, 260261 influenza vaccine, 694 ischemic acute tubular necrosis
nonspecific pneumonia, 210211 mucormycosis, 264 insulinoma, 144, 430 (ATN), 553
pulmonary fibrosis, 210 sporotrichosis, 261262 integrase inhibitors, 323. See also ischemic cardiomyopathy, 17
idiopathic intracranial hypertension, 614 parasites raltegravir ischemic cerebrovascular disease
idiopathic livedo reticularis, 111 helminths, 269270 interstitial lung diseases (ILDs), 205213 carotic endarterectomy, 638
idiopathic LV tachycardia, 16t protozoan parasites, 270271 categories, 205 carotid angioplasty with stent
idiopathic lymphedema syndromes, 218 rickettsiae, 259 causes of, 206b placement, 638
idiopathic nephrotic syndrome, 561 spirochetes diagnosis pathophysiologic mechanisms, 637
idiopathic orthostatic hypertension, 161t leptospirosis, 257 histopathology studies, 208 risk factors, 637638
idiopathic pseudo-obstruction, 167 Lyme disease, 257259 history, 205206 transient ischemic attacks, 638
idiopathic pulmonary embolism, 527 viruses imaging studies, 206207 treatment, 638639
idiopathic pulmonary fibrosis (IPF), 206, herpesviruses, 264268 laboratory studies, 207 ischemic colitis, 131
210, 225, 376b HTLV-I and II, 269 physical examination, 206 ischemic heart disease, 8097. See also
idiopathic pulmonary hemosiderosis measles (rubeola), 268 pulmonary function studies, 206 chronic stable angina
(IPH), 218, 219b, 223 mumps, 268269 drug-/therapy-induced acute coronary syndromes, 89
idiopathic pulmonary hypertension, 291 parvovirus B19, 269 amiodarone, 209 ST-segment elevation MI, 9197
idiopathic restrictive cardiomyopathy, rubella, 268 bleomycin lung toxicity, 209 unstable angina, nonST-segment
7879 infective endocarditis, 44t chemotherapy, radiotherapy, 209210 elevation MI, 8991
idiopathic stabbing headache, 624 bacterial endocarditis, prevention, 349 illicit substances, 209 atherosclerosis, mechanisms, 82
idiopathic thrombocytopenic purpura, cardiac valve replacement surgery, 345b methotrexate, 209 coronary artery spasm, 89
312f, 396397, 518 causative pathogens nitrofurantoin, 209 prevention, 8082
idiopathic trigeminal neuralgia, 625 B henselae, B quintana, 255 granulomatous ILDs risk factors, 8081, 81b
idiopathic ulcerative colitis, 164 Candida, 264 hypersensitivity pneumonitis, 212 stages of vascular injury, 82f
idiopathic viral pericarditis, 62 Coxiella burnetii, 259, 279, 340, 341b other diseases, 212 isolated nodal osteoarthritis, 382
IgA nephropathy, 559 enterococci, 345 sarcoidosis, 211212 isoniazid, 289
ILDs. See interstitial lung diseases Moraxella catarrhalis, 278 idiopathic ILDs, 206b itraconazole
iliac artery aneurysms, 105 non-influenza Haemophilus species, acute eosinophilic pneumonia, 211 for allergic bronchopulmonary
imaging, cardiac examination 345 acute interstitial pneumonia, 211 aspergillosis, 262
coronary angiography, 36 Staphylococcus aureus, 341 cryptogenic organizing pneumonia, for blastomycosis, 261
echocardiography, 3637 Streptococcus bovis, 132 211 for coccidioidomycosis, 260
electron beam computed tomography, 37 viridans group streptococci, 345 DIP/RB-ILD, 211 for sporotrichosis, 262
magnetic resonance imaging, 37 culture-negative endocarditis, 341b nonspecific pneumonia, 210211 Ixodes tick, 271, 666
INDEX 791
J Legionella species, 251t, 274 indications for, 614615 for seizure disorders, 619
jackhammer disease, 402 leg ulcer, 113, 113t in seizure disorders, 621 for spinal cord lesions, 613
Japanese encephalitis virus, 337t leiomyosarcomas, 214, 266 in spinal cord metastasis, 642 for thoracic aortic aneurysm, 99f
jugular venous pressure Leishmania braziliensis, 271 lung abscess, 281 for thyrotropin-producing tumors, 447
carcinoid heart disease and, 58 Leishmania donovani, 271 lung cancer for trauma, 612
congestive heart failure and, 67b Leishmania mexicana, 271 bloody eff usion in, 243 for trigeminal neuralgia, 625
constrictive pericarditis and, 63 leishmaniasis, 261, 271 bullous lung disease and, 238 for vascular diseases, 612
dilated cardiomyopathy and, 70 Leishmania tropica, 271 central diabetes insipidus and, 449 for white matter lesions, 613
evaluation, 31, 31f leptomeningeal lesions, 625 characteristics, histologic types, 482 major depressive disorder. See depressive
postcardiotomy syndrome and, 88 leukemia Cushing syndrome and, 455 disorders
in pregnancy, 60 acute myelogenous leukemia, 507 HIV/AIDS and, 31, 292 malabsorption
prerenal AKI and, 552 acute myeloid leukemia, 507, 535537 natural history, 482 in chronic pancreatitis, 43
restrictive cardiomyopathy and, 79 chronic lymphocytic leukemia, 388b, primary (x-rays), 226f in Crohn disease, 126
right ventricular infarction and, 96 505, 528529 problem magnitude, 482 in cystic fibrosis, 143
tamponade and, 62 eosinophilic fasciitis and, 402 risk factors, 435, 482 due to small intestine diseases
juvenile idiopathic arthritis, 393 eosinophilic leukemia, 588 rounded atelectasis and, 210 amyloidosis, 166167
esophageal infections and, 148 screening, 482, 689690 celiac disease, 165
K febrile neutropenia and, 249, 490t silicosis and, 210 eosinophilic gastroenteritis, 166
Kaposi sarcoma hairy cell leukemia, 529530 staging, 225, 238, 482 intestinal lymphangiectasia, 166
in AIDS patients, 291, 308, 311b, 312 human T-cell leukemia, 269 treatment, 482483 systemic mastocytosis, 166
description, 319 lymphocytic leukemia, 251t nonsmall cell lung cancer, 482483 tropical sprue, 165
differential diagnosis, 255 pericarditis and, 62 small cell lung cancer, 483 Whipple disease, 165166
pleural eff usion in, 292 pleural eff usion and, 243b lupus erythematosus (LE), 666 in Mycobacterium infection, 129
pneumothorax from, 291 progressive multifocal lupus nephritis, 396, 563 malaria, 271, 378b, 504, 505f
treatment options, 319 leukoencephalopathy and, 338 Lyme carditis, 60 male hypogonadism, adults, 459461
Kaposi sarcoma-associated virus (HHV-8), promyelocytic leukemia, 518 Lyme disease, 257259 clinical features, 460
268 secondary hyperuricemia and, 368b causes, 60 diagnosis, 460
ketoconazole, 129 secondary osteoporosis and, 468 clinical syndromes, 257258 etiology
kidney function, evaluation. See also secondary vasculitis and, 367 diagnosis, 258 central hypogonadotropism, 460
chronic kidney disease sweet syndrome and, 662 effects on the heart, 60 hypogonadotropic hypogonadism,
estimated GFR T-cell LGL leukemia, 530 epidemiology, 257 460
cystatin C, 568 T-cell prolymphocytic leukemia, 532 prevention, 258259 primary hypergonadotropic testicular
formula, 567 leukocytoclastic vasculitis, 372 treatment, 258 failure, 460
serum creatinine, 568 Lewy body dementia, 4t, 618, 646t, 683 lymphangiectasis, 219 hypergonadotropic hypogonadism,
measured GFR, 568 Lewy body disease, 618 lymphangioleiomyomatosis, 206, 212213, 459460
normal function, 567 Libman-Sacks endocarditis, 59 221b, 225 treatment, 461
normal functioning kidney, 567 light chain deposition disease, 565 lymphangioma, 219 malignancy-related myositis, 403
renal imaging Lindsay nails, 670 lymphangiomatosis, 218 malignant biliary obstruction, 187
arteriography, venography, 569 linear IgA bullous dermatosis, 658 lymphedema, 112113, 166, 168, 218, 478 malignant hematology
CT, 569 lipid disorders. See also lymphocytic interstitial pneumonitis, acute leukemias, 535536
DTPA, 569 hypercholesterolemia; 231, 291 chronic myeloid disorders, 536538
excretory urography, 569 hyperlipidemias lymphocytic leukemia, 250, 251t, 388, 505 lymphoproliferative disorders, 528533
gallium, indium scans, 569 clinical features, 420 lymphocytic thyroiditis, painless, 413414 plasma cell disorders, 533535
hippuran renal scanning, 569 diagnosis, 420, 422 lymphoproliferative disorders malignant melanoma, 63, 653654
MRI, 569 drug therapy, 422423 chronic lymphocytic leukemia, 528529 malignant otitis externa, 757
radiography, 569 etiology, 430 hairy cell leukemia, 529530 malingering, 599, 604
ultrasonography, 569 lifestyle changes, 422 Hodgkin lymphoma, 530531 Mallampati classification, airway
urinalysis, 568569 therapy, 422 large granular lymphocyte syndrome, management, 192f
discoloration causes, 569t treatment, 140, 324t, 420, 421t, 423 530 MALT lymphoma, 151, 152, 154, 532b,
Kingella species, 345 Lisch nodules of the iris, 665 non-Hodgkin lymphomas, 531533 533
Klebsiella pneumoniae, 301, 328 Listeria, 251t mania. See bipolar disorder and mania
Klinefelter syndrome, 676t Listeria monocytogenes, 251t, 304305, 336 M maraviroc (MVC), 326
Kniest dysplasia, 383t listeriosis, 250, 336337 macrocytic anemias Marfan syndrome, 383t, 676t
koilonychia (spoon nails), 670 livedo reticularis, 111112, 112f, 372 folate deficiency, 501 aortic root dilatation in, 39
lobular carcinoma (breast cancer), 476, vitamin B12 deficiency, 499500 effects on the heart, 59
L 476f macular degeneration. See age-related mitral valve prolapse in, 4546
labetalol, 104b locked-in syndrome, 617 macular degeneration pregnancy contraindication in, 6061,
Lambert-Eaton syndrome, 487 Loeys-Dietz syndrome, 98, 100 magnetic resonance imaging (MRI) 64
lapatinib, 479 Lffler endocarditis, 58 for adrenal incidentaloma, 459 thoracic aortic aneurysm and, 98
laryngeal tuberculosis, 283 Lfgren syndrome, 663 for adrenocortical failure, 453 mastocytosis, 587
latent syphilis, 295 long QT syndrome, 12, 17, 28f for aortic dissection, 102f, 104f measles (rubeola), 268
leaflets type mitral regurgitation, 44t long-term dialysis in ESRD for aortic regurgitation, 43f mechanical dysphagia, 145, 147148
left ventricular ejection fraction (LVEF), complications of, 573 for bacterial meningitis, 332f mechanical ventilation, for respiratory
17 overdoses and, 573b for breast cancer, 475476, 479 failure, 195198
left ventricular hypertrophy (LVH) loop diuretics, 467, 489, 542, 570 for cavernous hemangioma, 183 complications of, 196, 198
acute aortic regurgitation and, 40 lopinavir/ritonavir (LPV/r), 324t for cervical spondylosis, 629 intrinsic PEEP, 196
aortic dissection and, 102 lower esophageal ring (Schatzki ring), 148 for dementia, 613, 618 oxygen toxicity, 196
aortic stenosis and, 38, 39 lower urinary tract symptoms (LUTS), for disk evaluation, 613614 tracheostomy, 196, 198
coarctation of the aorta and, 53 697, 698t for erectile dysfunction, 703 ventilation-associated pneumonia,
exercise stress testing and, 83 lumbar puncture for hepatocellular carcinoma, 183 196
GH tumors and, 445 in Alzheimer disease, 682 for intracranial tumors, 613 modes of ventilation, 196
heart failure and, 66f, 70 in bacterial meningitis, 331, 332f for male hypogonadism, 460 CPAP, 197t
hypertension and, 115 in cryptococcal infections, 263, 315 for meningeal metastases, 642 initial, invasive settings, 197t
hypertrophic cardiomyopathy and, 75, in dementia diagnosis, 618 for normal pressure hydrocephalus, 618 positive end-expiratory pressure, 196
76, 77f in HIV-infection with syphilis, 317 for pheochromocytomas, 458 pressure control, 196, 197t
left ventricular myocardial dysfunction, 65 in neurological disorders for pituitary tumors, 443, 446 PSV, 197t
Legionella, 251t contraindications for, 615 for pulmonary conditions, 225 volume control, 196, 197t
792 INDEX
weaning from, 198 urinary tract infection and, 302 treatment, 45 in cavernous hemangioma, 183
Meckel diverticulum, 167 erectile dysfunction types of, 44t in chronic severe aortic regurgitation,
medical ethics, 769778 evaluation questions, 702t mitral stenosis 43f
beneficence principle, 770 history/physical examination, diagnosis, 4344, 44f in community-acquired bacterial
end-of-life considerations 702703 etiology, pathophysiology, 42 meningitis, 332f
defi nition of death, 778 medical management, 703705 left atrial tumors in, 63 in craniopharyngioma, 448
do-not-resuscitate orders, 777 nonmedical treatment, 705 physical examination, 42 in Cushing syndrome, 454, 456
incurable disease, death, 776777 physiology, 701702, 701f severe, pregnancy contraindication, 60 in dementia, 613
persistent vegetative state, 777 menstruation symptoms, 42 for focal cerebral, cerebellar processes,
physician-assisted death, 777778 amenorrhea and, 461 treatment, 44 614
withholding/withdrawing cancer antigen 125 and, 484 mitral valve prolapse in GH tumors, 446
treatments, 777 genetic hemochromatosis, 180 pathophysiology, nature history, 4546 in gonadotropin-producing tumors, 447
ethical dilemmas, 769 gonorrhea and, 298 physical examination, 46 in hepatocellular carcinoma, 183
nonmaleficence, applications iron deficiency and, 497 treatment, 4647, 49t in hypopituitarism, 441
confl ict of interest, 770 phases, 706 mixed connective tissue disease, 399 in intracranial tumors, 613
the impaired physician, 770 premenstrual syndrome and, 706 MMR vaccine, 695 in neurological disorders, 614
nonabandonment, 770 toxic shock syndrome and, 352 mnemonic memory devices in normal-pressure hydrocephalus, 618
rule of double effect, 770771 meperidine (Demerol), 141 for anion gap metabolic acidosis, 548, in peripheral artery disease, 106
patient autonomy meropenem, 328 549 in pheochromocytoma, 458
advance directives, 773 metabolic acidosis. See also anion gap for asthma, contributors of, 591, 591b in pituitary incidentalomas, 447
confidentiality, 775 metabolic acidosis for causes of aseptic necrosis of bone, in spinal cord compression, 490
conscientious objection, 773 acute kidney injury and, 556 384b in spinal cord lesions, 613
informed consent, exceptions, CKD and, 572 for causes of chylous eff usion, 243, 244 in thoracic aortic aneurysm, 99
774775 defi ned, 547 for causes of hypochromic microcytic in thyrotropin-producing tumors, 447
medical errors, 775 diabetic ketoacidosis and, 427 anemias, 497 in vascular diseases, 612
nonbeneficial treatment requests, GI hemorrhage and, 201 for heart sounds, valve sequence, 33 in white matter lesions, 613
775776 postoperative ileus and, 747 for hypochromic microcytic anemias, mucocutaneous candidiasis, 318
promoting, preserving, 771, 773 sepsis and, 200 497 mucormycosis (Rhizopus species,
surrogate decision making, 773774 metabolic syndrome for malignant melanoma, 654 Zygomycetes), 264
treatment refusal, 775776 defi nition, 114115 for MGUS/smoldering myeloma, 534 multidrug-resistant tuberculosis
truth telling, therapeutic privilege, heart failure and, 66f for plasma cell proliferative disorder, 533 (MDR-TB), 283
775 hypertension and, 637 for predominant upper lung opacities, multifocal motor neuropathy, 629, 630t
principles ischemic heart disease and, 8081, 81b 207 multinodular goiter, 414
beneficence, 770 lifestyle modification for, 117 for Wegener granulomatosis, clinical multiple endocrine neoplasia (MEN), 119
medullary carcinoma, 418 management, 81 features, 215, 369 multiple epiphyseal dysplasia (autosomal
medullary thyroid carcinoma, 119 uric acid stones and, 759 Mobiluncus species, 300 dominant), 383t
Megasphaera species, 300 metformin, 426 Model for End-Stage Liver Disease multiple myeloma, 56, 533534
membranoproliferative glomerulonephritis methicillin-resistant S aureus, 275, 328, (MELD) scoring system, 214 multiple-organ dysfunction syndrome
(MPGN), 559 349 MODS. See multiple-organ dysfunction (MODS), 200
membranous nephropathy, 562 methimazole, 414 syndrome multiple sclerosis, 146b, 647649
meningitis methotrexate, 379, 380 molluscum contagiosum, 671 multisystem organ failure, 200
acquired bacterial meningitis, methotrexate-induced ILDs, 209 monoclonal gammopathies of mumps, 268269, 405
276t277t, 331, 332f, 333t methyldopa, 62 undetermined significance, 533 mumps meningoencephalitis, 269
aseptic meningitis syndrome, 337338 metoprolol, 22, 104b mononucleosis, infectious, 265 murmurs, 3435, 35f
chronic meningitis syndrome, 338 metronidazole mood disorders, 599601. See also anxiety diastolic, 98
Coccidioides meningitis, 260 for bacterial vaginosis, 300 disorders; depressive disorders, evaluation recommendation, 35f
meningococcal meningitis, 277t, 331, for Entamoeba histolytica, 130, 270 adjustment disorder regurgitant, amyloidosis in, 56
335336 for Giardia lamblia, 130 with anxious mood, 602 muscle diseases
pneumococcal meningitis, 331, 336 for trichomoniasis, 300 with depressed mood, 600 acute muscle weakness, 635636
tuberculous meningitis, 283 mexiletine, 13t, 14t bipolar disorder, mania, 600601, 606 inflammatory myopathies, 403,
from untreated sinusitis, 580 MI. See myocardial infarction from general medical conditions, 601 634635
meningococcal meningitis, 277t, 331, microcytic anemias, 497498 substance-induced, 601 acute alcoholic myopathy, 635
335336 iron deficiency, 497498 Moraxella catarrhalis, 241 electrolyte imbalance, 635
meningococcal vaccine, 695 thalassemias, 498 morbilliform skin reaction, 586, 660 endocrine diseases, 635
meningoencephalitis, 216, 337 typical features of MCV, 498t motor dysphagia, 145, 146147 statin-induced myopathy, 635
menopause. See also perimenopause vitamin C deficiency, 498 motor neuron disease myasthenia gravis, 146b, 231, 549, 617,
breast cancer and, 476t microscopic polyangiitis, 218219, amyotrophic lateral sclerosis, 4t, 146b, 633, 634
endometrial cancer and, 713, 714b 366368, 368t 237, 629 mycobacterial and fungal joint infections
gout and, 388 clinical features, 366367 multifocal motor neuropathy, 629, 630t infected joint prosthesis, 405
hallmark symptoms, 719720 diagnosis, 367 movement disorders. See also Parkinson spinal septic arthritis, 405
HDL-C/LDL-C and, 423 features of, 368t disease mycobacterial infections. See pulmonary
hormone therapy, 720 outcome, 368 botulinum toxin therapy, 647 mycobacterial infections
osteoporosis and, 469 pathology, 366 essential tremors, 644645 Mycobacterium avium, 287288,
postmenopausal bleeding, 720 treatment, 367368 tremors, 644 314315
primary osteoarthritis and, 362 midodrine, 30 moxifloxacin, 274 Mycobacterium intracellulare, 314315
related terms, 719b migraine and tension headaches, 623624 MPGN. See membranoproliferative Mycobacterium kansasii, 287288
secondary amenorrhea, 462463 migratory polyarthralgias, 404 glomerulonephritis Mycobacterium leprae, 287
uterine fibroids and, 712 miliary tuberculosis, 282 MRI (magnetic resonance imaging) Mycobacterium species, 251t
mens health milrinone, 73 in abdominal aortic aneurysm, 101 Mycobacterium tuberculosis, 281284,
benign prostatic hyperplasia minimal change nephropathy, 559, 561 in acute aortic dissection, 104f 286287
differentiation difficulty, 484 minimally conscious state, 616 in Addison disease, 453 mycophenolate mofetil
evaluation, 699700 mitral regurgitation, 33 in ADH deficiency, 449 for cicatricial pemphigoid, 657
history/physical examination, differential diagnosis, 39 in adrenal gland disorders, 453 for classic polyarteritis nodosa, 367
697699 etiology, pathophysiology, 4445 in adrenal incidentaloma, 459 for microscopic polyangiitis, 367
medical management, 700701 management, severe patients, 46f in adult male hypogonadism, 460 T-cellmediated infections from, 250
overactive bladder and, 685 physical examination, 45 in brain trauma, 612 Mycoplasma pneumoniae, 274, 506
overflow incontinence and, 686 symptoms, 45 in breast cancer, 475476, 479 mycosis fungoides, 532b, 654, 655
INDEX 793
myelofibrosis presyncopal light headedness, neuropathy arthropathy (Charcot joint), nonulcer dyspepsia, 151
postpolycythemic myelofibrosis, 627628 384 Noonan syndrome, 52
537538 vertigo, dizziness, 626627 neurosyphilis, 295 nordihydropyridines (calcium channel
postthrombocythemic myelofibrosis, spinal level neutropenia, 264 blockers), 23. See also diltiazem;
537538 degenerative diseases, 623b, 630 NICE-SUGAR (Normoglycemia in verapamil
primary myelofibrosis, 537538 motor neuron disease, 629, 630t Intensive Care Evaluation normal-pressure hydrocephalus, 618, 682
myeloplastic syndromes, 501, 536 myelopathy, causes, 628629 Survival Using Glucose Algorithm normocytic anemias, 501
myocardial infarction (MI), 44t radiculopathy, 629 Regulation) trial, 201 Normoglycemia in Intensive Care
amiodarone for, 13 supratentorial level nicotine-replacement therapy, 756 EvaluationSurvival Using
-blockers for, 94 acute confusional states, 604, 614, nifedipine, 22 Glucose Algorithm Regulation
case fatality rate, 81f 617, 622, 683 nitrates (NICE-SUGAR) trial, 201
nitroglycerin for, 94 brain death, 614, 616, 778 for angina, 86 nosocomial pathogens, common
nonST-segment elevation MI, 8991 dementia, 617619 for coronary artery spasm, 89 coagulase-negative staphylococci, 249,
ST-segment elevation MI, 9197 headaches, facial pain, 622625 high dose, for dilated cardiomyopathy, 301, 330, 335t, 340341, 346t
U.S. data, 92 intracranial lesions, 625626 73 Staphylococcus aureus, 329330
myocardial ischemia, 82 locked-in syndrome, 617 nitric oxide (NO), 195 Stenotrophomonas maltophilia, 330
myocardium type mitral regurgitation, 44t minimally conscious state, 616 nitrofurantoin-induced ILDs, 209 nucleoside, nucleotide analogue reverse
myopathies persistent vegetative state, 617, 772t, nitroglycerin, 83, 86, 94, 150 transcriptase inhibitors,
drug-induced, 403 777 Nocardia infections, 213, 250t, 251t, 320322
inflammatory seizure disorders, 619622 256257, 261, 338 nystatin, 129
childhood type, 403 stupor and coma, 617 Nocardia pneumonia, 280
dermatomyositis, 403 ventricular system, 626 nonalcoholic fatty liver disease (NAFLD), O
malignancy-related myositis, 403 neurological disorders, categorized by 179 obesity
overlap connective tissues disease, 403 mechanism, 637650 nonallergenic rhinitis, 578 candidiasis and, 263
polymyositis, 403 cerebrovascular disease non-anion gap acidosis, 547. See also chronic hepatitis and, 171t
myotonia dystrophica, 146b hemorrhagic cerebrovascular disease, metabolic acidosis; renal tubular DVT/pulmonary embolism and, 219
myotonic dystrophy, 676t 640 acidoses health risk assessment for, 432
myxedema coma, 417 ischemic cerebrovascular disease, nonarticular rheumatism, 359372 heart failure and, 66f
637640 bursitis, 361362 hyperlipidemia and, 428t
N inflammatory/autoimmune disorders fibromyalgia, 359360 hypertension and, 114
NAFLD. See nonalcoholic fatty liver critical illness polyneuropathy, 649 low back pain, 360361, 361b hypertriglyceridemia and, 437
disease multiple sclerosis, 647649 polymyalgia rheumatica, 362363 hyperuricemia and, 387, 388b
narcotic addiction. See substance use neurology of sepsis, 649 vasculitic syndromes, 363372 ischemic heart disease and, 80, 81b
disorders neuromyelitis optica, 649 nonbacterial (thrombotic) marantic management
nasal polyposis, 579 septic encephalopathy, 649 endocarditis, 143 bariatric surgery, 433435
nasopharyngeal carcinoma, 266 movement disorders noncardiogenic syncope, 30 nutrition, 435437
natalizumab (Tysabri), 251 botulinum toxin therapy, 647 nonchlamydial nongonococcal urethritis, weight loss medications, 432433
nateglinide, 426 essential tremors, 644645 296 natriuretic peptide and, 68b
Necator americanus (hookworm), 270 Parkinson disease, 645647 nondiarrhea-associated hemolytic uremic nonalcoholic fatty liver disease and, 179
necrobiosis lipoidica diabeticorum, 668, tremors, 644 syndrome (D-HUS), 563564 sleep-related breathing disorders and,
669f neoplastic disease nonepileptic seizures (pseudoseizures), 619 120, 244, 245
necrolytic migratory erythema brain metastasis, 642 nonerosive nonspecific chronic gastritis, obesity-hypoventilation syndrome, 245
(glucagonoma syndrome), 661, 661f cancer treatment complications, 643 154 obsessive-compulsive disorder (OCD),
necrotizing fasciitis, 349 paraneoplastic disorders, 643, 643b, nongonococcal bacterial arthritis, 404 602603, 606
necrotizing pancreatitis, 139, 141, 144 643t nongonococcal urethritis, 296, 299 obstructive hydrocephalus, 442, 448, 626
Neisseria gonorrhoeae, 296, 298. See also primary CNS neoplasms, 640641 non-Hodgkin lymphoma. See also obstructive lung diseases, 238244. See
gonorrhea spinal cord metastasis, 642 cutaneous T-cell lymphoma also asthma; chronic obstructive
nelfi navir (NFV), 324t in systemic cancer patients, 641642 aggressive lymphomas, 532533 pulmonary disease
neoplastic disease neurological disorders, diagnosis in AIDS patients, 312 bronchiectasis
brain metastasis, 642 cerebrospinal fluid analysis, 614615 extranodal B-cell variant, 292 causes, associations, 242243
paraneoplastic disorders, 643, 643b, clinical evaluation, 611 in HIV infection, 312, 319320 complications, 242
643t history, 612b immunodeficiency and, 588 treatment, 242243
primary CNS neoplasms, 640641 localization of disorders, 612b low-grade lymphomas, 531532 bullous lung disease, 238, 239
spinal cord metastasis, 642 CT/MRI diagnostic testing obstructive lymphedema and, 112 cystic fibrosis, 143144, 223, 231f,
in systemic cancer patients, 641642 CTI/MRI comparison, 613b paraneoplastic disorders and, 643 241242, 287
neoplastic eosinophilia, 58 dementia, 613 Sjgren syndrome and, 381 distinguishing features, 238
neuraminidase inhibitors, 273. See also intracranial tumors, 613 nonischemic cardiomyopathy, 17 etiology, 239
oseltamivir; zanamivir spinal cord, 613 nonmelanoma skin cancer, 653, 654 pleural eff usion
neurocysticercosis, 269270 spine, 613614 nonnucleoside analogue reverse causes, 242, 243b
neurofibromatosis, 665 trauma, 612 transcriptase inhibitors, 322323, exudate/transudate, distinctions,
1 and 2, 677t vascular diseases, 612 322t 242243
in pheochromocytoma, 119 white matter lesions, 613 nonocclusive ischemic, 131 pleural fluid parameters, 243244
plexiform neurofibroma, 666f differential diagnosis formulation, nonpancreatic hyperamylasemia, 140 thoracentesis, complications of, 244
neurogenic thoracic outlet syndrome, 110 613t nonrheumatic atrial fibrillation, 23t obstructive lymphedema, 112
neurological disorders, anatomical EEG studies, 614 non-small cell lung cancer, 482483 obstructive sleep apnea (OSA)
involvement, 616636. See also electromyography studies, 614 nonsteroidal anti-inflammatory drugs defi nition, associations, 244
neurological disorders, categorized lumbar puncture (NSAIDs) GH tumors and, 446
by mechanism; neurological contraindications for, 615 for bypass arthritis, 393 hypertension and, 115t, 120, 637
disorders, diagnosis indications for, 614615 for fibromyalgia, 360 obesity and, 432, 433b
peripheral level nerve conduction studies, 614 for osteoarthritis, 385 Parkinson disease and, 647
acute muscle weakness, 635636, neuromuscular transmission disorders peptic ulcers from, 151, 153 pheochromocytoma and, 458
636b botulism, 252t, 634 for small cell vasculitis, 371 screening for, 730, 737
muscle diseases, 403, 634635 Lambert-Eaton myasthenic syndrome, nonST-segment elevation MI, 8991 treatment, 245
peripheral neuropathies, 630634 487, 488t, 633, 634, 643b nontoxic megacolon (intestinal pseudo- obstructive sleep apnea (OSA) hypopnea
posterior fossa level myasthenia gravis, 146b, 237, 549, obstruction), 133 syndrome, 244
brainstem lesions, 626 617, 633 nontuberculous mycobacteria (NTM), oculopharyngeal myopathy, 146b
cerebellar lesions, 626 neuromyelitis optica, 649 287289 odynophagia
794 INDEX
AIDS-related GI tract symptoms and, paraneoplastic syndromes, 487488, ovarian cancer basal ganglia abnormality and, 616, 628
128 488t cancer antigen 125, 483484 cytarabine (ara-C) neurotoxicity and,
Candida infections and, 129, 264, 318 prostate cancer, 112, 468, 484486, CKD complications and, 572 644t
CMV and, 128 485t outcome, 484 differential diagnosis, 644t
esophageal infections and, 148149 skin cancer, 529, 653 screening for, 484, 693 of plus syndromes, 646t
GERD with, 149 small cell lung cancer, 483 staging, 483 drug-related causes of, 644t, 645t
HSV infections and, 128129, 249 testicular cancer, 486 treatment, 484 mood disorders and, 601
medication-induced esophagitis, 149 thyroid cancer, 417418 ovarian disorders motor manifestations, 645t
oligoarthritis, asymmetric, 666 onycholysis, 655, 670 amenorrhea, 461463 management of, 646647, 646t
omalizumab, 594 opening snap (heart sounds), 34 polycystic ovary syndrome, 463 nonmotor manifestations, 645t
oncology, 475493 ophthalmology. See also retinitis; management of, 648t
breast cancer retinopathy P oropharyngeal dysphagia and, 146b
ductal/lobular carcinomas, 476, 476f age-related macular degeneration, pacemaker-mediated tachycardia, 17 secondary pseudo-obstruction and, 167
follow-up after curative therapy, 758759 Paget disease paromomycin
479480 glaucoma, 758 cutaneous manifestations, 661 for Cryptosporidium, 129
inflammatory bowel disease and, 136 red eye, 757758 diagnosis, 470 for Entamoeba histolytica, 270
natural history, prognostic factors, opioid analgesics, 385386 heart failure and, 69t paroxysmal nocturnal dyspnea, 42, 6768
477478 oral aphthous ulceration, 664 increased bone turnover in, 469 paroxysmal nocturnal hemoglobinuria,
pathology, 476 orbital/periorbital cellulitis, 580 sacroiliac involvement in, 392 507
plain chest radiography evaluation, organic solvents-related scleroderma, 402 secondary osteoarthritis and, 383 paroxysmal supraventricular tachycardia,
223 oropharyngeal dysphagia, 145, 146, 146b, therapy, 470 13, 24
problem magnitude, 475 148 Paget-Schroetter syndrome (subclavian parvovirus
recurrence patterns, 480 oseltamivir, 273 vein thrombosis), 110 focal segmental glomerulosclerosis
risk factors, 463, 465, 475, 476t Osler-Weber-Rendu syndrome (hereditary painless lymphocytic thyroiditis and, 561
screening, 223, 475476 hemorrhagic telangiectasia), 664, (postpartum thyroiditis), 413414 hemolytic anemia and, 504
staging, 476, 477b 677t palpable purpura, 372 rheumatoid arthritiss mimicking of, 407
cancer pain, 491493 osmotic diuresis, 428, 543 pamidronate, 479 parvovirus B19 infection, 269, 353, 378,
carcinoma of unknown primary origin, osteoarthritis pancreas, 139144 501
487 clinical features, 381382, 382f embryological development, 139 Pasteurella multocida, 350, 352353
cervical cancer, 312, 480, 716717 clinical subsets hemochromatosis involvement, 58 patent ductus arteriosus, 51
colorectal cancer apatite microcrystals, 384 susceptibility in cytomegalovirus, 128 patient autonomy considerations
diagnosis, 136137 avascular necrosis, 384385 pancreatic carcinoma, 131, 143 advance directives, 773
epidemiology, etiology, 135 erosive osteoarthritis, 382 pancreatic cholera, 144 confidentiality, 775
fecal occult blood testing for, 480 hemochromatosis, 383384 pancreatic cysts, 119 conscientious objection, 773
genetic factors, 135136 hypertrophic osteoarthropathy, 385 pancreatic endocrine tumors, 144 informed consent, exceptions, 774775
pathology, prognostic indicators, 136 isolated hip arthritis, 382 pancreatic phlegmon, 141 medical errors, 775
postoperative management, no isolated nodal osteoarthritis, 382 pancreatitis. See also acute pancreatitis; nonbeneficial treatment requests,
metastases, 137 neuropathy arthropathy, 384 chronic pancreatitis 775776
prevention strategy, 137138, 137t, primary osteoarthritis, 382 hereditary pancreatitis, 142, 143 promoting, preserving autonomy, 771,
138t secondary osteoarthritis, 382383 interstitial pancreatitis, 139 773
risk factors, 136, 480481 Wilson disease, 384 necrotizing pancreatitis, 139, 141, 144 surrogate decision making, 773774
staging and survival, 481t pathogenesis, 381 in pheochromocytoma, 119 treatment refusal, 775776
treatment, 137 radiographic features, 385 in ulcerative colitis s, 119 truth telling, therapeutic privilege, 775
complications, emergencies therapy for, 385386 panic disorder, 244, 601602, 606, PAVMs. See pulmonary arteriovenous
febrile neutropenia, 489490 osteogenesis imperfecta 728729 malformations
hypercalcemia, 488489 characteristics, 383t PAP. See pulmonary alveolar proteinosis pelvic inflammatory disease, 131, 254, 294,
spinal cord compression, 490491 effects on the heart, 60 papillary carcinoma, 417418 297t, 299300
tumor lysis syndrome, 489 osteoid osteoma, 393 papillary muscle rupture, 44t pemphigus vulgaris, 659, 663
endometrial cancer, 713714, 714b osteomalacia, 469470 para-articular osteoporosis, 386 penicillin-resistant S pneumoniae, 275
gastric cancer, 145, 152, 154155, clinical features, 470 paraganglioma. See pheochromocytoma, penile erythematous plaque, 666
154156 defi nition/etiology, 469470 paraganglioma peptic ulcer disease (PUD), 145, 151, 153
head and neck malignancy, 486487 therapy for, 470 Paragonimus westermani (paragonimiasis), percutaneous balloon valvuloplasty, 44, 52
hereditary polyposis syndromes, with osteomyelitis, 330, 349b, 353355, 384 290 percutaneous coronary intervention (PCI)
risk of cancer, 135 Candida osteomyelitis, 264 paraneoplastic disorders for chronic stable angina, 8687
lung cancer gummatous osteomyelitis, 295 cancer/syndromes antibody associations, intracoronary stent placement during,
bloody eff usion in, 243 osteoporosis, 468469 643t 87
bullous lung disease and, 238 ankylosing spondylitis and, 392 carcinoid syndrome, 487 for ST-segment elevation MI, 95
central diabetes insipidus and, 449 characteristics, 468 classification of, 488t, 643, 643b, 643t percutaneous transluminal coronary
characteristics, histologic types, 482 clinical features, 469 dermatomyositis, 488 angioplasty (PTCA), 8687
Cushing syndrome and, 455 Cushing syndrome and, 455 Lambert-Eaton syndrome, 487 perianal fistulas, 664
HIV/AIDS and, 31, 292 diagnosis, 469 paraneoplastic pemphigus, 663 perianal skin tags, 664
natural history, 482 etiology, 468 paraneoplastic limbic encephalitis, 641 periarticular osteoporosis, 378
primary (x-rays), 226f gonadotropin deficiency and, 440 paraproteinemia-associated renal diseases pericardial disease
problem magnitude, 482 male hypogonadism and, 460 amyloidosis, 5657, 166167, 534535, acute/subacute inflammatory
risk factors, 435, 482 para-articular osteoporosis, 386 565 pericarditis, 62
rounded atelectasis and, 210 periarticular osteoporosis, 378 light chain deposition disease, 565 constrictive pericarditis, 6263
screening, 482 prevention, treatment, 469 multiple myeloma, 56, 533534, pericardial eff usion, 56, 62
silicosis and, 210 primary hyperparathyroidism and, 466 564565 pericardial tamponade, 31, 62, 69t, 88,
nonmelanoma skin cancer, 653, 654 secondary, causes of, 468b parasagittal lesions, 626 96t, 102
non-small cell lung cancer, 482483 thiazolidinediones use and, 426 parasites pericardial tuberculosis, 283
ovarian cancer, 125, 483484, 572 ostium primum atrial septal defect, 50t helminths, 269270 perimenopause, 718719, 728
cancer antigen 125, 483484 ostium secundum atrial septal defect, 50t protozoan parasites, 270271 perinuclear ANCA (p-ANCA), 215216
CKD complications and, 572 otitis externa, acute and malignant, 757 pulmonary parasitic diseases, 290291 peripheral arterial conditions
outcome, 484 otorhinolaryngology parasitic diarrhea, 306 acute arterial occlusion, 107108
screening, 484 otitis externa, 757 Parkinson dementia, 4t peripheral artery aneurysms, 105
staging, 483 pharyngitis, 757 Parkinson disease peripheral artery disease, 105107,
treatment, 484 rhinosinusitis, 756757 antidepressants and, 606 116t, 422
INDEX 795
peripheral artery disease (PAD), 105107, prolactinoma, hyperprolactinemic varicella pneumonia, 272 pregnancy
116t, 422 syndrome, 444445 ventilator-associated pneumonia, 196, cardiac disease and, 6062, 64
ABI screening for, 106107 pituitary tumors 328329, 330 gestational diabetes and, 424, 429
differential diagnosis, 106t ACTH-producing tumors, 447 pneumonitis HELLP syndrome in, 120121
grading system, lower-extremities, 106t clinical features Q fever with, 259 hypertension and, 710
intermittent/pseudoclaudication endocrine associations, 443 from sporotrichosis, 261 immunizations and, 710
differential diagnosis, 106t hypersecretory states, 443 polio physiologic changes of, 60
medical management, 107 hypopituitarism, 443 oropharyngeal dysphagia from, 146b postpartum depression and, 599600,
symptoms, 105106, 107 inferior tumor extension, 442 postpolio syndrome, 245 728
peripheral neuropathies lateral tumor extension, 442 vaccine for, 338, 696 preconception counseling, 710
acute inflammatory demyelinating superior tumor extension, 442 poliovirus, 338 preeclampsia and, 120
polyradiculoneuropathy, 632 diagnosis, 443 pollen allergy, 580 SLE and, 396
autonomic neuropathy, 633 ectopic GH, GHRH tumor, 447 polyarteritis nodosa (PAN), 366368, T4 replacement, 416
chronic demyelinating neuropathies, GH-tumors: acromegaly, gigantism, 368t, 560561 thrombocytopenia and, 522
632 445447 characteristics of, 560 thromboembolic disease and, 710711
clinical features, 630t631t gonadotropin-producing tumors, 447 clinical features, 366367 thyroid disorders and, 711
diabetic neuropathy, 633 pituitary incidentalomas, 447 diagnosis of, 367, 561 venous thromboembolism and, 710
differential diagnosis, 630t631t therapy features of, 368t premature ventricular contractions, 13
evaluation of, 631b comorbidities, 447 HIV-associated vasculitis and, 406 premenstrual dysphoric disorder (PDD),
mononeuropathy, 632 medical therapy, 446447 mortality-related factors, 368b 707
mononeuropathy multiplex, 632 radiotherapy, 446 outcome, 367368 premenstrual syndrome (PMS)
neuromuscular transmission disorders, surgery, 446 pathology, 366 differential diagnosis, 706
146b, 487, 488t, 633634, 643b plague (Yersinia pestis), 252t, 254 rheumatoid vasculitis and, 376 management, 706707
painful neuropathy, 632633 plague vaccination, 696 scleritis and, 758 preoperative evaluation
pregabalin treatment, 359 plasma cell disorders (monoclonal Sjgren syndrome and, 381 anesthesia/surgical risk assessment,
peristomal pyoderma gangrenosum, 664 gammopathies) treatment, 367368 732, 732t
Peromyscus maniculatus, 273 amyloidosis, 534535 polychondritis, 393 cardiac risk assessments
persistent hyperamylasemia, 140 monoclonal gammopathies of polycystic liver disease, 566 coronary stent patients, 737
persistent vegetative state, 617, 772t, 777 undetermined significance, 533 polycystic ovary syndrome (PCOS) noncardiac surgery, 733t
personality disorders, 605606 multiple myeloma, 533534 adnexal mass differentiation, 714b patient-specific, 733
Peutz-Jeghers syndrome, 135, 664 Waldenstrm macroglobulinemia, 534 description, 464 perioperative ischemia monitoring,
pharyngitis, 757 Plasmodium falciparum, 271 endometrial cancer and, 714 736737
acute HIV-1 infection and, 310t Plasmodium knowlesi, 271 female infertility and, 710 resting echocardiography, 735
gonococcal pharyngitis, 296 Plasmodium malariae, 271 hirsutism and, 707 risk reduction strategies, 735736
group A -hemolytic S pyogenes, Plasmodium ovale, 271 secondary amenorrhea and, 462 stepwise approach, 733735
293294 Plasmodium vivax, 271 polycythemia vera, 538 stress test choice, 735
infectious mononucleosis and, 265, 266t platelet disorders, 518522. See also polymyalgia rheumatica, 362363 surgery-specific, 733
M pneumoniae and, 278 thrombocytopenia, due to features, differential diagnosis, 362 goals of, 730
streptococcal pharyngitis, 293 increased platelet destruction giant cell arteritis association, 362 history/review of systems for, 730731
phenytoin, 13t, 56 congenital platelet disorders, 521522 pathogenesis, 362 impression and plan, 731732
pheochromocytoma, paraganglioma, pseudothrombocytopenia, 518 systemic mimicking illnesses, 362b physical examination for, 731
457459 pleural eff usion treatment, 362363 pulmonary risk assessment
clinical features, 458 causes, 242, 243b polymyositis, 403 patient-/procedure-related, 737738
endocrine diagnosis, 458 exudate/transudate, distinctions, polyvinyl chloride disease, 402 procedures, 738
etiology, 457458 242243 popliteal artery aneurysms, 98, 105, 375 risk reduction strategies, 738
radiologic localization, 458 pleural fluid parameters, 243244 popliteal cyst, 375 testing guidelines
therapy, 458459 amylase, 243 porphyria cutanea tarda, 511t, 669670 chest radiography, 740
Philadelphia chromosome-negative cell counts, 243 porphyrias, 510511, 511t coagulation studies, 739
myeloproliferative neoplasms chylous eff usion, 243 porphyria variegata, 511t complete blood count, 740
essential thrombocythemia, 538 cultures, 244 portal systemic encephalopathy, 185186 creatinine, 740
polycythemia vera, 538 cytology, 243244 postcardiotomy syndrome, 88 ECG, 740
postpolycythemic myelofibrosis, glucose and pH, 243 postherpetic neuralgia, 268 electrolytes, 740
537538 pleural biopsy, 244 postinfectious glomerulonephritis, 559 glucose, 740
postthrombocythemic myelofibrosis, pleural tuberculosis, 282 postmyocardial infarction, 62 liver tests, 740
537538 Plummer-Vinson syndrome, 148 postpartum depression, 599600, 728 urinalysis, 740
primary myelofibrosis, 537538 pneumococcal meningitis, 331, 336 postpartum thyroiditis (painless venous thromboembolic prophylaxis,
phosphodiesterase inhibitors, 73, 240. See pneumococcal polysaccharide vaccine, 695 lymphocytic thyroiditis), 413414 738739
also milrinone; theophylline pneumococcal vaccine, 275 postpolio syndrome, 245 prerenal acute kidney injury (AKI),
phototherapy for psoriasis pneumoconioses, 207t, 210 postpolycythemic myelofibrosis, 537538 552553
narrow-band UVB, 655 Pneumocystis jiroveci infection, 250, 275, postprandial hypoglycemia, 430 presyncopal light headedness, 627628
psoralen, ultraviolet A, 655 290 postrenal acute kidney injury (AKI), 556 preventive medicine
ultraviolet light, 655 Pneumocystis pneumonia, 313 poststreptococcal reactive arthritis, 405 ACIP recommendations
physical urticaria, 582 pneumonia. See also community-acquired postthrombocythemic myelofibrosis, hepatitis A vaccine, 695
physician-assisted death (euthanasia), 771, pneumonia; hospital-acquired 537538 hepatitis B vaccine, 696
771t, 772t, 777778 pneumonia posttraumatic stress disorder (PTSD), 602, HPV vaccine, 695
pigment nephropathy, 554 acute eosinophilic pneumonia, 211 606, 728729 influenza vaccine, 694
piperacillin-tazobactam, 328 acute interstitial pneumonia, 211 potassium balance disorders meningococcal vaccine, 695
pituitary disorders, 439451 aspiration pneumonia, 280281 hyperkalemia, 544547 MMR vaccine, 695
adenomas, 153, 442443, 446, 455 from CMV, 266 hypokalemia, 544 pneumococcal polysaccharide
ADH deficiency: diabetes insipidus, cryptogenic organizing pneumonia, 211 potassium iodide, 262 vaccine, 695
448449 health careassociated pneumonia, 7, potassium-sparing diuretics, 545 polio vaccine, 696
ADH excess: SIADH, 449451 328329 prednisone rabies vaccine, 696
hypopituitarism, 439442 HSV in, 272 for giant cell arteritis, 364365 Td, Tdap vaccines, 694695
miscellaneous disorders Klebsiella pneumoniae, 301, 328 for nasal polyposis, 579 varicella vaccine, 695
craniopharyngioma, 447448 Mycoplasma pneumoniae, 274, 506 for polymyalgia rheumatica, 362363 cancer screening
lymphocytic hypophysitis, 448 Nocardia pneumonia, 280 for rheumatoid arthritis, 379 breast cancer, 690691
pituitary apoplexy, 448 nonspecific pneumonia, 210211 preeclampsia, 120, 522 cervical cancer, 693
796 INDEX
colorectal cancer, 691 macroprolactinoma, 445 vulvar itching and, 718 pulmonary diseases, common disorders.
lung cancer, 689690 microprolactinoma, 445 psoriatic arthritis, 392393, 666 See also obstructive lung diseases
ovarian cancer, 693 surgery, 445 psychiatry. See also Alzheimer disease; cough, 223
prostate cancer, 691693 proliferative retinopathy, 428 anorexia nervosa; anxiety exercise testing, 238
immunity, types of, 694 promyelocytic leukemia, 518 disorders; delirium; depressive function tests
immunizations, 693 propafenone disorders indications for, 227228
key concepts adverse effects of, 14t eating disorders, 604, 606, 756 interpretation of PFT results,
bias, 688 properties of, 13t electroconvulsive therapy, 607 235236, 237f
screening test features, 688689 relative effectiveness of, 13t factitious disorders, 603604 patient examples, 237238
types of prevention, 688 propranolol, 22, 104b malingering, 599, 604 provocation inhalation challenge,
potential bioterrorism agents vaccines, propylthiouracil, 414 mood disorders, 599601 228229
696 prostanoids, inhaled, 221 personality disorders, 605606 hemoptysis, 223
U.S. disease burden, 688 prostate cancer pharmacology history/physical examination, 224b
vaccines, types of, 694 follow-up recommendations, 486 antidepressants, 606 imaging diagnosis
Prevotella, 300 hypocalcemia and, 468 antipsychotics, 606607 computed tomography, 225
primary adrenocortical failure (Addison management benzodiazepines, 607 fluoroscopy, 225
disease), 452453 androgen deprivation, 485486 lithium, 607 MRI, 225
primary aldosteronism, 115t, 456457 bisphosphonates, 486 psychotic disorders, 602603 plain chest radiography, 223225
clinical features, 456 chemotherapy, 486 somatoform disorders, 603 pulmonary, bronchial angiography,
differential diagnosis, 457 prostatectomy, 485 substance use disorders, 604605 225226
endocrine diagnosis, 456457 radiation therapy, 485 suicidal patients, 605 radionuclide scans, 225226
etiologic diagnosis, 457 specific stages, 485 psychogenic polydipsia, 541 invasive testing, 238
etiology, 456 obstructive lymphedema and, 112 psychogenic spells (pseudoseizures), 619 percussion, auscultation fi ndings, 225t
therapy for, 457 prostate-specific antigen, 484485 psychotic disorders, 602603 pulmonary embolism, 31
primary biliary cirrhosis (PBC), 179 risk factors, 484 brief psychotic disorder, 603 diagnostic tests, 218220
primary cold agglutinin disease (cold screening for, 691693 psychosis (defi ned), 602 differential diagnosis, 68
agglutinin syndrome), 505506 potential harms, 692 schizophrenia/schizophrenia-like, etiology, 218
primary eosinophilia, 587 recommendations, 692693 602603 hypercapnic respiratory failure and, 193
primary hyperparathyroidism tests, 692 schizophreniform disorder, 603 treatment, 220, 527
clinical features, 465 staging, 485t PTH-dependent hypercalcemia, 465466 Wells probability prediction model, 525t
diagnosis, 465 prosthetic joint infections, 405 familial hypocalciuric hypercalcemia, pulmonary hemosiderosis, idiopathic, 219
etiology, 465 prosthetic valve endocarditis, 340341, 466 pulmonary hypertension (PH), 220222
therapy, 465466 346t primary hyperparathyroidism, 465466 in AIDS patients, 291
primary lymphedema, 112 causative organisms, 346t thiazide-induced hypercalcemia, 466 clinical classifications, 221t
primary myelofibrosis, 537538 treatment, 347t348t PTH-independent hypercalcemia diagnosis, 221
primary osteoarthritis, 382 prosthetic valves Addison disease, 467 hypercapnic respiratory failure and, 193
primary (partial atrioventricular canal) bioprosthetic valves, 4849 granulomatous disorders, 466 pregnancy contraindication in, 6061,
atrial septal defect, 5051 management in pregnancy, 61 hypercalcemia of malignancy, 466 64
primary Raynaud disease, 110111, 111t mechanical valves, 49, 50t hyperthyroidism, 467 sickle cell anemia and, 502
primary sclerosing cholangitis (PSC), protease inhibitors, 323, 324t. See sarcoidosis, lymphoma, 466 treatment, 221222
179180 also atazanavir; darunavir; vitamin D intoxication, 466 pulmonary Langerhans cell histiocytosis
prion-associated diseases, slow viruses fosamprenavir; indinavir; pulmonary alveolar proteinosis (PAP), 213 (PLCH), 212213
Creutzfeldt-Jakob disease, 339 lopinavir/ritonavir; nelfi navir; pulmonary arterial hypertension (PAH), pulmonary lymphatic disorders, 219
progressive multifocal ritonavir; saquinavir; tipranavir 220 pulmonary lymphatic dysplastic
leukoencephalopathy, 251, 311b, proteinuria, 571 pulmonary arteriovenous malformations syndromes, 219
318, 338339 Proteus mirabilis, 301 (PAVMs), 214 pulmonary lymphoid hyperplasia, 291
subacute sclerosing panencephalitis, 339 prothrombin G20210A, 523, 524b, pulmonary artery aneurysm, 214 pulmonary mycobacterial infections
procainamide 526527 pulmonary bacterial infections abdominal tuberculosis, 283
adverse effects of, 14t, 28 protozoan parasites, 270271 aspiration pneumonia, 280281 drug regimens, 284t
for cardiac issues in pregnancy, 61 protozoan pathogens, in AIDS community-acquired pneumonia, extensively drug-resistant tuberculosis,
properties of, 13t Blastocystis hominis, 130 274275 283284
relative effectiveness of, 13t Cryptosporidia belli, 129 antimicrobial therapy, 276t277t genitourinary tuberculosis, 283
in Wolff-Parkinson-White syndrome, Cryptosporidium, 129 Bordetella pertussis, 279 ileocecal tuberculosis, 283
with atrial fibrillation, 27 Entamoeba histolytica, 130 Burkholderia pseudomallei, 280 laryngeal tuberculosis, 283
procoagulant system defects Enterocytozoon bieneusi, 129 causes, 274 miliary tuberculosis, 282
increased VTE risks, 523 Giardia lamblia, 130 chlamydia, 278 multidrug-resistant tuberculosis, 283
inherited risk factors proximal tubular acidosis, 547 Enterobacter, 279 Mycobacterium tuberculosis, 281284,
factor V Leiden, 218, 219b, 523524, pseudoachondroplasia, 383t Francisella tularensis, 279280 286287
526527, 637 pseudocysts, 141 Klebsiella pneumoniae, 279 nontuberculous mycobacteria, 287289
prothrombin G20210A, 523, 524b, pseudogynecomastia, 461 Legionella, 278 pericardial tuberculosis, 283
526527 pseudohyperkalemia, 545 Moraxella, 278 pleural tuberculosis, 282
progressive multifocal pseudohypoparathyroidism, 467 Mycoplasma pneumoniae, 278 skeletal tuberculosis, 282283
leukoencephalopathy, 251, 311b, Pseudomonas aeruginosa, 249, 328 Serratia, 279 tuberculous lymphadenitis, 282
318, 338339 pseudopseudohypoparathyroidism, 467 treatments, 274275 tuberculous meningitis, 283
prolactinoma and hyperprolactinemic pseudoseizures, 614, 619 Yersinia pestis, 280 pulmonary parasitic diseases, 290291
syndrome, 444445 pseudothrombocytopenia, 518 lung abscess, 281 pulmonary shunting, 193
clinical features, 444 pseudoxanthoma elasticum, 663664 Nocardia pneumonia, 280 pulmonary stenosis, 52
diagnosis psoriasis pulmonary blastomycosis, 261 pulmonary valve regurgitation, 58
functional hypothalamic disorders, acute otitis externa and, 757 pulmonary capillary hemangiomatosis, 215 pulmonary vascular disease
444 exam question prep, 4t pulmonary diseases. See also pulmonary alveolar hemorrhage syndromes, 218
organic hypothalamic disorders, HIV-infection and, 310b, 671 diseases, common disorders arterial aneurysm, 214
444445 onycholysis and, 670 interstitial lung diseases, 205213 arteriovenous malformation, 214
pathologic hyperprolactinemia, 444 phototherapy in, 655, 671 respiratory critical care Behet disease, 217
physiologic hyperprolactinemia, 444 psoriatic arthritis and, 392393, 666 airway management, 191192 capillary hemangiomatosis, 215
treatment reactive arthritis and, 392 mechanical ventilation, 195198 Churg-Strauss syndrome, 216
dopamine agonists, 445 secondary hyperuricemia and, 387, 388b respiratory failure, 192195 giant cell arteritis, 216, 363365
idiopathic hyperprolactinemia, 445 targeted therapy in, 655 vascular diseases, 214222 Goodpasture syndrome, 218
INDEX 797
pulmonary vascular disease (Cont.) subjunctival hemorrhage, 757 ophthalmic abnormalities, 377 Schatzki ring (lower esophageal ring), 148
hepatopulmonary syndrome, 214 refeeding syndrome, 437, 743 pulmonary manifestations, 377 Schistosoma cercariae, 270
idiopathic pulmonary hemosiderosis, refractory sinusitis, 580 rheumatoid nodules, 376 Schistosoma haematobium, 304
219 refractory ventricular tachycardia, 2829 rheumatoid vasculitis, 376 Schistosoma japonicum, 290
lymphatic disorders, 219 Reiter syndrome, 205, 296, 666 laboratory fi ndings in, 377378 Schistosoma mansoni (schistosomiasis), 290
microscopic polyangiitis, 218219 relapsing polychondritis, 215, 663 musculoskeletal complications schistosomiasis, 270
Takayasu arteritis, 217218 Remicade (infl iximab), 251 carpal tunnel syndrome, 376 schizophreniform disorder, 603
vascular tumors, 214 renal artery stenosis, 115t, 118119, 457, cervical spine, 375 scleroderma (systemic sclerosis)
vasculitides, 215 548t, 562, 569 popliteal cyst, 375 clinical manifestations
Wegener granulomatosis, 215216 renal insufficiency, chronic, 502 tenosynovitis, 376 articular, 401
pulmonary vascular tumors, 214 renal papillary necrosis, 502, 503 natural history, 373374 cardiac, 401
pulmonary vasculitides, 215 renal parenchymal disease, 115t pathogenesis of, 374 gastrointestinal, 401
pulmonary viral infections, 272274 renal-pulmonary syndromes, 217 positive rheumatoid factorrelated interstitial lung diseases, 209
avian influenza A virus, 272 renal thrombotic microangiopathies, 564 diseases, 378b pulmonary, 401
hantavirus pulmonary syndrome, 273 renal tubular acidoses, 547, 547t radiographic fi ndings of, 378379 Raynaud phenomenon, 401
influenza, 273274 renovascular hypertension, 118119 related conditions renal, 401
severe acute respiratory syndrome, 273 respiratory acid-base alterations, 549550 adult-onset still disease, 380 skin, 400
viral pneumonia, 272 respiratory bronchiolitis-interstitial lung Felty syndrome, 241, 380, 530 diff use scleroderma, fi ndings, 402t
pustular psoriasis, 655 disease (RB-ILD), 211 seronegative rheumatoid arthritis, effects on the heart, 59
pyoderma gangrenosum, 661, 661f, 664 respiratory critical care 379 laboratory fi ndings, 401
pyostomatitis vegetans (gingival airway management, 191192 seronegative rheumatoid arthritis, of treatment, 401
granulomatous inflammation), 664 endotracheal intubation, 193b the elderly, 379380 scleroderma-like syndromes
pyrazinamide, 289 intubation difficulties, 192b Sjgren syndrome, 380381 environment-/occupation-related, 402
Mallampati classification, 192f treatment, pharmacologic, 379 eosinophilic fasciitis, 402
Q mask ventilation difficulties, 192b treatment, surgical, 379 metabolic/other causes, 402403
Q fever, 259 mechanical ventilation, 195198 uveitis and, 393 secondary adrenocortical failure, 452
quality improvement complications of, 196, 198 valvular aortic regurgitation and, 39 secondary hypertension, 115t, 117118
hospital medicine, 750751 modes of, 196, 197t rheumatoid arthritis-related ILDs, 208 secondary lymphedema, 112
LEAN methodology, 759760 weaning from, 198 rheumatoid factornegative (seronegative secondary osteoarthritis, 382383
patient safety, 750, 760762 pulmonary shunting, 193, 195 rheumatoid arthritis), 379 secondary Raynaud phenomenon, 111, 111t
Six Sigma/DMAIC approach, 760 respiratory failure, 192195 rheumatologic manifestations, in HIV secondary (reactive) eosinophilia, 587
tools for ARDS, 194195 AIDS-associated myopathy, 407 secondary syphilis, 295
control chart, 760, 760f hypercapnic, 193 diff use, infi ltrative lymphocytosis secondary urticaria, 581
Pareto chart, 760, 761f hypoxemic, 193 syndrome, 406 second-degree AV block, 1819, 18f, 19f, 29
root cause analysis, 760 response-to-injury hypothesis, for fibromyalgia, 407 second heart sound (S2), 32f, 34
value stream map, 760, 761f atherosclerosis, 82 HIV-associated vasculitis, 406 secundum atrial septal defect, 49
quinidine restrictive cardiomyopathy, 63, 7879 inflammatory articular syndrome, 407 sedative-hypnotic abuse, 605
adverse effects of, 14t, 28 anatomical, pathophysiologic processes, lupus-like illnesses, 406 seizure disorders. See also epilepsy
for cardiac issues in pregnancy, 61 70t reactive arthritis, 406 amantadine/renal disorders and, 274
properties of, 13t causes/categories, 7879 undifferentiated spondyloarthropathy, anticonvulsant therapy
relative effectiveness of, 13t diagnosis, 79 406 antiepileptic drugs, 619621, 620t
differential diagnosis, 79 rhinitis, chronic blood levels, 621
R signs and symptoms, 79 allergy tests, 578b starting and stopping, 621
rabies vaccine, 696 treatment, 79 differential diagnosis, 578b systemic side effects, 620t
radiation colitis, 131 retinitis medical history, 578 causes, 619
radioactive iodine, 414415 chorioretinitis, 266, 294, 316 treatment, 578579 eclampsia and, 120
radiographic contrast media reactions, 587 CMV retinitis, 250, 266267, 311b, 316 rhinitis medicamentosa (nasal spray EEG evaluation, 614
raltegravir (RAL), 325 Toxoplasma chorioretinitis, 270 rebound), 579 isoniazid/neuropathy and, 289
ranolazine (Ranexa), 86 retinitis pigmentosa (NARP), 678, 703 rhinosinusitis, 756757 mefloquine contraindication in, 271
rapidly progressive glomerulonephritis, retinopathy rickettsiae, 259 post-fi rst seizure risk factors, 621b
560 from antimalarial drug treatment, 377 rifampin, 289 pseudoseizures, 614, 619
Raynaud phenomenon, 400 diabetic retinopathy, 424, 428429, 562 RIFLE classification scheme for acute status epilepticus, 595, 614, 622
cryoglobulinemia and, 371 hypertensive target organ injury and, kidney injury, 552f syncope and, 29
differential diagnosis, 506 116t right-sided heart failure, 49, 58, 63 selective serotonin reuptake inhibitors
eosinophilic fasciitis, 402 proliferative retinopathy, 428 right ventricular hypertrophy, 31, 33, 43, (SSRIs)
giant cell arteritis and, 364 sickle cell anemia and, 502 44, 52, 58 for OCD, 602
hypertension and, 117 rhabdomyolysis, 545 rimantadine, 272274 for Parkinsonism, tremor, 645b, 648t
inflammatory myopathies and, 208 rheumatic aortic valve disease, 38 ritonavir (RTV), 324t for premenstrual dysphoric disorder, 707
mixed connective tissue disease and, 399 rheumatic diseases, autoantibodies in, 397t Rocky Mountain spotted fever, 259 for premenstrual syndrome, 706707
primary, 110111, 111t rheumatic fever rubella thiazide-induced hyponatremia and, 542
scleroderma and, 59, 147, 401 Jones diagnostic criteria, 294b patent ductus arteriosus and, 51 senile amyloidosis, 5657, 534
secondary, 111, 111t, 400b poststreptococcal reactive arthritis prodromal symptoms of, 268 sepsis
Sjgren syndrome and, 381b and, 405 vaccination for, 694, 695, 711b complications, 200
thromboangiitis obliterans and, 109 streptococcal pharyngitis and, 293 viral arthritis and, 353, 405406 description, 200
RB-ILD. See respiratory bronchiolitis- valvular aortic regurgitation and, 39 rupture of chordae, 44t neurology of, 649
interstitial lung disease rheumatoid arthritis RV outflow tract tachycardia, 16t treatment, 200201
reactive arthritis (spondyloarthropathy), amyloidosis in, 56 septic arthritis, 261, 403404
304, 390393 cardiac involvement in, 59 S septic bursitis, 361362
recurrent neurocardiogenic syncope clinical features of, 374375 Salmonella enteritidis, 129, 304 septic encephalopathy, 649
(vasovagal syncope), 30 connective tissue disease and, 111 Salmonella haematobium, 304 septic shock, 199f, 200, 332f
red eye constitutional features, 375 Salmonella species, 251t seronegative rheumatoid arthritis, 379
angle-closure glaucoma, 758 diagnosis, 378379, 378b Salmonella typhimurium, 129, 163, 304 of the elderly, 379380
blepharitis, 758 effects on the heart, 59 saquinavir (SQV), 324t in valvular aortic regurgitation, 39
conjunctivitis, 757758 extra-articular complications sarcomas, 214, 490. See also serotonin reuptake blockers, 30
episcleritis, 758 cardiac complications, 377 leiomyosarcomas Serratia Proteus, 328
iritis, 758 liver abnormalities, 377 SARS. See severe acute respiratory severe acute respiratory syndrome (SARS),
scleritis, 758 neurologic manifestations, 376 syndrome 273
798 INDEX
sexual assault, 729, 751b mimicking syndromes, 406, 407 multifocal motor neuropathy, 629, Streptococcus anginosus group, 293
sexually-transmitted infections rheumatoid factor in, 374, 378b, 397t 630t Streptococcus bovis endocarditis, 132
genital ulcers, lesions small vasculitis in, 370b spirochetes, 257259 Streptococcus mitis, 249250
chancroid, 294 skeletal tuberculosis, 282283 splenectomy, 275, 307, 335t, 336, 380, 498, Streptococcus pneumoniae (pneumococcus),
HSV, 294 skin and soft tissue infections, 349351 508, 520 241, 249, 273, 274, 275
HSV in pregnancy, 294295 cellulite, 349 splenic sequestration, 502 Streptococcus pyogenes, 293
syphilis, 295296 erysipelas, 349 spondyloarthropathies streptomycin, 290
gonorrhea, 296, 298299 folliculitis, 349 ankylosing spondylitis, 39, 59, 98, strokes. See also transient ischemic attacks
cervicitis, 294, 296, 299 impetigo, 349 391392 anaphylaxis and, 583
epididymitis, 296, 298t, 299, 302 necrotizing fasciitis, 349 characteristics, 390391 aspirin preventive therapy, 81
nongonococcal urethritis, 296, 299 unusual causes, 350, 352353 inflammatory bowel disease-associated atrial fibrillation and, 2224, 767
pelvic inflammatory disease, 131, 254, skin cancer, 529, 653 arthritis, 372, 392 atrial septal defect and, 49
294, 297t, 299300 SLE. See systemic lupus erythematosus psoriatic arthritis, 392393 carotid artery disease and, 108
urethritis syndromes, 296 sleep apnea. See central sleep apnea; reactive arthritis, 392 Cheyne-Stokes respiration and, 245
vaginitis obstructive sleep apnea spondyloepimetaphyseal dysplasia, 383t CT evaluation for, 612
bacterial vaginosis, 300 sleep hypoventilation syndrome, 245 spondyloepiphyseal dysplasia, 383t delirium and, 604
trichomoniasis, 300 sleep-related breathing disorders. See also spontaneous bacterial peritonitis, 184185 dementia and, 618
vulvovaginal candidiasis, 301 obstructive sleep apnea spoon nails (koilonychia), 670 diabetic ketoacidosis and, 427
Szary syndrome, 654 associated systemic disorders, 244b Sporothrix schenckii, 261262 Eisenmenger syndrome in, 52
Shigella fl exneri, 129, 163, 304 central sleep apnea, 244245 sporotrichosis, 261262 hormonal contraceptives and, 708t
shock obstructive sleep apnea hypopnea squamous cell carcinoma, 653 hypertension and, 114
classifications, 199t syndrome, 244 staphylococcal toxic shock syndrome, 352 illicit drug use and, 637
urgency of time factor, 198, 199f sleep hypoventilation syndrome, 245 Staphylococcus aureus, 162, 249, 274, mitral valve stenosis and, 44
SIADH (syndrome of inappropriate treatments, 245 302303, 328, 404, 655 oropharyngeal dysphagia and, 146, 146b
secretion of antidiuretic hormone), slow viruses, prion-associated diseases Staphylococcus lugdunensis, 301 PAVM and, 214
541 Creutzfeldt-Jakob disease, 339 Staphylococcus saprophyticus, 301 prosthetic valve endocarditis and, 341
clinical features, 450 progressive multifocal statin-induced myopathy, 635 pseudoxanthoma elasticum and, 603
diagnosis, 450 leukoencephalopathy, 251, 311b, statin therapy risk reduction measures, 767
etiology, 449 318, 338339 for ESRD, 571 sickle cell anemia and, 502
ectopic extrahypothalamic ADH subacute sclerosing panencephalitis, for increased LDL-C, 423 Sjgren syndrome and, 381b
excess, 449 339 for ischemic heart disease, 81 thoracic aortic atherosclerosis and, 105
exogenous ADH excess, 449 small bowel lymphoma, 663 for low HDL-C, 423 Strongyloides stercoralis, 270
hyponatremia and, 541 small cell lung cancer, 483 for peripheral artery disease, 107 struvite stones, 759
hypopituitarism and, 440 small cell vasculitis for primary hyperlipidemia, 421t ST-segment elevation myocardial
paraneoplastic syndromes and, 488t clinical features, 370371 for thoracic aortic aneurysm, 99 infarction, 9197
pathophysiology, 450 diagnosis, 371 for thoracic aortic atherosclerosis, 105 acute mechanical complications, 96
pituitary tumors and, 442 histopathology, 371 status epilepticus, 595, 614, 622 anticoagulation therapy for, 90
therapy, 450451 treatment and outcome, 371 steak house syndrome, 148 antiplatelet therapy for, 90
sick euthyroid syndrome, 418419 small intestines stem cell transplant management, 9395
sickle cell anemia, 304, 384, 387, 404, aortoenteric fistula, 167 for acute myeloid leukemia, 535 pathophysiology, 9193
637, 675 chronic intestinal pseudo-obstruction, for aggressive lymphomas, 533 percutaneous coronary intervention
sickle cell disorders 167168 for amyloidosis, 57, 565 for, 95
avascular necrosis of bone and, 384 malabsorption-related diseases for aplastic anemia, 501 prehospital-discharge evaluation,
classification, pathophysiology, 501502 amyloidosis, 166167 for Hodgkin lymphoma, 531 9697
community-acquired pneumonia and, celiac disease, 165 post-transplant infections, 250 presentation and diagnosis, 93
274 eosinophilic gastroenteritis, 166 for sickle cell disease, 503 reperfusion therapy, 9596
complications of, 502 intestinal lymphangiectasia, 166 Stenotrophomonas maltophilia, 330 TIMI risk score for, 89b
FSGS and, 561 systemic mastocytosis, 166 stents, 87, 87t Sturge-Weber-Dimitri syndrome, 666
membranoproliferative GN and, 559 tropical sprue, 165 Stevens-Johnson syndrome, 585, 659 subacute cutaneous lupus erythematosus,
Salmonella infections and, 353 Whipple disease, 165166 Stickler syndrome, 383t 666, 667f
S aureus infection and, 354 Meckel diverticulum, 167 stiff-hand syndrome, 669 subacute inflammatory pericarditis, 62
splenic abscesses and, 307 smallpox, 252t, 254 stiff man syndrome, 146b subacute painful thyroiditis (de Quervain
Streptococcal pneumonia and, 275 smallpox (vaccinia virus) vaccination, 696 oropharyngeal dysphagia from, 146b thyroiditis), 414
trait and compound states, 503 smoking cessation, 756 stinging insect allergies, 584585 subacute sclerosing panencephalitis
treatment, 502503 for carotid artery disease, 108 avoidance of, 585 (inclusion body encephalitis),
sick sinus syndrome, 21, 638b, 735 FDA-approved medications, 756 bees and vespids, 584 339, 614
sideroblastic anemias, 498499, 503 5 As approach, 756 testing, 584585 subarachnoid hemorrhage, 614, 638,
SIDS. See systemic inflammatory response for thoracic aortic aneurysm, 100 venom immunotherapy, 585 640641
syndrome for thromboangiitis obliterans, 109 stomach and duodenum subclavian steal syndrome, 105
silent thyroiditis (painless lymphocytic sodium balance, volume regulation dumping syndrome, 155 subclavian vein aneurysms, 110
thyroiditis), 413414 disorders, 541 gastric cancer, 154155 subclavian vein thrombosis (Paget-
silicosis, 205, 207, 210, 282, 286, 402 somatization disorder, 603 gastric polyps, 155 Schroetter syndrome), 110
silicosis pneumoconioses, 210 somatoform disorders gastroduodenal dysmotility syndromes, substance-induced mood disorders, 601
sinusitis conversion disorder, 603 155 substance use disorders, 604605. See also
causes, 580, 581b hypochondriasis, 603 Helicobacter pylori infection, 81, 145, alcohol abuse
complications, 580b somatization disorder, 603 151153, 152t anxiolytics, 605
diagnosis, 581, 581f somatostatinoma, 144 nonerosive nonspecific chronic gastritis, benzodiazepines, 605
refractory sinusitis, 580 sotalol, 13t, 14t, 28 154 sedative-hypnotics, 605
treatment, 581 spinal cord compression, 490491 NSAID-induced ulcers, 153 sudden death
sinus node dysfunction, 16b, 1718 spinal septic arthritis, 405 peptic ulcer disease, 145, 151 aneurysmal disease and, 98
sinus venosus atrial septal defect, 4950, spine ulcer diagnosis, management, 154 anorexia nervosa and, 604
50t degenerative diseases Zollinger-Ellison syndrome, 144, cardiac amyloidosis and, 5657
6-mercaptopurine, 127, 139, 389 cervical spondylosis, 623b, 630 153154 hypertrophic cardiomyopathy and,
Sjgren syndrome, 380381 lumbar spine disease, 630 streptococcal pharyngitis, 293 76, 676t
complications, 367, 377 motor neuron disease streptococcal psoriasis, 655 ischemic heart disease and, 80
differential diagnosis, 372b amyotrophic lateral sclerosis, 4t, streptococcal toxic shock syndrome, 352 severe aortic regurgitation and, 42t
features, 381b 146b, 237, 629 Streptococcus agalactiae, 337 ventricular arrhythmias and, 75
INDEX 799
superior vena cava syndrome, 31, 224b complications of, 397t third-degree AV block, 1920, 19f malignancy management, 418
supratentorial neurological disorders. See uveitis in, 393 third heart sound (S3), 34, 60 medullary carcinoma, 418
neurological disorders, anatomical systemic mastocytosis, 166 thoracic aortic aneurysm (TAA), 98100 thyroid gland disorders, 411419
involvement systemic sclerosis (scleroderma), 667 causes, symptoms, risk factors, 98 amiodarone, 419
supraventricular tachycardia clinical manifestations complications of, 9899 hyperthyroidism, 412415
catheter ablation for, 16t articular, 401 diagnosis, 99 hypothyroidism, 415417
differentiating SVT with aberrancy cardiac, 401 medical management, 99100 laboratory assessment
from VT, 2425 gastrointestinal, 401 thoracic aortic atherosclerosis, 105 radioactive iodine uptake, 412
paroxysmal SV tachycardia, 24 interstitial lung diseases, 209 thoracic aortic dissection, 101105 serum thyroglobulin, 412
in Wolff-Parkinson-White syndrome, pulmonary, 401 classifications, 103, 104f serum thyrotropin, 411
26f Raynaud phenomenon, 401 diagnosis, 102103, 102f, 103f test result interpretation, 412t
surgical treatment. See also coronary artery renal, 401 management, 104105, 104f thyroid hormone-binding proteins,
bypass grafting skin, 400 pharmacologic therapy, 104b 411
for abdominal aortic aneurysm, 101 diff use scleroderma, fi ndings, 402t presentation, 101102 thyroid scanning, 412
for carcinoid heart disease, 58 effects on the heart, 59 symptoms, 102 thyroid ultrasonography, 412
for chronic unstable angina, 8788 laboratory fi ndings, 401 thoracic outlet compression syndrome, thyrotropin receptor antibodies, 412
for coarctation of the aorta, 53 treatment, 401 109110 thyroxine, 411
for colorectal cancer, 481 thoracic outlet syndromeassociated upper total triiodothyronine, 411
for COPD, 241 T extremity arterial thrombosis, 110 sick euthyroid syndrome, 418419
for hyperthyroidism, 415 tabes dorsalis, 146b, 295 thromboangiitis obliterans (Buerger thyroid cancer, 417418
for malignant melanoma, 654 tachycardia-mediated cardiomyopathy, 28 disease), 108109, 109t, 369 thyroid nodules, 417
for mitral valve prolapse, 4748 tachycardias thrombocytopenia, 265 thyroid storm, 415
for pheochromocytoma, paraganglioma, atrial fibrillation, 2124 alveolar hemorrhage risks from, 217 thyrotoxicosis
458459 atrial flutter, 21 antiphospholipid antibody syndrome apathetic thyrotoxicosis, 413
for prolactinomas, 445 differentiating SVT with aberrancy and, 398399 atrial fibrillation and, 21
for rheumatoid arthritis, 379 from VT, 2425 chronic HIV infection and, 310 diarrhea and, 161t
for ulcerative colitis, 126127 paroxysmal SV tachycardia, 24 eosinophilic fasciitis and, 402 fi rst heart sound in, 33
of uterine fibroids, 712713 refractory ventricular tachycardia, 28 Epstein-Barr virus and, 265 follicular carcinoma and, 418
Surviving Sepsis Campaign, 200 tachycardia-mediated cardiomyopathy, fetal thrombocytopenia, 61 hypertension and, 114
sweet syndrome (acute febrile neutrophilic 28 hantavirus pulmonary syndrome and, hyperthyroidism and, 55, 467
dermatosis), 662 torsades de pointes, 28 273 iatrogenic thyrotoxicosis, 412
syncope ventricular ectopy, nonsustained VT, 27 HELLP syndrome and, 120 laboratory assessment, 411
in aortic stenosis, 39 ventricular tachycardia, fibrillation, in ICU patients, 203 thyrotropin-producing tumors and, 447
evaluation of, 2930 2728 paroxysmal nocturnal hemoglobinuria tipranavir (TPV), 324t
exercise-induced, 52 Wolff-Parkinson-White syndrome, and, 507 tobacco abuse, 80, 82, 487, 702. See also
major causes of, 29b 2527 SARS and, 273 smoking cessation
management of, 30 Taenia solium (pork tapeworm), 269270 SLE and, 395396, 397t torsades de pointes, 15f, 28, 95, 748
risk stratification, unexplained syncope, Takayasu arteritis, 365366 viral hemorrhagic fever and, 254 toxic epidermal necrolysis, 585
29b classification criteria, 366b thrombocytopenia, due to increased toxic oil syndrome, 402, 588b
syndrome of inappropriate secretion of clinical, laboratory features, 366 platelet destruction, 518521 toxic shock syndrome, 273, 352, 355, 708t
antidiuretic hormone (SIADH), description, 217218 autoimmune thrombocytopenic toxic thyroid adenoma, 414
541 thoracic aortic aneurysm and, 98 purpura, 518520 Toxoplasma chorioretinitis, 270
syphilis tamponade chemotherapy-associated Toxoplasma gondii, 270, 317
aortic root calcium association, 39 balloon tamponade therapy, 202 thrombocytopenia, 521 Toxoplasma gondii encephalitis, 312t, 317
diagnosis, 295296, 295t cardiac tamponade, 199t, 377 drug-induced thrombocytopenia, 204, toxoplasmosis
genital ulcers in, 294 cardiac trauma and, 60 520 AIDS patients and, 311b, 317318
treatment, 296 pericardial tamponade, 31, 62, 69t, 88, heparin-induced thrombocytopenia, infectious mononucleosis-like syndrome
syphilitic aortitis, 98 96t, 102 219b, 520521 and, 271
systemic inflammatory response syndrome shock and, 199t thrombolytic therapy primary prophylaxis for, 312t
(SIRS) T-cell clonal disorders, 501 for acute cerebral infarction, 639 primary toxoplasmosis, 270
in sepsis, 200 T-cell LGL leukemia, 530 for myocardial infarction, 9395 transmission risks, 752
in shock, 199f Td, Tdap vaccines, 694695 for pulmonary embolism, 526 transplant recipients and, 250
systemic lupus erythematosus (SLE) temporal arteritis. See giant cell arteritis for thoracic outlet compression treatment for, 250, 317t
alveolar hemorrhagic syndrome and, 217 tenosynovitis, 298, 376377, 404405 syndrome, 110 toxoplasmosis trichinosis, 635b
clinical manifestations tensor apparatus type mitral regurgitation, for venous thromboembolism, 220, transesophageal echocardiography, 23,
articular, 395 44t 525, 739 37, 104f
cardiopulmonary, 395 tertiary syphilis, 295 thrombophilia transfusional hemochromatosis, 502
general, 395 testicular cancer, 486, 493 anticoagulant system defects, 523527 transfusion reactions
interstitial lung diseases, 208 testicular disorders. See male defi ned, 523 acute hemolytic transfusion reactions,
neuropsychiatric, 395396 hypogonadism, adults procoagulant system defects, 523 509
treatments for, 397t tetanus, 146b, 255256 thrombotic microangiopathies, 507508 allergic transfusion reactions, 509510
diagnostic criteria, 394, 395b tetanus-diphtheria-acellular pertussis characteristics, 563 circulatory overload, 510
drug-induced lupus (Tdap) vaccine, 694695 hemolytic uremic syndrome, 508, delayed hemolytic transfusion reactions,
clinical features, 398 tetanus-diphtheria (Td) vaccine, 694695 563564 510
implicated agents, 398b tetracycline renal thrombotic microangiopathies, febrile transfusion reactions, 510
laboratory abnormalities, 398 for bypass arthritis, 393 564 infection, 510
metabolism, 398 pancreatitis caused by, 139 thrombotic thrombocytopenic purpura, porphyria, 510511
treatment, 398399 for syphilis, 296 508, 564 posttransfusion purpura, 510
effects on the heart, 59 thalassemias, 498, 675 thrombotic thrombocytopenic purpura transfusion-related acute lung injury, 510
epidemiology, etiology, 394 theophylline, 150, 239, 237, 242b, 289, 607 (TTP), 164, 194t, 506, 518, 564, transfusion-related acute lung injury
genetic factors, 394, 396t thiazide diuretics, 39, 139, 570571, 698t 639 (TRALI), 509
laboratory fi ndings, 396397 thiazide-induced hypercalcemia, 466 thymoma, 449, 643, 663 transient ischemic attacks (TIAs), 47, 49t,
outcome, 397 thiazolidinediones (TZDs), 426 thyroid cancer 108, 399, 638
pathogenesis, 394395 thin basement membrane nephropathy anaplastic carcinoma, 418 transmural myocardial infarction (MI), 91
in pregnancy, 396 (TBMN), 564 differentiated malignancies, 417418 transplants. See also stem cell transplant
renal involvement, 396 thionamides, 414. See also methimazole; follicular carcinoma, 418 allogenic hematopoietic stem cell
treatment, 397 propylthiouracil papillary carcinoma, 417418 transplant, 501
800 INDEX
heart patients, hyperlipidemias and, 74 Tysabri (natalizumab), 251 Td, Tdap vaccines, 694695 lymphedema, 112113
HSV infection and, 250t tetanus-diphtheria-acellular pertussis peripheral arterial conditions
transtelephonic event recording, 1112 U (Tdap), 694695 acute arterial occlusion, 107108
transthoracic echocardiography, 365f ulcerative colitis, 126127 tetanus-diphtheria (Td) vaccine, peripheral artery aneurisms, 105
transverse myelitis, 270 cholestasis and, 171 694695 peripheral artery disease, 105107
trastuzumab, 479 C jejuni and, 164 varicella vaccine, 695 Takayasu arteritis, 98, 217218,
Treponema pallidum, 295. See also syphilis colon cancer screening in, 137t for varicella-zoster virus, 268 365366
treprostinil, 221 CVID and, 588 vaginitis vasospastic disorders
trichinosis, 270, 635b description, 125 bacterial vaginosis, 300 chronic pernio, 112
Trichomonas vaginalis, 299 diarrhea and, 161t trichomoniasis, 300 livedo reticularis, 111112
trichomoniasis, 294, 300, 718 exam questions, 4t vulvovaginal candidiasis, 301 Raynaud syndrome, 110111
tricuspid regurgitation, 31, 32f, 48, 53, 74 idiopathic ulcerative colitis, 164165 Valsalva maneuver, 35, 39 vasculitic syndromes, 363372
tricuspid stenosis, 31, 48 primary sclerosing cholangitis and, 180 valvular heart disease, 3849 associated skin lesions, 372
tricuspid valve prolapse, 45, 48 treatment of, 126127 aortic regurgitation Buerger disease, 108109, 369
tricyclic antidepressants undifferentiated connective tissue disease, aortic root dilatation, 39 Churg-Strauss vasculitis, 59, 216,
for adjustment disorder with depressed 399 diagnosis, 40 368369
mood, 600 Ureaplasma urealyticum, 299 natural history of, 42t classic polyarteritis nodosa, 366368, 368t
adverse effects of, 28 uremia physical examination, 40 common clinical features, 363b
for fibromyalgia, 360 acute pseudo-obstruction and, 132 symptoms, 3940, 42t cryoglobulinemia, 371372
general principles, 606 ARDS and, 194t treatment, 4042 cutaneous vasculitis, 370371
for migraines, 623b bleomycin toxicity and, 210 valvular, 39 giant cell arteritis, 216, 363365
for postpartum depression, 729 Burr cells in, 504, 504f aortic stenosis hypocomplementemic vasculitis, 372
for urticaria, 583 CKD and, 570 diagnosis, 39 laboratory, radiographic abnormalities,
trimethoprim-sulfamethoxazole community-acquired pneumonia and, management strategy, 41f 364b
for brucellosis, 255 274 physical examination, 3839 leukocytoclastic vasculitis, 372
for Listeria monocytogenes, 336337 pericarditis and, 62 severity quantitation, 40t microscopic polyangiitis, 366368, 368t
for Nocardia infection, 280 pseudomembranous enterocolitis and, symptoms, 38 mimicking syndromes, 363
for Salmonella in AIDS, 129 130 treatment, 39, 40t small cell vasculitis, 370371, 370b
for Shigella fl exneri, 129 urethritis syndromes, 296 types, 38 Takayasu arteritis, 365366
for sinusitis, 581 uric acid stones, 759 with atrial fibrillation, 21 Wegener granulomatosis, 215216,
for Tropheryma whipplei infection, 407 urinary incontinence mitral regurgitation 369370
for UTIs in females, 301 evaluation of, 685 etiology, pathophysiology, 4445 vasospastic disorders
Tropheryma whipplei, 407 treatment, 686 management, 46f chronic pernio, 112
tropical sprue, 165 types of, 685686 physical examination, 45 livedo reticularis, 111112
tuberculosis urinary tract infections (UTIs) symptoms, 45 Raynaud syndrome, 110111
abdominal tuberculosis, 283 catheter-associated UTIs, 746747 treatment, 45 vasovagal syncope (recurrent
amyloidosis in, 56 in the elderly, 687 types of, 44t neurocardiogenic syncope), 30
antituberculosis drug toxicity, 289290 in females, 301302 mitral stenosis venom immunotherapy, 585
culture-negative pulmonary TB, 288f in males, 302 diagnosis, 4344, 44f venous thromboembolism (VTE),
diarrhea in, 132 urolithiasis etiology, pathophysiology, 42 524527
drug-resistant tuberculosis, 283 calcium oxalate stones, 759 physical examination, 42 disseminated intravascular coagulation
fi rst-line drugs, 285t calcium phosphate stones, 759 symptoms, 42 and, 517
genitourinary tuberculosis, 283 stone expulsion, 759 treatment, 44 evaluation of patients for, 525526
in HIV-infection, 314 struvite stones, 759 mitral valve prolapse hospital-acquisition of, 745
ileocecal tuberculosis, 283 uric acid stones, 759 pathophysiology, nature history, from hospitalization, 745
laryngeal tuberculosis, 283 urticaria 4546 incidence of, 525t
miliary tuberculosis, 282 angioedema association, 581 physical examination, 46 in pregnancy, 710
Mycobacterium tuberculosis, 281284, C1 esterase inhibitor deficiency, 582 treatment, 4647 prevention, 220, 524525
286287 chronic, histopathology of, 582 prosthetic valves risk factors, 524, 525t, 709, 720b
pericardial tuberculosis, 283 food allergy in, 582 bioprosthetic valves, 4849 treatment
pericarditis and, 62 management, 582583 mechanical valves, 49, 50t calf-vein thrombosis, 527
skeletal tuberculosis, 282283 physical urticaria, 582 tricuspid regurgitation, 48 duration of warfarin anticoagulation,
targeted testing for latent infection, secondary urticaria, 581 tricuspid stenosis, 48 527
286t uterine bleeding tricuspid valve prolapse, 48 initial management, 526
XDR-TB, 283284 abnormal, 707708, 707b, 713, 714 valvular pulmonary stenosis, 52f long-term management, 527
tuberculous lymphadenitis, 282 dysfunctional, 708 valvular pulmonary stenosis, 52f proximal DVT, 527
tuberculous meningitis, 283 uterine diseases varicella pneumonia, 267, 272 pulmonary embolism, 527
tuberculous spondylitis, 283 endometrial cancer, 713714, 714b varicella vaccine, 695 ventilator-associated pneumonia (VAP),
tuberous sclerosis complex, 665, 677t endometriosis, 711712 varicella-zoster virus (VZV), 250 196, 328329, 330
tubulointerstitial disease, 558, 565566 uterine fibroids, 712713 treatment for, 267268 ventricular ectopy, nonsustained
tularemia (Francisella tularensis) infection, uveitis and rheumatologic diseases, 393 vaccines for, 268 ventricular tachycardia, 27
254 varicella-zoster virus (VZV) vaccine, 268 ventricular septal defect, 3334, 51, 52, 96
tumor lysis syndrome, 545 V variegate porphyria (mixed porphyria), 670 ventricular tachycardia, 25f. See also
tumor necrosis factor- antagonists, 379 vaccines vascular dementia, 613, 618b, 682, 683 supraventricular tachycardia
tumor necrosis factor- inhibitors, 128, adult recommendation schedule, 694f vascular heart diseases, 98113 anorexia nervosa and, 604
251, 260, 392, 393, 655 hepatitis A vaccine, 695 arterial occlusive disease catheter ablation for, 16t
Turcot syndrome, 135 hepatitis B vaccine, 696 thoracic outlet compression device therapy for, 16
Turner syndrome, 52, 98, 676t HPV vaccine, 695 syndrome, 109110 EP testing for, 12
tylosis, 148, 662 influenza vaccine, 694 thromboangiitis obliterans, 108109 fibrillation and, 2728
type 1 diabetes mellitus. See diabetes meningococcal vaccine, 695 carotid artery disease, 107108 heart failure and, 70
mellitus (DM), type 1 MMR vaccine, 695 diseases of the aorta hypertrophic cardiomyopathy and, 76
type 2 diabetes mellitus. See diabetes oral, for poliovirus, 338 aneurysmal disease, 98101 identifying factors, 26b
mellitus (DM), type 2 pneumococcal polysaccharide vaccine, thoracic aortic atherosclerosis, 105 management, 27
type 2 gastric carcinoids, 155 695 thoracic aortic dissection, 101105 nonsustained ventricular tachycardia,
type A gastritis (autoimmune gastritis), 154 pneumococcal vaccine, 275 edema, 112 28, 78
type B gastritis, 154 polio vaccine, 696 erythromelalgia, 112 polymorphic ventricular tachycardia,
types 1, 2, 3 gastric carcinoids, 155 rabies vaccine, 696 leg ulcer, 113 14, 15t
INDEX 801
ventricular tachycardia (Cont.) stepwise assessment approach, 514t conduction of sinus impulses in, 27f dysfunctional uterine bleeding, 708
refractory ventricular tachycardia, 28 variables affecting vWF levels, 514515 defi nition, 2526 intimate partner violence, 729
sustained ventricular tachycardia, 14t vulvar skin disorders, 717718 supraventricular tachycardia in, 26f menopause
ventricular tachycardia and fibrillation, vulvovaginal candidiasis, 301 treatment, 2526 hallmark symptoms, 719720
2728 womens health, 706729. See also breast hormone therapy, 720
verapamil, 23, 61, 78 W cancer; contraceptives, hormonal; postmenopausal bleeding, 720
vertebral infections, 354 Waldenstrm macroglobulinemia, 534 contraceptives, oral; infertility related terms, 719b
vespid allergies, 584 warfarin therapy (female); menopause; pregnancy menstruation, 706
Vibrio cholerae, 163, 302t, 305 acquired coagulation deficiencies, 517t abnormal uterine bleeding, 707708, perimenopause, 718719
Vibrio parahaemolyticus, 163, 164, 305 for antiphospholipid antibody 707b, 713, 714 premenstrual syndrome, 706707
Vibrio vulnifi cus, 165, 350, 353 syndrome, 400 adnexal masses, 714716, 714b sexual assault, 729
viral arthritis, 353, 405406 contraindication in pregnancy, 56 anxiety and depression, 728729 uterine diseases
viral diarrhea, 305306 for dilated cardiomyopathy, 74 breast conditions endometrial cancer, 713714, 714b
viral hemorrhagic fevers, 252t for ischemic cerebrovascular disease, 639 benign breast disease, 723 endometriosis, 711712
viral pathogens, in AIDS for mitral valve prolapse, 49t nipple discharge, 722723 uterine fibroids, 712713
adenovirus, 129 for venous thromboembolism, 527 nonpalpable mass evaluation, 721 vulvar skin disorders, 717718
cytomegalovirus, 128 water balance disorders. See diabetes pain, 721722
herpes simplex virus, 128129 insipidus; hypernatremia; palpable mass evaluation, 721 X
viral pneumonia, 272 hyponatremia; osmotic diuresis cardiovascular disease X-linked lymphoproliferative syndrome,
viridans group streptococci, 345 Wegener granulomatosis (granulomatosis atrial fibrillation, 728 266
visceral leishmaniasis, 271 with polyangiitis), 215216, clinical presentation, 727
vitamin C deficiency, 498 369370, 580 gender-based management, outcomes, Y
vitamin D deficiency, 571 Wells model for predicting pulmonary 727 yellow jacket stings, 584
von Hippel-Lindau disease, 119, 677t embolism, 525t heart failure, 728 yellow nail syndrome, 218
von Willebrand disease, 513515 West Nile virus encephalitis, 4t pathogenesis, 726727 Yersinia enterocolitica, 164, 264, 305
biochemistry, 514 Whipple disease, 165166, 407 primary/secondary prevention, Yersinia pestis (plague), 252t, 254
classification, 513 Wilson disease, 180182, 384 727728
clinical features, 514 Wiskott-Aldrich syndrome, 522 risk factors, 725726 Z
defi nition, 513 Wolff-Parkinson-White syndrome, 11 stress testing, 727 zanamivir, 273
function of, 514 adenosine/verapamil contraindication, cervical cancer screening, Zenker diverticulum, 146, 148, 151
inheritance of, 515 13 716717 zoledronic acid, 465, 479, 489
laboratory testing, 514 with atrial fibrillation, 21 contraception options, risks, 708710, Zollinger-Ellison syndrome, 144,
management, 515 atrial fibrillation in, 2627 708t 153154
802 INDEX