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Nursing Management of Patient with Undifferentiated Schizophrenia

Dela Cruz, Victor Jr S. BSN3Y3-9B

Our Lady of Fatima University Valenzuela City

C O L L E G E O F

Maam Rosario Fernando Clinical Instructor

N U R S I N G

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Nursing Management of Patient with Undifferentiated Schizophrenia

Introduction R.A, 34 years old, male from Concessionaires area, PNPA. Patient is the 5th siblings, 2nd year college level when he became mentally ill 12 years prior to admission. He had regular check-up at this center on January 27, 2003. Given drugs of monthly Levozepromazine. His last check-up was on March 17, 2008 and has subsequent check-up care of Trece Martines. Schizophrenia (from the Greek roots skhizein ("to split") and phrn ("mind") is a severe mental illness characterized by a variety of symptoms including but not limited to loss of contact with reality. Schizophrenia is not characterized by a changing in personality; it is characterized by a deteriorating personality. Simply stated, schizophrenia is one of the most profoundly disabling illnesses, mental of physical that the nurse will ever encounter (Keltner,2007). There are 5 subtypes of schizophrenia naming; paranoid, disorganized, catatonic, undifferentiated, and residual. Schizophrenia undifferentiated is the type of schizophrenia wherein characteristic symptoms (delusions, hallucinations, disorganized speech, grossly disorganized or catatonic behavior, and negative symptoms) are present, but criteria for paranoid, catatonic, or disorganized subtypes are not met.
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Schizophrenia is not a terribly common disease but it can be a serious and chronicone. Worldwide about 1 percent of the population is diagnosed with schizophrenia. About 1.5 million people will be diagnosed with schizophrenia this year around the world. Ninety-five percent (95%) suffer a lifetime; thirty-three percent (33%) of all homeless Americans suffer from schizophrenia; fifty percent (50%) experience serious side effects from medications; and ten percent (10%) kill themselves (Keltner, 2007). According the study of cureresearch.com done 697,543 out of 86,241,697 of Filipinos or approximately 0.8% are suffering from schizophrenia. 5 schizophrenia ranks among the top 10 causes of disability in developed countries worldwide. Schizophrenia is a disease that typically begins in early adulthood; between the ages of 15 and 25. Men tend to get develop schizophrenia slightly earlier than women; whereas most males become ill between 16 and 25 years old, most females develop symptoms several years later, and the incidence in women is noticeably higher in women after age 30. The average age of onset is 18 in men and 25 in women. Schizophrenia onset is quite rare for people under 10 years of age, or over 40 years of age.
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Anatomy and Physiology The nervous system is an intricate, highly organized network of billions of neurons and neuroglia. The structures that make up the nervous system include the brain, cranial nerves, spinal nerves, ganglia, enteric plexuses and sensory receptors. The two main subdivisions of the nervous system are the central nervous system and the peripheral nervous system. The central nervous system consists of the brain and spinal cord. The brain is the center for registering sensations, correlating them with one another and with stored information, making decisions and taking actions. It also is the center for the intellect, emotions, behavior, and memory. The major parts of the brain include: the brain stem, cerebellum, diencephalon, and cerebrum. The spinal cord is connected to a section of the brain called the brainstem and runs through the spinal canal. Cranial nerves exit the brainstem. Nerve roots exit the spinal cord to both sides of the body. The spinal cord carries signals (messages) back and forth between the brain and the peripheral nerves.
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The brain stem is continuous with the spinal cord and consists of the medulla oblongata, pons, and midbrain. The medulla oblongata forms the inferior part of the brain stem. The medulla contains the cardiac, respiratory, vomiting and vasomotor centers and deals with breathing, heart rate and blood pressure. The pons is a bridge that connects parts of the brain with one another. The midbrain extends from the pons to the diencephalon. The midbrain is a short section of the brainstem between the diencephalon and the pons. Posterior to the brain stem is the cerebellum. Traditionally, the cerebellum has been known to control equilibrium and coordination and contributes to the generation of muscle tone. It has more recently
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become evident, however, that the cerebellum plays more diverse roles such as participating in some types of memory and exert in a comples influence on musical and mathematical skills. Superior to the brainstem is the diencephalon, which consists of the thalamus, hypothalamus, and epithalamus. The thalamus acts a relay center for all sensory impulses, except smell to the cerebral cortex. The hypothalamus is involved in the acceleration or deceleration of the heart. Impulses from the posterior hypothalamus produce a rise in arterial blood pressure and increase of the heart rate. Impulses from the anterior portion have the opposite effect. The hypothalamus is also involved in body temperature regulation. If the arterial blood flowing through the anterior portion of the hypothalamus is above normal level, the hypothalamus initiates impulses that cause heat loss through sweating and vasodilation of cutaneous vessels of the skin. A below-normal blood temperature causes the hypothalamus to relay impulses that result in heat production and retention through the initiation of shivering, the contraction of cutaneous blood vessels. The hypothalamus is also involved in the regulation of hunger and control of gastrointestinal activity. Low levels of blood glucose, fatty acids and amino acids are partially responsible for the sensation of hunger elicited from the hypothalamus. When sufficient amounts of food have been ingested, the hypothalamus inhibits the feeding center. It also regulates sleeping and wakefulness. A specialized sexual
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center in the hypothalamus responds to sexual stimulation of the tactile receptors within the genital organs. Also, the hypothalamus is associated with specific emotional responses, such asanger, fear, pain and pleasure. The hypothalamus produces neurosecretory chemicals that stimulate the anterior pituitary gland to release various hormones. The epithalamus is the posterior portion of the diencephalon. Supported on the diencephalon and brain stem is the cerebrum, which is the largest part of the brain. The cerebrum is the largest part of the brain and controls voluntary actions, speech, senses, thought, and memory. The surface of the cerebral cortex has grooves or infoldings (called sulci), the largest of which are termed fissures. Some fissures separate lobes. The convolutions of the cortex give it a wormy appearance. Each convolution is delimited by two sulci and is also called a gyrus (gyri in plural). The cerebrum is divided into two halves, known as the right and left hemispheres. A mass of fibers called the corpus callosum links the hemispheres. The right hemisphere controls voluntary limb movements on the left side of the body, and the left hemisphere controls voluntary limb movements on the right side of the body. Almost every person has one dominant hemisphere. Each hemisphere is divided into four lobes, or areas, which are interconnected.
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The frontal lobes are located in the front of the brain and are responsible for voluntary movement and vie their connections with other lobes, participate in the execution of sequential tasks; speech output; organizational skills; and certain aspects of behavior, mood, and memory. The parietal lobes are located behind the frontal lobes and in front of the occipital lobes. They process sensory information such as temperature, pain, taste, and touch. In addition, the processing includes information about numbers, attentiveness to the position of ones body parts, the space around ones body, and one's relationship to this space. The temporal lobes are located on each side of the brain. They process memory and auditory (hearing) information and speech and language functions. The occipital lobes are located at the back of the brain. They receive and process visual information. Neurotransmitters are chemicals which relay, amplify, and modulate signals between a neuron and another cell. Some neurotransmitters are commonly described as "excitatory" or "inhibitory". The only direct effect of a neurotransmitter is to activate one or more types of receptors. Examples of neurotransmitters are acetylcholine, dopamine, gamma-aminobutyric acid, dopamine, glutamate, aspartate, and serotonin. The chemical compound acetylcholine is a neurotransmitter in both the peripheral nervous system (PNS) and central nervous system (CNS) in many organisms including humans.
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In the peripheral nervous system, acetylcholine activates muscles, and is a major neurotransmitter in the autonomic nervous system. In the central nervous system, acetylcholine and the associated neurons form a neurotransmitter system, the cholinergic system, which tends to cause excitatory actions. Gamma-Aminobutyric acid (GABA) is the chief inhibitory neurotransmitter in the mammalian central nervous system. It plays a role in regulating neuronal excitability throughout the nervous system. In humans, GABA is also directly responsible for the regulation of muscle tone. Dopamine has many functions in the brain, including important role in behavior and cognition, voluntary movement, motivation, punishment and reward, inhibition of prolactin production (involved in lactation and sexual gratification), sleep, mood, attention, working memory, and learning. In the frontal lobes, dopamine controls the flow of information from other areas of the brain. Dopamine disorders in this region of the brain can cause a decline in neurocognitive functions, especially memory, attention, and problem-solving. Reduced dopamine concentrations in the prefrontal cortex are thought to contribute to attention deficit disorder. Dopamine is commonly associated with the pleasure system of the brain, providing feelings of enjoyment and reinforcement to motivate a person proactively to perform certain activities. Dopamine is released (particularly in areas such as the nucleus accumbens and prefrontal cortex) by naturally rewarding experiences such as food, sex, drugs, and neutral stimuli that become associated with them. Recent
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studies indicate that aggression may also stimulate the release of dopamine in this way. This theory is often discussed in terms of drugs such as cocaine, nicotine, and amphetamines, which directly or indirectly lead to an increase of dopamine in the mesolimbic reward pathway of the brain, and in relation to neurobiological theories of chemical addiction (not to be confused with psychological dependence), arguing that this dopamine pathway is pathologically altered in addicted persons. Projection neurons that produce dopamine are found in the diencephalon and the brainstem. In the diencephalon, dopamine cell bodies give rise to tuberopophysial dopamine projections, which inhibit the release of prolactin and melanocyte-stimulating hormone from the anterior and intermediate lobes of the pituitary, respectively, and the incertohypothalamic projections, which connect the zona incerta in the posterodorsal diencephalon with the anterior hypothalamus and septal area. A third dopamine projection system arises from neurons scattered along the ventricular system in the periaqueductal gray, the dorsal motor of the nucleus of the vagus, and the nucleussolitarius. The preventricular system provides terminals in the gray matter along the course of theventricles.Longer dopamine projection systems arise from the substantia nigra and the ventral tegmentalarea (VTA) of the midbrain. The former, the nigrostriatal dopamine system, is a particularly important in the control of motor function. The function of the VTAs dopamine projections to the
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forebrain, called the mesolimbic and mesocortical systems, has been linked to the complex group of disease we refer to as schizophrenia. Sociability is also closely tied to dopamine neurotransmission. Low D2 receptor-binding is found in people with social anxiety. Traits common to negative schizophrenia (social withdrawal, apathy, anhedonia) are thought to be related to a hypodopaminergic state in certain areas of the brain. In instances of bipolar disorder, manic subjects can become hypersocial, as well as hypersexual. This is credited to an increase in dopamine, because mania can be reduced by dopamine-blocking anti-psychotics. The locus ceruleus at the rostal end of the floor of the fourth ventricle on each side marks the position of a nucleus with a rich vascular supply and consisting of neurons containing melanin pigment. The nucleus (also known as nucleus pigmentosus) is partly in the pons and partly in the midbrain, lying dorsolateral to the oral pontine reticular nucleus. The locus ceruleus is the largest of about a dozen nuclei I the brainstem that produce catecholamines. Most produce norepinephrine, but some of those in the medulla produce epinephrine. A third catecholamine is dopamine, a transmitter used by the large neurons of the substantia nigra and ventral tegmental area, and by certain nuclei of the hypothalamus. Serotonin or 5-Hydroxytryptamine (5-HT) is a monoamine neurotransmitter that is primarily found in the gastrointestinal (GI) tract and central nervous system (CNS) of humans and animals. Approximately 80 percent of the human
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bodys total serotonin is located in the enterochromaffin cells in the gut, where it is used to regulate intestinal movements. The remainder is synthesized in serotonergic neurons in the CNS where it has various functions, including the regulation of mood, appetite, sleep, muscle contraction, and some cognitive functions including memory and learning. Modulation of serotonin at synapses is a thought to be a major action of several classes of pharmacological antidepressants. Serotonin secreted from the enterochromaffin cells eventually finds its way out of tissues into the blood. There, it is actively taken up by blood platelets, which store it. When the platelets bind toa clot, they disgorge serotonin, where it serves as a vasoconstrictor and helps to regulate hemostasis and blood clotting. Serotonin also is a growth factor for some types of cells, which may give it a role in wound healing.

Psychopathology The pathophysiology of schizophrenia has long remained a mystery and still today, even with various hypotheses, remains somewhat uncertain: there are too many variants; not enough consistency in findings; and, despite research, a lack of documented proof. The most well-known and respected hypothesis with regards to the pathophysiology of schizophrenia began in the 1990s and consisted primarily

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of the notion there is a problem with the dopamine levels in the brain of schizophrenics. Dopamine is both a hormone and a neurotransmitter, which means that it activates five different receptors in the brain, aptly named D1, D2, D3, D4, and D5. That said, it may not be the only neurotransmitter involved in the pathophysiology of schizophrenia. Glutamate and Serotonin have also been
implicated.

Contributing to this hypothesis is the fact that drugs administered to aid dopaminergic activity bring on schizophrenic characteristics such as psychosis, in a patient, whereas drugs administered to block them help reduce, or eliminate symptoms of schizophrenia altogether. Additional studies affecting the pathophysiology of schizophrenia include suggestions that maternal factors such as infection, malnutrician, location of birth, season of birth, and delivery, may play a significant part in the formation and subsequent appearance of schizophrenia. Studies have shown that the worldwide rate of births affected with schizophrenia is up to 8% higher when occurring in spring or winter, though no explanation for this can be offered. Another aspect of the pathophysiology of schizophrenia that has been explored in relative detail is that of genetics, and their relation to the likelihood of immediate relatives being born with the disease. Shockingly, it has been found that 10% of all immediate family members of an infected person will be struck down with the disease. This is specifically in relation to parents, siblings, and
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children. With regards to twins or other multiple births, the chances they will share the disease is 50%. Genetic reports suggest that it is the X chromosome which determines whether or not a person is infected with schizophrenia, specifically, chromosomes 1, 3, 5, and 11, however further studies are needed in order to prove this theory. Though there are many theories and hypotheses regarding the pathophysiology of schizophrenia, there is, unfortunately, still no cure for the disease. The best a sufferer can hope for nowadays is to benefit from available medication which keeps the disease under control or in remission for the duration of time for which it is taken.

History R.A, 34 years old, male from Concessionaires area, PNPA admitted on February 7,2012. Patient is the 5th siblings, 2nd year college level when he became mentally ill 12 years prior to admission. He had regular check-up at this center on January 27, 2003. Given drugs of monthly Levozepromazine. His last check-up was on March 17, 2008 and has subsequent check-up care of Trece Martines. Medication just conditioned to be manifested. 1 week prior to admission, patient became assaultive and distractive infront of family.
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2 days prior to admission, patient strambulated father and was helpless to calls, restless and sleep hence brought to the center. According to mother nananakit, nanununtok, sina-sabal ang tatay, naghuhubad and di-nakatulog. According to patient check-up lang and hindi po totoo yun.

Mental Status Exams Name: R.A Schizophrenia Age: 34 Appearance 34 year-old Filipino, male, 57 in height. At the time of examination, patient was well groomed and dressed. He was not confined to bed. R.A was cooperative throughout the interview. He maintained eye contact, except during the times when recounting the history before he was admitted. Then, he appeared depressed. His level of personal hygiene was fairly good. The patients movements are organized and purposeful during the interview. He moves in a normal pace and does not show any signs of over and under activity. The Ward: Pavillion 6, Pay Ward 1-E
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Diagnosis: Undifferentiated

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patients facial expressions are very much appropriate to his verbal responses during the interview. He was composed and receptive to whatever the I ask him. Behavior Behavior was passively cooperative during examination. The patient was friendly and warm during the interview. He was sitting on chair calmly. Speech R.A articulated himself clearly. During the interview, he was pleasant and cooperative and displayed a positive attitude. He went into details, the circumstances surrounding his admission. He was able to maintain adequate eye contact. His speech was coherent, spontaneous and appropriate with normal rate, volume and rhythm. He described his mood as depressed. Affect and mood Patients affect was depressed and her range of mood reduced. He also appeared anxious and irritable. Thought Patients thought stream was decreased. It was also disturbed and his speech slowed down and content reduced significantly when mentioning past unhappiness. He did not exhibit any formal thought disorders. She was able to answer questions spontaneously and directly. She did not use any new or
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created words. He did experience thought block when exploring sensitivities in his past. No negative thought disorder was detected. Other than feeling of guilt, R.A has no other positive symptoms, such as delusions, phobias or compulsions. Suicidal ideation was not detected. Perception R.A exhibits normal perception. Symptoms such as illusions, misinterpretations, depersonalization and passivity phenomena were not elicited. Cognition His memory was intact for recent and remote events. He was able to answer questions and recall his past without difficulties. I was able to establish adequate rapport with him throughout the interview and he was able to follow directions. He denied any ideation of worthlessness or hopelessness. Insight and judgement When questioned about his condition, R.A accepted the fact that he is ill and requires treatment. He has cooperated with doctors and nurses and is compliant with management.
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Nursing Physical Assessment R.A, 34 years old, was conscious, not in cardiorespiratory distress. With a blood pressure of 120/80, respiratory rate of 22, temperature of 36.9 and has respiratory rate of 110. Abdomen is flat, soft, NABS (Normal Active Bowel Sounds), no masses and tenderness. Anicteric sclera pink palpebrable conjunctiva, no symmetric chest expansion, no retractions, clear breath sounds adynamic precordium. Has tachycardia, regular rhythm, no murmur. Flat, soft, normoactive bowel sounds. Grossly normal extremities, no cyanosis, no edema and has psychosocial problem.

Related Treatments The patient was given Haloperidol 5mg. OD, it is classified as Antipsychotics to alters the effects of dopamine in the CNS and also has anticholinergic and alpha-adrenergic blocking activity and diminished signs and symptoms of psychoses. It is indicated for organic psychoses, acute psychotic symptoms; relieve hallucinations, delusions, disorganized thinking, severe anxiety and seizures. Common side effects are: extrapyramidal symptom such as muscle rigidity or spasm, shuffling gait, posture leaning forward, drooling, masklike facial appearance, dysphagia, akathisia, tardive dyskinesia, headache, seizures, tachycardia, arrhythmias, hypertension, orthostatic hypertension. blurred vision, glaucoma, dry mouth, anorexia, nausea,
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vomiting, constipation, diarrhea, weight gain, urinary frequency, urine retention, impotence, enuresis, amenorrhea, gynecomastia, anemia, leucopenia, agranulocytosis, rash, dermatitis, and photosensitivity. It is contraindicated to seizure disorder glaucoma and elderly clients. Nursing considerations are;Assess mental status prior to and periodically during therapy. Monitor BP and pulse prior to and frequently during the period of dosage adjustment. May cause QT interval changes on ECG. Observe patient carefully when administering medication, to ensure that medication is actually taken and not hoarded. Monitor I&O ratios and daily eight. Assess patient for signs and symptoms of dehydration. Monitor for development of neuroleptic malignant syndrome (fever, respiratory distress, tachycardia, seizures, diaphoresis, hypertension or hypotension, pallor, tiredness, severe muscle stiffness, loss of bladder control. Report symptoms immediately. May also cause leukocytosis, elevated liver function tests, elevated CPK. Advise patient to take medication as directed. Take missed doses as soon as remembered, witih remaining doses evenly spaced throughout the day. May require several weeks to obtain desired effects. Do not increase dose or discontinue medication without consulting health care professional. Abrupt withdrawal may cause dizziness, nausea, vomiting, GI upset, trembling, or uncontrolled movements of mouth, tongue or jaw. Risperidone is an atypical antipsychotic drug that is used for treating schizophrenia, bipolar mania and autism. Atypical antipsychotics differ from
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typical antipsychotics due to the lesser degree of extrapyramidal (movement) side effects and constipation. Risperdal Consta is an injectable, long-acting form of risperidone. The exact mechanism of action of risperidone is not known, but, like other anti-psychotics, it is believed that risperidone affects the way the brain works by interfering with communication among the brain's nerves. Nerves communicate with each other by making and releasing chemicals called neurotransmitters. The neurotransmitters travel to other nearby nerves where they attach to receptors on the nerves. The attachment of the neurotransmitters either stimulates or inhibits the function of the nearby nerves. Risperidone blocks several of the receptors on nerves including dopamine type 2, serotonin type 2, and alpha 2 adrenergic receptors. It is believed that many psychotic illnesses are caused by abnormal communication among nerves in the brain and that by altering communication through neurotransmitters, risperidone can alter the psychotic state. Risperidone was approved by the FDA in December, 1993. Risperidone is used to treat schizophrenia, bipolar mania [as a sole therapy or combination therapy with lithium (Eskalith, Lithobid) or valproate (Depakene, Depacon) and for the treatment of irritability associated with autistic disorder in children and adolescents. Clinical studies involving small numbers of patients have shown some benefit in using risperidone for stuttering and Tourette syndrome (non FDA-approved uses). Another non-FDA approved use of risperidone is forobsessive-compulsive disorders. Risperidone can be administered once or
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twice daily. Initial dosing is generally 2 mg/day. Dose increases can occur in increments of 1-2 mg/day, as tolerated, to a recommended dose of 4-8 mg/day. In children, risperidone should be initiated at 0.5 mg once daily, and can be increased in increments of 0.5 or 1 mg/day, as tolerated, to a recommended dose of 2.5 mg/day. Risperidone can be given with or without meals. The recommended dose of Risperdal Consta is 25 mg injected into the deltoid or gluteal muscle every two weeks. Patients who have never received risperidone are started on oral risperidone in order to evaluate tolerability. Patients then may be transitioned to Risperdal Consta if oral risperidone is tolerated. Risperidone may interfere with elimination by the kidneys of clozapine (Clozaril), a different type of antipsychotic medication, causing increased levels of clozapine in the blood. This could increase the risk of side effects with clozapine. Biperiden hydrochloride is a prescription medication that belongs to a class of drugs called anticholinergics. Biperiden HCl is a weak peripheral anticholinergic agent. It has, therefore, some antisecretory, antispasmodic and mydriatic effects. In addition, Biperiden possesses nicotinolytic activity. Parkinsonism is thought to result from an imbalance between the excitatory (cholinergic) and inhibitory (dopaminergic) systems in the corpus striatum. The mechanism of action of centrally active anticholinergic drugs such as Biperiden is considered to relate to competitive antagonism of acetylcholine at cholinergic receptors in the corpus striatum, which then restores the balance. The
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parenteral form of Biperiden is an effective and reliable agent for the treatment of acute episodes of extrapyramidal disturbances sometimes seen during treatment with neuroleptic agents. Akathisia, akinesia, dyskinetic tremors, rigor, oculogyric crisis, spasmodic torticollis, and profuse sweating are markedly reduced or eliminated. With parenteral Biperiden, these druginduced disturbances are rapidly brought under control. Subsequently, this can usually be maintained with oral doses which may be given with tranquilizer therapy in psychotic and other conditions requiring an uninterrupted therapeutic program. Only limited pharmacokinetic studies of biperiden in humans are available. The serum concentration at 1 to 1.5 hours following a single, 4 mg oral dose was 4-5 ng/mL. Plasma levels (0.1-0.2 ng/mL) could be determined up to 48 hours after dosing. Six hours after an oral dose of 250 mg/kg in rats, 87% of the drug had been absorbed. The metabolism of Biperiden is also incompletely understood, but does involve hydroxylation. In normal volunteers a single 10 mg intravenous dose of biperiden seemed to cause a transient rise in plasma cortisol and prolactin. No change in GH, LH, FSH, or TSH levels were seen. Biperiden lactate (10 mg/mL) was not irritating to the tissue of rabbits when injected intramuscularly (1.0 mL) into the sacrospinalis muscles and intradermally (0.25 mL) and subcutaneously (0.5 mL) into the shaved abdominal skin. Should be taken with food. Overdosage may result in dilated and sluggish pupils; warm, dry skin; facial flushing; decreased secretions of the mouth, pharynx, nose, and bronchi;
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foul-smelling breath; elevated temperature, tachycardia, cardiac arrhythmias, decreased bowel sounds, and urinary retention. Neuropsychiatric signs include delirium, disorientation, anxiety, hallucinations, illusions, confusion, incoherence, agitation, loss of memory, paranoia, combativeness, and seizures. May progress to stupor, coma, paralysis, and cardiac and respiratory arrest and death. Treatment is sympotomatic and supportive. Contraindicated to Closed-angle glaucoma or narrow angle between iris and cornea; prostatic hyperplasia; myasthenia gravis except to reduce adverse muscarinic effects of an anticholinergic; hypersensitivity; bowel obstruction; megacolon. Another drug given is Diphenhydramine 50 mg HS, an antihistamine used for treating allergic reactions. Histamine is released by the body during several types of allergic reactions and--to a lesser extent--during some viral infections, such as the common cold. When histamine binds to its receptors on cells, it stimulates changes within the cells that lead to sneezing, itching, and increased mucus production. Antihistamines compete with histamine for cell receptors; however, when they bind to the receptors they do not stimulate the cells. In addition, they prevent histamine from binding and stimulating the cells. Diphenhydramine also blocks the action of acetylcholine (anticholinergic effect) and is used as a sedative because it causes drowsiness. The FDA originally approved diphenhydramine in 1946. Diphenhydramine is used for the relief of nasal and non-nasal symptoms of various allergic conditions such as seasonal allergic rhinitis. It is also used to alleviate cold symptoms and
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chronic urticaria(hives). Although antihistamines are the preferred class of drugs in allergic rhinitis, they only reduce symptoms by 40%-60%. Diphenhydramine also is used for allergic reactions involving the eyes (allergic conjunctivitis), to prevent or treat active motion sickness, and for mild cases of Parkinsonism, including drug-induced Parkinsonism. The last two uses (motion sickness and Parkinsonism) are based on the anticholinergic effects of diphenhydramine, and not its antihistamine effects. Diphenhydramine is also used for treating insomnia. Diphenhydramine has its maximal effect about one hour after it is taken. When used to combat insomnia, it is prescribed at bedtime. Patients over the age of 60 years are especially sensitive to the sedating and anticholinergic effects of diphenhydramine, and the dose should be reduced. Doses vary depending on formulation. A common regimen for treating adult allergic reaction is 25-50 mg every 4-6 hours not to exceed 300 mg daily. Diphenhydramine adds to (exaggerates) the sedating effects of alcohol and other drugs than can cause sedation such as the benzodiazepine class of anti-anxiety drugs.
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Recommendation To the patient: He is advised to take part in complying with the treatment; the medication and therapeutic regimen designed for his rehabilitation. He should realize the importance of complying with his medication and the benefits this practice would bring to the improvement of his well-being. To the patients family:

The patients family plays an important role in the patients mental illness and recovery. The family should make themselves physically present so that the patient would feel their support and concern. They are encouraged to continue interacting with the patient so that ideas of violence towards self and others will be diverted. In addition, it is of prime importance that they are orientedand educated regarding the patients mental illness so that they will understand him even better and assist him in his daily activities.
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References mentalhelp.net cureresearch.com World Health Organization, www.who.int schizophrenia.com


http://nursingcrib.com/pathophysiology/pathophysiology-of-schizophrenia/

medicinenet.com
http://wiki.medpedia.com http://www.mims.com
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