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Amyloid beta is produced from the cleavage of amyloid precursor protein by beta and gamma secretases. Amyloid beta aggregates to form plaques, which are thought to disrupt calcium homeostasis and induce neuronal apoptosis and death. Tau proteins stabilize microtubules in neurons, and plaques lead to tau hyperphosphorylation, aggregation into tangles, and microtubule destruction. Both plaques and tangles contribute to neuronal damage in Alzheimer's. Immunotherapy trials have aimed to clear plaques by inducing an immune response to amyloid beta, but early trials had safety issues. Current efforts include DNA vaccines and drugs targeting the beta-secretase enzyme involved in amyloid beta production.
Amyloid beta is produced from the cleavage of amyloid precursor protein by beta and gamma secretases. Amyloid beta aggregates to form plaques, which are thought to disrupt calcium homeostasis and induce neuronal apoptosis and death. Tau proteins stabilize microtubules in neurons, and plaques lead to tau hyperphosphorylation, aggregation into tangles, and microtubule destruction. Both plaques and tangles contribute to neuronal damage in Alzheimer's. Immunotherapy trials have aimed to clear plaques by inducing an immune response to amyloid beta, but early trials had safety issues. Current efforts include DNA vaccines and drugs targeting the beta-secretase enzyme involved in amyloid beta production.
Amyloid beta is produced from the cleavage of amyloid precursor protein by beta and gamma secretases. Amyloid beta aggregates to form plaques, which are thought to disrupt calcium homeostasis and induce neuronal apoptosis and death. Tau proteins stabilize microtubules in neurons, and plaques lead to tau hyperphosphorylation, aggregation into tangles, and microtubule destruction. Both plaques and tangles contribute to neuronal damage in Alzheimer's. Immunotherapy trials have aimed to clear plaques by inducing an immune response to amyloid beta, but early trials had safety issues. Current efforts include DNA vaccines and drugs targeting the beta-secretase enzyme involved in amyloid beta production.
Explain the molecular biology of amyloid-beta, plaques, tau protein and neuronal cell loss in Alzheimer's
disease, and the potential role of amyloid-beta immunotherapy
I. Amyloid Beta a) Amyloid beta is a product of the enzymatic degradation of Amyloid precursor protein i. APP is a transmembrane protein with unknown function. Theories include regulation of synapse formation, neural plasticity, or Iron transport ii. APP has three enzymatic cleavage sites for the enzymes , , and Secretase b) APP is always cleaved by Gamma, but only the combination of gamma and beta cleavage produces amyloid deposition i. Gamma/Alpha secretases cleave APP in the majority of cases, this is non-pathogenic. Alpha secretase is thought to be involved in memory formation ii. Gamma/Beta secretase cleavage produces the amyloid beta protein, which may exist as a monomer, but may spontaneously change conformation and aggregate with other A proteins, forming (generally) Extracellular amyloid plaques 1. It is thought that the Beta pathway is necessary for peripheral nerve myelination c) Not all people produce amyloid plaques, and the process by which the Beta pathway turns pathogenic is not greatly understood i. Several genetic causes have been found, though these arent the majority of cases ii. Mutations in APP, -secretase, or Apolipoprotein E are factors in hereditary Alzheimers iii. Extra copies of the APP increase risk (Down Syndrome) d) Exactly how plaques cause neuronal degeneration is unknown. Plaques may damage calcium homeostasis, induce apoptosis, or selectively accumulate in mitochondria causing energy dysregulation II. Tau Protein a) Tau protein is required to stabilize microtubules, which are important in neurotransmitter vesicle movement in neurons i. Mainly found in the axons of CNS neurons ii. A plaques and the damage they cause lead to a hyperphosphorylation of tau proteins, which causes aggregation in the dendrites, where they form neurofibrillary tangles, further contributing to neural damage iii. This process also leads to the destruction of microtubules in the neurons III. Immunotherapy, and new drug targets a) The first clinical trials for an Alzheimers vaccine were performed 15 years ago. i. Strong evidence for halting of disease progression, and even plaque clearing in mice. ii. Stopped at phase II. 6% chance of hydrocephalus in patients in trial iii. Current vaccine ideas include a DNA vaccine. Injecting the A gene in hopes that the protein will be produced in small amounts and an immune response is mounted b) Attempts to use immunoglobulin therapy are also being trialled c) New drug targets include the enyzmes involved in the production of A i. Two drugs are currently in clinical trial, to be completed in 2019, which target Beta-Secretase 1, called BACE inhibitors