Post on 24-Feb-2016
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VIII. NEURODEGENERATIVE DISEASES
- Are disorders characterized by the cellular degeneration of subsets of neurons that typically are related by function, rather than by physical location in the brain.
- Many of these disorders are associated with the accumulation of abnormal proteins, which serve as histologic hallmarks of specific disorders
- An important but unanswered question is why these abnormal proteins tend to affect particular neurons
, since the involved proteins are widely expressed throughout the nervous system
- The possible explanation that subtle differences among subtypes of neurons are presumed to explain why particular neurons are affected in specific disorders.
- The clinical manifestations of degenerative diseases are dictated by the pattern of neuronal dysfunction:
A. Those affect the cortical neurons result in dementia;
B. Those affect basal ganglia neurons result in movement disorders
C. Those that affect the cerebellum result in ataxiaNote: Although many degenerative diseases have
primary targets, other brain regions are often affected later in the course of the illness
Dementia := is defined as the development of memory
impairment and other cognitive deficits severe enough to decrease the affected person's capacity to function at the previous level despite a normal level of consciousness.
- It arises during the course of many neurodegenerative diseases; but it also accompany other diseases that injure the cerebral cortex such as:
1. Infectionsa. Prion disease & neurosyphilisb. HIV associated neurocognitive disorderc. Chronic meningitis2. Vascular and traumatic diseasesa. Multifocal cerebral infarctionb. b. Chronic traumatic encephalopathy
3. Metabolic and nutritional diseases- Thiamine , Vit B12 and Niacin deficiencies4. Miscellaneous such as toxicity from lead and
manganese
I. Alzheimer Disease (AD)- Is the most common cause of dementia in the
elderly population manifests with the insidious onset of impaired higher intellectual function, altered mood and behavior.
- Later, this progresses to disorientation, memory loss, and aphasia, findings indicative of severe cortical dysfunction,
- And over another 5 to 10 years, the patient becomes profoundly disabled, mute, and immobile.
- Death usually occurs from intercurrent pneumonia - Age is an important risk factor for AD;a. The incidence is 3% in persons 65 to 74 years old, b. 9% in 75 to 84 years old to 47% in those older than
84 - Most cases of AD are sporadic - 5% to 10% are familial. • Sporadic cases rarely present before 50 years of
age, but early onset is seen with some heritable forms
PATHOGENESIS :- Study of the familial forms of AD supports a model
in which Aβ amyloid, accumulates in the brain over time, initiating a chain of events that result in AD.
1- Aβ is created when the transmembrane protein amyloid precursor protein (APP) is sequentially cleaved by the enzymes β-amyloid converting enzyme (BACE) and γ-secretase
- APP also can be cleaved α-secretase and γ-secretase, which liberates a different peptide that is nonpathogenic
Aβ peptide genesis and consequences in AD
.How deposits of Aβ cause manifestation 1. While large deposits are a feature of end-stage
AD, small aggregates of Aβ may also be pathogenic, as
a. They alter neurotransmission and areb. Toxic to neurons and synaptic endings found in
the superficial cerebral cortex,
Large deposits, in the form of plaques,:1. elicite a local inflammatory response Lead to
neuronal death 2. And may cause altered region-to-region
communication through mechanical effects on axons and dendrites.
3. Aβ amyloid also leads to hyperphosphorylation of the neuronal microtubule binding protein tau and this increased level of phosphorylation causes tau to redistribute from axons into dendrites and cell bodies, where it aggregates into tangles, which also contribute to neuronal dysfunction and cell death.
Familial forms1. Mutations in APP or in components of γ-secretase
(presenilin-1 or presenilin-2) lead to familial AD by increasing the rate at which Aβ is generated.
2. The APP gene is located on chromosome 21, - The risk of AD is higher in Down syndrome: an
extra copy of the APP gene, is present in patients with trisomy 21
3. The other major genetic risk factor is a variant of apolipoprotein E called Εε4 (ApoE ε 4).
- Each ApoE ε 4 allele that is present increases the risk of AD by approximately 4 fold and also appears to lower the age of onset.
- How ApoE ε 4 influences Aβ accumulation is unknown;
a. It may increase Aβ aggregation or deposition,b. Or decrease Aβ clearance
Macroscopic examination of the brain1. Variable degree of cortical atrophy, most severe in
the frontal, temporal, and parietal lobes. 2. With significant atrophy, there is compensatory
ventricular enlargement (hydrocephalus ex vacuo). At the microscopic level, AD is diagnosed by the
presence 1. Of Amyloid plaques (an extracellular lesion) 2. And neurofibrillary tangles (an intracellular lesion)
. Note:- These lesions may also be present to a lesser
extent in the brains of elderly non-demented persons, so the current criteria for a diagnosis of AD are based on a combination of clinical and pathologic features.
- There is a fairly constant progressive involvement of different parts of the brain.:
Pathologic features of AD
Pathologic changes (specifically plaques, tangles, and the associated neuronal loss and glial reaction)
a. Are evident first in the entorhinal cortex b. Then in the hippocampal formation, c. And finally in the neocortex.
1. Neuritic plaques : - Are focal, spherical collections of dilated,
tortuous, silver-staining neuritic processes (dystrophic neurites), often around a central amyloid core
- Range in size from 20 to 200 μm in diameter - Plaques can be found in the hippocampus and
amygdala as well as in the neocortex
- There usually is relative sparing of primary motor and sensory cortices until late in the disease course.
2. Diffuse plaques: - Are Aβ deposits lacking the surrounding neuritic
reaction, typically are found in the superficial cerbral cortex, basal ganglia , and the cerebellar cortex
2..Neurofibrillary tangles :- Are bundles of paired helical filaments visible as
basophilic in the cytoplasm of the neurons that displace or encircle the nucleus;
- Tangles can persist after neurons die, becoming a form of extracellular pathology and are commonly found in:
a. In the entorhinal cortex,b. In pyramidal cells of the hippocampus and
amygdala, c. The basal forebrain, and the raphe nuclei. - A major component of paired helical filaments is abnormally hyperphosphorylated tau- Tangles are not specific to AD, being found in
other degenerative diseases