Lecture 2 Flashcards
What is dementia and AD?
problem-solving or language.
Gradual onset & progressive
AD is the commonest cause of dementia but not all dementia is due to AD.
Alois Alzheimer - 1906
Post-mortem: the cerebral cortex was thinner and senile plaque, previously only encountered in elderly people, were found along with neurofibrillary tangles.
Alzheimers Pathology
Amyloid Plaques around neuronal bodies
Test for plaques
A) Plaque evident on routine H&E stained section of frontal cortex;
(B) tangle in a hippocampal pyramidal neuron on routine H&E stained section;
(D) immunohistochemistry against Aβ highlights plaques;
(E) immunohistochemistry against tau highlights tangles;
Pathology overlap
25% of all patients with AD develop parkinsonism.
50% of all cases of PD develop AD-type dementia after 65 years of age (Hansen et al. 1990).
70% of patients with sporadic AD display Parkinson’s pathology (Lippa et al. 1998; Trojanowski et al. 1998; Hamilton 2000
NINCDS– ADRDA criteria -1984
(1) the clinical diagnosis of AD could only be designated as “probable” while the patient was alive and could not be made definitively until AD confirmed at PM
(2) the clinical diagnosis of AD could be assigned only when the disease had advanced to the point of causing significant functional disability and met the threshold criterion of dementia.
Psychiatric changes in AD
Subtle behaviour changes: inattentiveness, mild cognitive dulling, social withdrawal, emotional withdrawal and agitation
Apathy (most freq change), disengagement
Psychotic symptoms: delusions (delusions of theft) or hallucinations
Agitation, anxiety.
Specific clinical phenotype
Presence of an early and significant episodic memory impairment (isolated or associated with other cognitive or behavioural changes that are suggestive of a mild cognitive impairment that includes the following features:
Gradual and progressive change in memory function reported by patient or informant over more than 6 months
Objective evidence of an amnestic syndrome of the hippocampal type,* based on significantly impaired performance on an episodic memory test with established specificity for AD, such as cued recall with control of encoding test
In vivo evidence of AD Pathology
Decreased Aβ1–42 together with increased T-tau or P-tau in CSF
Increased tracer retention on amyloid PET
AD autosomal dominant mutation present (in PSEN1, PSEN2, or APP)
AD affects what brain regions
Early degenrationof medial temporal lobe before degeneration spreads to temporal neocortex, frontal and parietal association areas.
Cognitive Profile in AD
Episodic memory: frequent intrusions and repetition errors, and high numbers of false positive errors in recall
Complex attention/executive function
Disproportionate impairment of category fluency as compared to phonemic fluency
Differentials
Vascular/Mixed Dementia
Sub-cortical-frontal pattern (attention difficulties, motor/cognitive slowing and executive problems) and visuo-spatial difficulties
Dementia with Lewy Bodies
Fluctuating cognition, pronounced disturbances in attention and concentration, working memory and early visuoperceptual deficits, visual hallucinations and spontaneous Parkinsonism
Depressive pseudo dementia
Sub-types of dementia
Alzheimer’s disease (AD) - 62%
Vascular dementia (VaD) - 17%
Mixed dementia (AD & VaD) - 10%
Dementia with Lewy Bodies (DLB) - 4%
Fronto-temporal lobe dementias - 2%
Parkinson’s dementia - 2%
Other types - 3%
Non- memory dysfunction in AD
(I) Apraxia / visuospatial dysfunction 12%:
(II) Language dysfunction- 9%
(III) Aphasic-apraxic-agnosic syndrome
(IV) Posterior cortical atrophy (PCA- 1%):
(V) Dysexecutive syndrome- 2
(I) Apraxia / visuospatial dysfunction 12%:
difficulties in spatial orientation, resulting in getting lost
(II) or problems in praxis, for example dressing apraxia
