Behavioral Science: Dementia 1-3

Question 1

Age-associated cognitive changes

Answer 1

• Difficulty retrieving words and names
• Slower processing speed
• Difficulty sustaining attention when faced with competing environmental stimuli
• Learning new shit takes more effort
• No functional impairment

Question 2

Mild cognitive impairment

Answer 2

• memory complaint corroborated by an informant
• objective memory impairment for age and education
• preserved general cognition
• normal ADL
• NOT demented

Question 3

Amnestic MCI

Answer 3

• Memory loss not meeting criteria for dementia
• Progresses to AD at a rate of 10-15%/year (vs. 1-3% incidence in gen pop)
• May be earliest phase of AD
• Clinical dx (no formal test)

Question 4

Dementia

Answer 4

Memory decline/impairment and at least one of the following:

• Aphasia
• Apraxia
• Impaired executive fxn
• Agnosia

Cognitive deficits must impact social and occupational function

Dx must be made in presence of a clear sensorium

Question 5

Early onset AD

Answer 5

• ages 30-60
• rare, MC familial
• gene mutations: 1 (presenilin 2), 14 (presenilin 1), 21 (amyloid precursor protein) are abnormal

Question 6

Late onset AD

Answer 6

• MC form
• After age 60
• Combination of factors
• Chromosome 19- apolipoprotein E4 gene implicated

Question 7

Alzheimers disease

Answer 7

• MCC dementia, presents w/ deficits in recent memory, progressing to global impairment of cognition
• Usually sporadic and late onset
• AD
• Neuronal and synaptic loss affecting cortical and some subcortical areas (ex. nucleus basalis of Meynert)

Question 8

Gross findings of AD

Answer 8

Cerebral atrophy especially affecting temporal, parietal, and frontal areas, with ventricular enlargement

Question 9

Microscopic findings in AD

Answer 9

• Amyloid plaques consisting of extracellular deposits of beta-amyloid peptides, often associated w/ dystrophic plaques
• Amyloid Beta deposits in cortical and leptomeningeal arteries and arterioles
• Filamentous intracellular inclusions of tau protein called neurofibrillary tangles and neuropil threads
• Granulovacuolar degeneration
• Hirano bodies

Question 10

Frontotemporal lobar degeneration

Answer 10

Types: Tau (MC), TDP, FUS

• Earlier onset than AD
• Lobar degeneration affects anterior frontal and superior temporal lobes, spares occipital and parietal lobes
• gross “knife edge” appearance

Question 11

AD risk factors

Answer 11

• increasing age
• females
• family history of dementia
• less education, income, SES
• depression
• head injury
• low folate, B12
• elevated plasma homocysteine
• apolipoprotein E4 allele
• postoperative delirium
• alcohol abuse

Question 12

Early symptoms of Ad

Answer 12

Cognitive: trouble keeping appointments, difficulty finding words, misplacing objects

Functional: difficulty driving, difficulty selecting clothes, missing appointments, problems at work

Behavioral: Subtle personality changes, social withdrawal, depression

Question 13

Differences between depression v dementia

Answer 13

Depressed patients:

• demonstrate less motivation during cognitive testing
• Express cognitive complaints that exceed measured deficits
• Maintain language and motor skills

Question 14

Brain imaging for AD

Answer 14

• Not routinely indicating, only considered when: focal findings on exam, rapid onset/decline, or Hx of falls/head trauma
• Nonspecific findings common in AD: lacunar infarcts, small vessel and white matter disease

Question 15

Frontotemporal Dementia vs. Alzheimers

Answer 15

Frontotemporal dementia has:

• insidious onset, gradual progression
• early decline in social interpersonal conduct
• early impairment in regulation of personal conduct w/ lack of insight
• early emotional blunting
• characterized by behavioral abnormalities
• memory loss occurs LATER

Question 16

Drugz for frontotemporal dementia

Answer 16

• No role for cholinesterase inhibitors
• Careful use of atypical antipsychotics
• Divalproex for behavioral control
• SSRIs for irritability, depression, impulsive behaviors

Question 17

Drugz for Alzheimers

Answer 17

• Cholinergic therapy
• NMDA receptor antagonists
• Investigational agents
• Tx of neuropsychiatric sx

Question 18

Why do anticholinesterases work in Alzheimers?

Answer 18

Because Alzheimers-associated degeneration of the basal nucleus of Meynert results in widespread Ach deficiency –> memory defects

Blocking degeneration of Ach leaves enough in synapse to slow progression of memory loss

Question 19

Cholinesterase inhibitors for mild-moderate AD

Answer 19

• Tacrine (now obsolete)
• Donepezil
• Rivastigmine
• Galantamine

Question 20

Glutaminergic tx for AD

Answer 20

• Memantine

Question 21

Vascular dementia

Answer 21

• Multi-infarct dementia
• Cerebral amyloid angiopathy
• HTN-related small vessel disease

Question 22

Hypertensive small vessel disease

Answer 22

• Arteriosclerosis of small arteries and arterioles supplying deep grey and white matter
• Lacunar infarcts
• Subcortical leukoencephalopathy
• Subcortical dementia: cognitive slowing, impaired problem solving, visuospatial abnormalities, disturbances of mood and affect

Question 23

Vascular dementia sx

Answer 23

• “step-wise progression” - can be abrupt after CVA
• Usually seen w/ cardiovascular risk factors
• “Mixed” dementia with AD or Lewy Body is not unusual
• Emotional lability

Question 24

Vascular Dementia tx

Answer 24

• Control cardiovascular risk factors: control BP, statins, stop smoking, control blood sugar, diet, exercise
• Cholinesterase inhibitors

Question 25

Lewy bodies

Answer 25

Characterized by intracellular, fibrillar deposits of a presynaptic terminal protein called a-synuclein

Question 26

Parkinsons Disease

Answer 26

• MC sporadic
• Resting tremor, akinesia, bradykinesia, rigidity, shuffling gait, postural instability
• Dopaminergic deficit
• Responsive to L-Dopa

Question 27

Gross and microscopic neuropathology of PD

Answer 27

Gross: pallor of the substantia nigra

Microscopic: Degeneration and loss of the pigmented, dopaminergic neurons of the SNpc and other pigmented neurons of the brainstem, eg. locus coeruleus. Often contain 1+ eosinophilic inclusions called Lewy Bodies. Striatum, thalamus, and some cortical regions are FUNCTIONALLY AFFECTED by the loss of dopaminergic input.

Question 28

Pathogenesis of PD

Answer 28

• a-synuclein is a pre-synaptic protein involved in regulation of synaptic vesicle trafficking
• Lewy bodies are composed primarily of fibrillar aggregates of a-synuclein (if in neural processes–> Lewy neurites)
• Aggregates are toxic and cause impairment of protein degradation, inhibition of oxidative phosphorylation, impairment of axonal transport, and cause oxidative stress
• Pesticide may be risk factor

Question 29

Dementia with Lewy Bodies

Answer 29

• Sporadic, primarily late onset
• Memory frequently less affected than AD
• Frontal and subcortical features like deficits in attention and alertness are prominent
• Pronounced fluctuations and variations in symptoms
• Neuropsychiatric symptoms: visual hallucinations + delusions
• Motor symptoms of PD are variably present

Question 30

Gross and microscopic neuropathology of Dementia w/ Lewy Bodies

Answer 30

Gross: Nigral pallor. Cortical atrophy is less severe than AD. Atrophy of limbic areas is often significant.

Microscopic:

1. “Cortical”-type LBs in frontal, temporal, insular cortex, limbic areas
2. Nigral LBs
3. LNs, esp in hippocampus and striatum
4. Plaques and tangles, dual dx of DLB and AD applies in most cases

Question 31

Clinical Sx of LBD

Answer 31

• Short term memory loss, gradual onset
• Visual hallucinations
• Cognitive fluctuations
• REM sleep disorder
• Frequent falls
• Autonomic dysfunction

Question 32

Drugz for LBD

Answer 32

• Cholesterase inhibitors for symptomatic support
• Trial of carbidopa/levodopa for severe movement sx
• AVOID antipsychotics (increased sensitivity)
• REM sleep disorder: clonazepam

Question 33

Lewy Body dementia vs Parkinson’s dementia

Answer 33

LB: Onset of dementia WITHIN 12 months of parkinsonism
PD: Onset of dementia MORE THAN 12 months after Dx of

Question 34

MMSE

Answer 34

• Standardized 30 point rating scale
• Screening tool, NOT diagnostic
• Not specific for dementia type
• Scoring can be impacted by age, education, ethnicity:
  Normal 30-27
  Mild 27-20
  Moderate 20-10
  Severe 10 or lower

Question 35

MoCA

Answer 35

• Standardized 30 point rating scale
• Screening tool, NOT diagnostic
• Not specific for dementia type
• Scoring can be impacted by age, education, ethnicity:
  Normal >26
  Mild 18-26
  Moderate 10-17
  Severe

Question 36

ADL vs IADL

Answer 36

ADL: walking, bathing, dressing, toileting, eating, etc.

IADL: cooking, driving, using computer, managing finances, managing medications

Question 37

Adult home

Answer 37

• provides room and meals
• can add on assistance with daily activities
• no complex medical problems
• not always licensed or monitored by authorities
• cash only

Question 38

Assisted living facility

Answer 38

• assistance with IADL
• can add on some basic ADL for extra fees
• No medical or nursing care onsite
• Cash only, not covered by medicaid/medicare

Question 39

Skilled nursing facility

Answer 39

• Daily skilled nursing care, onsite medical care
• Dependent in all basic ADL
• Most patients have advanced dementia
• Cash until money is depleted
• Most residents on Medicaid