Neurology: Dementia

Question 1

What is Dementia?

Answer 1

Clinical syndrome with multiple causes defined by:

• Acquired loss of higher mental function affecting two or more cognitive domains including episode memory, language function, frontal executive function, visuospatial function, apraxia
• Being of sufficient severity to affect ADLs
• Chronic condition (>6 months)

Dementia robs patients of their independence and serious burden on carers and a major socioeconomic challenge for society as a whole

Question 2

What are key parts of taking a dementia history?

Answer 2

• Memory:
  
  • Is the patient repetitive, e.g. with questions?
  • Is there a temporal gradient of amnesia – preservation of more distant memories with amnesia for recent events?
  • Is there difficulty learning to use new devices, e.g. computer, mobile phone?
• Functional ability:
  
  • Has work performance or ability to cook and do domestic tasks declined?
  • Has responsibility for finances and administration shifted to the spouse?
  • Does the patient get easily muddled?
• Personality and frontal lobe function:
  
  • Has personality altered?
  • More aggressive/apathetic/lacking initiative
  • Disinhibition
  • Change in food preference or religiosity
• Language:
  
  • Difficulty with word finding or remembering names
• Visuospatial ability:
  
  • Does the patient get lost in familiar places?
  • Difficulty dressing, e.g. putting jacket on the wrong way round
• Psychiatric features:
  
  • Features of depression
• Tempo of progression
• Family history of dementia
• Alcohol and drug use
• Medication
• Any other neurological problems, e.g. parkinsonism, gait disorder, strokes

Question 3

What are examinations for Dementia?

Answer 3

• Bedside Cognitive Assessment
  
  • Mini-mental state examination
    
    • commonly used to assess cognitive function but has its limitations such as relative insensitivity to milder cognitive impairment and to frontal lobe dysfunction
  • ACE is a tool used to address deficiencies of MMSE
    
    • Clock drawing for visuospatial function
    • Naming and reading tasks for language function
    • Verbal fluency
    • Frontal assessment battery: Conceptual similarity to abstract thinking and stop-go tasks
  • Check for primitive reflexes such as grasp, palmo-mental and pout reflexes and preservation or utilization behaviour with frontal lobe involvement
• Test
  
  • Limb praxis – copying hand gestures and miming tasks
  • Oro-buccal praxis – show me how you would blow out candle

Question 4

What are investigations for Dementia?

Answer 4

• Blood Tests: Full blood count, Erythrocyte sedimentation rate, Vitamin B12, Urea and electrolytes, Glucose, Liver Biochemistry, Serum Calcium, Thyroid Stimulating Hormone, T3, T4, HIV Serology, Syphilis Serology
• Imaging: CT or MRI brain scan to exclude structural tumours or hydrocephalus. Radionuclide scan can also directly visualize the amyloid depositions
• Other (selected patients only): Cerebrospinal fluid, Genetic Studies, Electroencephalography, Brain Biopsy
• Detailed neuropsychiatric assessment: appropriate in most this quantification of relative involvement of different cognitive domains
• Younger patients (<65 years): more intensive investigation may be necessary such as EEG, Genetic tests, Voltage-gated potassium channel antibodies, anti-neuronal antibodies, HIV serology and metabolic tests
• CSF examination:
  
  • Alzheimer’s disease – raised tau and reduced Aβ42
  • Creutzfeldt-Jakob disease – Protein 14-3-3 increased

Question 5

What are the risk factors for Alzheimer’s Disease?

Answer 5

Genetics

• 1^st degree relative with Alzheimer’s disease confers doubled lifetime risk of AD. Rare autosomal dominant monogenic ear-onset forms of familial AD with high penetrance caused by mutations in specific genes taken together for 1% of AD.
• Other genes are E4 allele, Amyloid precursor protein, Presenilin 1 and 2

Environmental

• Age
• Head trauma
• Vascular risk factors increase

Question 6

What are clinical features of Alzheimer’s Disease?

Answer 6

• Memory Impairment: episodic memory is affected. Progressive loss of ability to learn, retain and process new information. Relative preservation of distant memory and amnesia for more recent events.
• Language: Usually become impaired as disease advances. Difficulty with word finding characteristic.
• Apraxia: ability to carry out skilled motor activities is impaired
• Agnosia: failure to recognise object such as clothing and place or people
• Frontal executive function: organising, planning and sequencing is impaired
• Parietal presentation: visuospatial difficulties and difficulty with orientation in space and navigation may occur typically in later stages of disease
• Posterior Cortical Atrophy: least common presentation of AD. Memory initially well preserved
• Personality: basic personality and social behaviour remain intact until late AD
• Anosognosia: lack of insight by patient into their difficulties is common
• Tempo: onset insidious and progression gradual but inexorable over decade or longer with eventual deVere deficits in multiple cognitive domains
• Late non-cognitive features: myoclonus may develop followed by seizures. Sleep-wake cycle reversal and incontinence may place strain on carers. Motor function usually strikingly preserved so patient capable of wandering and getting lost

Question 7

What is the molecular pathology and aetiology of Alzheimer’s Disease?

Answer 7

• Deposition of β-amyloid (Aβ) in amyloid plaques in the cortex. Amyloid may also be laid down in cerebral blood vessels lead to amyloid angiopathy
• Structural and conformation changes in Tau protein which are binding blocks of neurofibrillary tangle. The protein aggregates damages synapses and ultimately lead to neuronal death

Question 8

What are investigations for Alzheimer’s Disease?

Answer 8

• MRI – characteristic atrophy of mesial temporal lobe structures including hippocampi, progressing eventually to generalized cerebral atrophy
• CSF tau and β-amyloid measurement is helpful in cases of diagnostic difficulty but not yet widely available

Question 9

What are early features of dementia with lewy bodies and parkinson’s diseases dementia?

Answer 9

• Visual hallucinations: often take form of people or animals or sense of presence
• Fluctuating cognition with variation in attention and alertness
• Sleep disorders
• Dysautonomia
• Parkinsonism
• Memory loss may be absent in early stages. Delusion and transient loss of consciousness occur.
• Lewy bodies, inclusion containing aggregates of protein α-synuclein first described in Parkinson’s disease, are found in the cortex.

Question 10

What are differences between dementia with lewy bodies and Parkinson’s disease dementia?

Answer 10

• In dementia with Lewy bodies
  
  • cognitive features dominate
  • parkinsonism may evolve later and is typically mild.
• In Parkinson’s disease dementia
  
  • cognitive problems are late feature occurring at least 1 year after onset and usually after age of 75.

Both conditions respond to cholinesterase inhibitors. Patient with DLB may be very sensitive to neuroleptic drugs with dramatic worsening

Question 11

What is Vascular Dementia?

Answer 11

• Multiple infarct dementia, cerebral small-vessel disease and post stroke dementia. Most vascular dementias are of mixed cause
• Vascular dementia distinguished from AD by its clinical features and imaging

Question 12

What is the history of Vascular Dementia?

Answer 12

• Dementia can be progressive and similar to AD. Sometimes history of TIAs or dementia follow succession of cerebrovascular events and has stepwise course
• Apraxic gait disorder, pyramidal signs and urinary incontinence are common additional features

Question 13

What is the investigation for Vascular Dementia?

Answer 13

• Widespread small-vessel disease seen on MRI and may produce variety of cognitive deficits reflecting site of ischemic damage

Question 14

What is Frontotemporal dementia (Pick’s Disease)?

Answer 14

• Describe group of neurodegenerative disorders characterised by asymmetric frontal lobe and temporal lobe atrophy on MRI and at post-mortem
• There is no cure or specific treatment presently

Question 15

What is the pathology of Frontotemporal dementia (Pick’s Disease)?

Answer 15

• 25% cases are familial associated with mutations in tau and progranulin gene and C9ORF72 gene.
• Consists of deposition of abnormally aggerated proteins: phosphorylated tau, transactive response DNA-binding protein 43 or fused in sarcoma. 10% of patients have overlap syndrome with motor neurone disease or parkinsonian disorders such as progressive supranuclear palsy.

Question 16

What is the presentation of Frontotemporal Dementia?

Answer 16

• Frontal presentation is characterised by
  
  • Personality change
  • Emotional blunting
  • Disinhibition
  • Carelessness
  • Behavioural change
  • Striking preservation of episodic memory
• Temporal presentation:
  
  • Primary progressive aphasia characterised by progressive impaired of language function.
  • Involvement of left temporal lobe produces with semantic dementia with fluent speech lacking in meaningful content and progressive difficulty with comprehending meaning of words.
  • Second temporal lobe presentation is progressive non-fluent aphasia due to peri-sylvian atrophy with verbal loss of cerebral fluency and increasingly telegrammatic speech

Question 17

What are types of Creutzfeldt-Jakob Disease (CJD)?

Answer 17

• Sporadic CJD
• Iatrogenic CJD
• Familial CJD
• Variant CJD

Question 18

What are features of Sporadic CJD?

Answer 18

• Most common form occurring over 50 years of age through to due to spontaneous somatic mutations in PRNP gene or stochastic conformational changes.
• Rapidly progressive dementia leads to death within 6 months onset. Rapidly progressive cognitive decline should always lead to CJD suspicion.
• Presence of myoclonus is a clinical clue

Question 19

What are features of Iatrogenic CJD?

Answer 19

• Transmitted from neurosurgical instruments, transplant material and cadaveric pituitary-derived growth hormone taken from patients with CJD or pre-symptomatic CJD.
• There is a long incubation period of several years.

Question 20

What is the key features of Familial CJD?

Answer 20

Associated with PRNP gene mutations

Question 21

What are key features of Variant CJD?

Answer 21

• Patients are younger than sporadic cases with mean age of 29 and it has a longer disease course.
• Early symptoms are neuropsychiatric, followed by ataxia and dementia with myoclonus or chorea.
• Diagnosis confirmed by tonsillar biopsy, but sensitive blood test has been developed.
• Caused by the same prion strain as BSE. Transmission by blood transfusion may also occur

Question 22

What are principles of treatment for Dementia mangement?

Answer 22

• Reversible causes are normal pressure hydrocephalus or frontal meningioma.
• Management of other conditions is supportive to preserve dignity and provide care for as long as possible in familiar home environment.
• Dementia clinical nurse form central part of multidisciplinary team. Burden of disease frequently falls on relative

Question 23

What is the management for Dementia?

Answer 23

• General measures
  
  • Participation in cognitively demanding activities in later life may protect against or delay onset of dementia. High dose B vitamin may help
• Cognitive Enhancing Drugs
  
  • Cholinesterase inhibitors
  • Memantine
• Psychiatric and behavioural problems
• Financial and legal issues: Set up lasting power of attorney to allow spouse or relative to deal with their financial affairs on their behalf when they lose capacity
• Driving: Inform DVLA for driving safety assessment

Question 24

What is the mechanism of action and side effects of Cholinesterase Inhibitors?

Answer 24

• Mechanism of Action
  
  • Increase brain acetylcholine levels by inhibiting CNS acetylcholinesterase. Patients with AD have central cholinergic deficit.
  • Small but significant improvement in memory, cognition and function
  • Can be effective in Dementia Lewy body and Parkinson’s dementia
• Side effect:
  
  • Particularly cholinergic gastrointestinal symptoms.
  • ECG should be performed to exclude cardiac conduction deficits before starting therapy

Question 25

What are mechnisms of actions of Memantine?

Answer 25

• NMDA receptor antagonist and used in moderate or severe AD or where cholinesterase inhibitors are not tolerated.
  
  • Generally, well tolerated.

Question 26

What are psychiatric and behavioural problems in dementia?

Answer 26

• Depression is common and may be hard to differentiate from dementia syndrome.
  
  • Trial of antidepressant may be appropriate
• Behavioural disturbance and hallucination may occur in late stage disease.
  
  • Use of antipsychotic medication significantly increases stroke risk in patient in dementia and only used last result