Dementia: Difference between revisions
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== |
== Background == |
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=== Definition === |
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* Acquired cognitive decline that impairs activities of daily living (ADLs) |
* Acquired cognitive decline that impairs activities of daily living (ADLs) |
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* Without impairment of ADLs, it is referred to as mild cognitive impairment (MCI) |
* Without impairment of ADLs, it is referred to as mild cognitive impairment (MCI) |
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* Early-onset is prior to 65 years |
* Early-onset is prior to 65 years |
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== Etiologies == |
=== Etiologies === |
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* '''[[Alzheimer disease]]''': insidious onset and gradual progression, usually starting with memory and learning but also behavioural and psychological manifestations |
* '''[[Alzheimer disease]]''': insidious onset and gradual progression, usually starting with memory and learning but also behavioural and psychological manifestations |
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* '''[[Vascular dementia]]''' |
* '''[[Vascular dementia]]''' |
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* Less common |
* Less common |
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** Vitamin deficiencies |
** Vitamin deficiencies |
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*** Thiamine (B1), |
*** Thiamine (B1), causing [[Wernicke encephalopathy]] |
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*** Cobalamin (B12), causing subacute combined degeneration |
*** Cobalamin (B12), causing subacute combined degeneration |
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*** Niacin (B3), causing pellagra |
*** Niacin (B3), causing [[pellagra]] |
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** Endocrinopathy |
** Endocrinopathy |
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*** Hypothyroidism |
*** [[Hypothyroidism]] |
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*** Adrenal insufficiency and Cushing |
*** [[Adrenal insufficiency]] and [[Cushing syndrome]] |
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*** |
*** [[Hypoparathyroidism]] and [[hyperparathyroidism]] |
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** Organ failure |
** Organ failure |
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*** Renal failure |
*** Renal failure |
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*** Pulmonary failure |
*** Pulmonary failure |
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** Chronic infections |
** Chronic infections |
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*** HIV |
*** [[HIV]] |
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*** Neurosyphilis |
*** [[Neurosyphilis]] |
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*** |
*** [[JC virus]], causing progressive multifocal leukoencephalopathy (PML) |
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*** Tuberculosis, fungal infections, and protozoa |
*** [[Tuberculosis]], fungal infections, and protozoa |
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*** Whipple |
*** [[Whipple disease]] |
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** Head trauma and diffuse |
** Head trauma and diffuse brain damage |
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*** Dementia pugilistica |
*** [[Dementia pugilistica]] |
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*** Chronic subdural hematoma |
*** [[Chronic subdural hematoma]] |
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*** Postanoxia |
*** Postanoxia |
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*** Postencephalitis |
*** Postencephalitis |
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*** Normal |
*** [[Normal pressure hydrocephalus]] |
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** Neoplastic |
** Neoplastic |
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*** Primary or secondary brain tumour |
*** Primary or secondary brain tumour |
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*** Paraneoplastic limbic encephalitis |
*** [[Paraneoplastic limbic encephalitis]] |
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** Toxins |
** Toxins |
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*** Drug, medication, and narcotic overdose |
*** Drug, medication, and narcotic overdose |
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*** Organic toxins |
*** Organic toxins |
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** Psychiatric |
** Psychiatric |
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*** Depression (pseudodementia) |
*** [[Depression]] (pseudodementia) |
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*** Schizophrenia |
*** [[Schizophrenia]] |
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*** Conversion disorder |
*** [[Conversion disorder]] |
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** Degenerative disorders |
** Degenerative disorders |
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*** Huntington |
*** [[Huntington disease]] |
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*** [['''Dementia with Lewy bodies''']] |
*** [[Dementia with Lewy bodies|'''Dementia with Lewy bodies''']] |
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*** Progressive supranuclear palsy |
*** [[Progressive supranuclear palsy]] |
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*** Multisystem atrophy |
*** [[Multisystem atrophy]] |
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*** Hereditary ataxias |
*** [[Hereditary ataxia|Hereditary ataxias]] |
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*** Motor neuron disease, such as amyotrophic lateral sclerosis (ALS) |
*** Motor neuron disease, such as [[amyotrophic lateral sclerosis]] (ALS) |
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*** '''[[Frontal lobe dementia]]''' |
*** '''[[Frontal lobe dementia]]''' |
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*** Corticobasal degeneration |
*** [[Corticobasal degeneration]] |
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*** Multiple sclerosis |
*** [[Multiple sclerosis]] |
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*** Adult Down syndrome with Alzheimer disease |
*** Adult [[Down syndrome]] with Alzheimer disease |
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*** ALS Parkinson dementia complex of Guam |
*** ALS Parkinson dementia complex of Guam |
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*** Prion disease (Creutzfeld-jakob and Gerstmann-Straussler-Scheinker diseases) |
*** [[Prion disease]] (Creutzfeld-jakob and Gerstmann-Straussler-Scheinker diseases) |
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** Miscellaneous |
** Miscellaneous |
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*** Sarcoidosis |
*** [[Sarcoidosis]] |
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*** Vasculitis |
*** [[Vasculitis]] |
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*** Cerebral autosomal dominant arteriopathy with subcortical infarcts and leukoencephalopathy (CADASIL) |
*** [[Cerebral autosomal dominant arteriopathy with subcortical infarcts and leukoencephalopathy]] (CADASIL) |
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*** Acute intermittent porphyria |
*** [[Acute intermittent porphyria]] |
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*** Recurrent non-convulsive seizures |
*** Recurrent non-convulsive seizures |
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* About 20% have a reversible cause (primarily depression, hydrocephalus, and alcohol abuse) |
* About 20% have a reversible cause (primarily depression, hydrocephalus, and alcohol abuse) |
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== Clinical |
== Clinical Manifestations == |
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{| class="wikitable" |
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{| |
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! Disease |
! Disease |
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! Early symptoms |
! Early symptoms |
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| Posterior parietal atrophy; hippocampi larger than in AD |
| Posterior parietal atrophy; hippocampi larger than in AD |
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|- |
|- |
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| |
| Creutzfeldt-Jakob disease |
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| Dementia, mood, anxiety, movement disorder |
| Dementia, mood, anxiety, movement disorder |
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| Variable, frontal/executive, focal cortical, memory |
| Variable, frontal/executive, focal cortical, memory |
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*** Brain biopsy |
*** Brain biopsy |
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== Management == |
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* Symptoms include psychosis, aggression, agitation, mania, apathy |
* Symptoms include psychosis, aggression, agitation, mania, apathy |
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* History most important |
* History most important |
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** Risperidone for severe behaviours, but increases risk of death |
** Risperidone for severe behaviours, but increases risk of death |
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** Document their behaviours over several weeks to document benefit or harm, then reassess every three months if antipsychotics are used |
** Document their behaviours over several weeks to document benefit or harm, then reassess every three months if antipsychotics are used |
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== Further Reading == |
== Further Reading == |
Latest revision as of 16:34, 15 October 2022
Background
Definition
- Acquired cognitive decline that impairs activities of daily living (ADLs)
- Without impairment of ADLs, it is referred to as mild cognitive impairment (MCI)
- At least one cognitive domain affected (complex attention, executive function, learning and memory, language, perceptual-motor, social cognition), with poor ADLs and iADLs and no other cause identified
- Early-onset is prior to 65 years
Etiologies
- Alzheimer disease: insidious onset and gradual progression, usually starting with memory and learning but also behavioural and psychological manifestations
- Vascular dementia
- Multi-infarct
- Diffuse white matter disease (Binswanger's)
- Chronic alcohol use
- Parkinson disease
- Drug or medication intoxication
- Less common
- Vitamin deficiencies
- Thiamine (B1), causing Wernicke encephalopathy
- Cobalamin (B12), causing subacute combined degeneration
- Niacin (B3), causing pellagra
- Endocrinopathy
- Organ failure
- Renal failure
- Liver failure
- Pulmonary failure
- Chronic infections
- HIV
- Neurosyphilis
- JC virus, causing progressive multifocal leukoencephalopathy (PML)
- Tuberculosis, fungal infections, and protozoa
- Whipple disease
- Head trauma and diffuse brain damage
- Dementia pugilistica
- Chronic subdural hematoma
- Postanoxia
- Postencephalitis
- Normal pressure hydrocephalus
- Neoplastic
- Primary or secondary brain tumour
- Paraneoplastic limbic encephalitis
- Toxins
- Drug, medication, and narcotic overdose
- Heavy metal intoxication
- Dialysis dementia (aluminum)
- Organic toxins
- Psychiatric
- Depression (pseudodementia)
- Schizophrenia
- Conversion disorder
- Degenerative disorders
- Huntington disease
- Dementia with Lewy bodies
- Progressive supranuclear palsy
- Multisystem atrophy
- Hereditary ataxias
- Motor neuron disease, such as amyotrophic lateral sclerosis (ALS)
- Frontal lobe dementia
- Corticobasal degeneration
- Multiple sclerosis
- Adult Down syndrome with Alzheimer disease
- ALS Parkinson dementia complex of Guam
- Prion disease (Creutzfeld-jakob and Gerstmann-Straussler-Scheinker diseases)
- Miscellaneous
- Sarcoidosis
- Vasculitis
- Cerebral autosomal dominant arteriopathy with subcortical infarcts and leukoencephalopathy (CADASIL)
- Acute intermittent porphyria
- Recurrent non-convulsive seizures
- Vitamin deficiencies
Epidemiology
- About 20% have a reversible cause (primarily depression, hydrocephalus, and alcohol abuse)
Clinical Manifestations
Disease | Early symptoms | Mental status | Neuropsych | Neuro | Imaging |
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Alzheimer dementia | Memory loww | Episodic memory loss | Initially normal | Initially normal | Entorhinal cortex and hippocampal atrophy |
Frontal-temporal dementia | Apathy, poo judgement/insight, speech and language, hyperorality | Frontal/executive, language; spares drawing | Apathy, disinhibition, hyperorality, euphoria, depression | May have vertical gaze palsy, axial rigidity, dystonia, alien hand, or MND | Frontal, insular, and/or temporal atrophy; spares posterior parietal lobe |
Lewy body dementia | Visual hallucinations, REM sleep disorder, delirium, Capgras (imposter) syndrome, parkinsonism | Drawing and frontal/executive; spares memory; delirium-prone | Visual hallucinations, depression, sleep disorder, delusions | Parkinsonism | Posterior parietal atrophy; hippocampi larger than in AD |
Creutzfeldt-Jakob disease | Dementia, mood, anxiety, movement disorder | Variable, frontal/executive, focal cortical, memory | Depression, anxiety | Myoclonus, rigidity, parkinsonism | Cortical ribboning and basal ganglia or thalamus hyperintensity on MRI |
Vascular dementia | Often but not always sudden and stepwise; variable early symptoms; apathy, falls, focal weaknesses | Frontal/executive, cognitive slowing; can spare memory | Apathy, delusions, anxiety | Usually motor slowing, spasticity; can be normal | Cortical and subcortical infarcts, confluent white matter disease |
Physical Examination
- Mental status examination, including affect
- Full neurological examination
- Cranial nerves, including eye movements
- Motor exam, with axial and appendicular rigidity and rule out stroke and UMN signs (as would be seen in ALS)
- Sensory examination, first light touch before cortical sensory function
- Comment on signs of Parkinsonism
- Cerebellar examination
Investigations
- The goal is to rule out reversible causes
- Laboratory
- TSH to rule out hypothyroidism
- Vitamin B12 to rule out B12 deficiency
- CBC for anemia and occult infection
- Electrolytes
- Imaging
- CT or MRI brain to rule out strokes, NPH, and tumour(s)
- Age <60
- Rapid, unexplained decline (1-2 months)
- Short duration of dementia (<2 years)
- Recent head trauma
- New neurological symptoms
- History of cancer
- ...
- ...
- CT or MRI brain to rule out strokes, NPH, and tumour(s)
- Optional
- Laboratory
- Lumbar puncture
- Liver and renal function
- Urine toxicology
- HIV
- Apolipoprotein E
- Syphilis screen
- Parathyroid function
- Adrenal function
- Urine for heavy metals
- ESR
- Imaging
- Chest x-ray
- Angiogram
- PET or SPECT
- Other
- EEG
- Psychometric testing
- Brain biopsy
- Laboratory
Cognitive Testing
- Clock draw is the most sensitive for executive dysfunction, and also tests visuospatial and language domains
- MoCA is the only one with a clock, so MoCA tests executive function (also, abstraction)
- Diagnosis is based on clinical history, though, not from cognitive testing
Management
Behavioural and Psychological Symptoms of Dementia (BPSD)
- Symptoms include psychosis, aggression, agitation, mania, apathy
- History most important
- Triggers for behaviour
- Reversible causes
- Risks of harm to self or others
- Non-pharmacologic interventions
- Make the environment nice
- Caregiver education
- Try not to use drugs, but can try...
- Risperidone for severe behaviours, but increases risk of death
- Document their behaviours over several weeks to document benefit or harm, then reassess every three months if antipsychotics are used