Alzheimer disease: Difference between revisions
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* Gene mutations: APP, PS-1, PS-2, and Apo epsilon-4 |
* Gene mutations: APP, PS-1, PS-2, and Apo epsilon-4 |
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== Clinical |
== Clinical Manifestations == |
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* History |
* History |
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Latest revision as of 07:14, 16 July 2020
Pathophysiology
- Build-up of beta amyloid plaques with neurofibrillary tangles
- Degeneration of the transentorhinal region, followed by hippocampus then lateral and posterior temporal and parietal neocortex
Differential Diagnosis
- See Dementia
Epidemiology
- Most prevalent dementia syndrome
Risk Factors
- Age
- Gene mutations: APP, PS-1, PS-2, and Apo epsilon-4
Clinical Manifestations
- History
- Typically begins with memory loss
- Later, aphasia and navigational problems
- Signs & Symptoms
Management
Symptomatic Treatments
- Cholinesterase inhibitors for AD with stroke, and as an option for Parkinson disease dementia
- Not indicated in vascular dementia
- No specific preferred cholinesterase inhibitor
- Modest improvements in cognition but does not delay nursing home
- Side effects include bradycardia, syncope, GI intolerance, urinary incontinence, and abnormal dreams
- NMS and rhabdomyolysis are rare but reported
- Combination with memantine appears safe
- Can either add memantine to cholinesterase inhibitor, or replace it
- Trial of antidepressent can be considered in patients with depression, severe dysthymia, or emotional lability
- Antipsychotics should be reserved for cases where the patient's agitated causes a risk of harm to themselves or others
Discontinuation of Acetylcholinesterase Inhibitors
- May worsen cognition, but should be considered if there are adverse side effects, or the dementia has progressed past the point where they would be helpful
- If stopped for non-effectiveness, they should be tapered before stopping, then monitored for cognitive decline
