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DONEPEZIL: TOLERABILITY AND SAFETY IN ALZHEIMER'S DISEASE

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SUMMARYThe tolerability and safety of donepezil HCI in patients with mild to moderate Alzheimer's disease (AD) were examined in an integrated analysis of phase ll/lll placebo‐controlled trials. Patients with mild to moderately severe AD (n=1920) were randomised to receive donepezil (n=1291) or placebo (n=629). Adverse events, physical examinations and clinical laboratory tests were assessed. A high completion rate (79%) was achieved in these trials. Of the 1291 patients receiving donepezil only, 142 (11%) withdrew because of an adverse event compared with 43 of the 629 (7%) placebo patients. The most common adverse events included nausea, diarrhoea, headache, insomnia, dizziness, rhinitis, vomiting, asthenia/fatigue and anorexia. Donepezil had no clinically significant effect on any laboratory evaluations and was not associated with hepatotoxicity. These results demonstrate that donepezil is well tolerated and has a favourable safety profile at clinically effective, once‐daily doses of 5 mg and 10 mg.
Title: DONEPEZIL: TOLERABILITY AND SAFETY IN ALZHEIMER'S DISEASE
Description:
SUMMARYThe tolerability and safety of donepezil HCI in patients with mild to moderate Alzheimer's disease (AD) were examined in an integrated analysis of phase ll/lll placebo‐controlled trials.
Patients with mild to moderately severe AD (n=1920) were randomised to receive donepezil (n=1291) or placebo (n=629).
Adverse events, physical examinations and clinical laboratory tests were assessed.
A high completion rate (79%) was achieved in these trials.
Of the 1291 patients receiving donepezil only, 142 (11%) withdrew because of an adverse event compared with 43 of the 629 (7%) placebo patients.
The most common adverse events included nausea, diarrhoea, headache, insomnia, dizziness, rhinitis, vomiting, asthenia/fatigue and anorexia.
Donepezil had no clinically significant effect on any laboratory evaluations and was not associated with hepatotoxicity.
These results demonstrate that donepezil is well tolerated and has a favourable safety profile at clinically effective, once‐daily doses of 5 mg and 10 mg.

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