Acetylcholinesterase inhibitors and risk of bleeding and acute ischemic events in non-hypertensive Alzheimer’s patients
Article [Version of Record]
Abstract(s)
Introduction: Acetylcholinesterase inhibitors (AChEIs) are commonly used to treat
mild to moderate cases of Alzheimer disease (AD). To the best of our knowledge, there
has been no study estimating the risk of bleeding and cardiovascular events in patients
with non-hypertensive AD. Therefore, this study aimed to estimate the association
between AChEIs and the risk of bleeding and cardiovascular ischemic events in patients
with non-hypertensive AD.
Methods: A nested case-control study was conducted to estimate the risk of bleeding
and ischemic events (angina, myocardial infarction [MI], and stroke) in patients with
AD. This study was conducted using the UK Clinical Practice Research Datalink and
Hospital Episode Statistics (HES) databases. The study cohort consisted of AD patients
≥65 years of age. The case groups included all AD subjects in the database who had
a bleeding or ischemic event during the cohort follow-up. Four controls were selected
for each case. Patients were classified as current users or past users based on a 60-day
threshold of consuming the drug. Simple and multivariable conditional logistic regression analyses were used to calculate the adjusted odds ratio for bleeding events and
cardiovascular events.
Results: We identified 507 cases and selected 2028 controls for the bleeding event
cohort and 555 cases and 2220 controls for the ischemic event cohort. The adjusted
odds ratio (OR) (95% confidence interval [CI]) for the association of AChEI use was 0.93
(0.75 to 1.16) for bleeding events, 2.58 (1.01 to 6.59) for angina, and 1.89 (1.07 to 3.33)
for MI. Past users of AChEIs were also at increased risk of stroke (1.51 [1.00 to 2.27]).
Discussion: This is the first study assessing the risk of bleeding and cardiovascular
events in patients with non-hypertensive AD. Our findings could be of great interest
for clinicians and researchers working on AD.