Stroke, Vol 19, 704-708, Copyright © 1988 by American Heart Association
R Joseph, TJ Steiner, LU Schultz and F Clifford Rose
Migraine is associated with increased platelet activity and an incidence of
cerebrovascular ischemic events. Because cerebrovascular events might
result from platelet aggregation, enhancing platelet activity further in
the treatment of migraine is not desirable. beta- Adrenoceptor blockers
effective in migraine prophylaxis include propranolol (nonselective) and
metoprolol (beta 1-selective), but it is uncertain how beta-receptor
subtype selectivity might influence platelet behavior in migraine. In 29
patients, comparable clinical responses were obtained with therapeutic
doses during 1 month of treatment with propranolol, metoprolol, and the
beta 2-selective Li 32- 468. Propranolol increased and metoprolol decreased
platelet aggregation and ATP release, and the effect of Li 32-468 could be
related to that of propranolol. These actions can be largely explained in
terms of what is known of platelet beta-receptors and therefore can be
generalized to other effective beta-blockers. Since altered platelet
activity does not account for the efficacy of these agents in migraine, the
actions of beta-blockers on platelets should be considered as side effects.
Those beta-blockers inhibiting platelet activity should be preferred in
migraine treatment, assuming equal efficacy, which implies the use of beta
1-selective blockers.
ARTICLES
Platelet activity and selective beta-blockade in migraine prophylaxis
Princess Margaret Migraine Clinic, Charing Cross Hospital, London, United Kingdom.
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