Stroke, Vol 22, 56-60, Copyright © 1991 by American Heart Association
FM Faraci, WG Mayhan and DD Heistad
Studies in vitro suggest that the basilar artery has distinctive responses
to endothelium-dependent stimuli. Our first goal was to examine the effects
of acetylcholine on diameter of the basilar artery in vivo. Because
aggregating platelets may have important effects on cerebral arteries, our
second goal was to examine the effects on the basilar artery of products
that are released by platelets (thromboxane, serotonin, and adenosine
5'-diphosphate). Diameter of the basilar artery was measured through a
cranial window in anesthetized rats (n = 25). Baseline diameter of the
basilar artery was 247 +/- 10 microns mean +/- SEM. Topical application of
acetylcholine at 10(-6) and 10(-5) M dilated the basilar artery by 13 +/-
2% and 19 +/- 2%, respectively. The thromboxane analogue U46619 at 10(-8)
and 10(-7) M reduced the diameter of the basilar artery by 18 +/- 5% and 29
+/- 4%, respectively. At 10(-8) and 10(-7) M, serotonin had little effect
on pial arterioles on the cerebrum but constricted the basilar artery by 18
+/- 2% and 29 +/- 4%, respectively. At 10(-6) and 10(-5) M, adenosine
5'-diphosphate produced marked dilatation of pial arterioles on the
cerebrum (9 +/- 2% and 20 +/- 3%, respectively) but had little effect on
the basilar artery (increased diameter by 4 +/- 2% and 6 +/- 2%,
respectively). Thus, in contrast to some studies of the basilar artery in
vitro, acetylcholine produces dilatation of the basilar artery in vivo.
Potent constrictor responses to thromboxane and serotonin, in combination
with the minimal dilator effect of adenosine 5'-diphosphate, suggest that
release of these products during platelet aggregation would favor
constriction of the basilar artery.
ARTICLES
Responses of rat basilar artery to acetylcholine and platelet products in vivo
Department of Internal Medicine, Veterans Administration Medical Center, Iowa City, Iowa.
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