Stroke, Vol 19, 1267-1274, Copyright © 1988 by American Heart Association
K Tanaka, F Gotoh, Y Fukuuchi, T Amano, N Suzuki, D Uematsu, J Kawamura, T Yamawaki, N Itoh and K Obara
We evaluated the effect of a stable synthetic prostacyclin analogue,
TRK-100, on the microcirculatory derangement occurring in feline pial
vessels with endothelial damage after middle cerebral artery occlusion.
Fifteen adult cats were divided into an untreated group (Group 1, n = 8)
and a treated group (Group 2, n = 7). Thirty minutes after 10 minutes of
ultraviolet irradiation, which selectively damaged endothelium in the pial
vessels, the middle cerebral artery was occluded in both groups and
maintained for 30 minutes. In Group 2, 50 ng/kg/min TRK-100 was
continuously infused intravenously following ultraviolet irradiation. In
both the pial arteries and veins, platelet aggregate adhesion to the
endothelium with subsequent thrombus formation was significantly (p less
than 0.01 and p less than 0.05, respectively) inhibited during middle
cerebral artery occlusion in Group 2 compared with Group 1. Similarly,
blood flow stasis in the pial veins was effectively prevented in Group 2
during occlusion. Furthermore, the pial artery diameter returned to the
control level during the late period of occlusion, whereas in Group 1 the
pial artery remained constricted. Our data suggest that TRK-100 can prevent
microcirculatory derangement in the acute stage of ischemic stroke.
ARTICLES
Stable prostacyclin analogue preventing microcirculatory derangement in experimental cerebral ischemia in cats
Department of Neurology, School of Medicine, Keio University, Tokyo, Japan.