Stroke, Vol 20, 488-494, Copyright © 1989 by American Heart Association
D Martz, G Rayos, GP Schielke and AL Betz
Free radicals have been shown to play an important role in ischemia-
reperfusion injury in several organ systems; however, the role of free
radicals in central nervous system ischemia has been less well studied.
Many potential free radical-generating systems exist. The primary products
of these reactions, superoxide and hydrogen peroxide, may combine to
produce hydroxyl radicals. Of the many potential sources of free radical
generation, the enzyme xanthine oxidase has been shown to be important in
ischemia in noncerebral tissue. We investigated the effect of the hydroxyl
radical scavenger dimethylthiourea and the xanthine oxidase inhibitor
allopurinol on infarct volume in a model of continuous partial ischemia.
Male Sprague-Dawley rats were treated with dimethylthiourea or allopurinol
before middle cerebral artery occlusion. Infarct volume was measured by
triphenyltetrazolium chloride staining of brains removed 3 or 24 hours
after occlusion. Stroke volume was reduced by 30% after dimethylthiourea
treatment and by 32-35% after allopurinol treatment. At 24 hours after
stroke, cortical tissue was more effectively protected than caudate tissue
with both agents. Pretreatment with dimethylthiourea and allopurinol also
significantly reduced cerebral edema formation and improved blood-brain
barrier function as measured by fluorescein uptake. Our results imply that
hydroxyl radicals are important in tissue injury secondary to partial
cerebral ischemia and that xanthine oxidase may be the primary source of
these radicals.
ARTICLES
Allopurinol and dimethylthiourea reduce brain infarction following middle cerebral artery occlusion in rats
Department of Surgery, University of Michigan, Ann Arbor.
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