Stroke, Vol 23, 394-398, Copyright © 1992 by American Heart Association
R Joseph, C Tsering and KM Welch
BACKGROUND AND PURPOSE: The mechanism of ischemic neuronal injury is not
fully resolved. The present view is that vascular occlusion per se does not
fully account for the extent of neurological dysfunction. We previously
hypothesized that platelet secretory products might contribute to neuronal
injury in the central nervous system. Our preliminary studies using
organotypic rat spinal cord cultures exposed to human platelet and its
secretory products revealed that platelet products had neurotoxic
properties. METHODS: Further studies, using the same methods, were
conducted, with the addition of several refinements such as use of
gel-filtered platelets (as opposed to washed platelets) and adding
additional relevant controls including platelet membranes, red blood cells,
and washed rat platelets. RESULTS: Exposure of spinal cord explant cultures
to platelet secretory products resulted in reduced number of neurons per
ventral horn compared with control. CONCLUSIONS: Our findings suggest that
platelet secretory products have neurotoxic properties. This effect was
seen with platelet secretion obtained from physiological platelet
concentrations. It appears possible that more abundant release of platelet
products at the site of thrombus formation could have pathological
significance in vivo.
ARTICLES
Study of platelet-mediated neurotoxicity in rat brain
Department of Neurology, Henry Ford Hospital and Health Sciences Center, Detroit, Mich. 48202.
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