Subtle Neuronal Death in Striatum After Short Forebrain Ischemia in Rats Detected by In Situ End-Labeling for DNA Damage

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Stroke. 1997;28:163-170

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(Stroke. 1997;28:163-170.)
© 1997 American Heart Association, Inc.

Articles

Subtle Neuronal Death in Striatum After Short Forebrain Ischemia in Rats Detected by In Situ End-Labeling for DNA Damage

Rainald Schmidt-Kastner, MD; Henry Fliss, PhD Antoine M. Hakim, MD, PhD

the Neuroscience Research Institute (R.S.-K., A.M.H.) and the Department of Physiology (H.F.), Faculty of Medicine, University of Ottawa (Canada).

Correspondence to Dr Rainald Schmidt-Kastner, Cerebral Vascular Disease Research Center, Department of Neurology (D4-5), University of Miami School of Medicine, PO Box 016960, Miami, FL 33101.

Background and Purpose Neuronal cell death after global brainischemia occurs predominantly by necrosis, whereas only a minorfraction of cell death may occur through apoptosis. Brief ormoderate insults are thought to facilitate apoptosis, whichis associated with DNA fragmentation. After 10 minutes of four-vesselocclusion in rats, conventional neuropathological analysis showsneuronal cell death in hippocampal CA1 but not in the striatum.Thus, we compared hippocampus and striatum for occurrence ofcells with DNA fragmentation.

Methods A brief insult of 10 minutes of forebrain ischemia wasinduced in rats using four-vessel occlusion, and groups of brainswere studied at 1, 3, 6, and 12 hours and at 1, 3, and 7 daysafter ischemia. In situ end-labeling (ISEL) was used to detectneurons undergoing DNA fragmentation. The hippocampal CA1 areawas compared with the striatum. Conventional staining and immunohistochemicalmarkers served to exclude ischemic neuronal cell death in thestriatum.

Results Hippocampal CA1 neurons were ISEL-positive by 3 daysafter ischemia. In contrast, positive cells became evident inthe striatum between 3 hours to 3 days after ischemia. The ISEL-positivecells were scattered throughout the striatum with a preferencefor the dorsomedial areas and accounted for about 0.2% of theneurons per striatal area at 1 day. Conventional staining andimmunohistochemical markers failed to reveal areas of overtcell damage in the striatum.

Conclusions The scattered cell damage in the striatum afterbrief forebrain ischemia suggests the occurrence of an apoptoticprocess. The striatum therefore may be prone to subtle celldeath due to metabolic insults.

Editorial Comment

Myron D. Ginsberg, MD, Guest Editor

Cerebral Vascular Disease Research CenterUniversity of Miami School of MedicineMiami, Fla

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