Published online before print July 15, 2004, doi: 10.1161/01.STR.0000137412.35700.0e
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(Stroke. 2004;35:2177.)
© 2004 American Heart Association, Inc.
Original Contributions |
Mouse Model of Microembolic Stroke and Reperfusion
From the Cardiology Division and Cardiovascular Research Center (D.N.A., F.N., P.L.H.), Stroke and Neurovascular Regulation Laboratory, Department of Radiology (Y.G.-Ö., C.A., M.A.M.), and Athinoula A. Martinos Center (A.K.D.), Massachusetts General Hospital, Charlestown, Massachusetts; and the Institute for Environmental Medicine (J.C.M., T.K., V.R.M.) and the Department of Pharmacology (V.R.M.), University of Pennsylvania School of Medicine, Philadelphia, Pennsylvania.
Correspondence to Dr Paul L. Huang, Cardiovascular Research Center, Massachusetts General Hospital East, 149 Thirteenth St, Charlestown, MA 02129. E-mail phuang1{at}partners.org
Background and Purpose— To test the role of fibrinolysis in stroke, we used a mouse model in which preformed 2.5- to 3-µm-diameter fibrin microemboli are injected into the cerebral circulation. The microemboli lodge in the downstream precapillary vasculature and are susceptible to fibrinolysis.
Methods— We injected various doses of microemboli into the internal carotid artery in mice and characterized their distribution, effects on cerebral blood flow, neurological deficit, infarct area, and spontaneous dissolution. By comparing wild-type and tissue plasminogen activator (tPA) knockout (tPA–/–) mice, we analyzed the role of endogenous tPA in acute thrombotic stroke.
Results— Microemboli cause dose-dependent brain injury. Although moderate doses of microemboli are followed by spontaneous reperfusion, they result in reproducible injury. Gene knockout of tPA markedly delays dissolution of cerebral emboli and restoration of blood flow and aggravates ischemic thrombotic infarction in the brain.
Conclusions— We describe a microembolic model of stroke, in which degree of injury can be controlled by the dose of microemboli injected. Unlike vessel occlusion models, this model can be modulated to allow spontaneous fibrinolysis. Application to tPA–/– mice supports a key role of endogenous tPA in restoring cerebral blood flow and limiting infarct size after thrombosis.
Key Words: animal models • fibrinolysis • microemboli • stroke • stroke, embolic
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