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Induction of reproducible brain infarction by photochemically initiated thrombosis

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1985

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TLDR

A photochemical thrombosis model was created by intravenously injecting rose bengal and irradiating the left parietal skull with 560‑nm green light for 20 minutes, producing reproducible cerebral infarctions in rats that were observed from 30 minutes to 15 days post‑irradiation. The model produced rapid thrombotic occlusion, complete within 4 h, and reproducible infarct evolution characterized by platelet aggregation, red‑cell stasis, and macrophage infiltration, making it suitable for testing therapies and studying region‑specific stroke outcomes.

Abstract

Abstract We have used a photochemical reaction in vivo to induce reprodcible thrombosis leading to cerebral infarction in rats. After the intravenous injection of rose bengal, a potent photosensitzing dye, an ischemic lesion was formed by irradiating the left parietal convexity of the exposed skull for 20 minutes with green light(560nm) from a filtered xenon arc lamp. Animals were allowed to surivive form 30 minutes to 15 days after irradiation. Early microscopic alerations within the irradiated zone included the formation of thrombotic plugs and adjacent red blood cell stasis within pial and parenchymal vessels. Scanning electron microscopy revealed frequent platelet aggregates adhering to the vascular endothelium, often resulting in vascular occlusion. Carbon‐black brain perfusion demonstrated that occlusion of vascular channels progressed after irradiation and was complete within 4 hours. Histopathological examination at 1, 5, and 15 days revealed that the associated infarct evolved reproducibly through several characteristic stages, including a phase of massive macrophage infiltration. Although cerbral infarction in this model is initiated by thrombosis of small bolld vessels, the fact that the main pathological features of stroke are consistently reproduced should permit its use in assessing treatment regimens, Further, the capability of producing infarction in preselected cortiacal regions may facilitate the study of behavioral, functional, and structural consequences of acute and chronic stroke.

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