Arterial thrombosis after plaque disruption is the critical event leading to acute vascular syndromes, including myocardial infarction, unstable angina pectoris, and stroke. Stroke is the third largest cause of mortality in the world, and about 80 % of strokes are ischemic events due to the occlusion of a vessel. Although restoration of blood flow to an ischemic area is crucial to tissue survival, these harmful aspects of this returning blood flow have been termed reperfusion injury, and were presumed to be mediated by massive free radicals, leukocyte infiltration, and vasoactive compounds. In our study, we used two compounds, lycopene and inosine. (1) Lycopene is not only a pigment, but a very potent antioxidant. It could protect plants from damage of sun or air pollution, and also help us to fight against several degeneration diseases. (2) Inosine plays an important role in inflammation. In our experiments, we have established two animal models: (1) irradiation of the mesenteric microvessels in fluorescein sodium-pretreated mice, and (2) middle cerebral artery occlusion in the rat by intraluminal suture. We would use these models to evaluate whether lycopene or inosine had protective effect in thrombosis and transient focal cerebral infarction. These test included quantification of brain infarct volume, measurement of lipid peroxidation, neurological deficit and grip test. Our results showed that both lycopene and inosine could prolong the occlusion time of inducing platelet plug formation in mesenteric venules. These suggested that these two compounds could have antithrombotic activity. In middle cerebral occlusion model, lycopene could significantly reduce the infarct size at the dosage of 4 mg/kg twice, but not significantly change score in neurological deficit and grip test. Another, our data showed that inosine (100 mg/kg ip twice or 150 mg/kg ip once) could significantly reduce the infarct size. Although inosine did not change the neurological deficit, it could increase score in grip test.