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别嘌醇在冠状动脉闭塞后最初24小时所提供的保护作用在48小时后减弱。

Protection afforded by allopurinol in the first 24 hours of coronary occlusion is diminished after 48 hours.

作者信息

Miura T, Yellon D M, Kingma J, Downey J M

机构信息

Department of Physiology, College of Medicine, University of South Alabama, Mobile 36688.

出版信息

Free Radic Biol Med. 1988;4(1):25-30. doi: 10.1016/0891-5849(88)90007-x.

Abstract

Experiments were performed to test whether the reduction in infarct size afforded by allopurinol following 24 h of permanent coronary artery occlusion is sustained over the subsequent 24 h. A dog's coronary artery was occluded with an embolus followed by injection of radiomicrospheres into the left ventricle to mark the ischemic region and to measure regional blood flow. Dogs were sacrificed either 24 h or 48 hours after embolization. The infarcts were delineated by failure to stain with triphenyl tetrazolium chloride and the ischemic zones were visualized by autoradiography of the heart slices. Dogs in the treatment groups received 600 mg of allopurinol PO 18 h before surgery, and a 10 mg/kg IV bolus 15 minutes before embolization followed by constant IV infusion of 55 mg/kg/24 h until sacrifice. A close correlation in the control animals between the percent of the ischemic zone which infarcted and collateral blood flow was used to predict a nonintervention infarct size in each treatment animal. Allopurinol treatment caused 17.9 +/- 3.3% less of the risk zone to be tetrazolium negative after 24 hours of ischemia than that seen in untreated animals. Less allopurinol induced salvage was observed in the 48 hour drug group with only a 11.1 +/- 3.3% limitation in infarct size. Furthermore, the effect was inconsistent at 48 h with only 2 dogs showing salvage. We conclude that allopurinol delays but does not prevent infarction in the permanent occlusion model.

摘要

进行实验以测试在冠状动脉永久性闭塞24小时后别嘌醇所带来的梗死面积减小在随后的24小时内是否持续存在。用栓子阻塞犬的冠状动脉,随后向左心室注射放射性微球以标记缺血区域并测量局部血流。栓塞后24小时或48小时处死犬。梗死灶通过氯化三苯基四氮唑不着色来界定,缺血区域通过心脏切片的放射自显影来显示。治疗组的犬在手术前18小时口服600毫克别嘌醇,栓塞前15分钟静脉推注10毫克/千克,随后以55毫克/千克/24小时的速度持续静脉输注直至处死。利用对照动物中梗死的缺血区域百分比与侧支血流之间的密切相关性来预测每只治疗动物的非干预梗死面积。与未治疗的动物相比,别嘌醇治疗使缺血24小时后四氮唑阴性的危险区域减少了17.9±3.3%。在48小时药物组中观察到别嘌醇诱导的挽救作用较小,梗死面积仅受限11.1±3.3%。此外,48小时时效果不一致,只有2只犬显示有挽救作用。我们得出结论,在永久性闭塞模型中,别嘌醇可延迟但不能预防梗死。

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