Both animal models of experimental myocardial infarction and clinical studies on reperfusion therapy for acute myocardial infarction have provided evidence of impaired tissue perfusion at the microvascular level after initiation of reperfusion despite adequate restoration of epicardial vessel patency. Characteristics of this "no-reflow" phenomenon found in basic science investigations, such as distinct perfusion defects, progressive decrease of resting myocardial flow with ongoing reperfusion and functional vascular alterations are paralleled by clinical observations demonstrating similar features during the course of reperfusion. In experimental animal investigations of coronary occlusion and reperfusion, this no-reflow phenomenon could be characterized as a fundamental mechanism of myocardial ischemia and reperfusion. Major determinants of the amount of no-reflow are the duration of occlusion, infarct size, but also the length of reperfusion, as rapid expansion of perfusion defects occurs during reperfusion. Moreover, no-reflow appears to persist over a period of at least four weeks, a period when major steps of infarct healing take place. The significant association of the degree of compromised tissue perfusion at four weeks and indices of infarct expansion, found in chronic animal models of reperfused myocardial infarction, might be the pathoanatomic correlate for the prognostic significance observed in the clinical setting.

译文

:实验性心肌梗死的动物模型和急性心肌梗死的再灌注治疗的临床研究均提供了证据,表明尽管充分恢复了心外膜血管通畅性,再灌注开始后微血管水平的组织灌注受损。在基础科学研究中发现的这种“无回流”现象的特征,例如明显的灌注缺陷,随着进行中的再灌注而逐渐减少的静息心肌血流量和功能性血管改变,与在再灌注过程中表现出相似特征的临床观察结果相吻合。在对冠状动脉闭塞和再灌注的动物实验研究中,这种无再流现象可被表征为心肌缺血和再灌注的基本机制。决定是否再流的主要因素是闭塞的持续时间,梗塞面积以及再灌注的时间,因为在再灌注过程中会出现灌注缺陷的快速扩展。此外,在至少四周的时间内,即梗塞愈合的主要步骤发生时,无复流似乎会持续。在再灌注心肌梗死的慢性动物模型中发现,在四周时受损的组织灌注程度与梗塞扩展指数之间存在显着相关性,这可能与在临床环境中观察到的预后意义相关。

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