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链激酶对冠状动脉再灌注期间心肌内出血、梗死面积及无复流现象的影响。

The effect of streptokinase on intramyocardial hemorrhage, infarct size, and the no-reflow phenomenon during coronary reperfusion.

作者信息

Kloner R A, Alker K J

出版信息

Circulation. 1984 Sep;70(3):513-21. doi: 10.1161/01.cir.70.3.513.

Abstract

The purpose of this study was to determine whether streptokinase exacerbates intramyocardial hemorrhage during coronary reperfusion, has any intrinsic effect on myocardial infarct size other than its ability to lyse proximal thrombi in coronary arteries, and can abolish the no-reflow phenomenon. Anesthetized open-chest dogs underwent coronary occlusion for 3 hr followed by 3 hr of reperfusion. Area of infarct was assessed by tetrazolium staining, anatomic zone of no-reflow by injection of the fluorescent dye thioflavin S at the end of the reperfusion period, regional blood flow during occlusion and reperfusion by the radioactive microsphere technique, and extent of gross hemorrhage by assessment of photographic enlargements of the heart slices. Area of infarction of the left ventricle was similar in control (13.4 +/- 3.6%) and streptokinase-treated dogs (13.0 +/- 2.9%; p = NS). Seven of eight dogs in the untreated group had anatomic perfusion defects as assessed by thioflavin S at the end of the reperfusion phase; seven of eight dogs in the streptokinase group had anatomic perfusion defects. There was no difference in the extent of gross hemorrhage between the two groups (6.5 +/- 2.1% of left ventricle in controls and 5.7 +/- 2.3% in streptokinase-treated dogs). Severe depression of regional blood flow during reperfusion was present within the infarcted tissue and was associated with an anatomic perfusion defect as defined by thioflavin S; there was moderate depression of flow within the noninfarcted, salvaged subepicardium. In a separate series of experiments, infarcts were assessed for hemoglobin content. Intramyocardial hemoglobin levels were not higher after fibrinolytic therapy plus reperfusion compared with reperfusion alone.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

本研究的目的是确定链激酶在冠状动脉再灌注期间是否会加剧心肌内出血,除了其溶解冠状动脉近端血栓的能力外,对心肌梗死面积是否有任何内在影响,以及是否能消除无复流现象。对麻醉开胸犬进行冠状动脉闭塞3小时,随后再灌注3小时。通过四氮唑染色评估梗死面积,在再灌注期结束时注射荧光染料硫黄素S评估无复流的解剖区域,通过放射性微球技术评估闭塞和再灌注期间的局部血流,并通过评估心脏切片的放大照片来评估大体出血的程度。对照组(13.4±3.6%)和链激酶治疗组犬(13.0±2.9%;p=无显著性差异)左心室梗死面积相似。在再灌注期结束时,未经治疗组8只犬中有7只通过硫黄素S评估存在解剖灌注缺陷;链激酶组8只犬中有7只存在解剖灌注缺陷。两组之间大体出血程度无差异(对照组左心室为6.5±2.1%,链激酶治疗组为5.7±2.3%)。梗死组织内再灌注期间局部血流严重降低,且与硫黄素S定义的解剖灌注缺陷相关;非梗死的、挽救的心外膜下存在中度血流降低。在另一系列实验中,评估梗死灶的血红蛋白含量。与单纯再灌注相比,溶栓治疗加再灌注后心肌内血红蛋白水平并未更高。(摘要截短于250字)

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