晚期再灌注对梗死扩展和心室重构的限制。大鼠模型中的时间进程及机制研究。

Limitation of infarct expansion and ventricular remodeling by late reperfusion. Study of time course and mechanism in a rat model.

作者信息

Boyle M P, Weisman H F

机构信息

Johns Hopkins Medical Institutions, Baltimore, Md.

出版信息

Circulation. 1993 Dec;88(6):2872-83. doi: 10.1161/01.cir.88.6.2872.

DOI:10.1161/01.cir.88.6.2872

PMID:8252700

Abstract

BACKGROUND

Reperfusion of acutely infarcted myocardium may be beneficial in limiting infarct expansion and ventricular remodeling even if established after the time that salvage of ischemic myocardium is possible.

METHODS AND RESULTS

To examine the permanency, time course, and mechanism of this effect of late reperfusion, 200 rats were randomized into one of four groups: (1) infarction with reperfusion after 1 to 2 hours, (2) infarction with reperfusion after 6 to 8 hours, (3) infarction without reperfusion, and (4) sham operation. Surviving rats were killed at either 7 days, when infarct expansion has plateaued, or 21 days, when infarct healing is complete. In both 7- and 21-day analyses, late reperfusion did not reduce infarct size or degree of transmural necrosis but significantly limited infarct expansion, as measured by an index based on infarct endocardial segment lengthening and infarct wall thinning (expansion index at 7 days: no reperfusion, 2.73 +/- 0.25, n = 13; reperfusion after 1 to 2 hours, 1.56 +/- 0.13, n = 23, P < .001; reperfusion after 6 to 8 hours, 1.78 +/- 0.15, n = 16, P = .002; at 21 days: no reperfusion, 3.45 +/- 0.39, n = 13; reperfusion after 1 to 2 hours, 2.21 +/- 0.24, n = 15, P = .01; reperfusion after 6 to 8 hours, 2.02 +/- 0.20, n = 9, P = .01). Reperfusion after 6 to 8 hours was equally effective in limiting expansion as reperfusion after 1 to 2 hours. Late reperfusion also significantly reduced ventricular remodeling at 21 days, as measured by an index based on left ventricular cavity dilatation and noninfarcted myocardial hypertrophy (remodeling index at 21 days: no reperfusion, 2.67 +/- 0.15, n = 13; reperfusion after 1 to 2 hours, 2.20 +/- 0.15, n = 15, P = .035; reperfusion after 6 to 8 hours, 2.12 +/- 0.10, n = 9, P = .012). Histological examination revealed that reperfusion accelerated the clearance of residual dead myofibrils, suggesting an increase in the rate of healing, and increased the degree of myocytolysis but did not change the final degree of infarct healing, tissue density, or viable subepicardial cells.

CONCLUSIONS

Late reperfusion causes a permanent reduction in postinfarction expansion that is present even after complete infarct healing. The time after coronary occlusion in which reperfusion is of benefit in reducing subsequent expansion and remodeling is substantially longer than previously established. The mechanism by which late reperfusion limits expansion may involve changing the rate of healing and the nature of myocardial necrosis but does not involve preserving subepicardial cells.

摘要

背景

急性梗死心肌的再灌注可能有助于限制梗死扩展和心室重构，即便在缺血心肌挽救可能性消失之后才进行再灌注。

方法与结果

为研究晚期再灌注这一效应的持续性、时间进程及机制，将200只大鼠随机分为四组之一：（1）梗死后1至2小时再灌注；（2）梗死后6至8小时再灌注；（3）梗死但不进行再灌注；（4）假手术。存活大鼠在梗死扩展趋于平稳的7天或梗死愈合完成的21天时处死。在7天和21天的分析中，晚期再灌注均未减小梗死面积或透壁坏死程度，但通过基于梗死心内膜节段延长和梗死壁变薄的指数测量，显著限制了梗死扩展（7天时的扩展指数：无再灌注，2.73±0.25，n = 13；1至2小时后再灌注，1.56±0.13，n = 23，P <.001；6至8小时后再灌注，1.78±0.15，n = 16，P =.002；21天时：无再灌注，3.45±0.39，n = 13；1至2小时后再灌注，2.21±0.24，n = 15，P =.01；6至8小时后再灌注，2.02±0.20，n = 9，P =.01）。6至8小时后再灌注在限制扩展方面与1至2小时后再灌注同样有效。晚期再灌注在21天时也显著减轻了心室重构，通过基于左心室腔扩张和非梗死心肌肥厚的指数测量（21天时的重构指数：无再灌注，2.67±0.15，n = 13；1至2小时后再灌注，2.20±0.15，n = 15，P =.035；6至8小时后再灌注，2.12±0.1,0，n = 9，P =.012）。组织学检查显示，再灌注加速了残留坏死肌原纤维的清除，提示愈合速度加快，且增加了肌细胞溶解程度，但未改变梗死愈合的最终程度、组织密度或存活的心外膜下细胞数量。