再灌注3小时后无致死性再灌注损伤。一项在单犬心脏缺血-再灌注模型中的研究。

Absence of lethal reperfusion injury after 3 hours of reperfusion. A study in a single-canine-heart model of ischemia-reperfusion.

作者信息

Zahger D, Yano J, Chaux A, Fishbein M C, Ganz W

机构信息

Department of Medicine, Cedars-Sinai Medical Center, Los Angeles, CA, USA.

出版信息

Circulation. 1995 Jun 15;91(12):2989-94. doi: 10.1161/01.cir.91.12.2989.

DOI:10.1161/01.cir.91.12.2989

PMID:7796510

Abstract

BACKGROUND

Whether reperfusion can cause necrosis of previously viable myocytes (lethal reperfusion injury) remains controversial. Numerous studies examined the ability of various agents to prevent or limit reperfusion injury, but the results were contradictory. In a single-canine-heart model of ischemia-reperfusion, we previously demonstrated that 5 minutes of reperfusion does not increase the transmural extent of necrosis. Since the 5-minute period of reperfusion is considered by some to be too short for the full manifestation of reperfusion injury, we reexamined the issue of lethal reperfusion injury using a modification of the single-heart model of ischemia-reperfusion that allowed extending the reperfusion period to 3 hours.

METHODS AND RESULTS

In anesthetized, open-chest dogs, the distal half of the left anterior descending coronary artery (LAD) segment between the last diagonal branch and the apex was perfused via a shunt from the left carotid artery. The shunt was closed for periods of 90 to 180 minutes, depending on the ECG severity of ischemia, and reperfused for 3 hours. While the distal region was perfused from the carotid artery, the LAD was occluded proximal to the last diagonal branch for the same period of time as the distal region had been earlier. The time of occlusion was chosen such that the end of the occlusion period coincided with the end of the experiment. Thus, both regions of the LAD territory were subjected to identical periods of ischemia, but only the distal region was reperfused. At the end of the experiment, the boundary between the proximal (nonreperfused) and distal (reperfused) area was delineated by blue dye, and the heart was arrested, cut into slices 1 cm thick parallel to the LAD, and placed in triphenyltetrazolium chloride. The epicardial edges of necrosis in the reperfused and the nonreperfused regions were examined for any shift that might suggest a difference in the transmurality of necrosis. The areas of necrotic and viable myocardium were measured by planimetry within 1 cm on either side of the boundary. In all 14 dogs, the epicardial edges of necrosis ran as a single line across the boundary, and no shift was present. There was also no difference in the transmurality of necrosis between the reperfused and nonreperfused regions (64.9 +/- 20.7% versus 66.1 +/- 17.0% of left ventricular wall thickness, respectively, P = .32 by paired t test).

CONCLUSIONS

In a single-canine-heart model of ischemia-reperfusion, there was no evidence of lethal reperfusion injury after 3 hours of reperfusion.

摘要

背景

再灌注是否会导致先前存活的心肌细胞坏死（致死性再灌注损伤）仍存在争议。众多研究探讨了各种药物预防或限制再灌注损伤的能力，但结果相互矛盾。在犬单心脏缺血-再灌注模型中，我们先前证明5分钟的再灌注不会增加透壁性坏死范围。由于有人认为5分钟的再灌注时间对于再灌注损伤的充分表现来说太短，我们使用一种改良的单心脏缺血-再灌注模型重新审视了致死性再灌注损伤问题，该模型可将再灌注时间延长至3小时。

方法与结果

在麻醉开胸的犬中，通过左颈动脉分流灌注左前降支冠状动脉（LAD）在最后一个对角支与心尖之间的远端半段。根据心电图缺血严重程度，分流关闭90至180分钟，然后再灌注3小时。当远端区域由颈动脉灌注时，LAD在最后一个对角支近端被阻断相同的时间，该时间与远端区域先前缺血时间相同。选择阻断时间以使阻断期结束与实验结束时间一致。因此，LAD区域的两个部分经历相同时间的缺血，但只有远端区域进行再灌注。实验结束时，用蓝色染料勾勒出近端（未再灌注）和远端（再灌注）区域之间的边界，使心脏停搏，沿与LAD平行的方向切成1厘米厚的切片，并置于氯化三苯基四氮唑中。检查再灌注和未再灌注区域坏死的心外膜边缘是否有任何移位，这可能提示坏死透壁性存在差异。在边界两侧1厘米范围内通过面积测量法测量坏死和存活心肌的面积。在所有14只犬中，坏死的心外膜边缘在边界处呈一条直线，没有移位。再灌注和未再灌注区域之间坏死的透壁性也没有差异（分别为左心室壁厚度的64.9±20.7%和66.1±17.0%，配对t检验P = 0.32）。