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首页> 外文期刊>American Journal of Physiology >Adenosine A(1)-receptor induced late preconditioning and myocardial infarction: reperfusion duration is critical.
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Adenosine A(1)-receptor induced late preconditioning and myocardial infarction: reperfusion duration is critical.

机译:腺苷A(1)受体诱导晚期预处理和心肌梗塞:再灌注持续时间至关重要。

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摘要

We investigated the influence of coronary artery reperfusion (CAR) duration on the infarct-limiting properties of adenosine A(1)-receptor stimulation-induced delayed preconditioning (A(1)-DPC) compared with ischemia-induced delayed preconditioning (I-DPC). Sixty-one chronically instrumented conscious rabbits successfully underwent the following protocol. On day 1, rabbits were randomly divided into four groups: control (saline, iv), I-DPC (six 4-min coronary artery occlusion/4-min reperfusion cycles), A(1)-DPC(100) (N(6)-cyclopentyladenosine, 100 microg/kg iv), and A(1)-DPC(400) (N(6)-cyclopentyladenosine, 400 microg/kg iv). On day 2 (i.e., 24 h later), rabbits underwent a 30-min coronary artery occlusion after which CAR was started and maintained for either 3 or 72 h. Infarct size (percentage of the area at risk) was determined by triphenyltetrazolium chloride staining. After 3 h of CAR, I-DPC, A(1)-DPC(100), and A(1)-DPC(400) significantly decreased infarct size (36 +/- 5, 41 +/- 4, 38 +/- 5%, respectively) compared with control (55 +/- 3%). After 72 h of CAR, infarct sizes were not significantly different among the four groups. This result was confirmed by histologic analysis. Thus A(1)-DPC at the two investigated doses, as well as I-DPC, decreased infarct size after 3 h but not 72 h of CAR.
机译:我们调查了冠状动脉再灌注(CAR)持续时间对腺苷A(1)-受体刺激诱导的延迟预处理(A(1)-DPC)与缺血诱导的延迟预处理(I-DPC)的梗塞限制特性的影响)。六十一只经长期检测的清醒兔子已成功接受以下治疗方案。在第1天,将兔随机分为四组:对照组(生理盐水,静脉注射),I-DPC(六个4分钟冠状动脉闭塞/ 4分钟再灌注周期),A(1)-DPC(100)(N( 6)-环戊基腺苷,100微克/千克iv)和A(1)-DPC(400)(N(6)-环戊基腺苷,400微克/千克,iv)。在第2天(即24小时后),对兔子进行30分钟的冠状动脉闭塞,然后开始CAR,并维持3或72 h。通过氯化三苯基四唑鎓染色确定梗塞面积(危险区域的百分比)。 CAR 3小时后,I-DPC,A(1)-DPC(100)和A(1)-DPC(400)显着减少了梗死面积(36 +/- 5、41 +/- 4、38 + / -分别为5%)和对照组(55 +/- 3%)。 CAR 72小时后,四组之间的梗死面积无明显差异。组织学分析证实了该结果。因此,两个研究剂量的A(1)-DPC以及I-DPC在CAR的3小时后减少了梗死面积,但在72小时后却没有减少。

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