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使用阿片类镇痛药布托啡诺进行预处理可提高犬缺血预处理的阈值。

Premedication with the opioid analgesic butorphanol raises the threshold for ischemic preconditioning in dogs.

作者信息

Schwartz L M, Jennings R B, Reimer K A

机构信息

Department of Pathology, Duke University Medical Center, Durham, North Carolina 27710, USA.

出版信息

Basic Res Cardiol. 1997 Apr;92(2):106-14. doi: 10.1007/BF00805571.

Abstract

Elucidation of the subcellular mechanism of myocardial ischemic preconditioning should be facilitated by precise knowledge of the biology of the cardioprotective response. Any proposed molecular mechanism for preconditioning must be initiated during the required ischemic stress period. The studies reported in this paper were undertaken to determine whether the infarct-limiting effect of four 5-min episodes of ischemia interspersed by reperfusion can be achieved by a single 5-min episode. Adult open-chest mongrel dogs, premedicated with the analgesic butorphanol, and anesthetized with sodium pentobarbital, underwent occlusion of the circumflex coronary artery for 60 min, followed by reperfusion of 3 h. Treated dogs were preconditioned with one, two or four cycles of 5-min occlusion followed by reperfusion. Additional dogs, not premedicated with butorphanol, were either untreated (not preconditioned) or preconditioned with one cycle of ischemia. Infarcts were identified using triphenyl-tetrazolium chloride (TTC) macrochemistry and infarct size (as % of area-at-risk, AAR) was measured and analyzed (using analysis of covariance [ANCOVA]) with respect to coronary collateral blood flow (measured using radioactive microspheres). Four 5-min cycles of preconditioning ischemia markedly limited infarct size. Two cycles were as effective as four. In contrast, infarct size was not different from control infarct size after a single episode of preconditioning ischemia. However, when pentobarbital anesthesia was used without premedication with butorphanol, a single 5-min ischemic stress did induce cardioprotection. Thus, the ischemic stress required for myocardial preconditioning in dogs is dependent on the anesthetic and premedication protocol employed. A single 5-min stimulus is effective in dogs anesthetized with pentobarbital. Premedication with the opioid analgesic, butorphanol, increases the threshold for induction of cardioprotection.

摘要

对心脏保护反应生物学的精确了解应有助于阐明心肌缺血预处理的亚细胞机制。任何提出的预处理分子机制都必须在所需的缺血应激期启动。本文报道的研究旨在确定单次5分钟的缺血发作是否能实现四个5分钟缺血发作并穿插再灌注所产生的梗死限制效应。成年开胸杂种犬,先用镇痛剂布托啡诺预处理,再用戊巴比妥钠麻醉,对其左旋冠状动脉进行60分钟的闭塞,随后再灌注3小时。处理过的犬接受一个、两个或四个5分钟闭塞后再灌注的周期进行预处理。另外一些未用布托啡诺预处理的犬,要么未接受处理(未预处理),要么接受一个缺血周期的预处理。使用氯化三苯基四氮唑(TTC)宏观化学方法识别梗死灶,并测量和分析梗死面积(以危险区面积的百分比表示,AAR),同时考虑冠状动脉侧支血流(使用放射性微球测量)。四个5分钟的预处理缺血周期显著限制了梗死面积。两个周期与四个周期的效果相同。相比之下,单次预处理缺血发作后的梗死面积与对照梗死面积没有差异。然而,当使用戊巴比妥麻醉而未用布托啡诺预处理时,单次5分钟的缺血应激确实诱导了心脏保护作用。因此,犬心肌预处理所需的缺血应激取决于所采用的麻醉和预处理方案。单次5分钟的刺激对用戊巴比妥麻醉的犬有效。用阿片类镇痛药布托啡诺预处理会提高诱导心脏保护的阈值。

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