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缺血预处理具有显著的抗心律失常作用。

Pronounced antiarrhythmic effects of ischemic preconditioning.

作者信息

Parratt J, Vegh A

机构信息

Department of Pharmacology, Albert Szent-Gyorgyi Medical School of Szeged, Hungary.

出版信息

Cardioscience. 1994 Mar;5(1):9-18.

PMID:8204800
Abstract

Brief periods of ischemia, induced either by complete coronary artery occlusion or by rapid ventricular pacing, greatly reduce the severity of those live-threatening ventricular arrhythmias that occur during a subsequent more prolonged occlusion of a major branch of the left coronary artery. The increased tolerance achieved by brief ischemia, either regional or global, has been termed ischemic preconditioning. This was originally defined as the reduction in ultrastructural changes and infarct size resulting from coronary artery occlusion and reperfusion by prior, brief, usually multiple ischemic periods. The reduction in the severity of arrhythmias by preconditioning, which has been described in several different species using both in vivo and in vitro models, depends on the duration and number of the short preconditioning occlusions and also on the time between the preconditioning period and the subsequent prolonged coronary artery occlusion. Under optimal conditions the antiarrhythmic effect of ischemic preconditioning is as pronounced as that with standard antiarrhythmic drugs. Unfortunately, the protection if also short-lived (usually less than 1 hour). If, however, we understood the precise mechanisms involved, we might be able to exploit them to ultimate therapeutic advantage. At least in the dog, the evidence suggests that the protection involves the release (from coronary vascular endothelial cells?) of endogenous myocardial protective substances such as bradykinin, nitric oxide and prostacyclin.

摘要

短暂的缺血期,无论是由冠状动脉完全闭塞还是快速心室起搏诱发,都能大大降低在随后左冠状动脉主要分支更长时间闭塞期间发生的那些危及生命的室性心律失常的严重程度。短暂缺血(局部或整体)所实现的耐受性增加被称为缺血预处理。这最初被定义为通过先前短暂的、通常是多次的缺血期,冠状动脉闭塞和再灌注导致的超微结构变化和梗死面积的减少。预处理对心律失常严重程度的降低,已在使用体内和体外模型的几种不同物种中得到描述,这取决于短暂预处理闭塞的持续时间和次数,也取决于预处理期与随后延长的冠状动脉闭塞之间的时间。在最佳条件下,缺血预处理的抗心律失常作用与标准抗心律失常药物一样显著。不幸的是,这种保护也是短暂的(通常少于1小时)。然而,如果我们了解其中的确切机制,我们或许能够利用它们获得最终的治疗益处。至少在狗身上,证据表明这种保护涉及内源性心肌保护物质如缓激肽、一氧化氮和前列环素的释放(来自冠状血管内皮细胞?)。

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