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活性氧在心脏亚细胞器缺血预处理中的作用。

Role of reactive oxygen species in ischemic preconditioning of subcellular organelles in the heart.

作者信息

Saini Harjot K, Machackova Jarmila, Dhalla Naranjan S

机构信息

Institute of Cardiovascular Sciences, St. Boniface General Hospital Research Centre, Faculty of Medicine, University of Manitoba, Winnipeg, Manitoba, Canada.

出版信息

Antioxid Redox Signal. 2004 Apr;6(2):393-404. doi: 10.1089/152308604322899468.

Abstract

Ischemic preconditioning (IPC) is an endogenous adaptive mechanism and is manifested by early and delayed phases of cardioprotection. Brief episodes of ischemia-reperfusion during IPC cause some subtle functional and structural alterations in sarcolemma, mitochondria, sarcoplasmic reticulum, myofibrils, glycocalyx, as well as nucleus, which render these subcellular organelles resistant to subsequent sustained ischemia-reperfusion insult. These changes occur in functional groups of various receptors, cation transporters, cation channels, and contractile and other proteins, and may explain the initial effects of IPC. On the other hand, induction of various transcriptional factors occurs to alter gene expression and structural changes in subcellular organelles and may be responsible for the delayed effects of IPC. Reactive oxygen species (ROS), which are formed during the IPC period, may cause these changes directly and indirectly and act as a trigger of IPC-induced cardioprotection. As ROS may be one of the several triggers proposed for IPC, this discussion is focused on the current knowledge of both ROS-dependent and ROS-independent mechanisms of IPC. Furthermore, some events, which are related to functional preservation of subcellular organelles, are described for a better understanding of the IPC phenomenon.

摘要

缺血预处理(IPC)是一种内源性适应性机制,表现为心脏保护的早期和延迟阶段。IPC期间短暂的缺血再灌注发作会导致肌膜、线粒体、肌浆网、肌原纤维、糖萼以及细胞核发生一些细微的功能和结构改变,使这些亚细胞器对随后的持续缺血再灌注损伤具有抗性。这些变化发生在各种受体、阳离子转运体、阳离子通道以及收缩蛋白和其他蛋白质的功能组中,可能解释了IPC的初始效应。另一方面,各种转录因子的诱导会改变基因表达以及亚细胞器的结构变化,可能是IPC延迟效应的原因。在IPC期间形成的活性氧(ROS)可能直接和间接导致这些变化,并作为IPC诱导的心脏保护的触发因素。由于ROS可能是提出的几种IPC触发因素之一,因此本讨论聚焦于当前关于IPC的ROS依赖性和ROS非依赖性机制的知识。此外,还描述了一些与亚细胞器功能保存相关的事件,以便更好地理解IPC现象。

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