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关于P2Y受体在心肌缺血再灌注损伤心脏保护作用中的当前知识。

Current knowledge on the role of P2Y receptors in cardioprotection against ischemia-reperfusion.

作者信息

Djerada Zoubir, Feliu Catherine, Richard Vincent, Millart Hervé

机构信息

Department of Pharmacology, E.A.3801, SFR CAP-santé, Reims University Hospital, 51, rue Cognacq-Jay, 51095 Reims Cedex, France.

Department of Pharmacology, E.A.3801, SFR CAP-santé, Reims University Hospital, 51, rue Cognacq-Jay, 51095 Reims Cedex, France.

出版信息

Pharmacol Res. 2017 Apr;118:5-18. doi: 10.1016/j.phrs.2016.08.009. Epub 2016 Aug 9.

Abstract

During ischemia, numerous effective endogenous extracellular mediators have been identified, particularly, nucleosides such as adenosine as well as purinergic and pyrimidinergic nucleotides. They may play important regulatory roles within the cardiovascular system and notably as cardio-protectants. Indeed, the distribution of the P2Y receptors in mammalian heart includes several cellular constituents relevant for the pathophysiology of myocardial ischemia. Beside the well-known cardioprotective effect of adenosine, the additional protective role of P2Y receptors has emerged. However, interpretation of experimental results may be sometimes perplexing. This is due to the variability of: the experimental models, the endpoints criteria, the chemical structure of agonist and antagonist ligands and their concentrations, the sequences of drug administration with respect to the model used (before and/or during and/or after ischemia). The net effect may be in the opposite direction after a transient or a prolonged stimulation. Nevertheless, the overall reading of published data highlights the beneficial role of the P2Y receptor stimulation, the useful and synergistic role of P2Y receptor activation and even of the P2Y receptor alone in cardioprotection. More, the P2Y receptor could be involved in counter-regulation of profibrotic processes. Paradoxically, transient P2X receptor stimulation could contribute to the net cardioprotective effect of ATP. Recently, experimental data have shown that blocking the P2Y receptor after ischemia confers cardioprotection independently of platelet antiaggregatory effect. This suggests for P2Y receptors an important role in primary prevention and as a therapeutic target in myocardial protection during ischemia and reperfusion.

摘要

在缺血期间,已鉴定出许多有效的内源性细胞外介质,特别是核苷,如腺苷以及嘌呤能和嘧啶能核苷酸。它们可能在心血管系统中发挥重要的调节作用,尤其是作为心脏保护剂。事实上,P2Y受体在哺乳动物心脏中的分布包括与心肌缺血病理生理学相关的几种细胞成分。除了众所周知的腺苷心脏保护作用外,P2Y受体的额外保护作用也已显现。然而,对实验结果的解释有时可能令人困惑。这是由于以下因素的变异性:实验模型、终点标准、激动剂和拮抗剂配体的化学结构及其浓度、给药顺序与所用模型的关系(缺血前和/或期间和/或后)。短暂或长期刺激后,净效应可能方向相反。尽管如此,对已发表数据的总体解读突出了P2Y受体刺激的有益作用、P2Y受体激活甚至单独的P2Y受体在心脏保护中的有益和协同作用。此外,P2Y受体可能参与纤维化过程的反调节。矛盾的是,短暂的P2X受体刺激可能有助于ATP的净心脏保护作用。最近,实验数据表明,缺血后阻断P2Y受体可独立于血小板抗聚集作用而赋予心脏保护作用。这表明P2Y受体在一级预防中以及作为缺血和再灌注期间心肌保护的治疗靶点具有重要作用。

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