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连接蛋白和富含组氨酸的钙离子结合蛋白:在心力衰竭和心律失常发生中的潜在作用。

Junctin and the histidine-rich Ca2+ binding protein: potential roles in heart failure and arrhythmogenesis.

作者信息

Pritchard Tracy J, Kranias Evangelia G

机构信息

Department of Pharmacology and Cell Biophysics, University of Cincinnati College of Medicine, OH 45267-0575, USA.

出版信息

J Physiol. 2009 Jul 1;587(Pt 13):3125-33. doi: 10.1113/jphysiol.2009.172171. Epub 2009 Apr 29.

Abstract

Contractile dysfunction and ventricular arrhythmias associated with heart failure have been attributed to aberrant sarcoplasmic reticulum (SR) Ca(2+) cycling. The study of junctin (JCN) and histidine-rich Ca(2+) binding protein (HRC) becomes of particular importance since these proteins have been shown to be critical regulators of Ca(2+) cycling. Specifically, JCN is a SR membrane protein, which is part of the SR Ca(2+) release quaternary structure that also includes the ryanodine receptor, triadin and calsequestrin. Functionally, JCN serves as a bridge between calsequestrin and the Ca(2+) release channel, ryanodine receptor. HRC is a SR luminal Ca(2+) binding protein known to associate with both triadin and the sarcoplasmic reticulum Ca(2+)-ATPase, and may thus mediate the crosstalk between SR Ca(2+) uptake and release. Indeed, evidence from genetic models of JCN and HRC indicate that they are important in cardiophysiology as alterations in these proteins affect SR Ca(2+) handling and cardiac function. In addition, downregulation of JCN and HRC may contribute to Ca(2+) cycling perturbations manifest in the failing heart, where their protein levels are significantly reduced. This review examines the roles of JCN and HRC in SR Ca(2+) cycling and their potential significance in heart failure.

摘要

与心力衰竭相关的收缩功能障碍和室性心律失常被认为与异常的肌浆网(SR)钙(Ca2+)循环有关。连接蛋白(JCN)和富含组氨酸的钙(Ca2+)结合蛋白(HRC)的研究变得尤为重要,因为这些蛋白质已被证明是钙(Ca2+)循环的关键调节因子。具体而言,JCN是一种肌浆网膜蛋白,是肌浆网钙(Ca2+)释放四级结构的一部分,该结构还包括兰尼碱受体、三联蛋白和肌集钙蛋白。在功能上,JCN充当肌集钙蛋白和钙(Ca2+)释放通道兰尼碱受体之间的桥梁。HRC是一种肌浆网腔钙(Ca2+)结合蛋白,已知与三联蛋白和肌浆网钙(Ca2+)-ATP酶都有关联,因此可能介导肌浆网钙(Ca2+)摄取和释放之间的相互作用。确实,来自JCN和HRC基因模型的证据表明,它们在心脏生理学中很重要,因为这些蛋白质的改变会影响肌浆网钙(Ca2+)的处理和心脏功能。此外,JCN和HRC的下调可能导致在衰竭心脏中出现的钙(Ca2+)循环紊乱,在衰竭心脏中它们的蛋白质水平显著降低。这篇综述探讨了JCN和HRC在肌浆网钙(Ca2+)循环中的作用及其在心力衰竭中的潜在意义。

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