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HERG1 通道病。

HERG1 channelopathies.

机构信息

Department of Physiology, Nora Eccles Harrison Cardiovascular Research & Training Institute, University of Utah, 95 South 2000 East, Salt Lake, UT 84112, USA.

出版信息

Pflugers Arch. 2010 Jul;460(2):265-76. doi: 10.1007/s00424-009-0758-8. Epub 2009 Nov 22.

Abstract

Human ether a go-go-related gene type 1 (hERG1) K+ channels conduct the rapid delayed rectifier K+ current and mediate action potential repolarization in the heart. Mutations in KCNH2 (the gene that encodes hERG1) causes LQT2, one of the most common forms of long QT syndrome, a disorder of cardiac repolarization that predisposes affected subjects to ventricular arrhythmia and increases the risk of sudden cardiac death. Hundreds of LQT2-associated mutations have been described, and most cause a loss of function by disrupting subunit folding, assembly, or trafficking of the channel to the cell surface. Loss-of-function mutations in hERG1 channels have also recently been implicated in epilepsy. A single gain-of-function mutation has been described that causes short QT syndrome and cardiac arrhythmia. In addition, up-regulation of hERG1 channel expression has been demonstrated in specific tumors and has been associated with skeletal muscle atrophy in mice.

摘要

人类 ether-a-go-go 相关基因 1 型 (hERG1) K+ 通道传导快速延迟整流 K+电流,并介导心脏动作电位复极化。KCNH2 基因突变(编码 hERG1 的基因)导致 LQT2,这是长 QT 综合征最常见的形式之一,是一种心脏复极障碍,使受影响的个体易发生室性心律失常,并增加心脏性猝死的风险。已经描述了数百种与 LQT2 相关的突变,大多数通过破坏亚基折叠、组装或通道向细胞表面的运输来导致功能丧失。hERG1 通道的功能丧失突变最近也与癫痫有关。已经描述了一种单一的功能获得性突变,它导致短 QT 综合征和心律失常。此外,hERG1 通道表达的上调已在特定肿瘤中得到证实,并与小鼠的骨骼肌萎缩有关。

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