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KCNE2钾离子通道调节亚基:广泛影响,复杂病理生物学

The KCNE2 K⁺ channel regulatory subunit: Ubiquitous influence, complex pathobiology.

作者信息

Abbott Geoffrey W

机构信息

Bioelectricity Laboratory, Dept. of Pharmacology, School of Medicine, University of California, Irvine, CA, USA; Dept. of Physiology and Biophysics, School of Medicine, University of California, Irvine, CA, USA.

出版信息

Gene. 2015 Sep 15;569(2):162-72. doi: 10.1016/j.gene.2015.06.061. Epub 2015 Jun 27.

Abstract

The KCNE single-span transmembrane subunits are encoded by five-member gene families in the human and mouse genomes. Primarily recognized for co-assembling with and functionally regulating the voltage-gated potassium channels, the broad influence of KCNE subunits in mammalian physiology belies their small size. KCNE2 has been widely studied since we first discovered one of its roles in the heart and its association with inherited and acquired human Long QT syndrome. Since then, physiological analyses together with human and mouse genetics studies have uncovered a startling array of functions for KCNE2, in the heart, stomach, thyroid and choroid plexus. The other side of this coin is the variety of interconnected disease manifestations caused by KCNE2 disruption, involving both excitable cells such as cardiomyocytes, and non-excitable, polarized epithelia. Kcne2 deletion in mice has been particularly instrumental in illustrating the potential ramifications within a monogenic arrhythmia syndrome, with removal of one piece revealing the unexpected complexity of the puzzle. Here, we review current knowledge of the function and pathobiology of KCNE2.

摘要

KCNE单跨膜亚基由人类和小鼠基因组中的五个成员基因家族编码。KCNE亚基主要因与电压门控钾通道共同组装并在功能上对其进行调节而被人们所认识,它们在哺乳动物生理学中的广泛影响与其小尺寸形成反差。自我们首次发现KCNE2在心脏中的作用及其与遗传性和获得性人类长QT综合征的关联以来,它就受到了广泛研究。从那时起,生理学分析以及人类和小鼠遗传学研究揭示了KCNE2在心脏、胃、甲状腺和脉络丛中惊人的一系列功能。与此相对的是,KCNE2功能破坏会引发各种相互关联的疾病表现,涉及心肌细胞等可兴奋细胞以及非兴奋、极化上皮细胞。小鼠中Kcne2基因的缺失对于阐明单基因心律失常综合征中的潜在后果尤为重要,去除其中一个部分就揭示了这个谜题意想不到的复杂性。在此,我们综述了关于KCNE2功能和病理生物学的当前知识。

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