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人类钾通道的异源多聚体组装。瞬时外向电流的分子基础?

Heteromultimeric assembly of human potassium channels. Molecular basis of a transient outward current?

作者信息

Po S, Roberds S, Snyders D J, Tamkun M M, Bennett P B

机构信息

Department of Pharmacology, Vanderbilt University Medical School, Nashville, Tenn. 37232-2171.

出版信息

Circ Res. 1993 Jun;72(6):1326-36. doi: 10.1161/01.res.72.6.1326.

DOI:10.1161/01.res.72.6.1326
PMID:8495559
Abstract

To gain insight into the molecular basis of cardiac repolarization, we have expressed K+ channels cloned from ventricular myocardium in Xenopus oocytes. A recently identified human cardiac K+ channel isoform (human Kv1.4) has properties similar to the 4-aminopyridine-sensitive calcium-insensitive component of the cardiac transient outward current. However, these channels recovered from inactivation much slower than native channels. Hybrid channels consisting of subunits from different K+ channel clones (delayed rectifier channels [Kv1.1, Kv1.2, and Kv1.5] and Kv1.4) were created by coinjection of cRNAs in oocytes. Multimeric channels consisting of Kv1.4:Kv1.1, Kv1.4:Kv1.2, and Kv1.4:Kv1.5 were expressed and compared. The hybrid channels displayed characteristics of heterotetrameric channels with kinetics that more closely resembled a native cardiac transient outward current. The inactivation and recovery from inactivation of the heteromeric channels indicated that the presence of a single inactivating subunit (Kv1.4) was probably sufficient to cause channel inactivation. The results demonstrate that expression of different K+ channel genes can produce channel protein subunits that assemble as heteromultimers with unique properties. It is shown that certain combinations of voltage-gated K+ channels probably do not contribute to native transient outward current. However, one combination of subunits could not be excluded. Therefore, this mechanism of channel assembly may underlie some of the functional diversity of potassium channels found in the cardiovascular system.

摘要

为深入了解心脏复极化的分子基础,我们已将从心室肌克隆的钾通道在非洲爪蟾卵母细胞中进行表达。最近鉴定出的一种人类心脏钾通道亚型(人类Kv1.4)具有与心脏瞬时外向电流中对4 - 氨基吡啶敏感且对钙不敏感的成分相似的特性。然而,这些通道从失活状态恢复的速度比天然通道慢得多。通过在卵母细胞中共注射cRNA,构建了由来自不同钾通道克隆(延迟整流通道[Kv1.1、Kv1.2和Kv1.5]以及Kv1.4)的亚基组成的杂合通道。表达并比较了由Kv1.4:Kv1.1、Kv1.4:Kv1.2和Kv1.4:Kv1.5组成的多聚体通道。这些杂合通道表现出异源四聚体通道的特征,其动力学更类似于天然心脏瞬时外向电流。异源多聚体通道的失活及从失活状态恢复表明,单个失活亚基(Kv1.4)的存在可能足以导致通道失活。结果表明,不同钾通道基因的表达可产生作为具有独特特性的异源多聚体组装的通道蛋白亚基。研究表明,电压门控钾通道的某些组合可能对天然瞬时外向电流没有贡献。然而,有一种亚基组合不能被排除。因此,这种通道组装机制可能是心血管系统中钾通道功能多样性的部分基础。

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