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可分离的Kvβ亚基结构域改变钾通道的表达和门控。

Separable Kvbeta subunit domains alter expression and gating of potassium channels.

作者信息

Accili E A, Kiehn J, Yang Q, Wang Z, Brown A M, Wible B A

机构信息

Rammelkamp Center for Research, MetroHealth Campus, Case Western Reserve University, Cleveland, Ohio 44109-1998, USA.

出版信息

J Biol Chem. 1997 Oct 10;272(41):25824-31. doi: 10.1074/jbc.272.41.25824.

Abstract

Kvbeta subunits have been shown to affect kinetic properties of voltage-gated K+ channel Kv1alpha subunits and increase the number of cell surface dendrotoxin-binding sites when coexpressed with Kv1. 2. Here, we show that Kvbeta1.2 alters both current expression and gating of Kvalpha1 channels and that each effect is mediated by a distinct Kvbeta1.2 domain. The Kvbeta1.2 N terminus or Kvalpha1-blocking domain introduced steady state current block, an apparent negative shift in steady state activation, and a slowing of deactivation along with a dramatic reduction in single channel open probability. N-terminal deletions of Kvbeta1.2 no longer altered channel kinetics but promoted dramatic increases in Kv1.2 current. The conserved Kvbeta1 C terminus or Kvalpha1 expression domain alone was sufficient to increase the number of functional channels. The same effect was observed with the normally noninactivating subunit, Kvbeta2. By contrast, Kv1.5 currents were reduced when coexpressed with either the Kvbeta1 C terminus or Kvbeta2, indicating that the Kvalpha1 expression domain has Kvalpha1 isoform-specific effects. Our results demonstrate that Kvbeta subunits consist of two domains that are separable on the basis of both primary structure and functional modulation of voltage-gated K+ channels.

摘要

Kvβ亚基已被证明可影响电压门控性钾通道Kv1α亚基的动力学特性,并在与Kv1.2共表达时增加细胞表面树突毒素结合位点的数量。在此,我们表明Kvβ1.2会改变Kvα1通道的电流表达和门控特性,且每种效应均由Kvβ1.2的不同结构域介导。Kvβ1.2的N端或Kvα1阻断结构域会引起稳态电流阻断、稳态激活的明显负向偏移、失活减慢以及单通道开放概率的显著降低。Kvβ1.2的N端缺失不再改变通道动力学,但会促使Kv1.2电流显著增加。保守的Kvβ1 C端或Kvα1表达结构域单独就足以增加功能性通道的数量。与通常不发生失活的亚基Kvβ2共表达时也观察到了相同的效应。相比之下,当与Kvβ1 C端或Kvβ2共表达时,Kv1.5电流会降低,这表明Kvα1表达结构域对Kvα1亚型具有特异性效应。我们的结果表明,Kvβ亚基由两个结构域组成,这两个结构域在电压门控性钾通道的一级结构和功能调节方面均可分离。

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