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Ca(2+)/CaM:Kv7.4 (KCNQ4) B-螺旋复合物的结构为 M 电流调节提供了深入了解。

Structure of a Ca(2+)/CaM:Kv7.4 (KCNQ4) B-helix complex provides insight into M current modulation.

机构信息

Cardiovascular Research Institute, University of California, San Francisco, CA 94158-2156, USA.

出版信息

J Mol Biol. 2013 Jan 23;425(2):378-94. doi: 10.1016/j.jmb.2012.11.023. Epub 2012 Nov 23.

DOI:10.1016/j.jmb.2012.11.023
PMID:23178170
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3540129/
Abstract

Calmodulin (CaM) is an important regulator of Kv7.x (KCNQx) voltage-gated potassium channels. Channels from this family produce neuronal M currents and cardiac and auditory I(KS) currents and harbor mutations that cause arrhythmias, epilepsy, and deafness. Despite extensive functional characterization, biochemical and structural details of the interaction between CaM and the channel have remained elusive. Here, we show that both apo-CaM and Ca(2+)/CaM bind to the C-terminal tail of the neuronal channel Kv7.4 (KCNQ4), which is involved in both hearing and mechanosensation. Interactions between apo-CaM and the Kv7.4 tail involve two C-terminal tail segments, known as the A and B segments, whereas the interaction between Ca(2+)/CaM and the Kv7.4 C-terminal tail requires only the B segment. Biochemical studies show that the calcium dependence of the CaM:B segment interaction is conserved in all Kv7 subtypes. X-ray crystallographic determination of the structure of the Ca(2+)/CaM:Kv7.4 B segment complex shows that Ca(2+)/CaM wraps around the Kv7.4 B segment, which forms an α-helix, in an antiparallel orientation that embodies a variation of the classic 1-14 Ca(2+)/CaM interaction motif. Taken together with the context of prior studies, our data suggest a model for modulation of neuronal Kv7 channels involving a calcium-dependent conformational switch from an apo-CaM form that bridges the A and B segments to a Ca(2+)/CaM form bound to the B-helix. The structure presented here also provides a context for a number of disease-causing mutations and for further dissection of the mechanisms by which CaM controls Kv7 function.

摘要

钙调蛋白(CaM)是 Kv7.x(KCNQx)电压门控钾通道的重要调节因子。该家族的通道产生神经元 M 电流和心脏及听觉 I(KS)电流,并携带导致心律失常、癫痫和耳聋的突变。尽管进行了广泛的功能表征,但 CaM 与通道相互作用的生化和结构细节仍然难以捉摸。在这里,我们表明 apo-CaM 和 Ca(2+)/CaM 均可与神经元通道 Kv7.4(KCNQ4)的 C 端尾部结合,该尾部参与听觉和机械感觉。apo-CaM 与 Kv7.4 尾部之间的相互作用涉及两个 C 端尾部片段,称为 A 和 B 片段,而 Ca(2+)/CaM 与 Kv7.4 C 端尾部的相互作用仅需要 B 片段。生化研究表明,CaM:B 片段相互作用的钙离子依赖性在所有 Kv7 亚型中均得到保守。Ca(2+)/CaM:Kv7.4 B 片段复合物的 X 射线晶体结构测定表明,Ca(2+)/CaM 环绕 Kv7.4 B 片段,B 片段形成α-螺旋,以反平行方式排列,体现了经典的 1-14 Ca(2+)/CaM 相互作用基序的一种变体。结合先前研究的背景,我们的数据表明,神经元 Kv7 通道的调节模型涉及一种钙依赖性构象转换,从桥接 A 和 B 片段的 apo-CaM 形式转换为与 B-螺旋结合的 Ca(2+)/CaM 形式。这里呈现的结构也为许多致病突变提供了一个背景,并为进一步剖析 CaM 控制 Kv7 功能的机制提供了一个背景。

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