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Kv4钾离子通道的两个N端结构域调节与KChIP1的结合及受其调控。

Two N-terminal domains of Kv4 K(+) channels regulate binding to and modulation by KChIP1.

作者信息

Scannevin Robert H, Wang KeWei, Jow Flora, Megules Jennifer, Kopsco David C, Edris Wade, Carroll Karen C, Lü Qiang, Xu Weixin, Xu Zhangbao, Katz Alan H, Olland Stephane, Lin Laura, Taylor Meggin, Stahl Mark, Malakian Karl, Somers Will, Mosyak Lydia, Bowlby Mark R, Chanda Pranab, Rhodes Kenneth J

机构信息

Neuroscience Discovery Research, Wyeth Research CN-8000, Princeton, NJ 08543, USA.

出版信息

Neuron. 2004 Feb 19;41(4):587-98. doi: 10.1016/s0896-6273(04)00049-2.

Abstract

The family of calcium binding proteins called KChIPs associates with Kv4 family K(+) channels and modulates their biophysical properties. Here, using mutagenesis and X-ray crystallography, we explore the interaction between Kv4 subunits and KChIP1. Two regions in the Kv4.2 N terminus, residues 7-11 and 71-90, are necessary for KChIP1 modulation and interaction with Kv4.2. When inserted into the Kv1.2 N terminus, residues 71-90 of Kv4.2 are also sufficient to confer association with KChIP1. To provide a structural framework for these data, we solved the crystal structures of Kv4.3N and KChIP1 individually. Taken together with the mutagenesis data, the individual structures suggest that that the Kv4 N terminus is required for stable association with KChIP1, perhaps through a hydrophobic surface interaction, and that residues 71-90 in Kv4 subunits form a contact loop that mediates the specific association of KChIPs with Kv4 subunits.

摘要

名为KChIPs的钙结合蛋白家族与Kv4家族的钾离子通道相关联,并调节其生物物理特性。在此,我们利用诱变和X射线晶体学方法,探究Kv4亚基与KChIP1之间的相互作用。Kv4.2 N端的两个区域,即第7至11位氨基酸残基和第71至90位氨基酸残基,对于KChIP1对Kv4.2的调节作用以及二者之间的相互作用是必需的。当将Kv4.2的第71至90位氨基酸残基插入到Kv1.2的N端时,其也足以介导与KChIP1的结合。为了给这些数据提供一个结构框架,我们分别解析了Kv4.3N和KChIP1的晶体结构。结合诱变数据来看,单独的结构表明,Kv4的N端可能通过疏水表面相互作用与KChIP1稳定结合是必需的,并且Kv4亚基中的第71至90位氨基酸残基形成一个接触环,介导KChIPs与Kv4亚基的特异性结合。

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