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首页> 外文期刊>Nature Communications >Dynamic switching of calmodulin interactions underlies Ca2+ regulation of CaV1.3 channels.
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Dynamic switching of calmodulin interactions underlies Ca2+ regulation of CaV1.3 channels.

机译:钙调蛋白相互作用的动态切换是CaV1.3通道Ca2 +调节的基础。

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Calmodulin regulation of CaV channels is a prominent Ca(2+) feedback mechanism orchestrating vital adjustments of Ca(2+) entry. The long-held structural correlation of this regulation has been Ca(2+)-bound calmodulin, complexed alone with an IQ domain on the channel carboxy terminus. Here, however, systematic alanine mutagenesis of the entire carboxyl tail of an L-type CaV1.3 channel casts doubt on this paradigm. To identify the actual molecular states underlying channel regulation, we develop a structure-function approach relating the strength of regulation to the affinity of underlying calmodulin/channel interactions, by a Langmuir relation (individually transformed Langmuir analysis). Accordingly, we uncover frank exchange of Ca(2+)-calmodulin to interfaces beyond the IQ domain, initiating substantial rearrangements of the calmodulin/channel complex. The N-lobe of Ca(2+)-calmodulin binds an N-terminal spatial Ca(2+) transforming element module on the channel amino terminus, whereas the C-lobe binds an EF-hand region upstream of the IQ domain. This system of structural plasticity furnishes a next-generation blueprint for CaV channel modulation.Registry Number/Name of Substance 0 (Calcium Channels, L-Type). 0 (Calmodulin). 0 (alpha1D (Cav1.3) L-type calcium channel, human). 7440-70-2 (Calcium).
机译:CaV通道的钙调蛋白调节是一个突出的Ca(2+)反馈机制,协调Ca(2+)进入的生命力调节。长期存在的这种调节的结构相关性是Ca(2+)结合的钙调蛋白,单独与通道羧基末端的IQ结构域复合。然而,在这里,L型CaV1.3通道整个羧基尾部的系统丙氨酸诱变使人们对该模式产生了怀疑。为了确定潜在的通道调控的实际分子状态,我们开发了一种结构函数方法,通过朗缪尔关系(单独转换的朗缪尔分析),将调控的强度与潜在的钙调蛋白/通道相互作用的亲和力联系起来。因此,我们发现Ca(2 +)-钙调蛋白到IQ范围以外的接口的坦率交换,启动钙调蛋白/通道复合物的大量重排。 Ca(2 +)-钙调蛋白的N瓣与通道氨基末端上的N末端空间Ca(2+)转化元件模块结合,而C瓣与IQ域上游的EF手区域结合。该结构可塑性系统为CaV通道的调制提供了下一代蓝图。注册号/物质0的名称(钙离子通道,L型)。 0(钙调蛋白)。 0(alpha1D(Cav1.3)L型钙通道,人类)。 7440-70-2(钙)。

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