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首页> 外文期刊>Nature Communications >Structure of the human sodium leak channel NALCN in complex with FAM155A
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Structure of the human sodium leak channel NALCN in complex with FAM155A

机译:伴有FAM155A复合物中人钠泄漏通道NALCN的结构

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摘要

NALCN, a sodium leak channel expressed mainly in the central nervous system, is responsible for the resting Na permeability that controls neuronal excitability. Dysfunctions of the NALCN channelosome, NALCN with several auxiliary subunits, are associated with a variety of human diseases. Here, we report the cryo-EM structure of human NALCN in complex with FAM155A at an overall resolution of 3.1 angstroms. FAM155A forms extensive interactions with the extracellular loops of NALCN that may help stabilize NALCN in the membrane. A Na ion-binding site, reminiscent of a Ca2 binding site in Cav channels, is identified in the unique EEKE selectivity filter. Despite its ‘leaky’ nature, the channel is closed and the intracellular gate is sealed by S6I, II-III linker and III-IV linker. Our study establishes the molecular basis of Na permeation and voltage sensitivity, and provides important clues to the mechanistic understanding of NALCN regulation and NALCN channelosome-related diseases. NALCN, a sodium leak channel, plays a key role in regulating the resting membrane potential and controlling neuronal excitability. Here the authors report a cryo-EM structure of human NALCN in complex with FAM155A, that with complementary functional analyses provide insights on its ion selectivity, voltage sensing and specific interactions with auxiliary subunits.
机译:NALCN,一种主要在中枢神经系统中表达的钠泄漏通道,负责控制神经元兴奋性的遗传性耐磁性。 NALCN通道组的功能障碍,具有几个辅助亚基的NALCN,与各种人类疾病有关。在这里,我们以3.1埃的总分辨率报告与FAM155A的复合物中人NALCN的Cryo-EM结构。 FAM155A与NALCN的细胞外环形成了广泛的相互作用,其可帮助稳定膜中的NALCN。在独特的EEKE选择性过滤器中鉴定了Na离子结合位点,使Ca2结合位点上鉴定。尽管其“泄漏”性质,但通道关闭,细胞内栅极由S6I,II-III接头和III-IV接头密封。我们的研究确定了NA渗透和电压敏感性的分子基础,并为NALCN调节和NALCN感觉组相关疾病提供了重要的线索。 NALCN,钠泄漏通道,在调节静止膜电位和控制神经元兴奋方面起着关键作用。这里作者报告了人NALCN的络合物与FAM155A中的Cryo-EM结构,互补功能分析提供了对其离子选择性,电压感测和与辅助亚基的特定相互作用的见解。

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