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首页> 外文期刊>Science Advances >K2P channel C-type gating involves asymmetric selectivity filter order-disorder transitions
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K2P channel C-type gating involves asymmetric selectivity filter order-disorder transitions

机译:K2P通道C型门控包括不对称选择性过滤序列障碍转换

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Ksub2P/sub potassium channels regulate cellular excitability using their selectivity filter (C-type) gate. C-type gating mechanisms, best characterized in homotetrameric potassium channels, remain controversial and are attributed to selectivity filter pinching, dilation, or subtle structural changes. The extent to which such mechanisms control C-type gating of innately heterodimeric Ksub2P/subs is unknown. Here, combining Ksub2P/sub2.1 (TREK-1) x-ray crystallography in different potassium concentrations, potassium anomalous scattering, molecular dynamics, and electrophysiology, we uncover unprecedented, asymmetric, potassium-dependent conformational changes that underlie Ksub2P/sub C-type gating. These asymmetric order-disorder transitions, enabled by the Ksub2P/sub heterodimeric architecture, encompass pinching and dilation, disrupt the S1 and S2 ion binding sites, require the uniquely long Ksub2P/sub SF2-M4 loop and conserved “M3 glutamate network,” and are suppressed by the Ksub2P/sub C-type gate activator ML335. These findings demonstrate that two distinct C-type gating mechanisms can operate in one channel and underscore the SF2-M4 loop as a target for Ksub2P/sub channel modulator development.
机译:k <亚> 2p 钾通道使用其选择性滤波器(c型)栅极调节细胞兴奋性。 C型门控机构,最能表征在同源化钾通道中,保持争议,归因于选择性过滤器夹紧,扩张或微妙的结构变化。这种机制控制I型型术的机制的程度尚未二二聚体K 2p S未知。在此,将K 2p 2.1(Trek-1)X射线晶体中的不同钾浓度,钾异常散射,分子动力学和电生理学中的X射线晶体结合,我们揭示前所未有的,不对称的,不对称的钾依赖性的构象变化k 2p c型门控。这些不对称秩序转换,由K 2p 异二聚体架构,包括夹持和扩张,破坏S1和S2离子结合位点,要求独特的LONG k 2p sf2 -m4环和保守的“M3谷氨酸网络”,并被k 2p c型栅极活化剂ml335抑制。这些发现表明,两个不同的C型门控机构可以在一个通道中运行,并且向SF2-M4循环下划为K 2P 通道调制器开发的目标。

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