Structures and gating mechanism of human TRPM2

IF 44.7 1区综合性期刊 Q1 MULTIDISCIPLINARY SCIENCES Science Pub Date : 2018-11-22 DOI:10.1126/science.aav4809

Longfei Wang, Tian-Min Fu, Yiming Zhou, Shiyu Xia, Anna Greka, Hao Wu

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引用次数: 109

Abstract

Transient receptor potential (TRP) melastatin 2 (TRPM2) is a cation channel associated with numerous diseases. It has a C-terminal NUDT9 homology (NUDT9H) domain responsible for binding adenosine diphosphate (ADP)–ribose (ADPR), and both ADPR and calcium (Ca²⁺) are required for TRPM2 activation. Here we report cryo–electron microscopy structures of human TRPM2 alone, with ADPR, and with ADPR and Ca²⁺. NUDT9H forms both intra- and intersubunit interactions with the N-terminal TRPM homology region (MHR1/2/3) in the apo state but undergoes conformational changes upon ADPR binding, resulting in rotation of MHR1/2 and disruption of the intersubunit interaction. The binding of Ca²⁺ further engages transmembrane helices and the conserved TRP helix to cause conformational changes at the MHR arm and the lower gating pore to potentiate channel opening. These findings explain the molecular mechanism of concerted TRPM2 gating by ADPR and Ca²⁺ and provide insights into the gating mechanism of other TRP channels.

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人类 TRPM2 的结构和门控机制

瞬时受体电位（TRP）美拉司他丁 2（TRPM2）是一种与多种疾病相关的阳离子通道。它有一个 C 端 NUDT9 同源（NUDT9H）结构域，负责结合二磷酸腺苷（ADP）-核糖（ADPR），TRPM2 的激活需要 ADPR 和钙（Ca2+）。在此，我们报告了人类 TRPM2 单独、与 ADPR 以及与 ADPR 和 Ca2+ 的冷冻电镜结构。在apo状态下，NUDT9H与N端TRPM同源区（MHR1/2/3）形成了亚基内和亚基间的相互作用，但在与ADPR结合时发生了构象变化，导致MHR1/2旋转并破坏了亚基间的相互作用。结合 Ca2+ 后，跨膜螺旋和保守的 TRP 螺旋进一步参与，导致 MHR 臂和较低的门孔发生构象变化，从而促进通道开放。这些发现解释了ADPR和Ca2+协同TRPM2门控的分子机制，并为其他TRP通道的门控机制提供了启示。

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来源期刊

Science 综合性期刊-综合性期刊

CiteScore

61.10

自引率

0.90%

发文量

审稿时长

2.1 months

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