【2h】

The Orai Pore Opening Mechanism

机译:奥莱孔开启机构

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摘要

Cell survival and normal cell function require a highly coordinated and precise regulation of basal cytosolic Ca2+ concentrations. The primary source of Ca2+ entry into the cell is mediated by the Ca2+ release-activated Ca2+ (CRAC) channel. Its action is stimulated in response to internal Ca2+ store depletion. The fundamental constituents of CRAC channels are the Ca2+ sensor, stromal interaction molecule 1 (STIM1) anchored in the endoplasmic reticulum, and a highly Ca2+-selective pore-forming subunit Orai1 in the plasma membrane. The precise nature of the Orai1 pore opening is currently a topic of intensive research. This review describes how Orai1 gating checkpoints in the middle and cytosolic extended transmembrane regions act together in a concerted manner to ensure an opening-permissive Orai1 channel conformation. In this context, we highlight the effects of the currently known multitude of Orai1 mutations, which led to the identification of a series of gating checkpoints and the determination of their role in diverse steps of the Orai1 activation cascade. The synergistic action of these gating checkpoints maintains an intact pore geometry, settles STIM1 coupling, and governs pore opening. We describe the current knowledge on Orai1 channel gating mechanisms and summarize still open questions of the STIM1–Orai1 machinery.
机译:细胞存活和正常细胞功能需要高度协调和精确的基础细胞溶胶Ca2 +浓度的调节。 Ca2 +进入细胞的主要来源由Ca2 +剥离活化的Ca2 +(CRAC)通道介导。响应于内部Ca2 +储存耗尽而刺激其作用。 CRAC通道的基本成分是Ca2 +传感器,基质相互作用分子1(STIM1)锚固在内质网中,以及质膜中的高度Ca2 + - 选择性孔形成亚基OraI1。 Orai1孔隙开放的确切性质目前是一项集中研究的主题。该综述描述了中间和细胞源延伸跨膜区域中的ORAI1 Gating检查点如何以协调的方式行动,以确保开放允许的ORAI1通道构象。在这种情况下,我们突出了当前已知的众所周知的orai1突变的影响,这导致了识别一系列门控检查点和它们在orai1激活级联的不同步骤中的作用。这些门控检查点的协同作用维持完整的孔隙几何形状,沉降Stim1耦合,并控制孔隙开口。我们描述了关于ORAI1渠道门控机制的当前知识,并总结了STIM1-ORAI1机械的开放性问题。

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