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Progress in the structural understanding of voltage-gated calcium channel (Ca-V) function and modulation

机译:对电压门控钙离子通道(Ca-V)功能和调节的结构理解的进展

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摘要

Voltage-gated calcium channels (Ca(V)s) are large, transmembrane multiprotein complexes that couple membrane depolarization to cellular calcium entry. These channels are central to cardiac action potential propagation, neurotransmitter and hormone release, muscle contraction and calcium-dependent gene transcription. Over the past six years, the advent of high-resolution structural studies of Ca-V components from different isoforms and Ca-V modulators has begun to reveal the architecture that underlies the exceptionally rich feedback modulation that controls Ca-V action. These descriptions of Ca-V molecular anatomy have provided new, structure-based insights into the mechanisms by which particular channel elements affect voltage-dependent inactivation (VDI), calcium-dependent inactivation (CDI) and calcium-dependent facilitation (CDF). The initial successes have been achieved through structural studies of soluble channel domains and modulator proteins and have proven most powerful when paired with biochemical and functional studies that validate ideas inspired by the structures. Here, we review the progress in this growing area and highlight some key open challenges for future efforts.
机译:电压门控钙通道(Ca(V)s)是大型跨膜多蛋白复合物,可将膜去极化与细胞钙进入耦合。这些通道是心脏动作电位传播,神经递质和激素释放,肌肉收缩和钙依赖性基因转录的核心。在过去的六年中,对来自不同同工型和Ca-V调节剂的Ca-V组分进行高分辨率结构研究的问世,开始揭示出这种结构是控制Ca-V作用的异常丰富的反馈调制的基础。 Ca-V分子解剖学的这些描述为特定通道元素影响电压依赖性灭活(VDI),钙依赖性灭活(CDI)和钙依赖性促进(CDF)的机理提供了新的,基于结构的见解。最初的成功是通过可溶性通道域和调节蛋白的结构研究获得的,与生物化学和功能研究相结合时,最成功的方法是有力的,这些研究验证了受结构启发的思想。在这里,我们回顾了这一增长领域的进展,并着重指出了未来工作中一些关键的开放挑战。

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