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花生四烯酸、ARC通道和Orai蛋白。

Arachidonic acid, ARC channels, and Orai proteins.

作者信息

Shuttleworth Trevor J

机构信息

Department of Pharmacology and Physiology, University of Rochester Medical Center, Rochester, NY 14642, USA.

出版信息

Cell Calcium. 2009 Jun;45(6):602-10. doi: 10.1016/j.ceca.2009.02.001. Epub 2009 Mar 17.

Abstract

A critical role for arachidonic acid in the regulation of calcium entry during agonist activation of calcium signals has become increasingly apparent in numerous studies over the past 10 years or so. In particular, low concentrations of this fatty acid, generated as a result of physiologically relevant activation of appropriate receptors, induces the activation of a unique, highly calcium-selective conductance now known as the ARC channel. Activation of this channel is specifically dependent on arachidonic acid acting at the intracellular surface of the membrane, and is entirely independent of any depletion of internal calcium stores. Importantly, a specific role of this channel in modulating the frequency of oscillatory calcium signals in various cell types has been described. Recent studies, subsequent to the discovery of STIM1 and the Orai proteins and their role in the store-operated CRAC channels, have revealed that these same proteins are also integral components of the ARC channels and their activation. However, unlike the CRAC channels, activation of the ARC channels depends on the pool of STIM1 that is constitutively resident in the plasma membrane, and the pore of these channels is comprised of both Orai1 and Orai3 subunits. The clear implication is that CRAC channels and ARC channels are closely related, but have evolved to play unique roles in the modulation of calcium signals-largely as a result of their entirely distinct modes of activation. Given this, although the precise details of how arachidonic acid acts to activate the channels remain unclear, it seems likely that the specific molecular features of these channels that distinguish them from the CRAC channels--namely Orai3 and/or plasma membrane STIM1--will be involved.

摘要

在过去约10年的众多研究中,花生四烯酸在激动剂激活钙信号过程中对钙内流调节的关键作用已日益明显。特别是,由于适当受体的生理相关激活而产生的低浓度这种脂肪酸,会诱导一种独特的、高度钙选择性电导的激活,现在已知其为ARC通道。该通道的激活特别依赖于花生四烯酸作用于膜的细胞内表面,并且完全独立于内部钙库的任何耗竭。重要的是,已经描述了该通道在调节各种细胞类型中振荡钙信号频率方面的特定作用。在发现STIM1和Orai蛋白及其在储存操纵性CRAC通道中的作用之后的近期研究表明,这些相同的蛋白也是ARC通道及其激活的组成部分。然而,与CRAC通道不同,ARC通道的激活取决于组成性驻留在质膜中的STIM1池,并且这些通道的孔由Orai1和Orai3亚基组成。明显的含义是CRAC通道和ARC通道密切相关,但已进化为在钙信号调节中发挥独特作用——很大程度上是由于它们完全不同的激活模式。鉴于此,尽管花生四烯酸如何作用于激活通道的精确细节仍不清楚,但似乎这些通道与CRAC通道不同的特定分子特征——即Orai3和/或质膜STIM1——将参与其中。

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