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动物细胞中受体激活的钙离子内流:多种为满足不同细胞内钙离子信号需求而量身定制的途径。

Receptor-activated Ca2+ inflow in animal cells: a variety of pathways tailored to meet different intracellular Ca2+ signalling requirements.

作者信息

Barritt G J

机构信息

Department of Medical Biochemistry, School of Medicine, Faculty of Health Sciences, Flinders University, G.P.O. Box 2100, Adelaide, South Australia 5001, Australia.

出版信息

Biochem J. 1999 Jan 15;337 ( Pt 2)(Pt 2):153-69.

Abstract

Receptor-activated Ca2+ channels (RACCs) play a central role in regulation of the functions of animal cells. Together with voltage-operated Ca2+ channels (VOCCs) and ligand-gated non-selective cation channels, RACCs provide a variety of pathways by which Ca2+ can be delivered to the cytoplasmic space and the endoplasmic reticulum (ER) in order to initiate or maintain specific types of intracellular Ca2+ signal. Store-operated Ca2+ channels (SOCs), which are activated by a decrease in Ca2+ in the ER, are a major subfamily of RACCs. A careful analysis of the available data is required in order to discern the different types of RACCs (differentiated chiefly on the basis of ion selectivity and mechanism of activation) and to properly develop hypotheses for structures and mechanisms of activation. Despite much intensive research, the structures and mechanisms of activation of RACCs are only now beginning to be understood. In considering the physiological functions of the different RACCs, it is useful to consider the specificity for Ca2+ of each type of cation channel and the rate at which Ca2+ flows through a single open channel; the locations of the channels on the plasma membrane (in relation to the ER, cytoskeleton and other intracellular units of structure and function); the Ca2+-responsive enzymes and proteins; and the intracellular buffers and proteins that control the distribution of Ca2+ in the cytoplasmic space. RACCs which are non-selective cation channels can deliver Ca2+ directly to specific regions of the cytoplasmic space, and can also admit Na+, which induces depolarization of the plasma membrane, the opening of VOCCs and the subsequent inflow of Ca2+. SOCs appear to deliver Ca2+ specifically to the ER, thereby maintaining oscillating Ca2+ signals.

摘要

受体激活的钙离子通道(RACCs)在动物细胞功能调节中起核心作用。与电压门控钙离子通道(VOCCs)和配体门控非选择性阳离子通道一起,RACCs提供了多种途径,通过这些途径钙离子可以被输送到细胞质空间和内质网(ER),以启动或维持特定类型的细胞内钙离子信号。由内质网中钙离子减少激活的储存操纵性钙离子通道(SOCs)是RACCs的一个主要亚家族。需要仔细分析现有数据,以便辨别不同类型的RACCs(主要根据离子选择性和激活机制区分),并正确地提出关于其激活结构和机制的假设。尽管进行了大量深入研究,但RACCs的激活结构和机制直到现在才开始被理解。在考虑不同RACCs的生理功能时,考虑每种阳离子通道对钙离子的特异性以及钙离子通过单个开放通道的流速;通道在质膜上的位置(相对于内质网、细胞骨架和其他细胞内结构与功能单位);钙离子反应性酶和蛋白质;以及控制细胞质空间中钙离子分布的细胞内缓冲液和蛋白质是很有用的。作为非选择性阳离子通道的RACCs可以将钙离子直接输送到细胞质空间的特定区域,还可以允许钠离子进入,这会导致质膜去极化、VOCCs开放以及随后钙离子的流入。SOCs似乎将钙离子特异性地输送到内质网,从而维持振荡的钙离子信号。

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