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钠离子内流以及钠/钙交换的调节作为瞬时受体电位通道C型(TRPC)信号传导的关键机制。

Na(+) entry and modulation of Na(+)/Ca(2+) exchange as a key mechanism of TRPC signaling.

作者信息

Eder Petra, Poteser Michael, Romanin Christoph, Groschner Klaus

机构信息

Institute of Pharmaceutical Sciences, Pharmacology and Toxicology, Karl-Franzens-University of Graz, Universitaetsplatz 2, 8010 Graz, Austria.

出版信息

Pflugers Arch. 2005 Oct;451(1):99-104. doi: 10.1007/s00424-005-1434-2. Epub 2005 May 28.

Abstract

Ion channels formed by canonical transient receptor potential (TRPC) proteins are considered to be key players in cellular Ca(2+) homeostasis. As permeation of Ca(2+) through TRPC homo- and/or heteromeric channels has been repeatedly demonstrated, analysis of the physiological role of TRPC proteins was so far based on the concept that these proteins form regulated Ca(2+) entry channels. The well-recognized lack of cation selectivity of TRPC channels and the ability to generate substantial monovalent conductances that govern membrane potential and cation gradients were barely appreciated as a physiologically relevant issue. Nonetheless, recent studies suggest monovalent, specifically Na(+) permeation through TRPC cation channels as an important event in TRPC signaling. TRPC-mediated Na(+) entry may be converted into a distinct pattern of cellular Ca(2+) signals by interaction with Na(+)/Ca(2+) exchanger proteins. This review discusses current concepts regarding the link between Na(+) entry through TRPC channels and cellular Ca(2+) signaling.

摘要

由典型瞬时受体电位(TRPC)蛋白形成的离子通道被认为是细胞钙(Ca2+)稳态的关键参与者。由于Ca2+通过TRPC同源和/或异源通道的通透已被反复证实,迄今为止,对TRPC蛋白生理作用的分析基于这些蛋白形成受调控的Ca2+进入通道这一概念。TRPC通道缺乏阳离子选择性以及产生控制膜电位和阳离子梯度的大量单价电导的能力,几乎未被视为一个生理相关问题。尽管如此,最近的研究表明,单价阳离子,特别是Na+通过TRPC阳离子通道的通透是TRPC信号传导中的一个重要事件。TRPC介导的Na+进入可能通过与Na+/Ca2+交换蛋白相互作用而转化为一种独特的细胞Ca2+信号模式。本综述讨论了关于通过TRPC通道的Na+进入与细胞Ca2+信号传导之间联系的当前概念。

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