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Proteomics to Identify Proteins Interacting with P2X2 Ligand-Gated Cation Channels

机译:蛋白质组学鉴定与P2X2配体门控阳离子通道相互作用的蛋白质

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摘要

Ligand-gated ion channels underlie synaptic communication in the nervous system1. In mammals there are three families of ligand-gated channels: the cys loop, the glutamate-gated and the P2X receptor channels2. In each case binding of transmitter leads to the opening of a pore through which ions flow down their electrochemical gradients. Many ligand-gated channels are also permeable to calcium ions3, 4, which have downstream signaling roles5 (e.g. gene regulation) that may exceed the duration of channel opening. Thus ligand-gated channels can signal over broad time scales ranging from a few milliseconds to days. Given these important roles it is necessary to understand how ligand-gated ion channels themselves are regulated by proteins, and how these proteins may tune signaling. Recent studies suggest that many, if not all, channels may be part of protein signaling complexes6. In this article we explain how to identify the proteins that bind to the C-terminal aspects of the P2X2 receptor cytosolic domain.P2X receptors are ATP-gated cation channels and consist of seven subunits (P2X1-P2X7). P2X receptors are widely expressed in the brain, where they mediate excitatory synaptic transmission and presynaptic facilitation of neurotransmitter release7. P2X receptors are found in excitable and non-excitable cells and mediate key roles in neuronal signaling, inflammation and cardiovascular function8. P2X2 receptors are abundant in the nervous system9 and are the focus of this study. Each P2X subunit is thought to possess two membrane spanning segments (TM1 & TM2) separated by an extracellular region7 and intracellular N and C termini (Fig 1a)7. P2X subunits10 (P2X1-P2X7) show 30-50% sequence homology at the amino acid level11. P2X receptors contain only three subunits, which is the simplest stoichiometry among ionotropic receptors. The P2X2 C-terminus consists of 120 amino acids (Fig 1b) and contains several protein docking consensus sites, supporting the hypothesis that P2X2 receptor may be part of signaling complexes. However, although several functions have been attributed to the C-terminus of P2X2 receptors9 no study has described the molecular partners that couple to the intracellular side of this protein via the full length C-terminus. In this methods paper we describe a proteomic approach to identify the proteins which interact with the full length C-terminus of P2X2 receptors.
机译:配体门控离子通道是神经系统 1 中突触通讯的基础。在哺乳动物中,存在三个家族的配体门控通道:cys环,谷氨酸门控和P2X受体通道 2 。在每种情况下,发射器的结合都会导致开孔,离子通过该开孔沿其电化学梯度向下流动。许多配体门控通道也可渗透钙离子 3,4 ,其下游信号传导作用 5 (例如基因调控)可能超过通道开放的持续时间。因此,配体门控的通道可以在几毫秒到几天的宽范围内发出信号。鉴于这些重要的作用,有必要了解配体门控离子通道本身是如何被蛋白质调控的,以及这些蛋白质如何调节信号传导。最近的研究表明,许多(即使不是全部)通道可能是蛋白质信号复合物 6 的一部分。在本文中,我们解释了如何鉴定与P2X2受体胞质结构域C端结合的蛋白质.P2X受体是ATP门控的阳离子通道,由七个亚基(P2X1-P2X7)组成。 P2X受体在大脑中广泛表达,介导兴奋性突触传递和神经递质释放 7 的突触前促进。 P2X受体存在于兴奋性和非兴奋性细胞中,并在神经元信号传导,炎症和心血管功能中起关键作用 8 。 P2X2受体在神经系统 9 中含量很高,是本研究的重点。每个P2X亚基被认为具有两个跨膜段(TM1和TM2),这些跨膜段由细胞外区域 7 和细胞内N和C末端分隔(图1a) 7 。 P2X亚基 10 (P2X1-P2X7)在氨基酸水平 11 上具有30-50%的序列同源性。 P2X受体仅包含三个亚基,这是离子型受体中最简单的化学计量。 P2X2 C末端包含120个氨基酸(图1b),并包含几个蛋白质对接共有位点,支持P2X2受体可能是信号复合物一部分的假设。然而,尽管P2X2受体 9 的C末端具有多种功能,但尚无研究描述通过全长C末端与该蛋白的细胞内结合的分子伴侣。在此方法论文中,我们描述了一种蛋白质组学方法来鉴定与P2X2受体的全长C末端相互作用的蛋白质。

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