Section on Cellular Signaling, Program in Developmental Neuroscience, NICHD, National Institutes of Health, Bldg. 49, Room 6A-36, 49 Convent Drive, Bethesda, MD 20892-4510, USA.
Cell Mol Neurobiol. 2010 Nov;30(8):1251-8. doi: 10.1007/s10571-010-9568-y. Epub 2010 Nov 25.
The P2X4 receptor (P2X4R) is a member of a family of ATP-gated cation channels that are composed of three subunits. Each subunit has two transmembrane (TM) domains linked by a large extracellular loop and intracellularly located N- and C-termini. The receptors are expressed in excitable and non-excitable cells and have been implicated in the modulation of membrane excitability, calcium signaling, neurotransmitter and hormone release, and pain physiology. P2X4Rs activate rapidly and desensitize within the seconds of agonist application, both with the rates dependent on ATP concentrations, and deactivate rapidly and independently of ATP concentration. Disruption of conserved cysteine ectodomain residues affects ATP binding and gating. Several ectodomain residues of P2X4R were identified as critical for ATP binding, including K67, K313, and R295. Ectodomain residues also account for the allosteric regulation of P2X4R; H140 is responsible for copper binding and H286 regulates receptor functions with protons. Ivermectin sensitized receptors, amplified the current amplitude, and slowed receptor deactivation by binding in the TM region. Scanning mutagenesis of TMs revealed the helical topology of both domains, and suggested that receptor function is critically dependent on the conserved Y42 residue. In this brief article, we summarize this study and re-interpret it using a model based on crystallization of the zebrafish P2X4.1 receptor.
P2X4 受体(P2X4R)是 ATP 门控阳离子通道家族的成员,由三个亚基组成。每个亚基有两个跨膜(TM)结构域,由一个大的细胞外环和细胞内的 N 端和 C 端连接。该受体在兴奋和非兴奋细胞中表达,并与膜兴奋性、钙信号、神经递质和激素释放以及疼痛生理学的调节有关。P2X4R 在激动剂应用后的几秒钟内迅速激活并脱敏,其速率取决于 ATP 浓度,并且快速独立于 ATP 浓度失活。保守的半胱氨酸胞外域残基的破坏会影响 ATP 的结合和门控。已经确定 P2X4R 的几个胞外域残基对于 ATP 结合至关重要,包括 K67、K313 和 R295。胞外域残基也负责 P2X4R 的变构调节;H140 负责铜结合,H286 通过质子调节受体功能。伊维菌素结合在 TM 区域,敏化受体,放大电流幅度,并减缓受体失活。TM 的扫描突变揭示了两个结构域的螺旋拓扑结构,并表明受体功能严重依赖于保守的 Y42 残基。在这篇简短的文章中,我们总结了这项研究,并使用基于斑马鱼 P2X4.1 受体晶体的模型重新解释了这项研究。