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缝隙连接半通道和连接蛋白通道的电生理学:它们有何不同?

Connexin hemichannel and pannexin channel electrophysiology: how do they differ?

机构信息

Department of Pharmacology, SUNY Upstate Medical University, Syracuse, NY 13210, United States.

Department of Pharmacology, SUNY Upstate Medical University, Syracuse, NY 13210, United States.

出版信息

FEBS Lett. 2014 Apr 17;588(8):1372-8. doi: 10.1016/j.febslet.2013.12.023. Epub 2014 Jan 14.

Abstract

Connexin hemichannels are postulated to form a cell permeabilization pore for the uptake of fluorescent dyes and release of cellular ATP. Connexin hemichannel activity is enhanced by low external [Ca(2+)]o, membrane depolarization, metabolic inhibition, and some disease-causing gain-of-function connexin mutations. This paper briefly reviews the electrophysiological channel conductance, permeability, and pharmacology properties of connexin hemichannels, pannexin 1 channels, and purinergic P2X7 receptor channels as studied in exogenous expression systems including Xenopus oocytes and mammalian cell lines such as HEK293 cells. Overlapping pharmacological inhibitory and channel conductance and permeability profiles makes distinguishing between these channel types sometimes difficult. Selective pharmacology for Cx43 hemichannels (Gap19 peptide), probenecid or FD&C Blue #1 (Brilliant Blue FCF, BB FCF) for Panx1, and A740003, A438079, or oxidized ATP (oATP) for P2X7 channels may be the best way to distinguish between these three cell permeabilizing channel types. Endogenous connexin, pannexin, and P2X7 expression should be considered when performing exogenous cellular expression channel studies. Cell pair electrophysiological assays permit the relative assessment of the connexin hemichannel/gap junction channel ratio not often considered when performing isolated cell hemichannel studies.

摘要

缝隙连接半通道被假定为形成细胞通透性孔,用于摄取荧光染料和释放细胞内 ATP。缝隙连接半通道活性可被低细胞外[Ca(2+)]o、膜去极化、代谢抑制和一些致病的连接蛋白功能获得性突变所增强。本文简要综述了缝隙连接半通道、连接蛋白 1 通道和嘌呤能 P2X7 受体通道在外源表达系统(包括非洲爪蟾卵母细胞和哺乳动物细胞系如 HEK293 细胞)中的电生理通道电导、通透性和药理学特性。重叠的药理学抑制和通道电导及通透性特征使得区分这些通道类型有时变得困难。对于 Cx43 半通道(Gap19 肽)、丙磺舒或 FD&C Blue #1(亮蓝 FCF,BB FCF)用于 Panx1,以及 A740003、A438079 或氧化型 ATP(oATP)用于 P2X7 通道的选择性药理学可能是区分这三种细胞通透性通道类型的最佳方法。在进行外源细胞表达通道研究时,应考虑内源性连接蛋白、连接蛋白和 P2X7 的表达。细胞对电生理测定可相对评估缝隙连接半通道/缝隙连接通道的比值,而在进行分离的细胞半通道研究时通常不会考虑这一点。

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