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一种新型细菌环核苷酸门控(bCNG)离子通道家族的鉴定与实验验证。

Identification and experimental verification of a novel family of bacterial cyclic nucleotide-gated (bCNG) ion channels.

作者信息

Caldwell David B, Malcolm Hannah R, Elmore Donald E, Maurer Joshua A

机构信息

Department of Chemistry, Washington University in St. Louis, St. Louis, MO 63130, USA.

出版信息

Biochim Biophys Acta. 2010 Sep;1798(9):1750-6. doi: 10.1016/j.bbamem.2010.06.001. Epub 2010 Jun 8.

Abstract

Studies of bacterial ion channels have provided significant insights into the structure-function relationships of mechanosensitive and voltage-gated ion channels. However, to date, very few bacterial channels that respond to small molecules have been identified, cloned, and characterized. Here, we use bioinformatics to identify a novel family of bacterial cyclic nucleotide-gated (bCNG) ion channels containing a channel domain related by sequence homology to the mechanosensitive channel of small conductance (MscS). In this initial report, we clone selected members of this channel family, use electrophysiological measurements to verify their ability to directly gate in response to cyclic nucleotides, and use osmotic downshock to demonstrate their lack of mechanosensitivity. In addition to providing insight into bacterial physiology, these channels will provide researchers with a useful model system to investigate the role of ligand-gated ion channels (LGICs) in the signaling processes of higher organisms. The identification of these channels provides a foundation for structural and functional studies of LGICs that would be difficult to perform on mammalian channels. Moreover, the discovery of bCNG channels implies that bacteria have cyclic nucleotide-gated and cyclic nucleotide-modulated ion channels, which are analogous to the ion channels involved in eukaryotic secondary messenger signaling pathways.

摘要

对细菌离子通道的研究为机械敏感和电压门控离子通道的结构-功能关系提供了重要见解。然而,迄今为止,已鉴定、克隆并表征的对小分子有反应的细菌通道非常少。在这里,我们利用生物信息学鉴定了一个新的细菌环核苷酸门控(bCNG)离子通道家族,该家族包含一个与小电导机械敏感通道(MscS)在序列同源性上相关的通道结构域。在本初步报告中,我们克隆了该通道家族的选定成员,用电生理学测量来验证它们对环核苷酸直接门控的能力,并利用渗透压骤降来证明它们缺乏机械敏感性。除了有助于深入了解细菌生理学外,这些通道还将为研究人员提供一个有用的模型系统,以研究配体门控离子通道(LGICs)在高等生物信号传导过程中的作用。这些通道的鉴定为LGICs的结构和功能研究奠定了基础,而这些研究在哺乳动物通道上难以进行。此外,bCNG通道的发现意味着细菌具有环核苷酸门控和环核苷酸调节的离子通道,这类似于参与真核生物第二信使信号通路的离子通道。

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