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用于研究CFTR通道门控及其调节的电生理、生化和生物信息学方法。

Electrophysiological, biochemical, and bioinformatic methods for studying CFTR channel gating and its regulation.

作者信息

Csanády László, Vergani Paola, Gulyás-Kovács Attila, Gadsby David C

机构信息

Department of Medical Biochemistry, Semmelweis University, Budapest, Hungary.

出版信息

Methods Mol Biol. 2011;741:443-69. doi: 10.1007/978-1-61779-117-8_28.

Abstract

CFTR is the only member of the ABC (ATP-binding cassette) protein superfamily known to function as an ion channel. Most other ABC proteins are ATP-driven transporters, in which a cycle of ATP binding and hydrolysis, at intracellular nucleotide binding domains (NBDs), powers uphill substrate translocation across the membrane. In CFTR, this same ATP-driven cycle opens and closes a transmembrane pore through which chloride ions flow rapidly down their electrochemical gradient. Detailed analysis of the pattern of gating of CFTR channels thus offers the opportunity to learn about mechanisms of function not only of CFTR channels but also of their ABC transporter ancestors. In addition, CFTR channel gating is subject to complex regulation by kinase-mediated phosphorylation at multiple consensus sites in a cytoplasmic regulatory domain that is unique to CFTR. Here we offer a practical guide to extract useful information about the mechanisms that control opening and closing of CFTR channels: on how to plan (including information obtained from analysis of multiple sequence alignments), carry out, and analyze electrophysiological and biochemical experiments, as well as on how to circumvent potential pitfalls.

摘要

囊性纤维化跨膜传导调节因子(CFTR)是已知作为离子通道发挥作用的ATP结合盒(ABC)蛋白超家族的唯一成员。大多数其他ABC蛋白是ATP驱动的转运蛋白,其中在细胞内核苷酸结合结构域(NBDs)处的ATP结合和水解循环为底物跨膜的上坡转运提供动力。在CFTR中,同样的ATP驱动循环打开和关闭一个跨膜孔,氯离子通过该孔迅速顺着其电化学梯度流动。因此,对CFTR通道门控模式的详细分析不仅提供了了解CFTR通道功能机制的机会,也提供了了解其ABC转运蛋白祖先功能机制的机会。此外,CFTR通道门控受到CFTR特有的细胞质调节结构域中多个共有位点处激酶介导的磷酸化的复杂调控。在这里,我们提供一份实用指南,以提取有关控制CFTR通道开闭机制的有用信息:关于如何规划(包括从多序列比对分析中获得的信息)、进行和分析电生理和生化实验,以及如何规避潜在陷阱。

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