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普雷斯汀和SLC26转运蛋白中阴离子相互作用的分子结构及结构基础。

Molecular architecture and the structural basis for anion interaction in prestin and SLC26 transporters.

作者信息

Gorbunov Dmitry, Sturlese Mattia, Nies Florian, Kluge Murielle, Bellanda Massimo, Battistutta Roberto, Oliver Dominik

机构信息

1] Department of Neurophysiology, Institute of Physiology and Pathophysiology, Philipps University, 35037 Marburg, Germany [2].

1] Department of Chemical Sciences, University of Padua, via Marzolo 1, Padova 35131, Italy [2].

出版信息

Nat Commun. 2014 Apr 8;5:3622. doi: 10.1038/ncomms4622.

Abstract

Prestin (SLC26A5) is a member of the SLC26/SulP anion transporter family. Its unique quasi-piezoelectric mechanical activity generates fast cellular motility of cochlear outer hair cells, a key process underlying active amplification in the mammalian ear. Despite its established physiological role, it is essentially unknown how prestin can generate mechanical force, since structural information on SLC26/SulP proteins is lacking. Here we derive a structural model of prestin and related transporters by combining homology modelling, MD simulations and cysteine accessibility scanning. Prestin's transmembrane core region is organized in a 7+7 inverted repeat architecture. The model suggests a central cavity as the substrate-binding site located midway of the anion permeation pathway, which is supported by experimental solute accessibility and mutational analysis. Anion binding to this site also controls the electromotile activity of prestin. The combined structural and functional data provide a framework for understanding electromotility and anion transport by SLC26 transporters.

摘要

Prestin(SLC26A5)是SLC26/SulP阴离子转运蛋白家族的成员。其独特的准压电机械活性产生耳蜗外毛细胞的快速细胞运动,这是哺乳动物耳朵中主动放大的关键过程。尽管其生理作用已得到确立,但由于缺乏SLC26/SulP蛋白的结构信息,目前基本上还不清楚Prestin如何产生机械力。在这里,我们通过结合同源建模、分子动力学模拟和半胱氨酸可及性扫描,推导出了Prestin和相关转运蛋白的结构模型。Prestin的跨膜核心区域以7+7反向重复结构组织。该模型表明,在阴离子渗透途径中间位置有一个中央腔作为底物结合位点,这得到了实验性溶质可及性和突变分析的支持。阴离子与该位点的结合也控制着Prestin的电运动活性。结构和功能数据相结合,为理解SLC26转运蛋白的电运动和阴离子转运提供了一个框架。

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