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溶质:钠离子同向转运体的第一个跨膜片段中的保守酪氨酸参与 Na+ 偶联底物共转运。

Conserved tyrosine in the first transmembrane segment of solute:sodium symporters is involved in Na+-coupled substrate co-transport.

机构信息

Department of Physiology and Biophysics, Weill Cornell Medical College, New York, New York 10065.

Center for Molecular Recognition & Department of Psychiatry, Columbia University College of Physicians and Surgeons, New York, New York 10032, and the New York State Psychiatric Institute, Division of Molecular Therapeutics, New York, New York 10032.

出版信息

J Biol Chem. 2011 Aug 19;286(33):29347-29355. doi: 10.1074/jbc.M111.263327. Epub 2011 Jun 24.

Abstract

Solute:sodium symporters (SSSs) transport vital molecules across the plasma membrane of all living organisms. vSGLT, the Na(+)/galactose transporter of Vibrio parahemeolyticus, is the only SSS for which high resolution structural information is available, revealing a LeuT-like fold and a Na(+)-binding site analogous to the Na2 site of LeuT. Whereas the core transmembrane segments (TMs) of SSSs share high structural similarity with other transporters of LeuT-like fold, TM1 does not correspond to any TM in those structural homologs and was only resolved for the backbone atoms in the initial vSGLT structure (Protein Data Bank code 3DH4). To assess the role of TM1 in Na(+)-coupled substrate symport by the SSSs, here we have studied the role of a conserved residue in TM1 by computational modeling in conjunction with radiotracer transport and binding studies. Based on our sequence alignment and much topological data for homologous PutP, the Na(+)/proline transporter, we have simulated a series of vSGLT models with shifted TM1 residue assignments. We show that in two converged vSGLT models that retained the original TM1 backbone conformation, a conserved residue, Tyr-19, is associated with the Na(+) binding interaction network. In silico and in vitro mutagenesis of homologous Tyr-14 in PutP revealed the involvement of this conserved residue in Na(+)-dependent substrate binding and transport. Thus, our combined computational and experimental data provide the first clues about the importance of a conserved residue in TM1, a unique TM in the proteins with LeuT-like fold, in the Na(+)-coupled symport mechanism of SSSs.

摘要

溶质

钠协同转运蛋白(SSSs)将重要分子运输穿过所有生物体的质膜。副溶血性弧菌的 Na(+)/半乳糖转运蛋白 vSGLT 是唯一具有高分辨率结构信息的 SSSs,其揭示了一种 LeuT 样折叠和类似于 LeuT 的 Na2 位点的 Na(+)结合位点。尽管 SSSs 的核心跨膜片段(TMs)与 LeuT 样折叠的其他转运蛋白具有高度结构相似性,但 TM1 与这些结构同源物中的任何 TM 都不对应,并且仅在初始 vSGLT 结构(蛋白质数据银行代码 3DH4)中解析为骨干原子。为了评估 TM1 在 SSSs 介导的 Na(+)-偶联底物协同转运中的作用,我们通过计算建模结合放射性示踪转运和结合研究来研究 TM1 中保守残基的作用。基于我们的序列比对和同源 PutP(Na(+)/脯氨酸转运蛋白)的大量拓扑数据,我们模拟了一系列具有移位 TM1 残基分配的 vSGLT 模型。我们表明,在保留原始 TM1 骨干构象的两个收敛的 vSGLT 模型中,一个保守残基 Tyr-19 与 Na(+)结合相互作用网络相关。同源 Tyr-14 在 PutP 中的计算和体外诱变揭示了该保守残基在 Na(+)依赖性底物结合和转运中的参与。因此,我们的组合计算和实验数据首次提供了关于 LeuT 样折叠蛋白中独特的 TM1 中保守残基在 SSSs 的 Na(+)-偶联协同转运机制中的重要性的线索。

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本文引用的文献

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Biology of human sodium glucose transporters.人类钠-葡萄糖转运体的生物学特性。
Physiol Rev. 2011 Apr;91(2):733-94. doi: 10.1152/physrev.00055.2009.
7
Ion-releasing state of a secondary membrane transporter.次级膜转运蛋白的离子释放态。
Biophys J. 2009 Dec 2;97(11):L29-31. doi: 10.1016/j.bpj.2009.09.005.
9
Structure and function of Na(+)-symporters with inverted repeats.具有反向重复序列的钠离子同向转运体的结构与功能
Curr Opin Struct Biol. 2009 Aug;19(4):425-32. doi: 10.1016/j.sbi.2009.06.002. Epub 2009 Jul 22.
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