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钠离子依赖型亮氨酸转运蛋白LeuT中离子-离子和离子-底物偶联的分子机制

Molecular mechanism of ion-ion and ion-substrate coupling in the Na+-dependent leucine transporter LeuT.

作者信息

Caplan David A, Subbotina Julia O, Noskov Sergei Yu

机构信息

Institute for Biocomplexity and Informatics, and Department of Biological Sciences, University of Calgary, Calgary, Alberta, Canada.

出版信息

Biophys J. 2008 Nov 15;95(10):4613-21. doi: 10.1529/biophysj.108.139741. Epub 2008 Aug 15.

Abstract

Ion-coupled transport of neurotransmitter molecules by neurotransmitter:sodium symporters (NSS) play an important role in the regulation of neuronal signaling. One of the major events in the transport cycle is ion-substrate coupling and formation of the high-affinity occluded state with bound ions and substrate. Molecular mechanisms of ion-substrate coupling and the corresponding ion-substrate stoichiometry in NSS transporters has yet to be understood. The recent determination of a high-resolution structure for a bacterial homolog of Na(+)/Cl(-)-dependent neurotransmitter transporters, LeuT, offers a unique opportunity to analyze the functional roles of the multi-ion binding sites within the binding pocket. The binding pocket of LeuT contains two metal binding sites. The first ion in site NA1 is directly coupled to the bound substrate (Leu) with the second ion in the neighboring site (NA2) only approximately 7 A away. Extensive, fully atomistic, molecular dynamics, and free energy simulations of LeuT in an explicit lipid bilayer are performed to evaluate substrate-binding affinity as a function of the ion load (single versus double occupancy) and occupancy by specific monovalent cations. It was shown that double ion occupancy of the binding pocket is required to ensure substrate coupling to Na(+) and not to Li(+) or K(+) cations. Furthermore, it was found that presence of the ion in site NA2 is required for structural stability of the binding pocket as well as amplified selectivity for Na(+) in the case of double ion occupancy.

摘要

神经递质

钠同向转运体(NSS)对神经递质分子的离子偶联转运在神经元信号调节中发挥着重要作用。转运循环中的一个主要事件是离子与底物的偶联以及与结合离子和底物形成高亲和力的堵塞状态。NSS转运体中离子与底物偶联的分子机制以及相应的离子与底物化学计量关系尚不清楚。最近对Na(+)/Cl(-)依赖性神经递质转运体的细菌同源物LeuT的高分辨率结构的测定,为分析结合口袋内多离子结合位点的功能作用提供了独特的机会。LeuT的结合口袋包含两个金属结合位点。位点NA1中的第一个离子直接与结合的底物(亮氨酸)偶联,相邻位点(NA2)中的第二个离子距离仅约7埃。在明确的脂质双层中对LeuT进行了广泛的、全原子的分子动力学和自由能模拟,以评估底物结合亲和力作为离子负载(单占据与双占据)和特定单价阳离子占据情况的函数。结果表明,结合口袋需要双离子占据以确保底物与Na(+)偶联,而不是与Li(+)或K(+)阳离子偶联。此外,还发现位点NA2中离子的存在对于结合口袋的结构稳定性以及在双离子占据情况下对Na(+)的增强选择性是必需的。

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