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通过粗粒度模拟探索乳糖通透酶在糖结合和质子转移时的构象变化。

Exploration of conformational changes in lactose permease upon sugar binding and proton transfer through coarse-grained simulations.

作者信息

Jewel Yead, Dutta Prashanta, Liu Jin

机构信息

School of Mechanical and Materials Engineering, Washington State University, Pullman, Washington, 99164.

出版信息

Proteins. 2017 Oct;85(10):1856-1865. doi: 10.1002/prot.25340. Epub 2017 Jul 6.

DOI:10.1002/prot.25340
PMID:28639287
Abstract

Escherichia coli lactose permease (LacY) actively transports lactose and other galactosides across cell membranes through lactose/H symport process. Lactose/H symport is a highly complex process that involves sugar translocation, H transfer, and large-scale protein conformational changes. The complete picture of lactose/H symport is largely unclear due to the complexity and multiscale nature of the process. In this work, we develop the force field for sugar molecules compatible with PACE, a hybrid and coarse-grained force field that couples the united-atom protein models with the coarse-grained MARTINI water/lipid. After validation, we implement the new force field to investigate the binding of a β-d-galactopyranosyl-1-thio- β-d-galactopyranoside (TDG) molecule to a wild-type LacY. Results show that the local interactions between TDG and LacY at the binding pocket are consistent with the X-ray experiment. Transitions from inward-facing to outward-facing conformations upon TDG binding and protonation of Glu269 have been achieved from ∼5.5 µs simulations. Both the opening of the periplasmic side and closure of the cytoplasmic side of LacY are consistent with double electron-electron resonance and thiol cross-linking experiments. Our analysis suggests that the conformational changes of LacY are a cumulative consequence of interdomain H-bonds breaking at the periplasmic side, interdomain salt-bridge formation at the cytoplasmic side, and the TDG orientational changes during the transition.

摘要

大肠杆菌乳糖通透酶(LacY)通过乳糖/质子同向转运过程将乳糖和其他半乳糖苷主动转运穿过细胞膜。乳糖/质子同向转运是一个高度复杂的过程,涉及糖的转运、质子转移以及大规模的蛋白质构象变化。由于该过程的复杂性和多尺度性质,乳糖/质子同向转运的全貌在很大程度上尚不清楚。在这项工作中,我们开发了与PACE兼容的糖分子力场,PACE是一种混合粗粒度力场,它将联合原子蛋白质模型与粗粒度的MARTINI水/脂质相结合。经过验证后,我们应用新的力场来研究β-D-吡喃半乳糖基-1-硫代-β-D-吡喃半乳糖苷(TDG)分子与野生型LacY的结合。结果表明,TDG与LacY在结合口袋处的局部相互作用与X射线实验结果一致。通过约5.5微秒的模拟,实现了TDG结合以及Glu269质子化后从内向构象到外向构象的转变。LacY周质侧的开放和胞质侧的关闭均与双电子-电子共振和硫醇交联实验结果一致。我们的分析表明,LacY的构象变化是周质侧结构域间氢键断裂、胞质侧结构域间盐桥形成以及转变过程中TDG取向变化的累积结果。

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Exploration of conformational changes in lactose permease upon sugar binding and proton transfer through coarse-grained simulations.通过粗粒度模拟探索乳糖通透酶在糖结合和质子转移时的构象变化。
Proteins. 2017 Oct;85(10):1856-1865. doi: 10.1002/prot.25340. Epub 2017 Jul 6.
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