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Molecular dynamic study of MlaC protein in Gram‐negative bacteria: conformational flexibility solvent effect and protein‐phospholipid binding

机译:革兰氏阴性细菌中MlaC蛋白的分子动力学研究:构象柔性溶剂作用和蛋白磷脂结合

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摘要

The composition of the outer membrane in Gram‐negative bacteria is asymmetric, with the lipopolysaccharides found in the outer leaflet and phospholipids in the inner leaflet. The MlaC protein transfers phospholipids from the outer to inner membrane to maintain such lipid asymmetry in the Mla pathway. In this work, we have performed molecular dynamics simulations on apo and phospholipid‐bound systems to study the dynamical properties of MlaC. Our simulations show that the phospholipid forms hydrophobic interactions with the protein. Residues surrounding the entrance of the binding site exhibit correlated motions to control the site opening and closing. Lipid binding leads to increase of the binding pocket volume and precludes entry of the water molecules. However, in the absence of the phospholipid, water molecules can freely move in and out of the binding site when the pocket is open. Dehydration occurs when the pocket closes. This study provides dynamic information of the MlaC protein and may facilitate the design of antibiotics against the Mla pathway of Gram‐negative bacteria.
机译:革兰氏阴性细菌的外膜组成是不对称的,外小叶中存在脂多糖,内小叶中存在磷脂。 MlaC蛋白将磷脂从外膜转移到内膜,以在Mla途径中维持此类脂质不对称性。在这项工作中,我们对载脂蛋白和磷脂结合的系统进行了分子动力学模拟,以研究MlaC的动力学性质。我们的模拟表明磷脂与蛋白质形成疏水相互作用。结合位点入口周围的残基表现出相关的运动,以控制位点的打开和关闭。脂质结合导致结合口袋体积的增加,并阻止水分子进入。然而,在没有磷脂的情况下,当口袋打开时,水分子可以自由地移入和移出结合位点。口袋闭合时会发生脱水。这项研究提供了MlaC蛋白的动态信息,并可能有助于针对革兰氏阴性细菌Mla途径的抗生素设计。

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