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首页> 外文期刊>Biophysical Chemistry: An International Journal Devoted to the Physical Chemistry of Biological Phenomena >Theoretical study of the interactions between the first transmembrane segment of NS2 protein and a POPC lipid bilayer
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Theoretical study of the interactions between the first transmembrane segment of NS2 protein and a POPC lipid bilayer

机译:NS2蛋白的第一个跨膜片段与POPC脂质双层相互作用的理论研究

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Non-structural protein 2 (NS2) plays a crucial role in the hepatitis C virus (HCV) assembly. NS2 was predicted to be composed of three transmembrane (TM) segments. However, the mechanism of interactions between TM segments of NS2 and surrounding lipid environment remains unclear. Molecular dynamics simulations were applied to investigate the conformation and orientation of the first transmembrane segment (TM1) as well as the interactions of TM1 with a zwitterionic POPC lipid bilayer which identifies several key residues that stabilize the position of TM1 within the membrane. Along with the charged residues R3 and K27, the S23 and H25 were found to be the key elements in establishing the conformation of TM1 inside the membrane. The peptide forms a stable alpha-helix (the sequence 12-21) connected to N-terminal haft in POPC bilayer. The results also reveal that TM1 induces the ordering of lipid and does not destabilize the lipid bilayer system. The hydrophobic mismatch in which the segment tilts an angle along the membrane normal was observed in this system. The binding free energy profile of TM1 to the membrane was also estimated using umbrella sampling. (C) 2016 Published by Elsevier B.V.
机译:非结构蛋白2(NS2)在丙型肝炎病毒(HCV)组装中起关键作用。预测NS2由三个跨膜(TM)段组成。然而,NS2的TM段和周围的脂质环境之间的相互作用的机制仍不清楚。应用分子动力学模拟研究了第一个跨膜片段(TM1)的构象和方向,以及TM1与两性离子POPC脂质双层的相互作用,该相互作用识别了几个稳定TM1在膜内位置的关键残基。与带电残基R3和K27一起,发现S23和H25是在膜内建立TM1构象的关键元素。该肽形成一个稳定的α-螺旋(序列12-21),该螺旋与POPC双层中的N末端柄相连。结果还表明,TM1诱导脂质有序化,并且不会破坏脂质双层系统的稳定性。在该系统中观察到疏水性不匹配,其中节段沿着膜法线倾斜一个角度。 TM1与膜的结合自由能分布也使用伞式采样进行了估计。 (C)2016由Elsevier B.V.发布

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