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Effect of Amphipathic HIV Fusion Inhibitor Peptides on POPC and POPC/Cholesterol Membrane Properties: A Molecular Simulation Study

机译:两亲性HIV融合抑制剂肽对POPC和POPC /胆固醇膜特性的影响:分子模拟研究

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摘要

T-20 and T-1249 fusion inhibitor peptides were shown to interact with 1-palmitoyl-2-oleyl-phosphatidylcholine (POPC) (liquid disordered, ld) and POPC/cholesterol (1:1) (POPC/Chol) (liquid ordered, lo) bilayers, and they do so to different extents. Although they both possess a tryptophan-rich domain (TRD), T-20 lacks a pocket binding domain (PBD), which is present in T-1249. It has been postulated that the PBD domain enhances FI interaction with HIV gp41 protein and with model membranes. Interaction of these fusion inhibitor peptides with both the cell membrane and the viral envelope membrane is important for function, i.e., inhibition of the fusion process. We address this problem with a molecular dynamics approach focusing on lipid properties, trying to ascertain the consequences and the differences in the interaction of T-20 and T-1249 with ld and lo model membranes. T-20 and T-1249 interactions with model membranes are shown to have measurable and different effects on bilayer structural and dynamical parameters. T-1249’s adsorption to the membrane surface has generally a stronger influence in the measured parameters. The presence of both binding domains in T-1249 appears to be paramount to its stronger interaction, and is shown to have a definite importance in membrane properties upon peptide adsorption.
机译:显示T-20和T-1249融合抑制剂肽与1-棕榈酰基-2-油基磷脂酰胆碱(POPC)(液体无序,ld)和POPC /胆固醇(1:1)(POPC / Chol)(液体有序)相互作用,lo)双层,它们的作用程度不同。尽管它们都具有富含色氨酸的结构域(TRD),但T-20缺少口袋结合域(PBD),该结构存在于T-1249中。据推测,PBD结构域增强了FI与HIV gp41蛋白和模型膜的相互作用。这些融合抑制剂肽与细胞膜和病毒包膜的相互作用对于功能即抑制融合过程是重要的。我们通过关注脂质性质的分子动力学方法解决了这个问题,试图确定后果以及T-20和T-1249与ld和lo模型膜相互作用的差异。 T-20和T-1249与模型膜的相互作用对双层结构和动力学参数具有可测量的不同影响。 T-1249在膜表面的吸附通常会对测量参数产生更大的影响。 T-1249中两个结合结构域的存在似乎对其更强的相互作用至关重要,并且在肽吸附后显示出对膜性质的绝对重要性。

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