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首页> 外文期刊>Journal of molecular graphics & modelling >Structural and binding insights into HIV-1 protease and P2-ligand interactions through molecular dynamics simulations, binding free energy and principal component analysis
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Structural and binding insights into HIV-1 protease and P2-ligand interactions through molecular dynamics simulations, binding free energy and principal component analysis

机译:通过分子动力学模拟的HIV-1蛋白酶和P2-配体相互作用的结构和结合洞察力,结合自由能和主要成分分析

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摘要

HIV-1 protease (HIV-1-pr) plays an important role in viral replication and maturation, making it one of the most attractive targets for anti-retroviral therapy. To design new effective inhibitors able to combat drug resistance in mutant HIV-1-pr variants, it is essential to gain further understanding about the mechanisms by which the recently proposed inhibitors deactivate the mutant HIV-1-pr variants. In the present work, we explored the interactions between two P2-ligands (DRV, and one new derivative, 4UY) with wild type (WT) and two multiple mutant HIV-1-pr variants (p20 and p51) with all atom molecular dynamics (MD) simulations, binding free energy calculations, and principal component analysis (PCA). The trajectories of MD simulations show that both 4UY and DRV primarily bind with the active sites, flap and 80s loop regions of HIV-1-pr variants through either hydrogen bonds or hydrophobic interactions. More hydrogen bonds and hydrophobic interactions were located for 4UY/HIV-1-pr complexes than for DRV/HIV-1-pr counterparts. More importantly, 4UY was found to have an extra hydrogen bond with the backbone of Gly48' in the flap region of the HIV-1-prs. The flap tip-tip distance (150-150') and flap tip active site distance (150-D25 and 150'-D25') indicate that the flaps turn more closed in 4UY bound HIV-1prs than DRV bound ones, and the former also have more compact hydrophobic cavities than the latter. Further, the vector projections from PCA indicate that 4UY/DRV inhibitor binding projects the closing of flap in HIV-1-pr variants. In line with the above trajectory analysis, the thermodynamics calculation with MM-PBSA method suggests much stronger binding affinity for 4UY/HIV-1-pr than DRV/HIV-1-pr by 4.3 -6.4 kcal/mol. Although p20 and p51 also induce weaker binding due to multiple mutants for 4UY inhibitor by 1.9-1.8 kcal/mol, their bindings to the new P2 ligand (4UY) are indeed significantly enhanced as compared to DRV. The thermodynamic components responsible
机译:HIV-1蛋白酶(HIV-1-PR)在病毒复制和成熟中起着重要作用,使其成为抗逆转录病毒治疗最具吸引力的目标之一。为了设计能够在突变体HIV-1-PR变体中对抗耐药性的新有效抑制剂,必须进一步了解最近提出的抑制剂失活的机制必须进一步了解突变体HIV-1-PR变体。在本作工作中,我们探讨了两种P2-配体(DRV和一个新衍生物,4UY)与野生型(WT)和两种多突变HIV-1-PR变体(P20和P51)之间的相互作用,所有原子分子动力学(MD)模拟,结合自由能量计算和主成分分析(PCA)。 MD模拟的轨迹表明,4UY和DRV通过氢键或疏水相互作用与HIV-1-PR变体的活性位点,襟翼和80S循环区域结合。对于DRV / HIV-1-PR对应物,位于4uY / HIV-1-PR复合物的更多氢键和疏水性相互作用。更重要的是,发现4UY在HIV-1-PRS的襟翼区域中具有额外的氢键与GLY48'的骨干。襟翼尖端距离(150-150')和翻盖尖端有源网站距离(150-d25和150'-d25')表明襟翼在4uy绑定的HIV-1PR中变得比DRV绑定的延伸更新,而前者还具有比后者更紧凑的疏水性腔。此外,来自PCA的载体突起表明4UY / DRV抑制剂结合突出了HIV-1-PR变体中的襟翼的闭合。根据上述轨迹分析,用MM-PBSA方法的热力学计算表明,对于40Y / HIV-1-PR,比DRV / HIV-1-PR为4.3 -6.4kcal / mol的更强的结合亲和力。尽管P20和P51也引起较弱的结合由于4uy抑制剂的多个突变体,但与DRV相比,它们与新P2配体(4UY)的结合确实显着提高。热力学组件负责

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