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Recovery of the wild type atomic flexibility in the HIV-1 protease double mutants

机译:HIV-1蛋白酶双突变体中野生型原子柔韧性的恢复

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摘要

The emergence of drug resistant mutations due to the selective pressure exerted by antiretrovirals, including protease inhibitors (PIs), remains a major problem in the treatment of AIDS. During PIs therapy, the occurrence of primary mutations in the wild type HIV-1 protease reduces both the affinity for the inhibitors and the viral replicative capacity compared to the wild type (WT) protein, but additional mutations compensate for this reduced viral fitness. To investigate this phenomenon from the structural point of view, we combined Molecular Dynamics and Normal Mode Analysis to analyze and compare the variations of the flexibility of C-alpha atoms and the differences in hydrogen bond (h-bond) network between the WT and double mutants. In most cases, the flexibility profile of the double mutants was more often similar to that of the WT than to that of the related single base mutants. All single mutants showed a significant alteration in h-bond formation compared to WT. Most of the significant changes occur in the border between the flap and cantilever regions. We found that all the considered double mutants have their h-bond pattern significantly altered in comparison to the respective single base mutants affecting their flexibility profile that becomes more similar to that of WT. This WT flexibility restoration in the double mutants appears as an important factor for the HIV-1 fitness recovery observed in patients. (C) 2015 Elsevier Inc. All rights reserved.
机译:由于包括蛋白酶抑制剂(PIs)在内的抗逆转录病毒药物施加的选择性压力,导致耐药性突变的出现仍然是治疗艾滋病的主要问题。在PIs治疗期间,与野生型(WT)蛋白相比,野生型HIV-1蛋白酶中主要突变的出现降低了与抑制剂的亲和力和病毒复制能力,但其他突变弥补了这种降低的病毒适应性。为了从结构的角度研究这种现象,我们结合分子动力学和正态分析来分析和比较C-alpha原子的柔韧性变化和WT与双键之间氢键(h-bond)网络的差异。突变体。在大多数情况下,与相关单碱基突变体相比,双突变体的柔韧性谱更常见于野生型。与WT相比,所有单个突变体均显示出h键形成的显着改变。大多数显着变化发生在襟翼和悬臂区域之间的边界。我们发现,与各个单碱基突变体相比,所有考虑的双突变体的h键模式均发生了显着变化,从而影响了它们的柔韧性,与WT相似。在双突变体中的这种WT灵活性恢复似乎是患者中观察到的HIV-1适应性恢复的重要因素。 (C)2015 Elsevier Inc.保留所有权利。

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