首页> 外文期刊>Journal of chemical theory and computation: JCTC >Study of the Conformational Dynamics of the Catalytic Loop of WT and G140A/G149A HIV-1 Integrase Core Domain Using Reversible Digitally Filtered Molecular Dynamics
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Study of the Conformational Dynamics of the Catalytic Loop of WT and G140A/G149A HIV-1 Integrase Core Domain Using Reversible Digitally Filtered Molecular Dynamics

机译:WT和G140A / G149A HIV-1整合核心结构域催化环构象动力学的可逆数字滤波分子动力学研究

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摘要

The HIV-1 IN enzyme is one of three crucial virally encoded enzymes (HIV-1 IN, HIV-1 PR, and HIV-1 RT) involved in the life-cycle of the HIV-1 virus, making it an attractive target in the development of drugs against the AIDS virus. The structure and mechanism of the HIV-1 IN enzyme is the least understood of the three enzymes due to the lack of three-dimensional structural information. X-ray cystallographic studies have not yet been able to resolve the full-length structure, and studies have been mainly focused on the catalytic domain. This central domain possesses an important catalytic loop observed to overhang the active site, and experimental studies have shown that its dynamics affects the catalytic activity of mutant HIV-1 IN enzymes. In this study, the enhanced sampling technique, Reversible Digitally Filtered Molecular Dynamics (RDFMD), has been applied to the catalytic domain of the WT and G140A/ G149A HIV-1 IN enzymes and has highlighted significant differences between the behavior of the catalytic loop which may explain the decrease of activity observed in experimental studies for this mutant.
机译:HIV-1 IN酶是参与HIV-1病毒生命周期的三种关键的病毒编码酶(HIV-1 IN,HIV-1 PR和HIV-1 RT)之一,使其成为HIV-1的有吸引力的靶标。开发抗艾滋病病毒的药物。由于缺乏三维结构信息,HIV-1 IN酶的结构和机理在这三种酶中了解最少。 X射线膀胱造影研究尚未能够解决全长结构,并且研究主要集中在催化领域。这个中央结构域具有一个重要的催化环,可以看到该环突出于活性位点,并且实验研究表明,其动力学影响了突变型HIV-1 IN酶的催化活性。在这项研究中,增强的采样技术,可逆数字滤波分子动力学(RDFMD),已应用于WT和G140A / G149A HIV-1 IN酶的催化域,并突显了催化环行为之间的显着差异。可以解释在该突变体的实验研究中观察到的活性降低。

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