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首页> 外文期刊>Organic & biomolecular chemistry >Three-dimensional structure of HIV-1 VIF constructed by comparative modeling and the function characterization analyzed by molecular dynamics simulation
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Three-dimensional structure of HIV-1 VIF constructed by comparative modeling and the function characterization analyzed by molecular dynamics simulation

机译:通过比较建模构建HIV-1 VIF的三维结构,并通过分子动力学模拟分析功能表征

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摘要

VIF is one of the six accessory proteins of HIV-1. It has been shown to be necessary for the survival of HIV-1 in the human body and for the retention of viral infectivity. It is strongly expected that a new therapeutic strategy against HIV-1 infection could be realized by blocking the biological pathway to VIF. In this paper, a three-dimensional model of VIF was constructed by comparative modeling based on two templates, VHL and NarL, which were used to construct the C-terminal domain and N-terminal domain of VIF, respectively. A model of the VIF-ElonginB-ElonginC complex was constructed, and molecular dynamics simulations were used to investigate the interactions between VIF and ElonginB-ElonginC. Mutagenesis was used to identify the function of some conserved residues in the putative SOCS-box. The results showed that the mutations of the critical residues led to the disruption of the interactions between VIF and ElonginB-ElonginC, consistent with experimental observations. These novel models of VIF and its complex has therefore provided structural information for investigating the function of VIF at the molecular level.
机译:VIF是HIV-1的六种辅助蛋白之一。已经证明它对于人体中HIV-1的存活和病毒感染力的保持是必需的。强烈期望可以通过阻断VIF的生物学途径来实现针对HIV-1感染的新治疗策略。本文通过基于两个模板VHL和NarL的比较建模,构建了VIF三维模型,分别用于构建VIF的C端结构域和N端结构域。建立了VIF-ElonginB-ElonginC复合物的模型,并使用分子动力学模拟研究了VIF和ElonginB-ElonginC之间的相互作用。诱变被用来鉴定推定的SOCS-box中一些保守残基的功能。结果表明,关键残基的突变导致VIF和ElonginB-ElonginC之间相互作用的破坏,与实验观察一致。因此,这些新颖的VIF模型及其复合物为研究VIF在分子水平上的功能提供了结构信息。

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