首页> 外文期刊>Journal of Computer-Aided Molecular Design >Source of oseltamivir resistance due to single E119D and double E119D/H274Y mutations in pdm09H1N1 influenza neuraminidase
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Source of oseltamivir resistance due to single E119D and double E119D/H274Y mutations in pdm09H1N1 influenza neuraminidase

机译:由于单一E119D和PDM09H1N1流感神经氨酸酶的单一E119D和Double E119D / H274Y突变引起的奥克拉米赖维尔抗性来源

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摘要

Influenza epidemics are responsible for an average of 3-5 millions of severe cases and up to 500,000 deaths around the world. One of flu pandemic types is influenza A(H1N1)pdm09 virus (pdm09H1N1). Oseltamivir is the antiviral drug used to treat influenza targeting at neuraminidase (NA) located on the viral surface. Influenza virus undergoes high mutation rates and leads to drug resistance, and thus the development of more efficient drugs is required. In the present study, all-atom molecular dynamics simulations were applied to understand the oseltamivir resistance caused by the single E119D and double E119D/H274Y mutations on NA. The obtained results in terms of binding free energy and intermolecular interactions in the ligand-protein interface showed that the oseltamivir could not be well accommodated in the binding pocket of both NA mutants and the 150-loop moves out from oseltamivir as an "open" state. A greater number of water molecules accessible to the binding pocket could disrupt the oseltamivir binding with NA target as seen be high mobility of oseltamivir at the active site. Additionally, our finding could guide to the design and development of novel NA inhibitor drugs.
机译:流感流行病人平均负责3-5万严重案件,全球最多可达500,000人死亡。流感大流行类型之一是流感A(H1N1)PDM09病毒(PDM09H1N1)。 Oseltamivir是用于治疗位于病毒表面上的神经氨酸酶(NA)的抗病毒药物。流感病毒经历高突变率并导致耐药性,因此需要更有效的药物的发展。在本研究中,应用全原子分子动力学模拟,以了解由单一E119D和NA上的双E119D / H274Y突变引起的Oseltamivir抗性。在配体 - 蛋白质界面的结合可自由能和分子间相互作用方面获得的结果表明,奥司他虫虫不能充分容纳在纳米突变体的结合口袋中,并且150环从Oseltamivir移出,作为“开放”状态。粘合口袋可获得更多的水分子可以破坏与Na靶标的奥司他韦结合,如活性位点在活性位点的高迁移率。此外,我们的发现可以指导新的Na抑制剂药物的设计和开发。

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