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Virtual screening based identification of novel small-molecule inhibitors targeted to the HIV-1 capsid.

机译:基于虚拟筛选的针对HIV-1衣壳的新型小分子抑制剂的鉴定。

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The hydrophobic cavity of the C-terminal domain (CTD) of HIV-1 capsid has been recently validated as potential target for antiviral drugs by peptide-based inhibitors; however, there is no report yet of any small molecule compounds that target this hydrophobic cavity. In order to fill this gap and discover new classes of ant-HIV-1 inhibitors, we undertook a docking-based virtual screening and subsequent analog search, and medicinal chemistry approaches to identify small molecule inhibitors against this target. This article reports for the first time, to the best of our knowledge, identification of diverse classes of inhibitors that efficiently inhibited the formation of mature-like viral particles verified under electron microscope (EM) and showed potential as anti-HIV-1 agents in a viral infectivity assay against a wide range of laboratory-adapted as well as primary isolates in MT-2 cells and PBMC. In addition, the virions produced after the HIV-1 infected cells were treated with two of the most active compounds showed drastically reduced infectivity confirming the potential of these compounds as anti-HIV-1 agents. We have derived a comprehensive SAR from the antiviral data. The SAR analyses will be useful in further optimizing the leads to potential anti-HIV-1 agents.
机译:HIV-1衣壳的C末端结构域(CTD)的疏水腔最近已被基于肽的抑制剂验证为抗病毒药物的潜在靶点;但是,尚无针对该疏水腔的小分子化合物的报道。为了填补这一空白并发现新型的ant-HIV-1抑制剂,我们进行了基于对接的虚拟筛选和后续类似物搜索,并采用了药物化学方法来识别针对此目标的小分子抑制剂。据我们所知,本文首次报道了鉴定各种抑制剂的方法,这些抑制剂可有效抑制电子显微镜(EM)验证的成熟样病毒颗粒的形成,并显示出作为抗HIV-1药物的潜力。针对MT-2细胞和PBMC中的各种实验室适应以及主要分离株的病毒感染性测定。此外,用两种最具活性的化合物处理HIV-1感染的细胞后产生的病毒体显示出大大降低的感染力,证实了这些化合物作为抗HIV-1药物的潜力。我们已经从抗病毒数据中得出了全面的SAR。 SAR分析将有助于进一步优化潜在的抗HIV-1药物的线索。

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