鉴定针对核衣壳蛋白的 HIV-1 抑制剂。
Identification of HIV-1 inhibitors targeting the nucleocapsid protein.
机构信息
Department of Molecular and Experimental Medicine, The Scripps Research Institute, 10550 North Torrey Pines Road, La Jolla, California 92037, United States.
出版信息
J Med Chem. 2012 Jun 14;55(11):4968-77. doi: 10.1021/jm201442t. Epub 2012 May 24.
Abstract
The HIV-1 nucleocapsid (NC) is a RNA/DNA binding protein encoded within the Gag polyprotein, which is critical for the selection and chaperoning of viral genomic RNA during virion assembly. RNA/DNA binding occurs through a highly conserved zinc-knuckle motif present in NC. Given the necessity of NC-viral RNA/DNA interaction for viral replication, identification of compounds that disrupt the NC-RNA/DNA interaction may have value as an antiviral strategy. To identify small molecules that disrupt NC-viral RNA/DNA binding, a high-throughput fluorescence polarization assay was developed and a library of 14,400 diverse, druglike compounds was screened. Compounds that disrupted NC binding to a fluorescence-labeled DNA tracer were next evaluated by differential scanning fluorimetry to identify compounds that must bind to NC or Gag to impart their effects. Two compounds were identified that inhibited NC-DNA interaction, specifically bound NC with nanomolar affinity, and showed modest anti-HIV-1 activity in ex vivo cell assays.
摘要
HIV-1 核衣壳(NC)是一种 RNA/DNA 结合蛋白,编码在 Gag 多聚蛋白内,对于病毒基因组 RNA 在病毒组装过程中的选择和伴侣作用至关重要。RNA/DNA 结合通过存在于 NC 中的高度保守的锌指模体发生。鉴于 NC-病毒 RNA/DNA 相互作用对于病毒复制的必要性,鉴定破坏 NC-RNA/DNA 相互作用的化合物可能作为一种抗病毒策略具有价值。为了鉴定破坏 NC-病毒 RNA/DNA 结合的小分子,开发了一种高通量荧光偏振测定法,并筛选了 14400 种不同的、类药性的化合物库。接下来,通过差示扫描荧光法评估破坏 NC 与荧光标记 DNA 示踪剂结合的化合物,以鉴定必须与 NC 或 Gag 结合才能发挥作用的化合物。鉴定出两种抑制 NC-DNA 相互作用的化合物,它们特异性地以纳摩尔亲和力结合 NC,并在体外细胞测定中显示出适度的抗 HIV-1 活性。
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