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首页> 外文期刊>Nature structural biology >STRUCTURE OF HIV-1 RT/TIBO R 86183 COMPLEX REVEALS SIMILARITY IN THE BINDING OF DIVERSE NONNUCLEOSIDE INHIBITORS
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STRUCTURE OF HIV-1 RT/TIBO R 86183 COMPLEX REVEALS SIMILARITY IN THE BINDING OF DIVERSE NONNUCLEOSIDE INHIBITORS

机译:HIV-1 RT / TIBO R 86183复杂揭示物在不同核苷抑制剂结合中的相似结构

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We report the structure of HIV-I reverse transcriptase (RT) complexed with the nonnucleoside inhibitor TIBO R 86183 at 3.0 Angstrom resolution. Comparing this structure with those of complexes of HIV-1 RT/alpha-APA R 95845 and HIV-1 RTevirapine provides a basis for understanding the nature of nonnucleoside inhibitor binding, the structure of the binding site and the interactions between the bound inhibitors and surrounding amino acid residues as well as for understanding mechanisms of inhibition by and resistance to nonnucleoside inhibitors. Ail three inhibitors considered assume a similar butterfly-like shape and bind to HIV-1 RT in a very similar way. important differences occur in the conformation of amino acid residues that form the binding pocket. [References: 33]
机译:我们报告了与非核苷抑制剂TIBO R 86183复合的HIV-1逆转录酶(RT)的结构,分辨率为3.0埃。将该结构与HIV-1 RT / alpha-APA R 95845和HIV-1 RT /奈韦拉平的复合物的结构进行比较,为理解非核苷抑制剂结合的性质,结合位点的结构以及结合的抑制剂之间的相互作用提供了基础和周围的氨基酸残基,以及用于理解非核苷抑制剂的抑制机制和耐药性。所考虑的所有三种抑制剂均呈现相似的蝴蝶状形状,并以非常相似的方式与HIV-1 RT结合。重要的差异发生在形成结合袋的氨基酸残基的构象上。 [参考:33]

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