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效应激酶偶联可实现对具有抗逆转录病毒活性的直接HIV-1 Nef拮抗剂的高通量筛选。

Effector kinase coupling enables high-throughput screens for direct HIV-1 Nef antagonists with antiretroviral activity.

作者信息

Emert-Sedlak Lori A, Narute Purushottam, Shu Sherry T, Poe Jerrod A, Shi Haibin, Yanamala Naveena, Alvarado John Jeff, Lazo John S, Yeh Joanne I, Johnston Paul A, Smithgall Thomas E

机构信息

Department of Microbiology and Molecular Genetics, University of Pittsburgh School of Medicine, Pittsburgh, PA 15219, USA.

出版信息

Chem Biol. 2013 Jan 24;20(1):82-91. doi: 10.1016/j.chembiol.2012.11.005.

DOI:10.1016/j.chembiol.2012.11.005
PMID:23352142
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3559019/
Abstract

HIV-1 Nef, a critical AIDS progression factor, represents an important target protein for antiretroviral drug discovery. Because Nef lacks intrinsic enzymatic activity, we developed an assay that couples Nef to the activation of Hck, a Src family member and Nef effector protein. Using this assay, we screened a large, diverse chemical library and identified small molecules that block Nef-dependent Hck activity with low micromolar potency. Of these, a diphenylpyrazolo compound demonstrated submicromolar potency in HIV-1 replication assays against a broad range of primary Nef variants. This compound binds directly to Nef via a pocket formed by the Nef dimerization interface and disrupts Nef dimerization in cells. Coupling of nonenzymatic viral accessory factors to host cell effector proteins amenable to high-throughput screening may represent a general strategy for the discovery of new antimicrobial agents.

摘要

HIV-1 Nef是一种关键的艾滋病进展因子,是抗逆转录病毒药物研发的重要靶蛋白。由于Nef缺乏内在酶活性,我们开发了一种检测方法,将Nef与Hck(一种Src家族成员和Nef效应蛋白)的激活偶联起来。利用该检测方法,我们筛选了一个大型多样的化学文库,并鉴定出了能够以低微摩尔效力阻断Nef依赖性Hck活性的小分子。其中,一种二苯基吡唑化合物在针对多种原发性Nef变体的HIV-1复制检测中表现出亚微摩尔效力。该化合物通过由Nef二聚化界面形成的口袋直接与Nef结合,并破坏细胞中的Nef二聚化。将非酶促病毒辅助因子与适合高通量筛选的宿主细胞效应蛋白偶联起来,可能是发现新型抗菌剂的一种通用策略。

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本文引用的文献

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Nef alleles from all major HIV-1 clades activate Src-family kinases and enhance HIV-1 replication in an inhibitor-sensitive manner.
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