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Chemical Library Screens Targeting an HIV-1 Accessory factor/Host Cell Kinase Complex Identify Novel Antiretroviral Compounds

机译:针对HIV-1辅助因子/宿主细胞激酶复合物的化学文库筛选确定了新型抗逆转录病毒化合物

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摘要

Nef is an HIV-1 accessory protein essential for AIDS progression and an attractive target for drug discovery. Lack of a catalytic function makes Nef difficult to assay in chemical library screens. We developed a high-throughput screening assay for Inhibitors of Nef function by coupling it to one of its host cell binding partners; the Src-family kinase Hck. Hck activation is dependent upon Nef in this assay, providing a direct readout of Nef activity in vitro. Using this screen; a unique diphenylfuropyrimidine was identified as a strong inhibitor of Nef-dependent Hck activation. This compound also exhibited remarkable antiretroviral effects, blocking Nef-dependent HIV replication in cell culture. Structurally related analogs were synthesized and shown to exhibit similar Nef-dependent antiviral activity, identifying the diphenylfuropyrimidine substructure as a new lead for antiretroviral drug development. This study demonstrates that coupling noncatalytic HIV accessory factors with host cell target proteins addressable by high-throughput assays may afford new avenues for the discovery of anti-HIV agents.
机译:Nef是艾滋病发展所必需的HIV-1辅助蛋白,也是药物发现的诱人靶标。缺乏催化功能使Nef难以在化学文库筛选中进行分析。通过将Nef功能抑制剂与其宿主细胞结合伴侣之一偶联,我们开发了一种Nef功能抑制剂的高通量筛选方法; Src家族激酶Hck。在此测定中,Hck激活依赖于Nef,可在体外直接读出Nef活性。使用此屏幕;独特的二苯基呋喃嘧啶被鉴定为Nef依赖性Hck激活的强抑制剂。该化合物还表现出显着的抗逆转录病毒作用,阻止了细胞培养中Nef依赖的HIV复制。合成了结构相关的类似物,并显示出类似的Nef依赖性抗病毒活性,从而确定了二苯基呋喃基嘧啶的亚结构是抗逆转录病毒药物开发的新先导。这项研究表明,通过高通量检测可将非催化性HIV辅助因子与宿主细胞靶蛋白偶联,可为发现抗HIV药物提供新途径。

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