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

  作者 EMERTSEDLAK LORI; KODAMA TOSHIAKI; LERNER EDWINA C; DAI WEIXIANG; FOSTER CALEB; DAY BILLY W; LAZO JOHN S; SMITHGALL THOMAS E  
  选自 期刊  ACS CHEMICAL BIOLOGY;  卷期  2009年4-11;  页码  939-947  
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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.

 
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