PCAF公司
化学
前病毒
激活剂(遗传学)
HIV长末端重复序列
转录因子
辅活化剂
病毒复制
病毒学
细胞生物学
基因
病毒
长终端重复
生物
生物化学
基因表达
基因组
作者
Lei Zeng,Jiaming Li,Michaela Müller,S.X. Yan,Shiraz Mujtaba,Chongfeng Pan,Zhiyong Wang,Ming‐Ming Zhou
摘要
Development of drug resistance from mutations in the targeted viral proteins leads to continuation of viral production by chronically infected cells, contributing to HIV-mediated immune dysfunction. Targeting a host cell protein essential for viral reproduction, rather than a viral protein, may minimize the viral drug resistance problem as observed with HIV protease inhibitors. We report here the development of a novel class of N1-aryl-propane-1,3-diamine compounds using a structure-based approach that selectively inhibit the activity of the bromodomain of the human transcriptional co-activator PCAF, of which association with the HIV trans-activator Tat is essential for transcription and replication of the integrated HIV provirus.
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