
pmid: 10425183
Vpr, an accessory gene product of HIV-1 which induces cell cycle abnormality leading to the increased HIV replication, is supposed to be a possible target for anti-AIDS drugs. We recently established a cell line (MIT-23) in which Vpr-induced cell cycle perturbation could be manipulated by a tetracycline promoter. Here, we screened anti-Vpr activity in 27 kinds of herb drugs using MIT-23 cells. One of the extracts prepared from Houttuyniae herba showed an inhibitory activity. Quercetin (QCT), a compound of this crude drug, efficiently inhibited Vpr function without affecting its expression. Furthermore, data suggested that Vpr-induced transcription from HIV-LTR was considerably abrogated by QCT. These data indicate that QCT, a flavonoid previously reported to inhibit HIV replication, also targets Vpr, implicating that MIT-23 cell provides a novel strategy for screening compounds possessing anti-Vpr activity which would be in turn utilized for clarifying the mechanism of Vpr function.
Anti-HIV Agents, Gene Products, vpr, Genes, vpr, Cell Cycle, Drug Evaluation, Preclinical, Gene Expression, vpr Gene Products, Human Immunodeficiency Virus, Cell Line, Mifepristone, Hormone Antagonists, HIV-1, Humans, Quercetin, Promoter Regions, Genetic, HIV Long Terminal Repeat, Phytotherapy
Anti-HIV Agents, Gene Products, vpr, Genes, vpr, Cell Cycle, Drug Evaluation, Preclinical, Gene Expression, vpr Gene Products, Human Immunodeficiency Virus, Cell Line, Mifepristone, Hormone Antagonists, HIV-1, Humans, Quercetin, Promoter Regions, Genetic, HIV Long Terminal Repeat, Phytotherapy
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