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Biased small-molecule ligands for selective inhibition of HIV-1 cell entry via CCR5.

Pharmacol Res Perspect. 2016-12; 
BergChristian,SpiessKatja,LüttichauHans R,RosenkildeMet
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Custom Vector Construction … cerevisiae. The GAL4‐VP16 gene was synthesized and cloned into the pUC57 vector by GenScript (Piscataway, NJ). The gene was then transferred into the pcDNA3.1(+) vector. The reading frame was confirmed by DNA sequencing … Get A Quote

摘要

Since the discovery of HIV's use of CCR5 as the primary coreceptor in fusion, the focus on developing small-molecule receptor for inhibition hereof has only resulted in one single drug, Maraviroc. We therefore investigated the possibility of using small-molecule CCR5 as HIV-1 fusion inhibitors. A virus-free cell-based fusion reporter assay, based on mixing "effector cells" (expressing HIV and luciferase activator) with "target cells" (expressing CD4, CCR5 wild type or a selection of well-described mutations, and luciferase reporter), was used as fusion readout. Receptor expression was evaluated by ELISA and fluorescence microscopy. On CCR5 WT, Maraviroc and Aplaviroc inhibited fusion with high ... More

关键词

CCR5,HIV‐1,drug development,efficacy switch,fusion,ligand bias,small‐molecule inhibi