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Literature DB >> 26332742

High-Throughput Screening, Discovery, and Optimization To Develop a Benzofuran Class of Hepatitis C Virus Inhibitors.

Shanshan He¹, Prashi Jain, Billy Lin¹, Marc Ferrer², Zongyi Hu¹, Noel Southall², Xin Hu², Wei Zheng², Benjamin Neuenswander, Chul-Hee Cho, Yu Chen, Shilpa A Worlikar, Jeffrey Aubé, Richard C Larock, Frank J Schoenen, Juan J Marugan², T Jake Liang¹, Kevin J Frankowski.

Abstract

Using a high-throughput, cell-based HCV luciferase reporter assay to screen a diverse small-molecule compound collection (∼ 300,000 compounds), we identified a benzofuran compound class of HCV inhibitors. The optimization of the benzofuran scaffold led to the identification of several exemplars with potent inhibition (EC50 < 100 nM) of HCV, low cytotoxicity (CC50 > 25 μM), and excellent selectivity (selective index = CC50/EC50, > 371-fold). The structure-activity studies culminated in the design and synthesis of a 45-compound library to comprehensively explore the anti-HCV activity. The identification, design, synthesis, and biological characterization for this benzofuran series is discussed.

Entities: CellLine Chemical Disease Gene Species

Keywords: HCV inhibitor; HCV replication; antiviral; benzofuran; hepatitis C

Mesh：

Substances：

Year: 2015 PMID： 26332742 PMCID： PMC6015500 DOI： 10.1021/acscombsci.5b00101

Source DB: PubMed Journal: ACS Comb Sci ISSN： 2156-8944 Impact factor: 3.784

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