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Literature DB >> 31179358

Novel inhibitors against wild-type and mutated HCV NS3 serine protease: an in silico study.

Ahmed A Ezat¹, Abdo A Elfiky¹, Wael M Elshemey¹, Noha A Saleh².

Abstract

In 2011, the FDA approved boceprevir as a hepatitis C virus (HCV) NS3 serine protease inhibitor. The sustained virological response rate for treatment with this approved compound is considerably low. Patients have not responded as much as expected to boceprevir therapy. In this in silico study, modified boceprevir compounds are suggested and tested on wild-type HCV NS3 protease and 19 mutated HCV NS3 proteases using molecular docking. Results reveal the superiority of two of the proposed modified compounds to boceprevir. One of which appears to be more potent than boceprevir itself concerning activity against wild-type NS3 and most of the examined mutated NS3 proteases.

Entities: Chemical Gene Species

Keywords: Boceprevir; Fluorinated sulfonamide; HCV; Molecular modeling; Mutated NS3 protease; Protein–ligand docking

Year: 2019 PMID： 31179358 PMCID： PMC6531565 DOI： 10.1007/s13337-019-00516-7

Source DB: PubMed Journal: Virusdisease ISSN： 2347-3584

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