Novel symmetrical phenylenediamines as potential anti-hepatitis C virus agents

Author:

Bassetto Marcella1,Ferla Salvatore1,Leyssen Pieter2,Neyts Johan2,Yerukhimovich Mark M3,Frick David N3,O’Donnell Rachel1,Brancale Andrea1

Affiliation:

1. Cardiff School of Pharmacy and Pharmaceutical Sciences, Cardiff, UK

2. Rega Institute for Medical Research, University of Leuven, Leuven, Belgium

3. Department of Chemistry and Biochemistry, University of Wisconsin-Milwaukee, Milwaukee, USA

Abstract

Background Despite the great progress made in the last 10 years, alternative strategies might help improving definitive treatment options against hepatitis C virus infection. Methods With the aim of identifying novel inhibitors of the hepatitis C virus-1b replication targeting the viral NS3 helicase, the structures of previously reported symmetrical inhibitors of this enzyme were rationally modified, and according to docking-based studies, four novel scaffolds were selected for synthesis and evaluation in the hepatitis C virus-1b subgenomic replicon assay. Results Among the newly designed compounds, one new structural family was found to inhibit the hepatitis C virus-1b replication in the micromolar range. This scaffold was chosen for further exploration and different novel analogues were synthesised and evaluated. Conclusions Different new inhibitors of the hepatitis C virus genotype 1b replication were identified. Some of the new compounds show mild inhibition of the NS3 helicase enzyme.

Publisher

SAGE Publications

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