| Literature DB >> 14578911 |
Daniel Lamarre1, Paul C Anderson, Murray Bailey, Pierre Beaulieu, Gordon Bolger, Pierre Bonneau, Michael Bös, Dale R Cameron, Mireille Cartier, Michael G Cordingley, Anne-Marie Faucher, Nathalie Goudreau, Stephen H Kawai, George Kukolj, Lisette Lagacé, Steven R LaPlante, Hans Narjes, Marc-André Poupart, Jean Rancourt, Roel E Sentjens, Roger St George, Bruno Simoneau, Gerhard Steinmann, Diane Thibeault, Youla S Tsantrizos, Steven M Weldon, Chan-Loi Yong, Montse Llinàs-Brunet.
Abstract
Hepatitis C virus (HCV) infection is a serious cause of chronic liver disease worldwide with more than 170 million infected individuals at risk of developing significant morbidity and mortality. Current interferon-based therapies are suboptimal especially in patients infected with HCV genotype 1, and they are poorly tolerated, highlighting the unmet medical need for new therapeutics. The HCV-encoded NS3 protease is essential for viral replication and has long been considered an attractive target for therapeutic intervention in HCV-infected patients. Here we identify a class of specific and potent NS3 protease inhibitors and report the evaluation of BILN 2061, a small molecule inhibitor biologically available through oral ingestion and the first of its class in human trials. Administration of BILN 2061 to patients infected with HCV genotype 1 for 2 days resulted in an impressive reduction of HCV RNA plasma levels, and established proof-of-concept in humans for an HCV NS3 protease inhibitor. Our results further illustrate the potential of the viral-enzyme-targeted drug discovery approach for the development of new HCV therapeutics.Entities:
Mesh:
Substances:
Year: 2003 PMID: 14578911 DOI: 10.1038/nature02099
Source DB: PubMed Journal: Nature ISSN: 0028-0836 Impact factor: 49.962