| Literature DB >> 20715823 |
Montse Llinàs-Brunet1, Murray D Bailey, Nathalie Goudreau, Punit K Bhardwaj, Josée Bordeleau, Michael Bös, Yves Bousquet, Michael G Cordingley, Jiamin Duan, Pat Forgione, Michel Garneau, Elise Ghiro, Vida Gorys, Sylvie Goulet, Ted Halmos, Stephen H Kawai, Julie Naud, Marc-André Poupart, Peter W White.
Abstract
C-Terminal carboxylic acid containing inhibitors of the NS3 protease are reported. A novel series of linear tripeptide inhibitors that are very potent and selective against the NS3 protease are described. A substantial contribution to the potency of these linear inhibitors arises from the introduction of a C8 substituent on the B-ring of the quinoline moiety found on the P2 of these inhibitors. The introduction of a C8 methyl group results not only in a modest increase in the cell-based potency of these inhibitors but more importantly in a much better pharmacokinetic profile in rats as well. Exploration of C8-substitutions led to the identification of the bromo derivative as the best group at this position, resulting in a significant increase in the cell-based potency of this class of inhibitors. Structure-activity studies on the C8-bromo derivatives ultimately led to the discovery of clinical candidate 29 (BI 201335), a very potent and selective inhibitor of genotype1 NS3 protease with a promising PK profile in rats.Entities:
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Year: 2010 PMID: 20715823 DOI: 10.1021/jm100690x
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446