Peptide backbone replacement of hepatitis C virus NS3 serine protease C-terminal cleavage product analogs: Discovery of potent succinamide inhibitors |
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| Authors: | Murray D. Bailey Josée Bordeleau Michel Garneau Mélissa Leblanc Christopher T. Lemke Jeff O’Meara Peter W. White Montse Llinàs-Brunet |
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| Affiliation: | Boehringer Ingelheim (Canada) Ltd, Research and Development, 2100 Cunard Street, Laval, Quebec H7S 2G5, Canada |
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| Abstract: | A number of potent peptidic inhibitors of the NS3 protease have been described in the literature based on a substrate-based approach. In an on-going effort to reduce the peptidic character of this class of inhibitors, two novel series of analogs have been prepared in which the usual P3 amino acid residue is replaced by a succinamide fragment. This new backbone modification not only reduces the peptidic nature of traditional inhibitors but also provides new SAR opportunities for the capping group. Optimization of each of these two series resulted in inhibitors with sub-nanomolar potencies. |
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| Keywords: | Hepatitis C NS3 protease Peptide backbone replacement Succinamide Peptidomimetic |
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