Discovery of a Potent and Selective Noncovalent Linear Inhibitor of the Hepatitis C Virus NS3 Protease (BI 201335)

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 introducti...

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Veröffentlicht in:	Journal of medicinal chemistry 2010-09, Vol.53 (17), p.6466-6476
Hauptverfasser:	Llinàs-Brunet, Montse, Bailey, Murray D, Goudreau, Nathalie, Bhardwaj, Punit K, Bordeleau, Josée, Bös, Michael, Bousquet, Yves, Cordingley, Michael G, Duan, Jiamin, Forgione, Pat, Garneau, Michel, Ghiro, Elise, Gorys, Vida, Goulet, Sylvie, Halmos, Ted, Kawai, Stephen H, Naud, Julie, Poupart, Marc-André, White, Peter W
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Sprache:	eng
Schlagworte:	Animals Antiviral Agents - chemical synthesis Antiviral Agents - pharmacokinetics Antiviral Agents - pharmacology Hepacivirus - enzymology Hepacivirus - genetics Humans Male Microsomes, Liver - metabolism Oligopeptides - chemical synthesis Oligopeptides - pharmacokinetics Oligopeptides - pharmacology Rats Rats, Sprague-Dawley Replicon - drug effects Serine Proteinase Inhibitors - chemical synthesis Serine Proteinase Inhibitors - pharmacokinetics Serine Proteinase Inhibitors - pharmacology Structure-Activity Relationship Thiazoles - chemical synthesis Thiazoles - pharmacokinetics Thiazoles - pharmacology Viral Nonstructural Proteins - antagonists & inhibitors
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creator	Llinàs-Brunet, Montse Bailey, Murray D Goudreau, Nathalie Bhardwaj, Punit K Bordeleau, Josée Bös, Michael Bousquet, Yves Cordingley, Michael G Duan, Jiamin Forgione, Pat Garneau, Michel Ghiro, Elise Gorys, Vida Goulet, Sylvie Halmos, Ted Kawai, Stephen H Naud, Julie Poupart, Marc-André White, Peter W
description	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.
doi_str_mv	10.1021/jm100690x
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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. 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Med. Chem</addtitle><description>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. 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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.</abstract><cop>United States</cop><pub>American Chemical Society</pub><pmid>20715823</pmid><doi>10.1021/jm100690x</doi><tpages>11</tpages></addata></record>
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subjects	Animals Antiviral Agents - chemical synthesis Antiviral Agents - pharmacokinetics Antiviral Agents - pharmacology Hepacivirus - enzymology Hepacivirus - genetics Humans Male Microsomes, Liver - metabolism Oligopeptides - chemical synthesis Oligopeptides - pharmacokinetics Oligopeptides - pharmacology Rats Rats, Sprague-Dawley Replicon - drug effects Serine Proteinase Inhibitors - chemical synthesis Serine Proteinase Inhibitors - pharmacokinetics Serine Proteinase Inhibitors - pharmacology Structure-Activity Relationship Thiazoles - chemical synthesis Thiazoles - pharmacokinetics Thiazoles - pharmacology Viral Nonstructural Proteins - antagonists & inhibitors
title	Discovery of a Potent and Selective Noncovalent Linear Inhibitor of the Hepatitis C Virus NS3 Protease (BI 201335)
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