Martin Trudeau
Vertex Pharmaceuticals
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Publication
Featured researches published by Martin Trudeau.
Journal of Medicinal Chemistry | 2008
Paul S. Charifson; Anne-Laure Grillot; Trudy H. Grossman; Jonathan D. Parsons; Michael Badia; Steve Bellon; David D. Deininger; Joseph Drumm; Christian H. Gross; Arnaud Letiran; Yusheng Liao; Nagraj Mani; David P. Nicolau; Emanuele Perola; Steven Ronkin; Dean Shannon; Lora Swenson; Qing Tang; Pamela R. Tessier; Ski-Kai Tian; Martin Trudeau; Tiansheng Wang; Yunyi Wei; Hong Zhang; Dean Stamos
The discovery of new antibacterial agents with novel mechanisms of action is necessary to overcome the problem of bacterial resistance that affects all currently used classes of antibiotics. Bacterial DNA gyrase and topoisomerase IV are well-characterized clinically validated targets of the fluoroquinolone antibiotics which exert their antibacterial activity through inhibition of the catalytic subunits. Inhibition of these targets through interaction with their ATP sites has been less clinically successful. The discovery and characterization of a new class of low molecular weight, synthetic inhibitors of gyrase and topoisomerase IV that bind to the ATP sites are presented. The benzimidazole ureas are dual targeting inhibitors of both enzymes and possess potent antibacterial activity against a wide spectrum of relevant pathogens responsible for hospital- and community-acquired infections. The discovery and optimization of this novel class of antibacterials by the use of structure-guided design, modeling, and structure-activity relationships are described. Data are presented for enzyme inhibition, antibacterial activity, and in vivo efficacy by oral and intravenous administration in two rodent infection models.
Bioorganic & Medicinal Chemistry Letters | 2010
Steven Ronkin; Michael C. Badia; Steve Bellon; Anne-Laure Grillot; Christian H. Gross; Trudy H. Grossman; Nagraj Mani; Jonathan D. Parsons; Dean Stamos; Martin Trudeau; Yunyi Wei; Paul S. Charifson
Bacterial DNA gyrase is an attractive target for the investigation of new antibacterial agents. Inhibitors of the GyrB subunit, which contains the ATP-binding site, are described in this communication. Novel, substituted 5-(1H-pyrazol-3-yl)thiazole compounds were identified as inhibitors of bacterial gyrase. Structure-guided optimization led to greater enzymatic potency and moderate antibacterial potency. Data are presented for the demonstration of selective enzyme inhibition of Escherichia coli GyrB over Staphylococcus aureus GyrB.
Archive | 2012
Patricia Hurter; William Rowe; Christopher Ryan Young; Adriana Costache; Patrick R. Connelly; Mariusz Krawiec; Yuchuan Gong; Yushi Feng; Martin Trudeau
Archive | 2001
Paul S. Charifson; Anne-Laure Grillot; Yusheng Liao; Dean Stamos; Martin Trudeau
Archive | 2005
Gerald J. Tanoury; Minzhang Chen; Andrew D. Jones; Philip L. Nyce; Martin Trudeau; David J. Guerin; John R. Snoonian
Archive | 2009
Michael Badia; Paul S. Charifson; Anne-Laure Grillot; Yusheng Liao; Dean Stamos; Martin Trudeau; グリロット アネラーレ; スタモス,ディーン; チャリフソン ポール; トルーデュー マーティン; バディア,マイケル; リアオ ユーシェン
Archive | 2006
Patricia Hurter; Yuchuan Gong; Christopher Ryan Young; Patrick R. Connelly; William Rowe; Adriana Costache; Mariusz Krawiec; Yushi Feng; Martin Trudeau
Archive | 2006
Patricia Hurter; Yuchuan Gong; Christopher Ryan Young; Patrick R. Connelly; William Rowe; Adriana Costache; Mariusz Krawiec; Yushi Feng; Martin Trudeau
Archive | 2005
Gerald J. Tanoury; Minzhang Chen; Andrew D. Jones; Philip L. Nyce; Martin Trudeau; David J. Guerin; John R. Snoonian
Archive | 2005
Gerald J. Tanoury; Minzhang Chen; Andrew D. Jones; Philip L. Nyce; Martin Trudeau; David J. Guerin; John R. Snoonian