Uwe D. Treuner
Bristol-Myers Squibb
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Publication
Featured researches published by Uwe D. Treuner.
Bioorganic & Medicinal Chemistry Letters | 2002
James C. Sutton; Scott A. Bolton; Karen S. Hartl; Ming-Hsing Huang; Glenn Anthony Jacobs; Wei Meng; Martin L. Ogletree; Zulan Pi; William A. Schumacher; Steven M. Seiler; William A. Slusarchyk; Uwe D. Treuner; Robert Zahler; Guohua Zhao; Gregory S. Bisacchi
A series of N1-activated C4-carboxy azetidinones was prepared and tested as inhibitors of human tryptase. The key stereochemical and functional features required for potency, serine protease specificity and aqueous stability were determined. From these studies compound 2, BMS-262084, was identified as a potent and selective tryptase inhibitor which, when dosed intratracheally in ovalbumin-sensitized guinea pigs, reduced allergen-induced bronchoconstriction and inflammatory cell infiltration into the lung.
Bioorganic & Medicinal Chemistry Letters | 2002
William A. Slusarchyk; Scott A. Bolton; Karen S. Hartl; Ming-Hsing Huang; Glenn Anthony Jacobs; Wei Meng; Martin L. Ogletree; Zulan Pi; William A. Schumacher; Steven M. Seiler; James C. Sutton; Uwe D. Treuner; Robert Zahler; Guohua Zhao; Gregory S. Bisacchi
The serine protease tryptase has been implicated in allergic and inflammatory diseases and associated with asthma. The synthesis and SAR of a series of N1-activated-4-carboxy azetidinones are described, resulting in identification of BMS-363131 (2) as a potent inhibitor of human tryptase (IC(50)<1.7 nM) with high selectivity (>3000-fold) for tryptase versus related serine proteases including trypsin.
Bioorganic & Medicinal Chemistry Letters | 2013
Scott A. Bolton; James Sutton; Rushith Anumula; Gregory S. Bisacchi; Bruce L. Jacobson; William A. Slusarchyk; Uwe D. Treuner; Shung C. Wu; Guohua Zhao; Zulan Pi; Steven Sheriff; Rebecca A. Smirk; Sharon N. Bisaha; Daniel L. Cheney; Anzhi Wei; William A. Schumacher; Karen S. Hartl; Eddie C.-K. Liu; Robert Zahler; Steven M. Seiler
In this Letter, we describe the synthesis of several nonamidine analogs of biaryl acid factor VIIa inhibitor 1 containing weakly basic or nonbasic P1 groups. 2-Aminoisoquinoline was found to be an excellent surrogate for the benzamidine group (compound 2) wherein potent inhibition of factor VIIa is maintained relative to most other related serine proteases. In an unanticipated result, the m-benzamide P1 (compounds 21a and 21b) proved to be a viable benzamidine replacement, albeit with a 20-40 fold loss in potency against factor VIIa.
Official Gazette of the United States Patent and Trademark Office Patents | 2001
Gregory S. Bisacchi; James C. Sutton; William A. Slusarchyk; Uwe D. Treuner; Guohua Zhao; Daniel L. Cheney; Yan Shi; Shung C. Wu
Bioorganic & Medicinal Chemistry Letters | 2004
Gregory S. Bisacchi; William A. Slusarchyk; Scott A. Bolton; Karen S. Hartl; Glenn Anthony Jacobs; Arvind Mathur; Wei Meng; Martin L. Ogletree; Zulan Pi; James C. Sutton; Uwe D. Treuner; Robert Zahler; Guohua Zhao; Steven M. Seiler
Archive | 1999
Gregory S. Bisacchi; William A. Slusarchyk; Uwe D. Treuner; James C. Sutton; Robert Zahler; Steven M. Seiler; David R. Kronenthal; Michael E. Randazzo; Mark D. Schwinden; Zhongmin Xu; Zhongping Shi
Archive | 2004
Peter W. Glunz; Gregory S. Bisacchi; George C. Morton; Alexandra A. Holubec; E. Scott Priestley; Xiaojun Zhang; Uwe D. Treuner
Archive | 1986
Hermann Breuer; William Henry Koster; Uwe D. Treuner; Robert Zahler
Archive | 1987
Uwe D. Treuner; Theodor Denzel; Hermann Breuer
Archive | 2001
Gregory S. Bisacchi; James C. Sutton; William A. Slusarchyk; Uwe D. Treuner; Guohua Zhao; Daniel L. Cheney; Shung C. Wu; Yan Shi
