Synthesis and SAR of 4-carboxy-2-azetidinone mechanism-based tryptase inhibitors

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

Synthesis and SAR of 4-carboxy-2-azetidinone mechanism-based tryptase inhibitors

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.

Keywords:

Potency
Organic chemistry
Tryptase
Biochemistry
Enzyme
Serine protease
Chemistry
Structure–activity relationship
Chemical synthesis
In vitro
Enzyme inhibitor
In vivo

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