5-Heteroatom substituted pyrazoles as canine COX-2 inhibitors. Part 1: Structure-activity relationship studies of 5-alkylamino pyrazoles and discovery of a potent, selective, and orally active analog

Subas M. Sakya,Kristin Lundy DeMello,Martha L. Minich,Bryson Rast,Andrei Shavnya,Robert J. Rafka,David A. Koss,Hengmiao Cheng,Jin Li,Burton H. Jaynes,Carl Bernard Ziegler,Donald W. Mann,Carol F. Petras,Scott B. Seibel,Annette M. Silvia,David M. George,Lisa A. Lund,Suzanne H. St. Denis,Anne Hickman,Michelle L. Haven,Michael P. Lynch

5-Heteroatom substituted pyrazoles as canine COX-2 inhibitors. Part 1: Structure-activity relationship studies of 5-alkylamino pyrazoles and discovery of a potent, selective, and orally active analog

2006

Abstract Structure–activity relationship (SAR) studies of the novel 2-[3-di and trifluoromethyl-5-alkylamino pyrazo-1-yl]-5-methanesulfonyl (SO 2 Me)/sulfamoyl (SO 2 NH 2 )-pyridine derivatives for canine COX enzymes are described. The studies led to the identification of 2e as lead with potent in vitro activity, selectivity, and in vivo activity in dogs and cats.

Keywords:

Enzyme
In vivo
Organic chemistry
Biochemistry
Chemical synthesis
Structure–activity relationship
Stereochemistry
In vitro
COX-2 inhibitor
Sulfone
Chemistry
Enzyme inhibitor
Heteroatom

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