Structure–activity relationships of anthranilamide-based factor Xa inhibitors containing piperidinone and pyridinone P4 moieties

James R. Corte,Tianan Fang,Donald J. P. Pinto,Wei Han,Zilun Hu,Xiang-Jun Jiang,Yun-Long Li,Jolicia F. Gauuan,Mark Hadden,Darren Orton,Alan R. Rendina,Joseph M. Luettgen,Pancras C. Wong,Kan He,Paul E. Morin,Chong-Hwan Chang,Daniel L. Cheney,Robert M. Knabb,Ruth R. Wexler,Patrick Y.S. Lam

Structure–activity relationships of anthranilamide-based factor Xa inhibitors containing piperidinone and pyridinone P4 moieties

2008

Abstract Introduction of the phenyl piperidinone and phenyl pyridinone P4 moieties in the anthranilamide scaffold led to potent, selective, and orally bioavailable inhibitors of factor Xa. Anthranilamide 28 displayed comparable efficacy to apixaban in the rabbit arteriovenous-shunt (AV) thrombosis model.

Keywords:

Enzyme
Factor Xa Inhibitor
Carboxamide
Molecular model
Enzyme inhibitor
Structure–activity relationship
Stereochemistry
Biochemistry
Hydrolase
Lactam
Chemistry
benzene derivatives

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