Author/Authors :
Valentine J. Klimkowski، نويسنده , , Brian M. Watson، نويسنده , , Michael R. Wiley، نويسنده , , John Liebeschuetz، نويسنده , , Jeffry B. Franciskovich، نويسنده , , Jothirajah Marimuthu، نويسنده , , Jolie A. Bastian، نويسنده , , Daniel J. Sall، نويسنده , , Jeffrey K. Smallwood، نويسنده , , Nikolay Y. Chirgadze، نويسنده , , Gerald F. Smith، نويسنده , , Ronald S. Foster، نويسنده , , Trelia Craft، نويسنده , , Philip Sipes، نويسنده , , Marcia Chastain، نويسنده , , Scott M. Sheehan، نويسنده ,
Abstract :
Analogs to a series of d-phenylglycinamide-derived factor Xa inhibitors were discovered. It was found that the S4 amide linkage can be replaced with an ether linkage to reduce the peptide character of the molecules and that this substitution leads to an increase in binding affinity that is not predicted based on modeling. Inhibitors which incorporate ether, amino, or alkyl S4 linkage motifs exhibit similar levels of binding affinity and also demonstrate potent in vitro functional activity, however, binding affinity in this series is strongly dependent on the nature of the S1 binding element.
Keywords :
Non-covalent inhibitors , Serine protease inhibitors , Coagulation cascade , Factor Xa
