化学
酰胺
凝血酶
直接凝血酶抑制剂的发现与发展
凝结
药理学
酶抑制剂
血栓
结构-活动关系
体外
胰蛋白酶
抗凝剂
抗凝血酶
效力
立体化学
生物化学
酶
肝素
内科学
血小板
医学
作者
William R. Ewing,Michael R. Becker,Vincent E. Manetta,Roderick S. Davis,Henry W. Pauls,Helen J. Mason,Yong Mi Choi-Sledeski,Daniel J. Green,Don Cha,Alfred P. Spada,Daniel L. Cheney,Jonathan Mason,S. Maignan,J.P. Guilloteau,Karen Brown,Dennis Colussi,Ross Bentley,Jeff Bostwick,Charles Kasiewski,Suzanne R. Morgan
摘要
The discovery of a series of non-peptide factor Xa (FXa) inhibitors incorporating 3-(S)-amino-2-pyrrolidinone as a central template is described. After identifying compound 4, improvements in in vitro potency involved modifications of the liphophilic group and optimizing the angle of presentation of the amidine group to the S1 pocket of FXa. These studies ultimately led to compound RPR120844, a potent inhibitor of FXa (K(i) = 7 nM) which shows selectivity for FXa over trypsin, thrombin, and several fibrinolytic serine proteinases. RPR120844 is an effective anticoagulant in both the rat model of FeCl(2)-induced carotid artery thrombosis and the rabbit model of jugular vein thrombus formation.
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