Author/Authors :
Yonghong Song، نويسنده , , Lane Clizbe، نويسنده , , Chhaya Bhakta، نويسنده , , Willy Teng، نويسنده , , Eric Dumbaugh & Wenhao Li، نويسنده , , Paul Wong، نويسنده , , Brian Huang، نويسنده , , Uma Sinha، نويسنده , , Gary Park، نويسنده , , Andrea Reed، نويسنده , , Robert M. Scarborough، نويسنده , , Bing-Yan Zhu، نويسنده ,
Abstract :
To overcome the low bioavailability of our substituted acrylamide P1 benzamidine factor Xa inhibitors reported previously, neutral and less basic groups were used to replace the benzamidine. As a result, a series of P1 aminoisoquinoline substituted acrylamide Xa inhibitors was identified to be potent, selective, and orally bioavailable. Modification of P4 moiety of these compounds further improved their pharmacokinetic properties.
