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Design and synthesis of factor Xa inhibitors and their prodrugs
Authors:Song Yonghong  Clizbe Lane  Bhakta Chhaya  Teng Willy  Wong Paul  Huang Brian  Tran Katherine  Sinha Uma  Park Gary  Reed Andrea  Scarborough Robert M  Zhu Bing Yan
Institution:Department of Medicinal Chemistry, Millennium Pharmaceuticals, Inc., 256 East Grand Ave., South, San Francisco, CA 94080, USA. song@mpi.com
Abstract:In addition to our previously reported fluoro acrylamides Xa inhibitors 2 and 3, a series of potent and novel cyclic diimide amidine compounds has been identified. In efforts to improve their oral bioavailability, replacement of the amidine group with methyl amidrazone gives compounds of moderate potency (14, IC(50)=0.028 microM). In the amidoxime prodrug approach, the amidoxime compounds show good oral bioavailability in rats and dogs. High plasma level of prodrug 26 and significant concentration of active drug 26a were obtained upon oral administration of prodrug 26 in rats.
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