| Literature DB >> 10715155 |
M R Wiley1, L C Weir, S Briggs, N A Bryan, J Buben, C Campbell, N Y Chirgadze, R C Conrad, T J Craft, J V Ficorilli, J B Franciskovich, L L Froelich, D S Gifford-Moore, T Goodson, D K Herron, V J Klimkowski, K D Kurz, J A Kyle, J J Masters, A M Ratz, G Milot, R T Shuman, T Smith, G F Smith, A L Tebbe, J M Tinsley.
Abstract
To enhance the potency of 1,2-dibenzamidobenzene-derived inhibitors of factor Xa (fXa), an amidine substituent was incorporated on one of the benzoyl side chains to interact with Asp189 in the S1 specificity pocket. Lead molecule 1 was docked into the active site of fXa to facilitate inhibitor design. Subsequently, iterative SAR studies and molecular modeling led to a 1000-fold increase in fXa affinity and a refined model of the new inhibitors in the fXa active site. Strong support for the computational model was achieved through the acquisition of an X-ray crystal structure using thrombin as a surrogate protein. The amidines in this series show high levels of selectivity for the inhibition of fXa relative to other trypsin-like serine proteases. Furthermore, the fXa affinity of compounds in this series (K(ass) = 50-500 x 10(6) L/mol) translates effectively into both anticoagulant activity in vitro and antithrombotic activity in vivo.Entities:
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Year: 2000 PMID: 10715155 DOI: 10.1021/jm9903287
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446