| Literature DB >> 16870455 |
Donnette D Staas1, Kelly L Savage, Vanessa L Sherman, Heidi L Shimp, Terry A Lyle, Lekhanh O Tran, Catherine M Wiscount, Daniel R McMasters, Philip E J Sanderson, Peter D Williams, Bobby J Lucas, Julie A Krueger, S Dale Lewis, Rebecca B White, Sean Yu, Bradley K Wong, Christopher J Kochansky, M Reza Anari, Youwei Yan, Joseph P Vacca.
Abstract
Previous reports from our laboratories described potent tripeptide thrombin inhibitors which incorporate heterocycle-substituted chlorophenyl groups in the P1 position. Using these as lead compounds for further optimization, we identified sites of metabolism and designed analogs with 4-fluoroproline in P2 and cyclopropane-containing side chains in P3 as an approach to reducing metabolism and improving their oral pharmacokinetic performance. The large (300-fold) difference in potency between analogs containing (4R)- and (4S)-4-fluoroproline was rationalized by analyzing inhibitor-enzyme interactions in crystal structures of related compounds and by molecular modeling which indicated that the more potent (4R)-4-fluoroproline isomer stabilizes a proline ring conformation that is preferred for binding to the enzyme. An optimal compound from this work, 41, exhibits high potency in a coagulation assay in human plasma (2xAPTT=190 nM), excellent selectivity versus the digestive enzyme trypsin (K(i)=3300 nM), and excellent oral bioavailability in dogs with moderate clearance (F=100%, CL=12 mL/min/kg).Entities:
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Year: 2006 PMID: 16870455 DOI: 10.1016/j.bmc.2006.06.040
Source DB: PubMed Journal: Bioorg Med Chem ISSN: 0968-0896 Impact factor: 3.641