Azepanone-Based Inhibitors of Human and Rat Cathepsin K

Robert W. Marquis , Yu Ru , Steven M. LoCastro , Robert W. Marquis , Yu Ru , Steven M. LoCastro , Jin Zeng , Dennis S. Yamashita , Hye-Ja Oh , Karl F. Erhard , Larry D. Davis , Thaddeus A. Tomaszek , David G. Tew , Kevin L. Salyers , Joel W. Proksch , Keith W. Ward , Brian R. Smith , Mark A. Levy , Maxwell D. Cummings , R. Curtis Haltiwanger , Gudrun Trescher , Bing Wang , Mark E. Hemling , Chad Quinn , H-Y. Cheng , Fan Lin , Ward W. Smith , Cheryl A. Janson , Baoguang Zhao , Michael S. McQueney , Karla D'Alessio , Chao‐Pin Lee , Antonia Marzulli , Robert A. Dodds , Simon Blake , Shing‐Mei Hwang , Ian E. James , Catherine J. Gress , Brian R. Bradley , Michael W. Lark , Maxine Gowen , Daniel F. Veber
2001 Journal of Medicinal Chemistry 102 citations

Abstract

The synthesis, in vitro activities, and pharmacokinetics of a series of azepanone-based inhibitors of the cysteine protease cathepsin K (EC 3.4.22.38) are described. These compounds show improved configurational stability of the C-4 diastereomeric center relative to the previously published five- and six-membered ring ketone-based inhibitor series. Studies in this series have led to the identification of 20, a potent, selective inhibitor of human cathepsin K (K(i) = 0.16 nM) as well as 24, a potent inhibitor of both human (K(i) = 0.0048 nM) and rat (K(i,app) = 4.8 nM) cathepsin K. Small-molecule X-ray crystallographic analysis of 20 established the C-4 S stereochemistry as being critical for potent inhibition and that unbound 20 adopted the expected equatorial conformation for the C-4 substituent. Molecular modeling studies predicted the higher energy axial orientation at C-4 of 20 when bound within the active site of cathepsin K, a feature subsequently confirmed by X-ray crystallography. Pharmacokinetic studies in the rat show 20 to be 42% orally bioavailable. Comparison of the transport of the cyclic and acyclic analogues through CaCo-2 cells suggests that oral bioavailability of the acyclic derivatives is limited by a P-glycoprotein-mediated efflux mechanism. It is concluded that the introduction of a conformational constraint has served the dual purpose of increasing inhibitor potency by locking in a bioactive conformation as well as locking out available conformations which may serve as substrates for enzyme systems that limit oral bioavailability.

Keywords

ChemistryStereochemistrySubstituentMolecular modelCathepsinBioavailabilityEnzyme inhibitorDiastereomerChemical synthesisEnzymeIn vitroBiochemistry

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Publication Info

Year
2001
Type
article
Volume
44
Issue
9
Pages
1380-1395
Citations
102
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Robert W. Marquis, Yu Ru, Steven M. LoCastro et al. (2001). Azepanone-Based Inhibitors of Human and Rat Cathepsin K. Journal of Medicinal Chemistry , 44 (9) , 1380-1395. https://doi.org/10.1021/jm000481x

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DOI
10.1021/jm000481x