| Literature DB >> 16302794 |
James T Palmer1, Clifford Bryant, Dan-Xiong Wang, Dana E Davis, Eduardo L Setti, Robert M Rydzewski, Shankar Venkatraman, Zong-Qiang Tian, Leland C Burrill, Rohan V Mendonca, Eric Springman, John McCarter, Tobee Chung, Harry Cheung, James W Janc, Mary McGrath, John R Somoza, Philip Enriquez, Z Walter Yu, Robert M Strickley, Liang Liu, Michael C Venuti, M David Percival, Jean-Pierre Falgueyret, Peppi Prasit, Renata Oballa, Denis Riendeau, Robert N Young, Gregg Wesolowski, Sevgi B Rodan, Colena Johnson, Donald B Kimmel, Gideon Rodan.
Abstract
We have prepared a series of achiral aminoacetonitriles, bearing tri-ring benzamide moieties and an aminocyclohexanecarboxylate residue at P2. This combination of binding elements resulted in sub-250 pM, reversible, selective, and orally bioavailable cathepsin K inhibitors. Lead compounds displayed single digit nanomolar inhibition in vitro (of rabbit osteoclast-mediated degradation of bovine bone). The best compound in this series, 39n (CRA-013783/L-006235), was orally bioavailable in rats, with a terminal half-life of over 3 h. 39n was dosed orally in ovariectomized rhesus monkeys once per day for 7 days. Collagen breakdown products were reduced by up to 76% dose-dependently. Plasma concentrations of 39n above the bone resorption IC50 after 24 h indicated a correlation between functional cellular and in vivo assays. Inhibition of collagen breakdown by cathepsin K inhibitors suggests this mechanism of action may be useful in osteoporosis and other indications involving bone resorption.Entities:
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Year: 2005 PMID: 16302794 DOI: 10.1021/jm058198r
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446