| Literature DB >> 21937229 |
Ruben A Tommasi1, Sven Weiler, Leslie W McQuire, Olivier Rogel, Mark Chambers, Kirk Clark, John Doughty, James Fang, Vishwas Ganu, Jonathan Grob, Ronald Goldberg, Robert Goldstein, Stacey Lavoie, Raviraj Kulathila, William Macchia, Richard Melton, Clayton Springer, Marc Walker, Jing Zhang, Lijuan Zhu, Michael Shultz.
Abstract
The matrix metalloproteinase enzyme MMP-13 plays a key role in the degradation of type II collagen in cartilage and bone in osteoarthritis (OA). An effective MMP-13 inhibitor would provide a disease modifying therapy for the treatment of arthritis, although this goal still continues to elude the pharmaceutical industry due to issues with safety. Our efforts have resulted in the discovery of a series of hydroxamic acid inhibitors of MMP-13 that do not significantly inhibit MMP-2 (gelatinase-1). MMP-2 has been implicated in the musculoskeletal side effects resulting from pan-MMP inhibition due to findings from spontaneously occurring human MMP-2 deletions. Analysis of the SAR of hundreds of previously prepared hydroxamate based MMP inhibitors lead us to 2-naphthylsulfonamide substituted hydroxamates which exhibited modest selectivity for MMP-13 versus MMP-2. This Letter describes the lead optimization of 1 and identification of inhibitors exhibiting >100-fold selectivity for MMP-13 over MMP-2.Entities:
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Year: 2011 PMID: 21937229 DOI: 10.1016/j.bmcl.2011.08.087
Source DB: PubMed Journal: Bioorg Med Chem Lett ISSN: 0960-894X Impact factor: 2.823