| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 1372960 | Bioorganic & Medicinal Chemistry Letters | 2011 | 7 Pages |
Abstract
A series of N-aryl pyridinone inhibitors of p38 mitogen activated protein (MAP) kinase were designed and prepared based on the screening hit SC-25028 (1) and structural comparisons to VX-745 (5). The focus of the investigation targeted the dependence of potency and metabolic stability on the benzyloxy connectivity, the role of the C-6 position and the substitution pattern on the N-phenyl ring. Further optimization produced the highly selective and potent pyridinones 2 and 3. These inhibitors exhibited activity in both acute and chronic models of inflammation.
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Related Topics
Physical Sciences and Engineering
Chemistry
Organic Chemistry
Authors
Shaun R. Selness, Terri L. Boehm, John K. Walker, Balekudru Devadas, Richard C. Durley, Ravi Kurumbail, Huey Shieh, Li Xing, Michael Hepperle, Paul V. Rucker, Kevin D. Jerome, Alan G. Benson, Laura D. Marrufo, Heather M. Madsen, Jeff Hitchcock,