| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 1366718 | Bioorganic & Medicinal Chemistry Letters | 2007 | 4 Pages |
Abstract
A novel class of selective Tie-2 inhibitors was derived from a multi-kinase inhibitor 1. By reversing the amide connectivity and incorporating aminotriazine or aminopyridine hinge-binding moieties, excellent Tie-2 potency and KDR selectivity could be achieved with 3-substituted terminal aryl rings. X-ray co-crystal structure analysis aided inhibitor design. This series was evaluated on the basis of potency, selectivity, and rat pharmacokinetic parameters.
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Related Topics
Physical Sciences and Engineering
Chemistry
Organic Chemistry
Authors
Brian L. Hodous, Stephanie D. Geuns-Meyer, Paul E. Hughes, Brian K. Albrecht, Steve Bellon, Sean Caenepeel, Victor J. Cee, Stuart C. Chaffee, Maurice Emery, Jenne Fretland, Paul Gallant, Yan Gu, Rebecca E. Johnson, Joseph L. Kim, Alexander M. Long,