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Synthesis and biological activity of quinolinone and dihydroquinolinone p38 MAP kinase inhibitors
Authors:Chen Meng-Hsin  Fitzgerald Patricia  Singh Suresh B  O'Neill Edward A  Schwartz Cheryl D  Thompson Chris M  O'Keefe Stephen J  Zaller Dennis M  Doherty James B
Affiliation:Department of Medicinal Chemistry, Merck Research Laboratories, PO Box 2000, Rahway, NJ 07065, USA. meng_hsin_chen@merck.com
Abstract:Synthesis and biological activities of some quinolinone and dihydroquinolinone p38 MAP kinase inhibitors are reported. Modifications to the dihydroquinolinone pharmacophore revealed that dihydroquinolinone may be replaced with a quinolinone pharmacophore and lead to enhanced p38 inhibitory activity. From a study of C-7 substitutions by amino acid side chains, a very potent series of compounds in the p38 enzyme assays was identified. Translation of the in vitro activity into reasonable whole blood activity can be improved in this series of compounds by judicious modification of the physical properties at appropriate regions of the lead.
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