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3-(7-Azaindolyl)-4-arylmaleimides as potent, selective inhibitors of glycogen synthase kinase-3 |
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| Authors: | Zhang Han-Cheng Ye Hong Conway Bruce R Derian Claudia K Addo Michael F Kuo Gee-Hong Hecker Leonard R Croll Diane R Li Jian Westover Lori Xu Jun Z Look Richard Demarest Keith T Andrade-Gordon Patricia Damiano Bruce P Maryanoff Bruce E |
| Affiliation: | Drug Discovery, Johnson & Johnson Pharmaceutical Research & Development, Spring House, PA 19477-0776, USA. hzhang@prdus.jnj.com |
| Abstract: | A novel series of acyclic 3-(7-azaindolyl)-4-(aryl/heteroaryl)maleimides was synthesized and evaluated for activity against GSK-3beta and selectivity versus PKC-betaII, as well as a broad panel of protein kinases. Compounds 14 and 17c potently inhibited GSK-3beta (IC(50)=7 and 26 nM, respectively) and exhibited excellent selectivity over PKC-betaII (325 and >385-fold, respectively). Compound 17c was also highly selective against 68 other protein kinases. In a cell-based functional assay, both 14 and 17c effectively increased glycogen synthase activity by inhibiting GSK-3beta. |
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