| Literature DB >> 23083119 |
Rajâa Boulahjar1, Aziz Ouach, Chiurato Matteo, Stephane Bourg, Myriam Ravache, Rémy le Guével, Séverine Marionneau, Thibauld Oullier, Olivier Lozach, Laurent Meijer, Christiane Guguen-Guillouzo, Saïd Lazar, Mohamed Akssira, Yves Troin, Gérald Guillaumet, Sylvain Routier.
Abstract
The development of CDK and GSK3 inhibitors has been regarded as a potential therapeutic approach, and a substantial number of diverse structures have been reported to inhibit CDKs and GSK-3β in recent years. Only a few molecules have gone through or are currently undergoing clinical trials as CDK and GSK inhibitors. In this paper, we prepared valmerins, a new family containing the tetrahydropyrido[1,2-a]isoindone core. The fused heterocycle was prepared with a straightforward synthesis that was functionalized by a (het)arylurea. Twelve valmerins inhibited the CDK5 and GSK3 with an IC(50) < 100 nM. A semiquantitative kinase scoring was realized, and a cellular screening was done. At the end of our study, we investigated the in vivo potency of one valmerin. Mice exhibited good tolerance to our lead, which proved its efficacy and clearly blocked tumor growth. Valmerins appear also as good candidates for further development as anticancer agents.Entities:
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Year: 2012 PMID: 23083119 DOI: 10.1021/jm3008536
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446