| Literature DB >> 24462666 |
Jeffrey W Johannes1, Claudio Chuaqui2, Scott Cowen3, Erik Devereaux4, Lakshmaiah Gingipalli2, Audrey Molina5, Tao Wang6, David Whitston4, Xiaoyun Wu7, Hai-Jun Zhang8, Michael Zinda4.
Abstract
The discovery and optimization of a series of 6-aryl-azabenzimidazole inhibitors of TBK1 and IKK-ε is described. Various internal azabenzimidazole leads and reported TBK1/IKK-ε inhibitors were docked into a TBK1 homology model. The resulting overlays inspired a focused screen of 6-substituted azabenzimidazoles against TBK1/IKK-ε. This screen resulted in initial hit compound 3. The TBK1/IKK-ε enzyme and cell potency of this compound was further improved using structure guided drug design. Systematic exploration of the C6 aryl group led to compound 19, a potent inhibitor of TBK1 with selectivity against cell cycle kinases CDK2 and Aurora B. Further elaboration and optimization gave compound 25, a single digit nM inhibitor of TBK1. These compounds may serve as in vitro probes to evaluate TBK1/IKK-ε as an oncology target.Entities:
Keywords: Azabenzimidazole; IKK-ε; Kinase inhibitor; TBK1
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Year: 2014 PMID: 24462666 DOI: 10.1016/j.bmcl.2013.12.123
Source DB: PubMed Journal: Bioorg Med Chem Lett ISSN: 0960-894X Impact factor: 2.823