| Literature DB >> 21341675 |
Jesús R Medina1, Christopher J Becker, Charles W Blackledge, Celine Duquenne, Yanhong Feng, Seth W Grant, Dirk Heerding, William H Li, William H Miller, Stuart P Romeril, Daryl Scherzer, Arthur Shu, Mark A Bobko, Antony R Chadderton, Melissa Dumble, Christine M Gardiner, Seth Gilbert, Qi Liu, Sridhar K Rabindran, Valery Sudakin, Hong Xiang, Pat G Brady, Nino Campobasso, Paris Ward, Jeffrey M Axten.
Abstract
Phosphoinositide-dependent protein kinase-1(PDK1) is a master regulator of the AGC family of kinases and an integral component of the PI3K/AKT/mTOR pathway. As this pathway is among the most commonly deregulated across all cancers, a selective inhibitor of PDK1 might have utility as an anticancer agent. Herein we describe our lead optimization of compound 1 toward highly potent and selective PDK1 inhibitors via a structure-based design strategy. The most potent and selective inhibitors demonstrated submicromolar activity as measured by inhibition of phosphorylation of PDK1 substrates as well as antiproliferative activity against a subset of AML cell lines. In addition, reduction of phosphorylation of PDK1 substrates was demonstrated in vivo in mice bearing OCl-AML2 xenografts. These observations demonstrate the utility of these molecules as tools to further delineate the biology of PDK1 and the potential pharmacological uses of a PDK1 inhibitor.Entities:
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Year: 2011 PMID: 21341675 DOI: 10.1021/jm101527u
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446