Discovery of a potent and highly selective PDK1 inhibitor via fragment-based drug discovery

Article ID	Journal	Published Year	Pages	File Type
1361963	Bioorganic & Medicinal Chemistry Letters	2011	6 Pages	PDF

Abstract

We report the use of a fragment-based lead discovery method, Tethering with extenders, to discover a pyridinone fragment that binds in an adaptive site of the protein PDK1. With subsequent medicinal chemistry, this led to the discovery of a potent and highly selective inhibitor of PDK1, which binds in the ‘DFG-out’ conformation.

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Keywords

PDK1 DFG-Out Selective Tethering Pyridinone Fragment-based drug discovery

Related Topics

Physical Sciences and Engineering Chemistry Organic Chemistry

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Discovery of a potent and highly selective PDK1 inhibitor via fragment-based drug discovery

Authors

Daniel A. Erlanson, Joseph W. Arndt, Mark T. Cancilla, Kathy Cao, Robert A. Elling, Nicki English, Jessica Friedman, Stig K. Hansen, Cathy Hession, Ingrid Joseph, Gnanasambandam Kumaravel, Wen-Cherng Lee, Ken E. Lind, Robert S. McDowell,