Discovery of a novel class of non-ATP site DFG-out state p38 inhibitors utilizing computationally assisted virtual fragment-based drug design (vFBDD)

Article ID	Journal	Published Year	Pages	File Type
1372173	Bioorganic & Medicinal Chemistry Letters	2011	11 Pages	PDF

Abstract

Discovery of a new class of DFG-out p38α kinase inhibitors with no hinge interaction is described. A computationally assisted, virtual fragment-based drug design (vFBDD) platform was utilized to identify novel non-aromatic fragments which make productive hydrogen bond interactions with Arg 70 on the αC-helix. Molecules incorporating these fragments were found to be potent inhibitors of p38 kinase. X-ray co-crystal structures confirmed the predicted binding modes. A lead compound was identified as a potent (p38α IC50 = 22 nM) and highly selective (≥150-fold against 150 kinase panel) DFG-out p38 kinase inhibitor.

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Keywords

PBM MAPK, mitogen activated protein kinase TNF-?, tumor necrosis factor alpha ATP, adenosine triphosphate RA, Rheumatoid Arthritis COPD, chronic obstructive pulmonary disease LPS, lipopolysaccharide

Related Topics

Physical Sciences and Engineering Chemistry Organic Chemistry

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Discovery of a novel class of non-ATP site DFG-out state p38 inhibitors utilizing computationally assisted virtual fragment-based drug design (vFBDD)

Authors

Kristofer Moffett, Zenon Konteatis, Duyan Nguyen, Rupa Shetty, Jennifer Ludington, Ted Fujimoto, Kyoung-Jin Lee, Xiaomei Chai, Haridasan Namboodiri, Michael Karpusas, Bruce Dorsey, Frank Guarnieri, Marina Bukhtiyarova, Eric Springman, Enrique Michelotti,