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. 2010 Aug 15;20(16):4819-24.
doi: 10.1016/j.bmcl.2010.06.102.

Optimization of alpha-ketoamide based p38 inhibitors through modifications to the region that binds to the allosteric site

Antonio Garrido Montalban  1 Erik BomanChau-Dung ChangSusana Conde CeideRussell DahlDavid DalesandroNancy G J DelaetEric ErbJustin T ErnstAndrew GibbsJeffrey KahlLinda KesslerJeff KucharskiChristopher LumJan LundströmStephen MillerHiroshi NakanishiEdward RobertsEddine SaiahRobert SullivanJan UrbanZhijun WangChristopher J Larson
Affiliations

Optimization of alpha-ketoamide based p38 inhibitors through modifications to the region that binds to the allosteric site

Antonio Garrido Montalban et al. Bioorg Med Chem Lett. .

Abstract

We have optimized a novel series of potent p38 MAP kinase inhibitors based on an alpha-ketoamide scaffold through structure based design that due to their extended molecular architecture bind, in addition to the ATP site, to an allosteric pocket. In vitro ADME, in vivo PK and efficacy studies show these compounds to have drug-like characteristics and have resulted in the nomination of a development candidate which is currently in phase II clinical trials for the oral treatment of inflammatory conditions.

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