Details

Autor(en) / Beteiligte

• Goldstein, David M
• Alfredson, Tom
• Bertrand, Jay
• Browner, Michelle F
• Clifford, Ken
• Dalrymple, Stacie A
• Dunn, James
• Freire-Moar, Jose
• Harris, Seth
• Labadie, Sharada S
• La Fargue, JoAnn
• Lapierre, Jean Marc
• Larrabee, Susan
• Li, Fujun
• Papp, Eva
• McWeeney, Daniel
• Ramesha, Chakk
• Roberts, Rick
• Rotstein, David
• San Pablo, Bong
• Sjogren, Eric B
• So, On-Yee
• Talamas, Francisco X
• Tao, Will
• Trejo, Alejandra
• Villasenor, Armando
• Welch, Mary
• Welch, Teresa
• Weller, Paul
• Whiteley, Phyllis E
• Young, Kelly
• Zipfel, Sheila

Titel

Discovery of S-[5-Amino-1-(4-fluorophenyl)-1H-pyrazol-4-yl]-[3-(2,3-dihydroxypropoxy)phenyl]methanone (RO3201195), an Orally Bioavailable and Highly Selective Inhibitor of p38 Map Kinase

Ist Teil von

• Journal of medicinal chemistry, 2006-03, Vol.49 (5), p.1562-1575

Ort / Verlag

Washington, DC: American Chemical Society

Erscheinungsjahr

2006

Link zum Volltext

Quelle

MEDLINE

Beschreibungen/Notizen

• A novel class of highly selective inhibitors of p38 MAP kinase was discovered from high throughput screening. The synthesis and optimization of a series of 5-amino-N-phenyl-1H-pyrazol-4-yl-3-phenylmethanones is described. An X-ray crystal structure of this series bound in the ATP binding pocket of unphosphorylated p38α established the presence of a unique hydrogen bond between the exocyclic amine of the inhibitor and threonine 106 which likely contributes to the selectivity for p38. The crystallographic information was used to optimize the potency and physicochemical properties of the series. The incorporation of the 2,3-dihydroxypropoxy moiety on the pyrazole scaffold resulted in a compound with excellent drug-like properties including high oral bioavailability. These efforts identified 63 (RO3201195) as an orally bioavailable and highly selective inhibitor of p38 which was selected for advancement into Phase I clinical trials.