2-Alkylamino- and alkoxy-substituted 2-amino-1,3,4-oxadiazoles-O-Alkyl benzohydroxamate esters replacements retain the desired inhibition and selectivity against MEK (MAP ERK kinase).

Joseph Scott Warmus,Cathlin Marie Flamme,Lu Yan Zhang,Stephen Douglas Barrett,Alexander James Bridges,Huifen Chen,Richard Gowan,Michael Kaufman,Judy Sebolt-Leopold,Wilbur R. Leopold,Ronald Merriman,Jeffrey F. Ohren,Alexander Pavlovsky,Sally Przybranowski,Haile Tecle,Heather Valik,Christopher Whitehead,Erli Zhang

2-Alkylamino- and alkoxy-substituted 2-amino-1,3,4-oxadiazoles-O-Alkyl benzohydroxamate esters replacements retain the desired inhibition and selectivity against MEK (MAP ERK kinase).

2008

Joseph Scott Warmus
Cathlin Marie Flamme
Lu Yan Zhang
Stephen Douglas Barrett
Alexander James Bridges
Huifen Chen
Richard Gowan
Michael Kaufman
Judy Sebolt-Leopold
Wilbur R. Leopold
Ronald Merriman
Jeffrey F. Ohren
Alexander Pavlovsky
Sally Przybranowski
Haile Tecle
Heather Valik
Christopher Whitehead
Erli Zhang

This paper reports a second generation MEK inhibitor. The previously reported potent and efficacious MEK inhibitor, PD-184352 (CI-1040), contains an integral hydroxamate moiety. This compound suffered from less than ideal solubility and metabolic stability. An oxadiazole moiety behaves as a bioisostere for the hydroxamate group, leading to a more metabolically stable and efficacious MEK inhibitor.

Keywords:

MEK inhibitor
Moiety
Organic chemistry
Oxadiazole
Alkoxy group
Aromatic amine
Hydroxamic acid
Biochemistry
Enzyme inhibitor
Stereochemistry
Bioisostere
Chemistry

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