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Merck

Discovery libraries targeting the major enzyme classes: the serine hydrolases.

Bioorganic & medicinal chemistry letters (2014-07-20)
Katerina Otrubova, Venkat Srinivasan, Dale L Boger
ABSTRACT

Two libraries of modestly reactive ureas containing either electron-deficient acyl anilines or acyl pyrazoles were prepared and are reported as screening libraries for candidate serine hydrolase inhibitors. Within each library is a small but powerful subset of compounds that serve as a chemotype fragment screening library capable of subsequent structural diversification. Elaboration of the pyrazole-based ureas provided remarkably potent irreversible inhibitors of fatty acid amide hydrolase (FAAH, apparent Ki=100-200 pM) complementary to those previously disclosed enlisting electron-deficient aniline-based ureas.

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Sigma-Aldrich
Serine Hydrolase Inhibitor-11, 95%
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Serine Hydrolase Inhibitor-1
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Serine Hydrolase Inhibitor-9
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