Optimization of the central heterocycle of α-ketoheterocycle inhibitors of fatty acid amide hydrolase

…, DG Hochstatter, I Hwang, DL Boger

文献索引：Garfunkle, Joie; Ezzili, Cyrine; Rayl, Thomas J.; Hochstatter, Dustin G.; Hwang, Inkyu; Boger, Dale L. Journal of Medicinal Chemistry, 2008 , vol. 51, # 15 p. 4392 - 4403

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被引用次数: 82

摘要

The synthesis and evaluation of a refined series of α-ketoheterocycles based on the oxazole 2 (OL-135) incorporating systematic changes in the central heterocycle bearing a key set of added substituents are described. The nature of the central heterocycle, even within the systematic and minor perturbations explored herein, significantly influenced the inhibitor activity: 1, 3, 4-oxadiazoles and 1, 2, 4-oxadiazoles 9> tetrazoles, the isomeric 1, 2, 4- ...

37729-18-3

2-([1,1'-联苯]-4-基)乙醇

~55%

61502-90-7

(9H-Fluoren-9-y...

Design, synthesis, and structure− affinity relationships of ...

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Structure–activity relationship of a new Series of reversibl...

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