Long_2010_J.Med.Chem_53_1830

Reference

Title : Characterization of tunable piperidine and piperazine carbamates as inhibitors of endocannabinoid hydrolases - Long_2010_J.Med.Chem_53_1830
Author(s) : Long JZ , Jin X , Adibekian A , Li W , Cravatt BF
Ref : Journal of Medicinal Chemistry , 53 :1830 , 2010
Abstract :

Monoacylglycerol lipase (MAGL) and fatty acid amide hydrolase (FAAH) are two enzymes from the serine hydrolase superfamily that degrade the endocannabinoids 2-arachidonoylglycerol and anandamide, respectively. We have recently discovered that MAGL and FAAH are both inhibited by carbamates bearing an N-piperidine/piperazine group. Piperidine/piperazine carbamates show excellent in vivo activity, raising brain endocannabinoid levels and producing CB1-dependent behavioral effects in mice, suggesting that they represent a promising class of inhibitors for studying the endogenous functions of MAGL and FAAH. Herein, we disclose a full account of the syntheses, structure-activity relationships, and inhibitory activities of piperidine/piperazine carbamates against members of the serine hydrolase family. These scaffolds can be tuned for MAGL-selective or dual MAGL-FAAH inhibition by the attachment of an appropriately substituted bisarylcarbinol or aryloxybenzyl moiety, respectively, on the piperidine/piperazine ring. Modifications to the piperidine/piperazine ring ablated inhibitory activity, suggesting a strict requirement for a six-membered ring to maintain potency.

PubMedSearch : Long_2010_J.Med.Chem_53_1830
PubMedID: 20099888

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Citations formats

Long JZ, Jin X, Adibekian A, Li W, Cravatt BF (2010)
Characterization of tunable piperidine and piperazine carbamates as inhibitors of endocannabinoid hydrolases
Journal of Medicinal Chemistry 53 :1830

Long JZ, Jin X, Adibekian A, Li W, Cravatt BF (2010)
Journal of Medicinal Chemistry 53 :1830