Litcius/Paper detail

Design, microwave‐assisted synthesis, biological evaluation and molecular modeling studies of 4‐phenylthiazoles as potent fatty acid amide hydrolase inhibitors

Stephanie Wilt, Mark Anthony Rodriguez, Thanh N. H. Le, Emily V. Baltodano, Adrián Salas, Stevan Pecic

2020Chemical Biology & Drug Design19 citationsDOI

Abstract

Endocannabinoids, anandamide (AEA) and 2-arachidonoylglycerol (2-AG), are endogenous lipids that activate cannabinoid receptors. Activation of these receptors produces anti-inflammatory and analgesic effects. Fatty acid amide hydrolase (FAAH) is a membrane enzyme that hydrolases endocannabinoids; thus, inhibition of FAAH represents an attractive approach to develop new therapeutics for treating inflammation and pain. Previously, potent rat FAAH inhibitors containing 2-naphthyl- and 4-phenylthiazole scaffolds were identified, but up to the present time, very little structure-activity relationship studies have been performed on these moieties. We designed and synthesized several analogs containing these structural motifs and evaluated their inhibition potencies against human FAAH enzyme. In addition, we built and validated a homology model of human FAAH enzyme and performed docking experiments. We identified several inhibitors in the low nanomolar range and calculated their ADME predicted values. These FAAH inhibitors represent promising drug candidates for future preclinical in vivo studies.

Topics & Concepts

Fatty acid amide hydrolaseAnandamideEndocannabinoid systemCannabinoid receptorChemistryCannabinoidEnzymeBiochemistryPharmacologyAmidaseADMEReceptorDocking (animal)In vivoIn vitroBiologyAntagonistMedicineBiotechnologyNursingCannabis and Cannabinoid ResearchPharmacological Receptor Mechanisms and EffectsNeurotransmitter Receptor Influence on Behavior