Journal
BRITISH JOURNAL OF PHARMACOLOGY
Volume 180, Issue 10, Pages 1316-1338Publisher
WILEY
DOI: 10.1111/bph.16014
Keywords
AEA; endocannabinoid system; FAAH; melatonin; N-acylethanolamines; neuroinflammation; OEA; PPAR alpha; TRPV1; URB597
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Inhibiting FAAH or stimulating melatonin receptors can enhance endocannabinoid and melatoninergic signaling, which may be beneficial for treating neuroinflammation and neurodegenerative diseases.
Background and Purpose: Devising novel strategies to therapeutically favour inflammation resolution and provide neuroprotection is an unmet clinical need. Enhancing endocannabinoid tone by inhibiting the catabolic enzyme fatty acid amide hydrolase (FAAH), or stimulating melatonin receptors has therapeutic potential to treat neuropathological states in which neuroinflammation plays a central role.Experimental Approach: A rodent hippocampal explant model of inflammatory injury was used to assess the effects of UCM1341, a dual-acting compound with FAAH inhibitory action and agonist activity at melatonin receptors, against neuroinflammatory damage. FAAH activity was measured by a radiometric assay, and N- acylethanolamine levels were assessed by HPLC-MS/MS methods. FAAH distribution, evolution of inflammation and the contribution of UCM1341 to the expression of proteins controlling macrophage behaviour were investigated by biochemical and confocal analyses.Key Results: UCM1341 exhibited greater neuroprotection against neuroinflammatory degeneration, compared with the reference compounds URB597 (FAAH inhibitor) and melatonin. During neuroinflammation, UCM1341 augmented the levels of anandamide and N-oleoylethanolamine, but not N-palmitoylethanolamine, up regulated PPAR-alpha levels, attenuated demyelination and prevented the release of TNF-alpha. UCM1341 modulated inflammatory responses by contributing to microglia/ macrophage polarization, stimulating formation of lipid-laden macrophages and regulating expression of proteins controlling cholesterol metabolism and efflux. The neuroprotective effects of UCM1341 were prevented by PPAR alpha, TRPV1 and melatonin receptor antagonists.Conclusion and Implications: UCM1341, by enhancing endocannabinoid and melatoninergic signalling, benefits neuroprotection and stimulates inflammation resolution pathways. Our findings provide an encouraging prospect of therapeutically targeting endocannabinoid and melatoninergic systems in inflammatory demyelinating states in the CNS.
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