| Literature DB >> 26888301 |
Margherita Brindisi1, Samuele Maramai1, Sandra Gemma1, Simone Brogi1, Alessandro Grillo1, Lorenzo Di Cesare Mannelli2, Emanuele Gabellieri1, Stefania Lamponi1, Simona Saponara3, Beatrice Gorelli3, Daniele Tedesco4, Tommaso Bonfiglio5, Christophe Landry6, Kwang-Mook Jung7, Andrea Armirotti8, Livio Luongo9, Alessia Ligresti10, Fabiana Piscitelli10, Carlo Bertucci4, Marie-Pierre Dehouck6, Giuseppe Campiani1, Sabatino Maione9, Carla Ghelardini2, Anna Pittaluga5,11, Daniele Piomelli7, Vincenzo Di Marzo10, Stefania Butini1.
Abstract
We report the discovery of compound 4a, a potent β-lactam-based monoacylglycerol lipase (MGL) inhibitor characterized by an irreversible and stereoselective mechanism of action, high membrane permeability, high brain penetration evaluated using a human in vitro blood-brain barrier model, high selectivity in binding and affinity-based proteomic profiling assays, and low in vitro toxicity. Mode-of-action studies demonstrate that 4a, by blocking MGL, increases 2-arachidonoylglycerol and behaves as a cannabinoid (CB1/CB2) receptor indirect agonist. Administration of 4a in mice suffering from experimental autoimmune encephalitis ameliorates the severity of the clinical symptoms in a CB1/CB2-dependent manner. Moreover, 4a produced analgesic effects in a rodent model of acute inflammatory pain, which was antagonized by CB1 and CB2 receptor antagonists/inverse agonists. 4a also relieves the neuropathic hypersensitivity induced by oxaliplatin. Given these evidence, 4a, as MGL selective inhibitor, could represent a valuable lead for the future development of therapeutic options for multiple sclerosis and chronic pain.Entities:
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Year: 2016 PMID: 26888301 DOI: 10.1021/acs.jmedchem.5b01812
Source DB: PubMed Journal: J Med Chem ISSN: 0022-2623 Impact factor: 7.446