4.7 Article

New potent and selective inhibitors of anandamide reuptake with antispastic activity in a mouse model of multiple sclerosis

Journal

BRITISH JOURNAL OF PHARMACOLOGY
Volume 147, Issue 1, Pages 83-91

Publisher

WILEY-BLACKWELL
DOI: 10.1038/sj.bjp.0706418

Keywords

cannabinoid; endocannabinoid; 2-arachidonoylglycerol; membrane transport; spasticity; multiple sclerosis

Funding

  1. Multiple Sclerosis Society [835, 541] Funding Source: Medline
  2. NIDA NIH HHS [R01 DA008904, DA-08904, DA-09789, P01 DA009789] Funding Source: Medline
  3. NATIONAL INSTITUTE ON DRUG ABUSE [R01DA008904, P01DA009789] Funding Source: NIH RePORTER

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1 We previously reported that the compound O-2093 is a selective inhibitor of the reuptake of the endocannabinoid anandamide (AEA). We have now re-examined the activity of O-2093 in vivo and synthesized four structural analogs (O-2247, O-2248, O-3246, and O-3262), whose activity was assessed in: (a) binding assays carried out with membranes from cells overexpressing the human CB(1) and CB(2) receptors; (b) assays of transient receptor potential of the vanilloid type-1 (TRPV1) channel functional activity (measurement of [Ca(2+)](i)); (c) [(14)C]AEA cellular uptake and hydrolysis assays in rat basophilic leukaemia (RBL-2H3) cells; (d) the mouse 'tetrad' tests (analgesia on a hot plate, immobility on a 'ring', rectal hypothermia and hypolocomotion in an open field); and (e) the limb spasticity test in chronic relapsing experimental allergic encephalomyelitis (CREAE) mice, a model of multiple sclerosis (MS). 2 O-2093, either synthesized by us or commercially available, was inactive in the 'tetrad' up to a 20 mg kg(-1) dose (i. v.). Like O-2093, the other four compounds exhibited low affinity in CB(1) (K(i) from 1.3 to > 10 mu M) and CB(2) binding assays (1.3 < K(i) < 8 mu M), low potency and efficacy in a TRPV1 functional assay (EC(50) > 10 mu M), very low potency as fatty acid amide hydrolase (FAAH) inhibitors (IC(50) > 25 mu M) and were inactive in the 'tetrad' up to a 30 mg kg(-1) dose (i. v.). 3 While O-2247 and O-2248 were poor inhibitors of [(14)C]AEA cellular uptake (IC(50) > 40 mu M), O-3246 and O-3262 were quite potent in this assay. O-3246, which exhibits only a very subtle structural difference with O-2093, is the most potent inhibitor of AEA uptake reported in vitro under our experimental conditions (IC(50) = 1.4 mu M) and is 12-fold more potent than O-2093. 4 When injected intravenously O-3246 and O-3262, again like O-2093 and unlike O-2247 and O-2248, significantly inhibited limb spasticity in mice with CREAE. 5 These data confirm the potential utility of selective AEA uptake inhibitors as anti-spasticity drugs in MS and, given the very subtle chemical differences between potent and weak inhibitors of uptake, support further the existence of a specific mechanism for this process.

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