The Endogenous Cannabinoid Anandamide Produces δ-9-Tetrahydrocannabinol-Like Discriminative and Neurochemical Effects That Are Enhanced by Inhibition of Fatty Acid Amide Hydrolase but Not by Inhibition of Anandamide Transport

Solinas, Marcello; Tanda, Gianluigi; Justinová, Zuzana; Wertheim, Carrie E.; Yaşar, Sevil; Piomelli, Daniele; Vadivel, Subramanian K.; Makriyannis, Alexandros; Goldberg, Steven R.

doi:10.1124/jpet.106.114124

Cited by 104 publications

(145 citation statements)

References 41 publications

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“…Rimonabant, however, did not affect the behavior maintained by cocaine when administered alone (140). In agreement with this report, Rimonabant pretreatment did not show any effect on cocaine self-administration under fixedratio schedules of behavior in squirrel monkeys (63), an effect that has been recently replicated and confirmed (141,142). In addition, Rimonabant did not affect the number of cocaine selfinjections in Wistar rats studied under a fixed-ratio 5 schedule of drug delivery (103,104).…”

Section: Effects Of Cannabinoids On Cocaine-maintained Self-administrsupporting

confidence: 78%

“…Anandamide is then metabolized into the cell by an intracellular enzyme, the fatty acid amide hydrolase (FAAH) (60,61), the blockade of which has been shown to prolong the behavioral/neurobiological effects of anandamide (4,61,62,63). In contrast, 2-AG is metabolized through the mono glyceril lipase enzyme (54).…”

Section: Overview On the Brain Endocannabinoid Systemmentioning

confidence: 99%

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Modulation of the endocannabinoid system: Therapeutic potential against cocaine dependence

Tanda

2007

Pharmacological Research

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Dependence on cocaine is still a main unresolved medical and social concern, and in spite of research efforts, no pharmacological therapy against cocaine dependence is yet available. Recent studies have shown that the endocannabinoid system participates in specific stages and aspects of drug dependence in general, and some of this evidence suggests an involvement of the cannabinoid system in cocaine effects. For example, cocaine administration has been shown to alter brain endocannabinoid levels, and the endocannabinoid system has been involved in long-term modifications of brain processes that might play a role in neuro/behavioral effects of psychostimulant drugs like cocaine. Human studies show that marijuana dependence is frequently associated with cocaine dependence, and that the cannabinoid receptor CNR1 gene polymorphism might be related to cocaine addiction. This article will review the main papers in the field showing how a modulation of different components of the cannabinoid system might interact with some of the neurobiological/behavioral effects of cocaine related to its reinforcing effects, evaluated in preclinical models or in clinical settings. The goal of this review will be to provide insights into the complex picture of cocaine abuse and addiction, and to extrapolate from such endocannabinoid-cocaine interactions useful information to test the therapeutic potential of cannabinoid ligands and endocannabinoid-level enhancers against cocaine dependence for future preclinical/clinical trials.

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Section: Effects Of Cannabinoids On Cocaine-maintained Self-administrsupporting

confidence: 78%

Section: Overview On the Brain Endocannabinoid Systemmentioning

confidence: 99%

Modulation of the endocannabinoid system: Therapeutic potential against cocaine dependence

Tanda

2007

Pharmacological Research

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“…The outcomes of the antagonism tests are reminiscent of previous studies assessing surmountable antagonism of rimonabant by mAEA (Järbe et al 2001); animals ceased responding before full generalization (≥80% drug lever responding) might have been achieved (see also Solinas et al 2007). When agonist dose was held constant, i.e., the mAEA training dose, both rimonabant and AM251 (1 to 3 mg/kg) reduced mAEA (10 mg/ kg) appropriate responding to around 25% or lower, suggesting CB 1 R mediation for the DD effect; this was accompanied by a downward trend in response rate (Järbe et al 2006a).…”

Section: Discussionmentioning

confidence: 88%

“…To account for such findings, it has been suggested that cannabinoid ligands interact with CB 1 R/CB 2 R through different binding motifs and/or through non-CB 1 R/CB 2 R cellular targets including additional cannabinoid subtypes or cannabinoid-like receptors and involvement of vanilloid receptor (VR 1 ) mechanisms (Howlett 2004;Pacher et al 2006;Oz 2006 for reviews). Of these, vanilloid mechanism(s) do not appear important for cannabinoid DD, as the VR 1 antagonist capsazepine did not antagonize the Δ9-THC-like discriminative stimulus effects of anandamide (Solinas et al 2007), nor did the VR 1 agonist O-1839 substitute for DDs maintained by the CB 1 R agonists Δ9-THC and O-1812 (ACEA), a CB 1 R selective anandamide analog ). All of the above postulated mechanisms may, however, affect response rate.…”

Section: Discussionmentioning

confidence: 99%

Discriminative stimulus effects of the cannabinoid CB1 receptor antagonist rimonabant in rats

Järbe

Vadivel

et al. 2008

Psychopharmacology

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Objective-To examine the discriminative stimulus effects of the cannabinoid CB 1 receptor (CB 1 R) antagonist/inverse agonist rimonabant (SR141716A) using a discriminated taste aversion (DTA) procedure.Materials and methods-Groups of rats were trained to discriminate between drug (5.6 or 3 mg/kg) and vehicle in DTA (t′=20 min). The 30-min drinking opportunity after rimonabant pretreatment was followed by injection of lithium chloride (120 mg/kg) in the experimental (EXP) animals. When offered fluid after vehicle pretreatment, EXP animals subsequently were given intraperitoneal saline (NaCl, 10 ml/kg). Post-drinking treatment for controls (CONT) was NaCl irrespective of the pretreatment condition (rimonabant or vehicle). Tests examined other doses and drugs (t′=20 min).Results-The rimonabant analog AM251 (1 to 5.6 mg/kg) substituted for rimonabant. AM281 also appeared to substitute, but interpretation is complicated by unconditioned effects (drinking suppressed also in the CONT group). The CB 2 R antagonists SR144528 (18 and 30 mg/kg), AM630 (1 to 10 mg/kg), and the CB 1 R agonist methanandamide (mAEA, 3 and 10 mg/kg) did not substitute. There was a dose-related attenuation of the rimonabant-induced suppression of saccharin drinking when Δ9-tetrahydrocannabinol (Δ9-THC; 0.3 to 5.6 mg/kg), but not mAEA (1 to 10 mg/kg), was given together with rimonabant (3 mg/kg). Unconditioned effects occurred with the mAEA-rimonabant combination, not evident for combinations of rimonabant and Δ9-THC. mAEA (10 mg/kg) plus AM251 (5.6 mg/kg) resulted in strong unconditioned effects.Conclusion-Rimonabant induces a discriminative stimulus in DTA that continues to show potential for further examination of cannabinoid receptor antagonism.

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“…The general procedure and apparatus have been described previously (Solinas et al, 2007). Rats were surgically implanted with a concentric dialysis probe aimed at the shell of the nucleus accumbens (2 mm anterior and 1.1 mm lateral from bregma, 8.0 mm below the dura) (Paxinos and Watson, 2005) under anesthesia.…”

Section: In Vivo Microdialysis In Freely Moving Ratsmentioning

confidence: 99%

Effects of Fatty Acid Amide Hydrolase (FAAH) Inhibitors in Non-Human Primate Models of Nicotine Reward and Relapse

Justinová

Panlilio

Moreno-Sanz

et al. 2015

Neuropsychopharmacol

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Inhibition of the enzyme fatty acid amide hydrolase (FAAH) counteracts reward-related effects of nicotine in rats, but it has not been tested for this purpose in non-human primates. Therefore, we studied the effects of the first-and second-generation O-arylcarbamatebased FAAH inhibitors, URB597 (cyclohexyl carbamic acid 3'-carbamoyl-3-yl ester) and URB694 (6-hydroxy-[1,1'-biphenyl]-3-ylcyclohexylcarbamate), in squirrel monkeys. Both FAAH inhibitors: (1) blocked FAAH activity in brain and liver, increasing levels of endogenous ligands for cannabinoid and α-type peroxisome proliferator-activated (PPAR-α) receptors; (2) shifted nicotine self-administration dose-response functions in a manner consistent with reduced nicotine reward; (3) blocked reinstatement of nicotine seeking induced by reexposure to either nicotine priming or nicotine-associated cues; and (4) had no effect on cocaine or food self-administration. The effects of FAAH inhibition on nicotine self-administration and nicotine priming-induced reinstatement were reversed by the PPAR-α antagonist, MK886. Unlike URB597, which was not self-administered by monkeys in an earlier study, URB694 was self-administered at a moderate rate. URB694 self-administration was blocked by pretreatment with an antagonist for either PPAR-α (MK886) or cannabinoid CB 1 receptors (rimonabant). In additional experiments in rats, URB694 was devoid of THC-like or nicotine-like interoceptive effects under drug-discrimination procedures, and neither of the FAAH inhibitors induced dopamine release in the nucleus accumbens shell-consistent with their lack of robust reinforcing effects in monkeys. Overall, both URB597 and URB694 show promise for the initialization and maintenance of smoking cessation because of their ability to block the rewarding effects of nicotine and prevent nicotine priming-induced and cue-induced reinstatement.

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The Endogenous Cannabinoid Anandamide Produces δ-9-Tetrahydrocannabinol-Like Discriminative and Neurochemical Effects That Are Enhanced by Inhibition of Fatty Acid Amide Hydrolase but Not by Inhibition of Anandamide Transport

Cited by 104 publications

References 41 publications

Modulation of the endocannabinoid system: Therapeutic potential against cocaine dependence

Modulation of the endocannabinoid system: Therapeutic potential against cocaine dependence

Discriminative stimulus effects of the cannabinoid CB1 receptor antagonist rimonabant in rats

Effects of Fatty Acid Amide Hydrolase (FAAH) Inhibitors in Non-Human Primate Models of Nicotine Reward and Relapse

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