Inhibition of Anandamide Hydrolysis by Cyclohexyl Carbamic Acid 3′-Carbamoyl-3-yl Ester (URB597) Reverses Abuse-Related Behavioral and Neurochemical Effects of Nicotine in Rats

Scherma, María; Panlilio, Leigh V.; Fadda, Paola; Fattore, Liana; Gamaleddin, Islamhany; Foll, Bernard Le; Justinová, Zuzana; Mikics, Éva; Haller, József; Medalie, Julie; Stroik, Jessica; Barnes, Chanel; Yaşar, Sevil; Piomelli, Daniele; Fratta, Walter; Goldberg, Steven R.

doi:10.1124/jpet.108.142224

Cited by 128 publications

(143 citation statements)

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“…Whether the phosphorylation leads to a reduced ion influx into the DA cell or to fewer nAChRs expressed on the surface of DA cell membranes, the outcome appears as a diminished/abolished response of VTA DA neurons to nicotine, as well as to endogenous acetylcholine [42]. This scenario would provide a plausible cellular mechanism for the lack of effect of nicotine in increasing extracellular DA levels in the shell of the NAcc following URB597 treatment [40]. Accordingly, synthetic PPARa ligands, such as lipid lowering fibrates, prevent nicotine-induced excitation of DA cells and increases of extracellular DA levels in the NAcc shell [73].…”

Section: Review Endocannabinoids and Dopamine Neurons M Melis And Mmentioning

confidence: 99%

“…However, because DA neurons might be sensitized to priming with drugs or with drug-associated cues, and might trigger reinstatement, one possibility is that potentiation of endocannabinoid signalling (rather than an indiscriminate activation of CB1 receptors by exogenous agonists) might blunt their stimulus-driven responses by selectively suppressing glutamate release from impinging excitatory axons. Accordingly, cue-induced reinstatement to nicotine self-administration is particularly sensitive to blockade by both FAAH inhibition, AM404 and VDM11 [40,107,108]. In regards to this, it must be pointed out that inhibition of FAAH enhances NAE levels that could depress responses to nicotine via modulation of nAChRs (see above).…”

Section: Review Endocannabinoids and Dopamine Neurons M Melis And Mmentioning

confidence: 99%

“…Nonetheless, previous anatomical, biochemical and electrophysiological studies have provided compelling evidence that the N-acylethanolamine anandamide and the endogenous ligands to peroxisome-proliferatoractivated receptor-alpha (PPARa; i.e. oleoylethanolamide, OEA; palmitoylethanolamide, PEA), as well as the endocannabinoid/vanilloid N-arachidonoyldopamine (NADA) are also present within the VTA [31,34,[38][39][40][41][42][43], thus suggesting discrete physiological roles for each endocannabinoid and cognate molecule in the modulation of DA neuron and its related behaviour.…”

Section: Endocannabinoid Systemmentioning

confidence: 99%

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Hub and switches: endocannabinoid signalling in midbrain dopamine neurons

Melis

Pistis

2012

Phil. Trans. R. Soc. B

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The last decade has provided a wealth of experimental data on the role played by lipids belonging to the endocannabinoid family in several facets of physiopathology of dopamine neurons. We currently suggest that these molecules, being intimately connected with diverse metabolic and signalling pathways, might differently affect various functions of dopamine neurons through activation not only of surface receptors, but also of nuclear receptors. It is now emerging how dopamine neurons can regulate their constituent biomolecules to compensate for changes in either internal functions or external conditions. Consequently, dopamine neurons use these lipid molecules as metabolic and homeostatic signal detectors, which can dynamically impact cell function and fitness. Because dysfunctions of the dopamine system underlie diverse neuropsychiatric disorders, including schizophrenia and drug addiction, the importance of better understanding the correlation between an unbalanced endocannabinoid signal and the dopamine system is even greater. Particularly, because dopamine neurons are critical in controlling incentive-motivated behaviours, the involvement of endocannabinoid molecules in fine-tuning dopamine cell activity opened new avenues in both understanding and treating drug addiction. Here, we review recent advances that have shed new light on the understanding of differential roles of endocannabinoids and their cognate molecules in the regulation of the reward circuit, and discuss their anti-addicting properties, particularly with a focus on their potential engagement in the prevention of relapse.

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Section: Review Endocannabinoids and Dopamine Neurons M Melis And Mmentioning

confidence: 99%

Section: Review Endocannabinoids and Dopamine Neurons M Melis And Mmentioning

confidence: 99%

Section: Endocannabinoid Systemmentioning

confidence: 99%

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Hub and switches: endocannabinoid signalling in midbrain dopamine neurons

Melis

Pistis

2012

Phil. Trans. R. Soc. B

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“…For example, although synthetic CB 1 agonists increase nicotine SA and enhance nicotine-seeking behavior (Gamaleddin et al, 2012), these nicotine-related behaviors are generally attenuated by enhancing endogenous eCB tone (eg, eCB clearance inhibition) (Forget et al, 2009;Gamaleddin et al, 2011;Scherma et al, 2008). The distinction between these influences may arise, in part, from differential regional patterns of CB1 activation.…”

Section: Endocannabinoid Levels Following Nicotine Exposure Mw Buczynmentioning

confidence: 99%

“…Moreover, in contrast to CB 1 -selective agonists, manipulations such as FAAH inhibition also enhance signaling through non-CB receptors (PPAR a , TRPV 1 , and so on) that may counter or modify the effects of concurrent CB 1 receptor signaling. Because the nature of nicotine-induced alterations in eCB signaling may differ at various stages of nicotine exposure (eg, acquisition vs maintenance of drug intake; dependence), and nicotineinduced eCB alterations may differ from eCB disruptions associated with nicotine-seeking behavior (induced by cues, drug priming, and/or stress), it is not surprising that the influence of eCB clearance inhibition on nicotine-related behaviors varies among these distinct phases of nicotine use (Forget et al, 2009;Scherma et al, 2008).…”

Section: Endocannabinoid Levels Following Nicotine Exposure Mw Buczynmentioning

confidence: 99%

The Volitional Nature of Nicotine Exposure Alters Anandamide and Oleoylethanolamide Levels in the Ventral Tegmental Area

Buczynski

Polis

Parsons

2012

Neuropsychopharmacol

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Cannabinoid-1 receptors (CB 1 ) have an important role in nicotine reward and their function is disrupted by chronic nicotine exposure, suggesting nicotine-induced alterations in endocannabinoid (eCB) signaling. However, the effects of nicotine on brain eCB levels have not been rigorously evaluated. Volitional intake of nicotine produces physiological and behavioral effects distinct from forced drug administration, although the mechanisms underlying these effects are not known. This study compared the effects of volitional nicotine self-administration (SA) and forced nicotine exposure (yoked administration (YA)) on levels of eCBs and related neuroactive lipids in the ventral tegmental area (VTA) and other brain regions. Brain lipid levels were indexed both by in vivo microdialysis in the VTA and lipid extractions from brain tissues. Nicotine SA, but not YA, reduced baseline VTA dialysate oleoylethanolamide (OEA) levels relative to nicotine-naïve controls, and increased anandamide (AEA) release during nicotine intake. In contrast, all nicotine exposure paradigms increased VTA dialysate 2-arachidonoyl glycerol (2-AG) levels. Thus, nicotine differentially modulates brain lipid (2-AG, AEA, and OEA) signaling, and these modulations are influenced by the volitional nature of the drug exposure. Corresponding bulk tissue analysis failed to identify these lipid changes. Nicotine exposure had no effect on fatty acid amide hydrolase activity in the VTA, suggesting that changes in AEA and OEA signaling result from alterations in their nicotine-induced biosynthesis. Both CB 1 (by AEA and 2-AG) and non-CB 1 (by OEA) targets can alter the excitability and activity of the dopaminergic neurons in the VTA. Collectively, these findings implicate disrupted lipid signaling in the motivational effects of nicotine.

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Using dopamine research to generate rational cannabinoid drug policy

Loewinger

Oleson

Cheer

2012

Drug Testing and Analysis

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The recent rise in the recreational use of synthetic cannabinoids (e.g. ‘K2’ and ‘Spice’) has been accompanied by a corresponding increase in regulation. Besides prohibition of specific compounds and general class bans in over forty states, five synthetic cannabinoids (CB) are federally regulated under a ‘temporary’ ban and are currently under a formal review to determine whether to permanently schedule them. Whether through explicit prohibition of specific chemicals, or potential de facto bans of unofficially scheduled compounds through the analogue act, scheduling CBs may significantly impede researching their therapeutic utility and elucidating physiological roles of the endogenous CB system. We argue that a review of neuroscience research suggests that synthetic CBs that act like Δ9-tetrahydrocannabinol (THC) by directly binding to and stimulating CB receptors (i.e. direct agonists), as well as novel drugs that indirectly stimulate these receptors by increasing levels of endogenous CB neurotransmitters (i.e. indirect agonists) have therapeutic value. Specifically, neurochemical research into how CBs influence mesolimbic dopamine release, a reliable and consistent marker of drugs’ rewarding/reinforcing effects, provides the most useful indication of CB abuse liability, and may have implications for the generation of rational drug policy. It demonstrates that direct CB receptor agonists, but not indirect agonists, increase mesolimbic dopamine release. Thus, while direct CB receptor agonists pose an abuse liability, indirect agonists do not. We recommend regulatory agencies revise policies that treat these separate CB classes similarly and to curb regulation aimed at any CB receptor agonists as Schedule I, as this ignores their medicinal properties.

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Inhibition of Anandamide Hydrolysis by Cyclohexyl Carbamic Acid 3′-Carbamoyl-3-yl Ester (URB597) Reverses Abuse-Related Behavioral and Neurochemical Effects of Nicotine in Rats

Cited by 128 publications

References 45 publications

Hub and switches: endocannabinoid signalling in midbrain dopamine neurons

Hub and switches: endocannabinoid signalling in midbrain dopamine neurons

The Volitional Nature of Nicotine Exposure Alters Anandamide and Oleoylethanolamide Levels in the Ventral Tegmental Area

Using dopamine research to generate rational cannabinoid drug policy

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