Involvement of 2‐arachidonoyl glycerol in the increased consumption of and preference for ethanol of mice treated with neurotoxic doses of methamphetamine

Gutiérrez-Ĺopez,; Llopis, Noemi; Feng, Shile; Barrett, David A.; O’Shea, Esther; Colado, M. Isabel

doi:10.1111/j.1476-5381.2010.00720.x

Cited by 19 publications

(12 citation statements)

References 49 publications

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“…In other investigations, the self‐administration of alcohol was demonstrated to increase the extracellular level of 2‐AG in the NAc, which is linked to the amount of alcohol consumed, but not of AEA in the same region (Caille, Alvarez‐Jaimes, Polis, Stouffer, & Parsons, ). Furthermore, a mouse model of methamphetamine‐induced neurotoxic lesioning of nigrostriatal dopaminergic projections exhibited increased alcohol intake and enhanced 2‐AG levels in the limbic forebrain tissues comprising the anterior cingulate and the NAc (Gutierrez‐Lopez et al, ). The pharmacological blockade of MAGL also enhanced alcohol consumption and preference (Serrano et al, ; Figure ).…”

Section: The Role Of the Ecb System In Alcohol Intake/self‐administramentioning

confidence: 99%

Distinct functions of endogenous cannabinoid system in alcohol abuse disorders

Basavarajappa

Joshi

Shivakumar

et al. 2019

British J Pharmacology

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Δ9‐tetrahydrocannabinol, the principal active component in Cannabis sativa extracts such as marijuana, participates in cell signalling by binding to cannabinoid CB1 and CB2 receptors on the cell surface. The CB1 receptors are present in both inhibitory and excitatory presynaptic terminals and the CB2 receptors are found in neuronal subpopulations in addition to microglial cells and astrocytes and are present in both presynaptic and postsynaptic terminals. Subsequent to the discovery of the endocannabinoid (eCB) system, studies have suggested that alcohol alters the eCB system and that this system plays a major role in the motivation to abuse alcohol. Preclinical studies have provided evidence that chronic alcohol consumption modulates eCBs and expression of CB1 receptors in brain addiction circuits. In addition, studies have further established the distinct function of the eCB system in the development of fetal alcohol spectrum disorders. This review provides a recent and comprehensive assessment of the literature related to the function of the eCB system in alcohol abuse disorders.

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Section: The Role Of the Ecb System In Alcohol Intake/self‐administramentioning

confidence: 99%

Distinct functions of endogenous cannabinoid system in alcohol abuse disorders

Basavarajappa

Joshi

Shivakumar

et al. 2019

British J Pharmacology

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“…Notably, self-administration of ethanol increases interstitial levels of 2-AG in the NAc that are correlated with the amount of ethanol consumed, but does not alter levels of AEA in this brain region (Caillé et al, 2007). Additionally, a methamphetamine-induced neurotoxic lesion of nigrostriatal dopaminergic projections (Granado et al, 2010; Sanchez et al, 2003) is associated with increased levels of ethanol consumption and preference, and this mouse model of enhanced ethanol intake displays increased tissue concentrations of 2-AG in limbic forebrain sections containing anterior cingulate and NAc (Gutierrez-Lopez et al, 2010). Furthermore, these investigators found that enhanced ethanol consumption and preference were also observed in intact mice treated with the MAGL inhibitor N- arachidonyl maleimide.…”

Section: Ethanol and The Ec Systemmentioning

confidence: 99%

A review of the interactions between alcohol and the endocannabinoid system: Implications for alcohol dependence and future directions for research

Pava

Woodward

2012

Alcohol

131

101

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Over the past fifty years a significant body of evidence has been compiled suggesting an interaction between the endocannabinoid (EC) system and alcohol dependence. However, much of this work has been conducted only in the past two decades following the elucidation of the molecular constituents of the EC system that began with the serendipitous discovery of the cannabinoid 1 receptor (CB1). Since then, novel pharmacological and genetic tools have enabled researchers to manipulate select components of the EC system, to determine their contribution to the motivation to consume ethanol. From these preclinical studies, it is evident that CB1 contributes the motivational and reinforcing properties of ethanol, and chronic consumption of ethanol alters EC transmitter levels and CB1 expression in brain nuclei associated with addiction pathways. These results are augmented by in vitro and ex vivo studies showing that acute and chronic treatment with ethanol produces physiologically relevant alterations in the function of the EC system. This report provides a current and comprehensive review of the literature regarding the interactions between ethanol and the EC system. We begin be reviewing the studies published prior to the discovery of the EC system that compared the behavioral and physiological effects of cannabinoids with ethanol in addition to cross-tolerance between these drugs. Next, a brief overview of the molecular constituents of the EC system is provided as context for the subsequent review of more recent studies examining the interaction of ethanol with the EC system. These results are compiled into a summary providing a scheme for the known changes to the components of the EC system in different stages of alcohol dependence. Finally, future directions for research are discussed.

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“…Although both anandamide and 2‐AG function as reinforcers in their own right when tested in squirrel monkeys (Justinova et al,2005; Justinova et al,2011), a growing body of evidence suggests that these molecules may exert opposing effects during particular circumstances of reward‐directed behavior. Augmenting 2‐AG levels increases dopamine neurotransmission (Oleson et al,2012) and facilitates reward‐directed behavior (Gutierrez‐Lopez et al,2010; Oleson et al,2012; Wakley and Rasmussen,2009). By contrast, augmenting anandamide levels reduces the potency of cues to motivate reward‐directed behavior.…”

Section: Discussionmentioning

confidence: 99%

Paradoxical effects of the endocannabinoid uptake inhibitor VDM11 on accumbal neural encoding of reward predictive cues

Oleson

Cheer

2012

Synapse

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A growing body of evidence implicates the endocannabinoid (eCB) system in brain reward function. Previous studies show that antagonizing eCB transmission decreases reward-directed behavior and nucleus accumbens (NAc) encoding of reward predictive cues. We therefore hypothesized that elevating eCB levels would uniformly facilitate NAc neural encoding of reward predictive cues and reward-directed behavior. Contrary to our expectations, the eCB transport uptake inhibitor, VDM11, dose-dependently decreased both measures.

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Involvement of 2‐arachidonoyl glycerol in the increased consumption of and preference for ethanol of mice treated with neurotoxic doses of methamphetamine

Cited by 19 publications

References 49 publications

Distinct functions of endogenous cannabinoid system in alcohol abuse disorders

Distinct functions of endogenous cannabinoid system in alcohol abuse disorders

A review of the interactions between alcohol and the endocannabinoid system: Implications for alcohol dependence and future directions for research

Paradoxical effects of the endocannabinoid uptake inhibitor VDM11 on accumbal neural encoding of reward predictive cues

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