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Endocannabinoid signalling in reward and addiction
by
Hurd, Yasmin L.
, Parsons, Loren H.
in
13/56
/ 42/41
/ 42/44
/ 631/378/1457/1284
/ 631/378/1595/1554
/ 631/378/1595/2618
/ 631/378/1689/5
/ 631/378/2591/2592
/ 631/378/2629/1788
/ 64/110
/ 64/60
/ 64/86
/ 82/51
/ 96/44
/ Addictions
/ Animal Genetics and Genomics
/ Animals
/ Behavior, Addictive - psychology
/ Behavioral Sciences
/ Biological Techniques
/ Biomedicine
/ Brain - physiology
/ Brain - physiopathology
/ Brain research
/ Cellular signal transduction
/ Endocannabinoids
/ Endocannabinoids - genetics
/ Endocannabinoids - physiology
/ Enzymes
/ Fatty acids
/ Health aspects
/ Humans
/ Ligands
/ Marijuana Abuse - physiopathology
/ Neural Pathways - physiopathology
/ Neurobiology
/ Neurons
/ Neurosciences
/ Properties
/ review-article
/ Reward
/ Reward (Psychology)
/ Risk factors
/ Signal Transduction - genetics
/ Signal Transduction - physiology
/ Substance abuse
2015
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Endocannabinoid signalling in reward and addiction
by
Hurd, Yasmin L.
, Parsons, Loren H.
in
13/56
/ 42/41
/ 42/44
/ 631/378/1457/1284
/ 631/378/1595/1554
/ 631/378/1595/2618
/ 631/378/1689/5
/ 631/378/2591/2592
/ 631/378/2629/1788
/ 64/110
/ 64/60
/ 64/86
/ 82/51
/ 96/44
/ Addictions
/ Animal Genetics and Genomics
/ Animals
/ Behavior, Addictive - psychology
/ Behavioral Sciences
/ Biological Techniques
/ Biomedicine
/ Brain - physiology
/ Brain - physiopathology
/ Brain research
/ Cellular signal transduction
/ Endocannabinoids
/ Endocannabinoids - genetics
/ Endocannabinoids - physiology
/ Enzymes
/ Fatty acids
/ Health aspects
/ Humans
/ Ligands
/ Marijuana Abuse - physiopathology
/ Neural Pathways - physiopathology
/ Neurobiology
/ Neurons
/ Neurosciences
/ Properties
/ review-article
/ Reward
/ Reward (Psychology)
/ Risk factors
/ Signal Transduction - genetics
/ Signal Transduction - physiology
/ Substance abuse
2015
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Endocannabinoid signalling in reward and addiction
by
Hurd, Yasmin L.
, Parsons, Loren H.
in
13/56
/ 42/41
/ 42/44
/ 631/378/1457/1284
/ 631/378/1595/1554
/ 631/378/1595/2618
/ 631/378/1689/5
/ 631/378/2591/2592
/ 631/378/2629/1788
/ 64/110
/ 64/60
/ 64/86
/ 82/51
/ 96/44
/ Addictions
/ Animal Genetics and Genomics
/ Animals
/ Behavior, Addictive - psychology
/ Behavioral Sciences
/ Biological Techniques
/ Biomedicine
/ Brain - physiology
/ Brain - physiopathology
/ Brain research
/ Cellular signal transduction
/ Endocannabinoids
/ Endocannabinoids - genetics
/ Endocannabinoids - physiology
/ Enzymes
/ Fatty acids
/ Health aspects
/ Humans
/ Ligands
/ Marijuana Abuse - physiopathology
/ Neural Pathways - physiopathology
/ Neurobiology
/ Neurons
/ Neurosciences
/ Properties
/ review-article
/ Reward
/ Reward (Psychology)
/ Risk factors
/ Signal Transduction - genetics
/ Signal Transduction - physiology
/ Substance abuse
2015
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Journal Article
Endocannabinoid signalling in reward and addiction
2015
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Overview
Key Points
Cannabinoid receptors and their endogenous ligands are widely expressed throughout the brain, with a particularly strong presence and influence in neuronal circuits such as the mesocorticolimbic pathways highly implicated in reward and addiction.
Cannabinoid 1 receptor (CB1R) signalling influences the motivation for both natural and drug rewards. In comparison to most drugs of abuse, CB1Rs exert only modest influence on psychostimulant intake.
Brain endocannabinoid (eCB) levels are increased by most drugs of abuse, although the nature of this effect differs between classes of drugs and across brain regions. The response contingency of drug exposure (volitional versus response-independent) seems to influence brain eCB production, suggesting contributions both of drug-related pharmacological effects and of neural activity engaged by active drug-seeking behaviour.
Chronic exposure to drugs of abuse generally results in impaired CB1R function, loss of eCB-mediated synaptic plasticity in addiction-related neural circuits, and negative affective states that can be ameliorated through pharmacologically enhanced eCB tone. The eCB system (ECS) has a strong role in modulating relapse-like behaviour induced by conditioned cues or reward priming, and this is evident for both natural and drug rewards.
Recent investigations of
CNR1
(which encodes CB1R) and fatty acid amide hydrolase (
FAAH
) variants generally suggest an association with endophenotypes implicated in addiction susceptibility, including reward sensitivity, impulsivity and negative affect. However, confounding factors, including restricted sample size, ethnicity and polysubstance use, limit interpretational power, and the functional consequences of the variants (causal or linked) are currently unknown.
Cannabinoid receptors and their endogenous ligands, the endocannabinoids, are widely expressed in the brain, particularly in regions that are implicated in mediating reward. In this Review, Parsons and Hurd explore the role of endocannabinoid signalling in natural and drug-induced reward, as well as in addiction.
Brain endocannabinoid (eCB) signalling influences the motivation for natural rewards (such as palatable food, sexual activity and social interaction) and modulates the rewarding effects of addictive drugs. Pathological forms of natural and drug-induced reward are associated with dysregulated eCB signalling that may derive from pre-existing genetic factors or from prolonged drug exposure. Impaired eCB signalling contributes to dysregulated synaptic plasticity, increased stress responsivity, negative emotional states and cravings that propel addiction. Understanding the contributions of eCB disruptions to behavioural and physiological traits provides insight into the eCB influence on addiction vulnerability.
Publisher
Nature Publishing Group UK,Nature Publishing Group
Subject
/ 42/41
/ 42/44
/ 64/110
/ 64/60
/ 64/86
/ 82/51
/ 96/44
/ Animal Genetics and Genomics
/ Animals
/ Behavior, Addictive - psychology
/ Cellular signal transduction
/ Endocannabinoids - physiology
/ Enzymes
/ Humans
/ Ligands
/ Marijuana Abuse - physiopathology
/ Neural Pathways - physiopathology
/ Neurons
/ Reward
/ Signal Transduction - genetics
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