The genetic versus pharmacological invalidation of the cannabinoid CB1 receptor results in differential effects on ‘non-associative’ memory and forebrain monoamine concentrations in mice

Thiemann, Gunnar; Fletcher, Ben; Ledent, Catherine; Molleman, Areles; Hasenöhrl, Rüdiger U.

doi:10.1016/j.nlm.2007.07.013

Cited by 11 publications

(5 citation statements)

References 33 publications

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“…Several studies reported increased anxiety-related behaviors after impaired CB1R signaling only when aversive stimulus cannot be avoided (Haller et al, 2004, 2009; Thiemann et al, 2007; Kamprath et al, 2009). However, little is known about how ECS modulation of the DAergic system could be involved in this effect.…”

Section: Discussionmentioning

confidence: 99%

The Dopamine and Cannabinoid Interaction in the Modulation of Emotions and Cognition: Assessing the Role of Cannabinoid CB1 Receptor in Neurons Expressing Dopamine D1 Receptors

Terzian

Drago

Wotjak

et al. 2011

Front. Behav. Neurosci.

113

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Although cannabinoid CB1 receptors (CB1Rs) are densely expressed in neurons expressing dopamine D1 receptors (D1Rs), it is not fully understood to what extent they modulate emotional behaviors. We used conditional CB1R knock-out animals lacking CB1Rs in neurons expressing D1R (D1–CB1−/−) in order to answer this question. To elucidate the behavioral effects of CB1R deficiency in this specific neuronal subpopulation, we subjected D1–CB1−/− mice to a battery of behavioral tests which included exploration-based tests, depressive-like behavioral tests, social behavior, and fear-related memory paradigms. D1–CB1−/− did not show any difference in the exploration-based paradigms such as open field, elevated plus maze, or novel object investigation test, except for an increase in novelty-induced grooming. By contrast, they showed a mild anhedonia-like state as described by the slightly decreased preference for sweet solution, as compared to wild-type control group. This decrease, however, could be observed only during the first day of exposure, thus suggesting increased neophobia as an alternative explanation. Accordingly, mutant mice performed normally in the forced swim test, a procedure widely used for evaluating behavioral despair in rodents. However, weak- to moderate anxiety-like phenotypes were evident when D1–CB1−/− mice were tested for social behavior. Most strikingly, D1–CB1−/− mice exhibited significantly increased contextual and auditory-cued fear, with attenuated within session extinction, suggesting that a specific reduction of endocannabinoid signaling in neurons expressing dopamine D1Rs is able to affect acute fear adaptation. These results provided first direct evidence for a cross-talk between dopaminergic D1Rs and endocannabinoid system in terms of controlling negative affect.

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Section: Discussionmentioning

confidence: 99%

The Dopamine and Cannabinoid Interaction in the Modulation of Emotions and Cognition: Assessing the Role of Cannabinoid CB1 Receptor in Neurons Expressing Dopamine D1 Receptors

Terzian

Drago

Wotjak

et al. 2011

Front. Behav. Neurosci.

113

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“…Consequently, there is the option that endocannabinoids modulate one-trial sensitization via their influence on memory processes (Riedel & Davies 2005). Attenuated CB1 signalling seems to coincide, among others, with increased short-term (Degroot et al 2005) and long-term habituation (Thiemann et al 2007) to an open field. Our data partially support these observations: Total-CB1-KO showed pronounced within-exposure habituation in the open field under bright light, but no differences to wild-type controls Genes, Brain and Behavior (2009) 8: 685-698 in between-exposure habituation.…”

Section: Discussionmentioning

confidence: 99%

“…Experiments were performed with mice lacking CB1 expression in the entire body (Total‐CB1‐KO; Marsicano et al 2002) or specifically in glutamatergic cortical neurons (CB 1 f/f;Nex−Cre = Glu‐CB1‐KO; Monory et al 2006). Because the endocannabinoid system was shown to mediate habituation to homotypic stressors (Patel et al 2005; Patel & Hillard 2008), including adaptation to aversive tones (Kamprath et al 2006), and to play a particular role during re‐exposure to exploration‐based anxiety tests, such as the elevated plus‐maze test (Rodgers et al 2005) and the open field test (Thiemann et al 2007), we additionally studied the consequences of repeated testing (i.e. familiarity) for test situations with avoidable (elevated plus‐maze) or unavoidable (open field) light exposure.…”

mentioning

confidence: 99%

Endocannabinoids render exploratory behaviour largely independent of the test aversiveness: role of glutamatergic transmission

Jacob

Yassouridis

Marsicano

et al. 2009

Genes Brain and Behavior

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To investigate the impact of averseness, controllability and familiarity of a test situation on the involvement of the endocannabinoid system in the regulation of exploratory behaviour, we tested conventional and conditional cannabinoid receptor type 1 (CB1)-deficient mice in behavioural paradigms with different emotional load, which depended on the strength of illumination and the ability of the animals to avoid the light stimulus. Complete CB1 null-mutant mice (Total-CB1-KO) showed an anxiogenic-like phenotype under circumstances where they were able to avoid the bright light such as the elevated plus-maze and the light/dark avoidance task. Conditional mutant mice lacking CB1 expression specifically in cortical glutamatergic neurons (Glu-CB1-KO), in contrast, failed to show a similar phenotype under the same experimental conditions. However, both mutant lines showed increased avoidance of open arm exploration during a second exposure to the elevated plus-maze. If tested in situations where the fear eliciting light could not be avoided, Total-CB1-KO mice showed increased thigmotaxis in an open field, decreased social investigation and decreased novel object exploration under aversive light conditions, but not under non-aversive low light. This time, Glu-CB1-KO also showed decreased exploratory behaviour towards objects and conspecific juveniles and increased thigmotaxis in the open field. Taking into consideration that the behavioural performance of wild-type mice was only marginally affected by changes in light intensities, these data indicate that the endocannabinoid system renders exploratory behaviour largely independent of the test averseness. This process differentially involves endocannabinoid-controlled glutamatergic transmission, depending on the controllability of the test situation.

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“…The fact that these effects were blocked by the administration of CB 1 r-antagonist, SR141716A, supports CB 1 r as being the target involved in the acute effects of cannabinoids on memory impairments (Da and Takahashi, 2002;Pamplona and Takahashi, 2006). Interestingly, pharmacological or genetic disruption of CB 1 r signaling enhances learning and memory in a variety of spatial and operant paradigms (Thiemann et al, 2007). Further studies revealed the modulation of GABA neurotransmission through the activation of CB 1 r located on GABA interneurons, the indirect activation of the mammalian target of rapamycin (mTOR)/70-kDa ribosomal protein S6 kinase (p70S6K) signaling cascade and NMDA receptors as the main mechanisms underlying the cognitive impairments produced by cannabinoids (Puighermanal et al, 2009).…”

Section: Introductionmentioning

confidence: 93%

Synaptic plasticity alterations associated with memory impairment induced by deletion of CB2 cannabinoid receptors

et al. 2013

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The genetic versus pharmacological invalidation of the cannabinoid CB1 receptor results in differential effects on ‘non-associative’ memory and forebrain monoamine concentrations in mice

Cited by 11 publications

References 33 publications

The Dopamine and Cannabinoid Interaction in the Modulation of Emotions and Cognition: Assessing the Role of Cannabinoid CB1 Receptor in Neurons Expressing Dopamine D1 Receptors

The Dopamine and Cannabinoid Interaction in the Modulation of Emotions and Cognition: Assessing the Role of Cannabinoid CB1 Receptor in Neurons Expressing Dopamine D1 Receptors

Endocannabinoids render exploratory behaviour largely independent of the test aversiveness: role of glutamatergic transmission

Synaptic plasticity alterations associated with memory impairment induced by deletion of CB2 cannabinoid receptors

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