共 96 条
Cannabidiol inhibits sucrose self-administration by CB1 and CB2 receptor mechanisms in rodents
被引:36
作者:

Bi, Guo-Hua
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机构:
NIDA, Addict Biol Unit, Mol Targets & Medicat Discoveries Branch, Intramural Res Program, Baltimore, MD 21224 USA NIDA, Addict Biol Unit, Mol Targets & Medicat Discoveries Branch, Intramural Res Program, Baltimore, MD 21224 USA

Galaj, Ewa
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h-index: 0
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NIDA, Addict Biol Unit, Mol Targets & Medicat Discoveries Branch, Intramural Res Program, Baltimore, MD 21224 USA NIDA, Addict Biol Unit, Mol Targets & Medicat Discoveries Branch, Intramural Res Program, Baltimore, MD 21224 USA

He, Yi
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h-index: 0
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NIDA, Addict Biol Unit, Mol Targets & Medicat Discoveries Branch, Intramural Res Program, Baltimore, MD 21224 USA NIDA, Addict Biol Unit, Mol Targets & Medicat Discoveries Branch, Intramural Res Program, Baltimore, MD 21224 USA

Xi, Zheng-Xiong
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h-index: 0
机构:
NIDA, Addict Biol Unit, Mol Targets & Medicat Discoveries Branch, Intramural Res Program, Baltimore, MD 21224 USA NIDA, Addict Biol Unit, Mol Targets & Medicat Discoveries Branch, Intramural Res Program, Baltimore, MD 21224 USA
机构:
[1] NIDA, Addict Biol Unit, Mol Targets & Medicat Discoveries Branch, Intramural Res Program, Baltimore, MD 21224 USA
关键词:
cannabidiol;
cannabinoid;
CB1;
receptor;
CB2;
feeding behavior;
sucrose self-administration;
DOPAMINE SYSTEM IMPLICATIONS;
FOOD-INTAKE;
ALLOSTERIC MODULATOR;
ENDOCANNABINOID SYSTEM;
INTERVAL PERFORMANCE;
BRAIN;
CANNABINOIDS;
ANANDAMIDE;
APPETITE;
MICE;
D O I:
10.1111/adb.12783
中图分类号:
Q5 [生物化学];
Q7 [分子生物学];
学科分类号:
071010 ;
081704 ;
摘要:
A growing number of studies suggest therapeutic applications of cannabidiol (CBD), a recently U.S. Food and Drug Administration (FDA)-approved medication for epilepsy, in treatment of many other neuropsychological disorders. However, pharmacological action and the mechanisms by which CBD exerts its effects are not fully understood. Here, we examined the effects of CBD on oral sucrose self-administration in rodents and explored the receptor mechanisms underlying CBD-induced behavioral effects using pharmacological and transgenic approaches. Systemic administration of CBD (10, 20, and 40 mg/kg, ip) produced a dose-dependent reduction in sucrose self-administration in rats and in wild-type (WT) and CB1(-/-) mice but not in CB2(-/-) mice. CBD appeared to be more efficacious in CB1(-/-) mice than in WT mice. Similarly, pretreatment with AM251, a CB1R antagonist, potentiated, while AM630, a selective CB2R antagonist, blocked CBD-induced reduction in sucrose self-administration, suggesting the involvement of CB1 and CB2 receptors. Furthermore, systemic administration of JWH133, a selective CB2R agonist, also produced a dose-dependent reduction in sucrose self-administration in WT and CB1(-/-) mice, but not in CB2(-/-) mice. Pretreatment with AM251 enhanced, while AM630 blocked JWH133-induced reduction in sucrose self-administration in WT mice, suggesting that CBD inhibits sucrose self-administration likely by CB1 receptor antagonism and CB2 receptor agonism. Taken together, the present findings suggest that CBD may have therapeutic potential in reducing binge eating and the development of obesity.
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