大麻素 1 型受体中性拮抗剂可减少 binge-like 酒精消费和酒精引起的伏隔核多巴胺能信号。
Cannabinoid-1 receptor neutral antagonist reduces binge-like alcohol consumption and alcohol-induced accumbal dopaminergic signaling.
机构信息
Department of Neurochemistry, Nathan Kline Institute for Psychiatric Research, Orangeburg, New York, NY, United States.
Division of Analytical Psychopharmacology, Nathan Kline Institute for Psychiatric Research, Orangeburg, New York, NY, United States.
出版信息
Neuropharmacology. 2018 Mar 15;131:200-208. doi: 10.1016/j.neuropharm.2017.10.040. Epub 2017 Nov 3.
Abstract
Binge alcohol (ethanol) drinking is associated with profound adverse effects on our health and society. Rimonabant (SR141716A), a CB1 receptor inverse agonist, was previously shown to be effective for nicotine cessation and obesity. However, studies using rimonabant were discontinued as it was associated with an increased risk of depression and anxiety. In the present study, we examined the pharmacokinetics and effects of AM4113, a novel CB1 receptor neutral antagonist on binge-like ethanol drinking in C57BL/6J mice using a two-bottle choice drinking-in-dark (DID) paradigm. The results indicated a slower elimination of AM4113 in the brain than in plasma. AM4113 suppressed ethanol consumption and preference without having significant effects on body weight, ambulatory activity, preference for tastants (saccharin and quinine) and ethanol metabolism. AM4113 pretreatment reduced ethanol-induced increase in dopamine release in nucleus accumbens. Collectively, these data suggest an important role of CB1 receptor-mediated regulation of binge-like ethanol consumption and mesolimbic dopaminergic signaling, and further points to the potential utility of CB1 neutral antagonists for the treatment of binge ethanol drinking.
摘要
binge 饮酒(乙醇)与我们的健康和社会的深远负面影响有关。利莫那班(SR141716A),一种 CB1 受体反向激动剂,以前被证明对戒烟和肥胖有效。然而,由于利莫那班与抑郁和焦虑风险增加有关,因此使用利莫那班的研究被停止。在本研究中,我们使用双瓶选择暗饮(DID)范式,在 C57BL/6J 小鼠中检查了新型 CB1 受体中性拮抗剂 AM4113 对 binge 样乙醇饮用量的药代动力学和影响。结果表明,AM4113 在大脑中的消除速度比在血浆中慢。AM4113 抑制乙醇消耗和偏好,而对体重、活动能力、对味觉剂(糖精和奎宁)和乙醇代谢的偏好没有显著影响。AM4113 预处理可减少乙醇诱导的伏隔核多巴胺释放增加。总之,这些数据表明 CB1 受体介导的调节 binge 样乙醇消耗和中脑边缘多巴胺信号的重要作用,并进一步表明 CB1 中性拮抗剂在治疗 binge 乙醇饮用量方面的潜在用途。
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