National Institute for Health and Welfare, Helsinki, Finland.
Alcohol Clin Exp Res. 2009 Oct;33(10):1711-20. doi: 10.1111/j.1530-0277.2009.01008.x. Epub 2009 Jul 1.
The central nervous system cannabinoid CB1 receptors have been implicated in regulation of alcohol consumption. Less data are available on the role of the endogenous ligands for these receptors, anandamide (AEA) and 2-arachidonoylglycerol (2-AG), in alcohol-related behaviors. The purpose of this study was to assess the effects of voluntary alcohol consumption on the levels of these endocannabinoids in key brain areas mediating alcohol reinforcement.
Female and male alcohol-preferring AA (Alko, Alcohol) rats were trained to drink 10% (v/v) alcohol during 90-min limited access sessions every second day. Following establishment of stable alcohol drinking, half of the subjects were killed immediately before the daily alcohol access ("pre-session" group), while the other half was killed after the drinking session ("post-session" group). A separate control group consisted of water-drinking rats. AEA and 2-AG levels were measured from prefrontal cortex (PFC), nucleus accumbens (NAc), caudate putamen (CPu), amygdala, and hippocampus using liquid chromatography-tandem mass spectrometry (LC/MS/MS).
Voluntary alcohol drinking caused widespread alterations in the levels of both AEA and 2-AG. Compared to the water group, increased AEA levels were seen in the pre-session group, but they were decreased immediately following limited access drinking in the female AA rats. Also 2-AG levels were significantly elevated after long alcohol exposure, and an additional increase was found after limited access drinking in PFC. In males, however, the only alterations caused by alcohol drinking were significantly elevated AEA levels in NAc and CPu in the post-session group. No changes were seen in the levels of 2-AG.
These results demonstrate that voluntary alcohol drinking modulates the levels of endocannabinoids in several brain areas implicated in alcohol reinforcement. AEA and 2-AG were differentially affected, suggesting that they could have partially separate modulatory roles. Alterations were more widespread in females than males, possibly reflecting their higher alcohol intake. Taken together, alcohol-induced release of endocannabinoids may have an important role in alcohol reinforcement and development of alcohol addiction.
中枢神经系统大麻素 CB1 受体参与了酒精消费的调节。关于这些受体的内源性配体,即花生四烯酸乙醇胺(AEA)和 2-花生四烯酸甘油(2-AG),在与酒精相关的行为中的作用的数据较少。本研究的目的是评估自愿饮酒对调节酒精强化的关键脑区中这些内源性大麻素水平的影响。
将雌性和雄性酒精偏好 AA(Alko,酒精)大鼠在每天 90 分钟的有限接触时段内接受 10%(v/v)酒精训练。在稳定饮酒后,一半的大鼠在每日酒精接触前立即被处死(“预接触”组),而另一半在饮酒后被处死(“接触后”组)。另一组为饮水大鼠的对照组。使用液相色谱-串联质谱法(LC/MS/MS)从前额叶皮质(PFC)、伏隔核(NAc)、尾壳核(CPu)、杏仁核和海马体中测量 AEA 和 2-AG 的水平。
自愿饮酒导致 AEA 和 2-AG 的水平广泛改变。与水组相比,预接触组大鼠的 AEA 水平升高,但在雌性 AA 大鼠进行有限接触饮酒后立即降低。此外,2-AG 水平在长期酒精暴露后显著升高,在 PFC 进行有限接触饮酒后进一步升高。然而,在雄性大鼠中,仅在接触后组中观察到酒精饮引起的 NAc 和 CPu 中 AEA 水平的显著升高。2-AG 水平没有变化。
这些结果表明,自愿饮酒调节了几个与酒精强化有关的脑区中内源性大麻素的水平。AEA 和 2-AG 受到不同程度的影响,表明它们可能具有部分分离的调节作用。女性的变化比男性更广泛,这可能反映了她们更高的酒精摄入量。总的来说,内源性大麻素的酒精诱导释放可能在酒精强化和酒精成瘾的发展中发挥重要作用。
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