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首页> 外文期刊>Neuropharmacology >Exposure to cannabinoid agonist WIN 55,212-2 during early adolescence increases alcohol preference and anxiety in CD1 mice
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Exposure to cannabinoid agonist WIN 55,212-2 during early adolescence increases alcohol preference and anxiety in CD1 mice

机译:暴露于大麻激动剂赢得55,212-2在青春期期间增加了CD1小鼠的酒精偏好和焦虑

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摘要

The endocannabinoid (eCB) system is involved in the modulation of the reward system and participates in the reinforcing effects of different drugs of abuse, including alcohol. The most abundant receptor of the eCB system in the central nervous system is the CB1 receptor (CB1R), which is predominantly expressed in areas involved in drug addiction, such as the nucleus accumbens, the ventral tegmental area, the substantia nigra and the raphe nucleus. CB1R is expressed in early stages during development, and reaches maximum levels during early adolescence. In addition, cannabinoid receptor 2 has been found expressed also in the central nervous system at postsynaptic level. In order to analyze the participation of the eCB system on ethanol (EtOH) preference, mice were exposed to cannabinoid agonist WIN 55,212-2 (WIN) for 5 consecutive days during early adolescence. Anxiety tests were performed the day after WIN treatment withdrawal, and EtOH preference was measured throughout adolescence. Mice exposed to WIN during early adolescence exhibited a significant increase in EtOH intake and preference after treatment. Moreover, WIN exposure during early adolescence induced an anxiogenic effect. Morphometric analysis revealed higher dendritic ramifications and fewer dendritic spines in neurons of the substantia nigra pars compacta in WIN-treated mice. On the other hand, immunohistochemical analysis revealed an increase in the number of tryptophan hydroxylase-expressing neurons in the dorsal raphe nucleus but no differences were found in the ventral tegmental area or substantia nigra pars compacta for tyrosine hydroxylase-expressing neurons. These results demonstrate that exposure to WIN in early adolescence can affect neural development and induce alcohol preference and anxiety-like behavior during late adolescence. (C) 2018 Elsevier Ltd. All rights reserved.
机译:EndoCannabinoid(ECB)系统参与了奖励系统的调制,并参与不同滥用药物的增强效果,包括酒精。中枢神经系统中ECB系统中最丰富的受体是CB1受体(CB1R),其主要在参与药物成瘾的地区,例如核心腺,腹侧腹部,基础,真主NIGRA和Raphe核心。 CB1R在发育期间的早期阶段表达,在青春期早期达到最大水平。此外,在突触水平的中枢神经系统中发现大麻素受体2已经发现。为了分析ECB系统对乙醇(ETOH)偏好的参与,在早期青春期连续5天将小鼠暴露于大麻素激动剂赢得55,212-2(Win)。焦虑测试在赢取治疗脱离后的一天进行,并在整个青春期测量EtOH偏好。暴露于青春期期间的小鼠在治疗后的EtOH摄入和偏好显着增加。此外,在青春期早期源于焦虑效应的终止造成焦虑作用。形态学分析显示在基础上的小鼠中的神经元中的神经元中的树突状肾脏和较少的树突刺。另一方面,免疫组织化学分析表明,背部拉皮核中表达色氨酸羟化酶的数量增加,但在腹侧脑结构区域或基础菌氏菌对酪氨酸羟化酶的神经元中没有发现差异。这些结果表明,早期青春期的胜利暴露会影响神经发育,并且在晚期青春期期间诱导醇偏好和焦虑的行为。 (c)2018年elestvier有限公司保留所有权利。

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