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青春期 CB1 受体拮抗和应激暴露对大鼠社会情感行为、神经内分泌应激反应以及海马和前额叶皮质相关蛋白表达的影响。

Effects of CB1 receptor antagonism and stress exposures in adolescence on socioemotional behaviours, neuroendocrine stress responses, and expression of relevant proteins in the hippocampus and prefrontal cortex in rats.

机构信息

Department of Biological Sciences, Brock University, 1812 Sir Isaac Brock Way, St. Catharines, Ontario L2S 3A1, Canada.

Department of Psychology, Brock University, 1812 Sir Isaac Brock Way, St. Catharines, Ontario L2S 3A1, Canada.

出版信息

Neuropharmacology. 2018 Jan;128:433-447. doi: 10.1016/j.neuropharm.2017.10.029. Epub 2017 Oct 29.

DOI:10.1016/j.neuropharm.2017.10.029
PMID:29092785
Abstract

Little is known about the consequences of altered endocannabinoid signalling in adolescence. We hypothesized that CB1 receptor antagonism (AM251, 1 mg/kg) and stress exposures (1 h confinement stress) in adolescence (daily, postnatal days 30-44) would interact to increase neuroendocrine stress responses and anxiety when investigated a minimum of 24 h after drug and stress treatments; these treatment effects were independent of each other. Changes in homecage behaviour and in weight gain confirmed that both males and females were sensitive to the treatments. Nevertheless, in males, repeated AM251 administration was without effect on any of the measures investigated in days post-treatment. Males had reduced corticosterone release to the repeated stress and had increased GAD67 expression in the ventral hippocampus under baseline conditions. In females, AM251 also reduced weight gain and increased stereotypic behaviours in the homecage; these same females showed increased sociality, reduced CB1 receptor expression in the dorsal hippocampus, and increased GAD67 expression in the prefrontal cortex. Further, females exposed to repeated stress had enhanced recovery to baseline corticosterone concentrations after stress. The inclusion of a non-injected comparison group also revealed stress of injection effects in both sexes that otherwise would have been masked. Together, the findings demonstrate effects of CB1 receptor antagonism and stress that were more evident in females than males, suggesting that females may be more vulnerable to the consequences of disrupted endocannabinoid signalling during adolescence.

摘要

关于青春期内内源性大麻素信号改变的后果知之甚少。我们假设 CB1 受体拮抗剂(AM251,1mg/kg)和应激暴露(1 小时禁闭应激)在青春期(每日,出生后第 30-44 天)会相互作用,增加神经内分泌应激反应和焦虑,至少在药物和应激处理后 24 小时进行调查;这些治疗效果是相互独立的。笼内行为和体重增加的变化证实,雄性和雌性都对这些治疗敏感。然而,在雄性中,重复给予 AM251 对处理后任何一天的任何措施都没有影响。雄性对重复应激的皮质酮释放减少,并且在基线条件下腹侧海马体中的 GAD67 表达增加。在雌性中,AM251 还减少体重增加和增加刻板行为在笼内;这些相同的雌性表现出增加的社交性,减少背侧海马体中的 CB1 受体表达,和增加前额叶皮层中的 GAD67 表达。此外,暴露于重复应激的雌性在应激后皮质酮浓度恢复到基线时有增强。包括非注射对照组也揭示了两性中注射应激的影响,否则这些影响会被掩盖。总之,这些发现表明 CB1 受体拮抗剂和应激的影响在雌性中比雄性中更为明显,这表明女性在青春期内内源性大麻素信号中断的后果中可能更为脆弱。

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