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Gender differences in the effects of cannabidiol on ethanol binge drinking in mice

机译:大麻大麻对小鼠乙醇狂欢饮用作用的性别差异

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Abstract The purpose of this study was to explore the effects of cannabidiol (CBD) on binge drinking and evaluate potential gender‐related differences. To this aim, male and female C57BL/6J mice (n?=?60 per sex) were exposed to the drinking in the dark (DID) model for 4?weeks (DID‐1 to DID‐4). Dose‐response effects of CBD on the ethanol intake were tested by acute (day‐4 of DID‐3) or repeated administration (day‐1 to 4 of DID‐4) (experiment 1: CBD 15, 30, and 60?mg/kg, i.p.; experiment 2: CBD 90?mg/kg, i.p.). Finally, we analyzed the relative gene expression of tyrosine hydroxylase ( TH ) and μ‐opioid receptor ( OPRM1 ) and cannabinoid CB1 receptor ( CB 1 r ) in the ventral tegmental area (VTA) and in the nucleus accumbens (NAc), respectively, by real‐time quantitative PCR. Females exhibited higher ethanol intake during each DID session. Interestingly, females also showed higher expression of TH and OPRM1 , without any difference in CB 1 r . Only the acute administration of CBD at the highest dose (90?mg/kg) reduced significantly ethanol consumption in both sexes. Chronic CBD administration (30, 60 and 90?mg/kg) reduced ethanol intake in males, whereas in females a significant reduction was only achieved with the highest dose (90?mg/kg). Repeated administration with CBD (60?mg/kg) significantly reduced TH and OPRM1 in males. In addition, CBD (30 and 60?mg/kg) significantly reduced CB 1 r in males. No effect was observed in females. Taken together, these findings suggest that CBD may be of interest for treating binge‐drinking patterns and that gender‐related difference may affect the treatment outcome.
机译:摘要本研究的目的是探讨Cannabidiol(CBD)对狂犬病饮酒和评估潜在性别相关差异的影响。对于这种目的,男性和雌性C57BL / 6J小鼠(N?=?60次)暴露在黑暗(DID)模型中的饮酒4?周(DID-1 DO-4)。 CBD对乙醇摄入量的剂量 - 反应效应通过急性(DID-3)或重复给药(DID-4日 - 4日 - 4日)(实验1:CBD 15,30和60μmG /千克,IP;实验2:CBD 90?Mg / kg,IP)。最后,我们分析了翼霉菌羟化酶(TH)和μ-ApiOID受体(OPRM1)和大麻素CB1受体(CB 1 R)的相对基因表达,分别在腹侧腹部区域(VTA)和核心宫内(NAC)中,通过实时定量PCR。女性在每次会议期间表现出更高的乙醇摄入量。有趣的是,女性也表现出更高的TH和OPRM1的表达,而没有任何CB 1 R的差异。只有在最高剂量(90×mg / kg)处只有急性癌症的急性施用在两性中的乙醇消耗明显减少。慢性CBD施用(30,60和90×mg / kg)降低乙醇的雌性摄入量,而在雌性中,仅通过最高剂量(90μmg/ kg)实现显着的减少。重复施用CBD(60?Mg / kg)显着减少了雄性中的TH和OPRM1。此外,CBD(30和60×mg / kg)显着降低了雄性的Cb 1 r。女性没有效果。这些发现结合在一起,表明CBD可能对治疗狂暴饮酒模式感兴趣,并且性别相关差异可能会影响治疗结果。

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