循环皮质酮水平介导了急性乙醇中毒与雄性大鼠 NF-κB 激活标志物之间的关系。
Circulating corticosterone levels mediate the relationship between acute ethanol intoxication and markers of NF-κB activation in male rats.
机构信息
Developmental Exposure Alcohol Research Center, Behavioral Neuroscience Program, Department of Psychology, Binghamton, NY, 13902-6000, USA.
Developmental Exposure Alcohol Research Center, Behavioral Neuroscience Program, Department of Psychology, Binghamton, NY, 13902-6000, USA.
出版信息
Neuropharmacology. 2022 Jun 1;210:109044. doi: 10.1016/j.neuropharm.2022.109044. Epub 2022 Mar 24.
Binge drinking is a harmful pattern of alcohol use that is associated with a number of serious health problems. Of particular interest are the rapid alterations in neuroimmune gene expression and the concurrent activation of the hypothalamic-pituitary-adrenal (HPA) axis activation associated with high intensity drinking. Using a rat model of acute binge-like ethanol exposure, the present studies were designed to assess the role of corticosterone (CORT) in ethanol-induced neuroimmune gene expression changes, particularly those associated with the NFκB signaling pathway, including rapid induction of IL-6 and IκBα, and suppression of IL-1β and TNFα gene expression evident after administration of moderate to high doses of ethanol (1.5-3.5 g/kg ip) during intoxication (3 h post-injection). Experiment 1 tested whether inhibition of CORT synthesis with metyrapone and aminoglutethimide (100 mg/kg each, sc) would block ethanol-induced changes in neuroimmune gene expression. Results indicated that rapid alterations in IκBα, IL-1β, and TNFα expression were completely blocked by pretreatment with the glucocorticoid synthesis inhibitors, an effect that was reinstated by co-administration of exogenous CORT (3.75 mg/kg) in Experiment 2. Experiment 3 assessed whether these rapid alterations in neuroimmune gene expression would be evident when rats were challenged with a subthreshold dose of ethanol (1.5 g/kg) in combination with 2.5 mg/kg CORT, which showed limited evidence for additive effects of low-dose CORT combined with a moderate dose of ethanol. Acute inhibition of mineralocorticoid (spironolactone) or glucocorticoid (mifepristone) receptors, alone (Experiment 4) or combined (Experiment 5) had no effect on ethanol-induced changes in neuroimmune gene expression, presumably due to poor CNS penetrance of these drugs. Finally, Experiments 6 and 7 showed that dexamethasone (subcutaneous; a GR agonist) recapitulated effects of ethanol. Overall, we conclude that ethanol-induced CORT synthesis and release is responsible for suppression of IL-1β, TNFα, and induction of IκBα in the hippocampus through GR signaling. Interventions designed to curb these changes may reduce drinking, and subdue detrimental neuroimmune activation induced by ethanol.
binge drinking 是一种与许多严重健康问题相关的有害饮酒模式。特别值得关注的是,高强度饮酒会导致神经免疫基因表达的快速改变和下丘脑-垂体-肾上腺 (HPA) 轴的激活。本研究采用急性 binge-like 乙醇暴露大鼠模型,旨在评估皮质酮 (CORT) 在乙醇诱导的神经免疫基因表达变化中的作用,特别是那些与 NFκB 信号通路相关的基因表达变化,包括在中等至高剂量乙醇(1.5-3.5 g/kg ip)给药期间,即醉酒期(注射后 3 小时),IL-6 和 IκBα 的快速诱导以及 IL-1β 和 TNFα 基因表达的抑制。实验 1 测试了用甲吡酮和氨鲁米特(100mg/kg,sc)抑制 CORT 合成是否会阻断乙醇诱导的神经免疫基因表达变化。结果表明,快速改变 IκBα、IL-1β 和 TNFα 的表达完全被糖皮质激素合成抑制剂预处理阻断,而在实验 2 中,同时给予外源性 CORT(3.75mg/kg)则恢复了这种作用。实验 3 评估了当大鼠接受亚阈值剂量乙醇(1.5 g/kg)与 2.5 mg/kg CORT 联合刺激时,这些神经免疫基因表达的快速改变是否会显现,结果表明低剂量 CORT 与中等剂量乙醇联合使用时,仅有有限的累加效应。单独(实验 4)或联合(实验 5)急性抑制盐皮质激素(螺内酯)或糖皮质激素(米非司酮)受体对乙醇诱导的神经免疫基因表达变化没有影响,这可能是由于这些药物在中枢神经系统中的穿透性较差。最后,实验 6 和 7 表明,地塞米松(皮下;GR 激动剂)再现了乙醇的作用。总体而言,我们得出结论,乙醇诱导的 CORT 合成和释放通过 GR 信号导致海马中 IL-1β、TNFα 的抑制和 IκBα 的诱导。设计用于抑制这些变化的干预措施可能会减少饮酒,并抑制乙醇诱导的有害神经免疫激活。
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