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Negative Affect and Excessive Alcohol Intake Incubate during Protracted Withdrawal from Binge-Drinking in Adolescent, But Not Adult, Mice

机译:青少年从暴饮暴食中长期戒断期间的负面影响和过度饮酒,但未成年小鼠

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Binge-drinking is common in underage alcohol users, yet we know little regarding the biopsychological impact of binge-drinking during early periods of development. Prior work indicated that adolescent male C57BL6/J mice with a 2-week history of binge-drinking (PND28-41) are resilient to the anxiogenic effects of early alcohol withdrawal. Herein, we employed a comparable Drinking-in-the-Dark model to determine how a prior history of binge-drinking during adolescence (EtOHadolescents) influences emotionality (assayed with the light-dark box, marble burying test, and the forced swim test) and the propensity to consume alcohol in later life, compared to animals without prior drinking experience. For additional comparison, adult mice (EtOHadults) with comparable drinking history (PND56-69) were subdivided into groups tested for anxiety/drinking either on PND70 (24 h withdrawal) or PND98 (28 days withdrawal). Tissue from the nucleus accumbens shell (AcbSh) and central nucleus of the amygdala (CeA) was examined by immunoblotting for changes in the expression of glutamate-related proteins. EtOHadults exhibited some signs of hyperanxiety during early withdrawal (PND70), but not during protracted withdrawal (PND98). In contrast, EtOHadolescents exhibited robust signs of anxiety-l and depressive-like behaviors when tested as adults on PND70. While all alcohol-experienced animals subsequently consumed more alcohol than mice drinking for the first time, alcohol intake was greatest in EtOHadolescents. Independent of drinking age, the manifestation of withdrawal-induced hyperanxiety was accompanied by reduced Homer2b expression within the CeA and increased Group1 mGlu receptor expression within the AcbSh. The present data provide novel evidence that binge-drinking during adolescence produces a state characterized by profound negative affect and excessive alcohol consumption that incubates with the passage of time in withdrawal. These data extend our prior studies on the effects of subchronic binge-drinking during adulthood by demonstrating that the increase in alcoholism-related behaviors and glutamate-related proteins observed in early withdrawal dissipate with the passage of time. Our results to date highlight a critical interaction between the age of binge-drinking onset and the duration of alcohol withdrawal in glutamate-related neuroplasticity within the extended amygdala of relevance to the etiology of psychopathology, including pathological drinking, in later life.
机译:暴饮暴食在未成年饮酒者中很普遍,但是我们对暴饮暴食在发育早期对生物心理的影响知之甚少。先前的工作表明,有2周暴饮暴食史(PND28-41)的青春期雄性C57BL6 / J小鼠对早期戒酒的焦虑作用具有抵抗力。在本文中,我们采用了类似的“黑暗中饮酒”模型来确定青春期(EtOH青少年)暴饮暴食的既往史如何影响情绪(通过浅色暗箱,大理石掩埋测试和强迫游泳测试进行分析)与没有饮酒经验的动物相比,在以后的生活中容易饮酒。为了进一步比较,将具有相似饮酒史(PND56-69)的成年小鼠(EtOHadults)分为PND70(戒断24小时)或PND98(戒断28天)进行焦虑/饮酒测试的组。通过免疫印迹检查伏隔核壳(AcbSh)和杏仁核中央核(CeA)的组织中谷氨酸相关蛋白表达的变化。 EtOH成人在早期戒断期间(PND70)表现出一些焦虑感,而在长期戒断期间(PND98)则没有。相反,当在PND70上成人测试时,EtOH青少年表现出强烈的焦虑-1和抑郁样行为迹象。尽管所有有酒精经验的动物随后的饮酒量都比第一次饮酒的小鼠要多,但酒精摄入量在EtOH青少年中最大。与饮酒年龄无关,戒断诱发的过度焦虑的表现伴随着CeA内Homer2b表达的减少和AcbSh内Group1 mGlu受体表达的增加。目前的数据提供了新颖的证据,表明青春期的暴饮暴食会产生一种以深刻的负面影响和过量的酒精消耗为特征的状态,随着戒断时间的流逝,这种状态会逐渐加剧。这些数据证明了在早期戒断中观察到的酒精中毒相关行为和谷氨酸相关蛋白的增加会随着时间的流逝而消失,从而扩展了我们对成年期亚慢性暴饮酒影响的先前研究。迄今为止,我们的结果突显了暴饮暴食的年龄与酒精中毒后谷氨酸相关的神经可塑性中的谷氨酸相关的神经可塑性持续时间之间的关键相互作用,杏仁核与心理病理学的病因(包括病理性饮酒)在以后的生活中有关。

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