青少年酒精会破坏孤束核中去甲肾上腺素能神经元的发育,并以性别特异性的方式增强成年小鼠的应激行为

Liz A. Aguilar , Caitlin R. Coker , Zari McCullers , Alexandra Evans , Opeyemi Showemimo , Mariam Melkumyan , Bailey N. Keller , Angela E. Snyder , Sarah S. Bingaman , Patrick A. Randall , Andras Hajnal , Kirsteen N. Browning , Amy C. Arnold , Yuval Silberman
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引用次数: 0

摘要

酒精使用障碍(AUD)是世界范围内常见的心理健康问题,并可能导致其他慢性疾病。压力是AUD发展和持续的主要因素,青少年饮酒会导致压力反应增强,并增加成年后AUD发展的风险。青春期、压力和酒精之间相互作用的确切机制尚不完全清楚,需要进一步研究。在这方面,孤束核(NTS)向延伸的杏仁核提供密集的去甲肾上腺素投射,为压力相关的酒精行为提供了关键途径。虽然已知NTS去甲肾上腺素神经元对酒精敏感,但青少年酒精是否会破坏NTS去乙肾上腺素神经元的发育,以及这是否与成年后压力敏感性和酒精偏好的改变有关,以前尚未进行过研究。在这里,我们在出生后第28-42天将雄性和雌性C57Bl/6J小鼠暴露于常用的青少年间歇性乙醇(AIE)蒸汽模型中,并检测AIE对以下方面的影响:1)不同年龄(出生后第21-90天)NTS中酪氨酸羟化酶(TH)mRNA的表达,2)成年期对急性应激的行为反应,3)成年期NTS TH神经元对急性应激和乙醇挑战的反应,以及4)成年期乙醇条件下的位置偏好行为。总的来说,研究结果表明,AIE以性别依赖的方式改变了NTS TH mRNA的表达,并增加了急性应激暴露后的焦虑样行为。这些mRNA表达和行为变化发生在没有AIE诱导的NTS TH神经元对急性应激或急性酒精暴露的敏感性变化或乙醇条件下的位置偏好变化的情况下。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Adolescent alcohol disrupts development of noradrenergic neurons in the nucleus of the tractus solitarius and enhances stress behaviors in adulthood in mice in a sex specific manner

Alcohol use disorders (AUDs) are common mental health issues worldwide and can lead to other chronic diseases. Stress is a major factor in the development and continuation of AUDs, and adolescent alcohol exposure can lead to enhanced stress-responsivity and increased risk for AUD development in adulthood. The exact mechanisms behind the interaction between adolescence, stress, and alcohol are not fully understood and require further research. In this regard, the nucleus of the tractus solitarius (NTS) provides dense norepinephrine projections to the extended amygdala, providing a key pathway for stress-related alcohol behaviors. While NTS norepinephrine neurons are known to be alcohol sensitive, whether adolescent alcohol disrupts NTS-norepinephrine neuron development and if this is related to altered stress-sensitivity and alcohol preference in adulthood has not previously been examined. Here, we exposed male and female C57Bl/6J mice to the commonly used adolescent intermittent ethanol (AIE) vapor model during postnatal day 28-42 and examined AIE effects on: 1) tyrosine hydroxylase (TH) mRNA expression in the NTS across various ages (postnatal day 21-90), 2) behavioral responses to acute stress in the light/dark box test in adulthood, 3) NTS TH neuron responses to acute stress and ethanol challenges in adulthood, and 4) ethanol conditioned place preference behavior in adulthood. Overall the findings indicate that AIE alters NTS TH mRNA expression and increases anxiety-like behaviors following acute stress exposure in a sex-dependent manner. These mRNA expression and behavioral changes occur in the absence of AIE-induced changes in NTS TH neuron sensitivity to either acute stress or acute alcohol exposure or changes to ethanol conditioned place preference.

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来源期刊
Addiction neuroscience
Addiction neuroscience Neuroscience (General)
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