雌雄小鼠基础动机行为、慢性乙醇摄入和杏仁核活性的性别差异。
Sex differences in basal motivated behavior, chronic ethanol drinking, and amygdala activity in female and male mice.
机构信息
Neuroscience Curriculum, University of North Carolina at Chapel Hill, Chapel Hill, NC 27599, USA; Bowles Center for Alcohol Studies, University of North Carolina at Chapel Hill, Chapel Hill, NC 27599, USA.
Bowles Center for Alcohol Studies, University of North Carolina at Chapel Hill, Chapel Hill, NC 27599, USA.
出版信息
Alcohol. 2024 Nov;120:85-97. doi: 10.1016/j.alcohol.2024.06.004. Epub 2024 Jun 13.
Alcohol use disorder (AUD) is a major public health concern that despite its prevalence, lacks a widely-effective treatment due to the complexity of AUD pathology. AUD is highly comorbid with other psychiatric conditions including anxiety and mood disorders, however it is unclear how these disorders influence each other. The underlying etiology of these comorbidities is difficult to decipher and factors including sex, stress, and the environment further complicate both diagnosis and treatment strategies. To understand more about this bidirectional relationship between AUD and comorbid psychiatric disorders, we ran male and female C57Bl/6j mice through baseline behavioral testing followed by intermittent access-two bottle choice (IA-2BC) drinking. We found no sex differences in basal anxiety-like or depressive-like behavior, however females displayed enhanced motivated feeding behavior. Females consumed more ethanol than males, at both 1hr and 24hr timepoints. Basal affective state did not predict subsequent ethanol intake in either sex, however exploratory behavior was positively correlated with drinking in males but not females. We then re-assessed negative affect behavior following chronic ethanol drinking to determine if drinking impacted subsequent affective behavior and found no relationship between ethanol intake and affective state in males or females. We also examined how chronic ethanol drinking affected central amygdala (CeA) and basolateral amygdala (BLA) neuronal activity in males and females. Ethanol-drinking females had a decrease in CeA neuronal activity, driven by reduced activity in the lateral (CeA) sub-region, while in males there was no significant difference in CeA activity compared to water controls. Neither males or females had a significant change in BLA neuronal activity following chronic ethanol drinking. Collectively, these results demonstrate sex differences in basal motivated behavior, drinking behavior, and subregion-specific amygdala neuronal activity following chronic ethanol drinking which may inform the sex differences seen in patients diagnosed with AUD and comorbid conditions.
酒精使用障碍(AUD)是一个主要的公共卫生关注点,尽管它很普遍,但由于 AUD 病理的复杂性,缺乏广泛有效的治疗方法。AUD 与其他精神疾病高度共病,包括焦虑和情绪障碍,但这些疾病如何相互影响尚不清楚。这些共病的潜在病因难以解释,包括性别、压力和环境在内的因素进一步使诊断和治疗策略复杂化。为了更深入地了解 AUD 和共病精神障碍之间的这种双向关系,我们对雄性和雌性 C57Bl/6j 小鼠进行了基线行为测试,然后进行间歇性双瓶选择(IA-2BC)饮酒。我们发现,雄性和雌性在基础焦虑样或抑郁样行为上没有性别差异,但雌性表现出增强的动机进食行为。雌性比雄性消耗更多的乙醇,无论是在 1 小时还是 24 小时时间点。基础情感状态并不能预测两性随后的乙醇摄入量,但探索性行为与雄性的饮酒量呈正相关,而与雌性无关。然后,我们在慢性乙醇饮酒后重新评估了消极情绪行为,以确定饮酒是否影响随后的情绪行为,结果发现雄性和雌性的乙醇摄入量与情绪状态之间没有关系。我们还检查了慢性乙醇饮酒如何影响雄性和雌性的中央杏仁核(CeA)和基底外侧杏仁核(BLA)神经元活动。乙醇饮用的雌性的 CeA 神经元活动减少,这是由外侧(CeA)亚区的活动减少驱动的,而雄性的 CeA 活动与水对照组相比没有显著差异。与水对照组相比,雄性和雌性的 BLA 神经元活动在慢性乙醇饮酒后均无显著变化。总的来说,这些结果表明,在慢性乙醇饮酒后,雄性和雌性在基础动机行为、饮酒行为和杏仁核亚区特定神经元活动方面存在性别差异,这可能为诊断为 AUD 和共病的患者中观察到的性别差异提供信息。
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