Voluntary alcohol consumption during distinct phases of adolescence differentially alters adult fear acquisition, extinction and renewal in male and female rats.

IF 2.6 4区心理学 Q2 BEHAVIORAL SCIENCES Stress-The International Journal on the Biology of Stress Pub Date : 2023-11-01 Epub Date: 2023-11-05 DOI:10.1080/10253890.2023.2278315

J Alex Grizzell, Maryam Vanbaelinghem, Jessica Westerman, Michael P Saddoris

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Abstract

Alcohol use during adolescence coincides with elevated risks of stress-related impairment in adults, particularly via disrupted developmental trajectories of vulnerable corticolimbic and mesolimbic systems involved in fear processing. Prior work has investigated the impact of binge-like alcohol consumption on adult fear and stress, but less is known about whether voluntarily consumed alcohol imparts differential effects based on adolescence phases and biological sex. Here, adolescent male and female Long Evans rats were granted daily access to alcohol (15%) during either early (Early-EtOH; P25-45) or late adolescence (Late-EtOH; P45-55) using a modified drinking-in-the-dark design. Upon adulthood (P75-80), rats were exposed to a three-context (ABC) fear renewal procedure. We found that male and female Early-EtOH rats showed faster acquisition of fear but less freezing during early phases of extinction and throughout fear renewal. In the extinction period specifically, Early-EtOH rats showed normal levels of freezing in the presence of fear-associated cues, but abnormally low freezing immediately after cue offset, suggesting a key disruption in contextual processing and/or novelty seeking brought by early adolescent binge consumption. While the effects of alcohol were most pronounced in the Early-EtOH rats (particularly in females), Late-EtOH rats displayed some changes in fear behavior including slower fear acquisition, faster extinction, and reduced renewal compared with controls, but primarily in males. Our results suggest that early adolescence in males and females and, to a lesser extent, late adolescence in males is a particularly vulnerable period wherein alcohol use can promote stress-related dysfunction in adulthood. Furthermore, our results provide multiple bases for future research focused on developmental correlates of alcohol mediated disruption in the brain.

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青春期不同阶段的自愿饮酒会不同程度地改变成年雄性和雌性大鼠的恐惧获取、消退和更新。

青春期饮酒与成年人压力相关障碍的风险增加相吻合，特别是通过参与恐惧处理的脆弱皮质边缘和中边缘系统的发育轨迹被打乱。先前的工作已经调查了酗酒对成年人恐惧和压力的影响，但对于自愿饮酒是否会根据青春期和生理性别产生不同的影响，人们知之甚少。在这里，青春期雄性和雌性Long Evans大鼠在青春期早期（早期EtOH；P25-45）或晚期（晚期EtOH；P45-55）使用改良的黑暗饮酒设计，每天获得酒精（15%）。成年后（P75-80），大鼠暴露于三情境（ABC）恐惧更新程序。我们发现，雄性和雌性早期EtOH大鼠在灭绝的早期阶段和整个恐惧更新过程中表现出更快的恐惧获得，但冷冻较少。特别是在灭绝期，早期EtOH大鼠在存在恐惧相关线索的情况下表现出正常水平的冷冻，但在线索抵消后立即表现出异常低的冷冻，这表明青少年早期的暴饮带来了上下文处理和/或新奇感寻求的关键中断。虽然酒精的影响在早期EtOH大鼠（尤其是雌性）中最为明显，但与对照组相比，晚期EtOH大白鼠在恐惧行为上表现出一些变化，包括恐惧获得较慢、消退较快和更新减少，但主要发生在雄性。我们的研究结果表明，男性和女性的青春期早期，以及在较小程度上男性的青春期晚期，是一个特别脆弱的时期，在这个时期，饮酒会促进成年后与压力相关的功能障碍。此外，我们的研究结果为未来研究酒精介导的大脑破坏的发育相关性提供了多个基础。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Stress-The International Journal on the Biology of Stress 医学-行为科学

CiteScore

5.60

自引率

0.00%

发文量

审稿时长

6-12 weeks

期刊介绍： The journal Stress aims to provide scientists involved in stress research with the possibility of reading a more integrated view of the field. Peer reviewed papers, invited reviews and short communications will deal with interdisciplinary aspects of stress in terms of: the mechanisms of stressful stimulation, including within and between individuals; the physiological and behavioural responses to stress, and their regulation, in both the short and long term; adaptive mechanisms, coping strategies and the pathological consequences of stress. Stress will publish the latest developments in physiology, neurobiology, molecular biology, genetics research, immunology, and behavioural studies as they impact on the understanding of stress and its adverse consequences and their amelioration. Specific approaches may include transgenic/knockout animals, developmental/programming studies, electrophysiology, histochemistry, neurochemistry, neuropharmacology, neuroanatomy, neuroimaging, endocrinology, autonomic physiology, immunology, chronic pain, ethological and other behavioural studies and clinical measures.