Bertagna Natalia B, Holmgren Eleanor B, Engi Sheila A, Ha Linh, Cruz Fabio C, Albrechet-Souza Lucas, Wills Tiffany A
Department of Cell Biology & Anatomy, School of Medicine, Louisiana State University Health Sciences Center, 533 Bolivar Street, New Orleans, LA, 70112, USA.
Department of Pharmacology, Federal University of São Paulo, São Paulo, SP, Brazil.
Psychopharmacology (Berl). 2024 Dec;241(12):2513-2523. doi: 10.1007/s00213-024-06693-8. Epub 2024 Sep 30.
Alcohol exposure during adolescence has been linked to long-lasting behavioral consequences, contributing to the development of alcohol use disorder. Negative affect and chronic pain during alcohol withdrawal are critical factors influencing problematic alcohol use and relapse. Our previous research demonstrated that adolescent intermittent ethanol (AIE) vapor exposure elicits sex-specific negative affect-like behavior in adult mice following stress exposure. Additionally, AIE induces persistent mechanical hypersensitivity, which is accompanied by increased activation of corticotropin-releasing factor receptor type 1 (CRFR1) neurons in the dorsolateral bed nucleus of the stria terminalis (dlBNST).
This study extends previous work by investigating plasma corticosterone levels and CRFR1 protein expression in the dlBNST following restraint stress exposure in adult mice with an AIE history. We also aim to explore the role of dlBNST CRFR1 signaling in mediating negative affect-like behavior and mechanical hypersensitivity.
Female mice exhibited elevated plasma corticosterone levels compared to males following restraint stress. Moreover, females with AIE history showed higher expression of CRFR1 protein in the dlBNST compared to air controls. Antagonism of CRFR1 in the dlBNST blocked AIE-induced mechanical hypersensitivity in adult females but did not affect stress-induced negative affect-like behavior. In alcohol-naïve females, intra-dlBNST administration of a CRFR1 agonist induced mechanical hypersensitivity.
These findings provide new insights into the neurobiological mechanisms underlying stress-induced negative affect and pain-related behavior, both influenced by a history of adolescent alcohol exposure. The results suggest that CRFR1 antagonists warrant further investigation for their potential in addressing alcohol-related chronic pain.
青春期饮酒与长期的行为后果有关,会导致酒精使用障碍的发展。酒精戒断期间的负面影响和慢性疼痛是影响酒精使用问题和复发的关键因素。我们之前的研究表明,青春期间歇性乙醇(AIE)蒸汽暴露会在成年小鼠应激暴露后引发性别特异性的类似负面影响的行为。此外,AIE会诱导持续的机械性超敏反应,同时伴有终纹床核背外侧(dlBNST)中促肾上腺皮质激素释放因子1型(CRFR1)神经元的激活增加。
本研究通过调查有AIE病史的成年小鼠在束缚应激暴露后血浆皮质酮水平和dlBNST中CRFR1蛋白表达,扩展了先前的工作。我们还旨在探讨dlBNST CRFR1信号在介导类似负面影响的行为和机械性超敏反应中的作用。
与雄性小鼠相比,雌性小鼠在束缚应激后血浆皮质酮水平升高。此外,有AIE病史的雌性小鼠与空气对照组相比,dlBNST中CRFR1蛋白表达更高。阻断dlBNST中的CRFR1可阻断成年雌性小鼠中AIE诱导的机械性超敏反应,但不影响应激诱导的类似负面影响的行为。在未接触过酒精的雌性小鼠中,向dlBNST内注射CRFR1激动剂可诱导机械性超敏反应。
这些发现为应激诱导的负面影响和疼痛相关行为的神经生物学机制提供了新的见解,这两者都受青春期饮酒史的影响。结果表明,CRFR1拮抗剂因其在解决酒精相关慢性疼痛方面的潜力值得进一步研究。
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