Department of Psychology, Center for Development and Behavioral Neuroscience, Binghamton University, Binghamton, NY, 13902, USA.
Developmental Exposure Alcohol Research Center, Binghamton University, Binghamton, NY, 13902, USA.
Neuropsychopharmacology. 2022 Nov;47(12):2140-2149. doi: 10.1038/s41386-022-01327-z. Epub 2022 Apr 27.
Anxiety disorders are highly prevalent among individuals with a history of prenatal alcohol exposure (PAE), and adolescent rodents demonstrate anxiety-like behavior following moderate PAE on Gestational Day (G) 12. A likely systemic target of PAE is the stress peptide corticotropin-releasing factor (CRF), as activation of CRF receptor 1 (CRFR1) in the medial nucleus of the central amygdala (CeM) is known to increase anxiety-like behavior in adults. To determine if CRF-CRFR1 interactions underly PAE-induced anxiety, functional changes in CRF system activity were investigated in adolescent male and female Sprague Dawley rats following G12 PAE. Compared to air-exposed controls, PAE increased basal spontaneous (s) inhibitory postsynaptic current (IPSC) frequency in the CeM of males, but not females. Furthermore, PAE blunted CRFR1-regulated miniature (m) IPSCs in a sex- and concentration-specific manner, and only PAE males demonstrated tonic CRFR1 activity in the CeM. It was further determined that G12 PAE decreased CRFR1 mRNA in the CeM of males while increasing regional expression in females. Finally, infusion of a CRFR1 agonist into the CeM of adolescents produced a blunted expression of CRFR1-induced anxiety-like behavior exclusively in PAE males, mirroring the blunted physiology demonstrated by PAE males. Cumulatively, these data suggest that CRFR1 function within the CeM is age- and sex-specific, and PAE not only increases the expression of anxiety-like behavior, but may reduce the efficacy of treatment for PAE-induced anxiety through CRFR1-associated mechanisms. Therefore, future research will be necessary to develop targeted treatment of anxiety disorders in individuals with a history of PAE.
焦虑障碍在有产前酒精暴露 (PAE) 史的个体中高度普遍,青春期啮齿动物在妊娠第 12 天 (G) 中度 PAE 后表现出类似焦虑的行为。PAE 的一个可能的系统靶点是应激肽促肾上腺皮质释放因子 (CRF),因为已知中杏仁核 (CeM) 中的 CRF 受体 1 (CRFR1) 的激活会增加成年期的类似焦虑行为。为了确定 CRF-CRFR1 相互作用是否是 PAE 引起的焦虑的基础,研究了 G12 PAE 后青春期雄性和雌性 Sprague Dawley 大鼠中 CRF 系统活性的功能变化。与空气暴露对照相比,PAE 增加了雄性 CeM 中基础自发 (s) 抑制性突触后电流 (IPSC) 的频率,但雌性则没有。此外,PAE 以性别和浓度特异性的方式削弱了 CRFR1 调节的微小 (m) IPSC,只有 PAE 雄性在 CeM 中表现出紧张的 CRFR1 活性。进一步确定 G12 PAE 降低了雄性 CeM 中的 CRFR1 mRNA,而增加了雌性的区域表达。最后,将 CRFR1 激动剂输注到青少年的 CeM 中,仅在 PAE 雄性中产生了 CRFR1 诱导的类似焦虑行为表达的减弱,这与 PAE 雄性表现出的生理功能减弱相匹配。总之,这些数据表明,CeM 中的 CRFR1 功能具有年龄和性别特异性,PAE 不仅增加了类似焦虑行为的表达,而且可能通过 CRFR1 相关机制降低 PAE 引起的焦虑的治疗效果。因此,未来的研究将有必要开发针对有 PAE 史的个体的焦虑障碍的靶向治疗。