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糖皮质激素受体拮抗剂 PT150 对早期生活应激后芬太尼自身给药的获得和升级的影响。

Effect of the glucocorticoid receptor antagonist PT150 on acquisition and escalation of fentanyl self-administration following early-life stress.

机构信息

Department of Psychology.

Research Triangle Institute.

出版信息

Exp Clin Psychopharmacol. 2023 Apr;31(2):362-369. doi: 10.1037/pha0000577. Epub 2022 May 19.

Abstract

There is comorbidity between posttraumatic stress disorder (PTSD) and opioid use disorder (OUD), perhaps because PTSD-like stressful experiences early in life alter the hypothalamic-pituitary-adrenal stress axis to increase the risk for OUD. The present study determined if the glucocorticoid receptor antagonist PT150 reduces the escalation of fentanyl intake in rats exposed to a "two-hit" model of early-life stress (isolation rearing and acute stress). Male and female rats were raised during adolescence in either isolated or social housing and then were given either a single acute stress (restraint and cold-water swim) or control treatment in young adulthood. Rats were then treated daily with PT150 (50 mg/kg, oral) or placebo and were tested for acquisition of fentanyl self-administration in 1-hr sessions, followed by escalation across 6-hr sessions. Regardless of PT150 treatment or sex, acquisition of fentanyl self-administration in 1-hr sessions was greater in isolate-housed rats compared to social-housed rats; the acute stress manipulation did not have an effect on self-administration even though it transiently increased plasma corticosterone levels. During the 6-hr sessions, escalation of fentanyl was observed across all treatment groups; however, there was a significant PT150 Treatment × Sex interaction. While males self-administered more than females overall, PT150 intake in males and intake in females, thus negating the sex difference. Although PT150 may serve as an effective treatment for reducing the risk of OUD following early-life stress in males, further work is needed to determine the mechanism underlying the differential effects of PT150 in males and females. (PsycInfo Database Record (c) 2023 APA, all rights reserved).

摘要

创伤后应激障碍(PTSD)和阿片类药物使用障碍(OUD)之间存在共病,这可能是因为生命早期类似 PTSD 的压力体验改变了下丘脑-垂体-肾上腺应激轴,增加了 OUD 的风险。本研究旨在确定糖皮质激素受体拮抗剂 PT150 是否会减少经历早期生活应激(隔离饲养和急性应激)“双打击”模型的大鼠中芬太尼摄入量的增加。雄性和雌性大鼠在青春期分别在隔离或社交环境中饲养,然后在成年早期接受单次急性应激(束缚和冷水游泳)或对照处理。然后,大鼠每天接受 PT150(50mg/kg,口服)或安慰剂治疗,并在 1 小时的时间段内接受芬太尼自我给药的获得测试,然后在 6 小时的时间段内进行递增测试。无论是否接受 PT150 治疗或性别如何,与社交饲养的大鼠相比,隔离饲养的大鼠在 1 小时的时间段内更易获得芬太尼自我给药;尽管急性应激处理会短暂增加血浆皮质酮水平,但对自我给药没有影响。在 6 小时的时间段内,所有治疗组均观察到芬太尼的递增;然而,存在显著的 PT150 治疗×性别交互作用。虽然雄性总体上自我给药多于雌性,但 PT150 摄入在雄性和 摄入在雌性中,从而消除了性别差异。虽然 PT150 可能作为一种有效的治疗方法,用于减少男性早期生活应激后 OUD 的风险,但仍需要进一步的工作来确定 PT150 在男性和女性中的差异作用的机制。(PsycInfo 数据库记录(c)2023 APA,保留所有权利)。

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