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大鼠强迫性样舒芬太尼蒸气自给药。

Compulsive-Like Sufentanil Vapor Self-Administration in Rats.

机构信息

Intramural Research Program, National Institute on Drug Abuse, National Institutes of Health, Baltimore, MD, USA.

La Jolla Alcohol Research, La Jolla, CA, USA.

出版信息

Neuropsychopharmacology. 2018 Mar;43(4):801-809. doi: 10.1038/npp.2017.172. Epub 2017 Aug 16.

Abstract

Opioid misuse is at historically high levels in the United States, with inhalation (ie, smoking and vaping) being one of the most common routes of consumption. We developed and validated a novel preclinical model of opioid self-administration by inhalation that does not require surgery and reliably produces somatic and motivational signs of dependence. Rats were trained to perform an operant response (nosepoke) to receive 10 s of vaporized sufentanil, a potent opioid, in 2 h daily sessions. Rats readily and concentration-dependently self-administered vaporized sufentanil. Rats exhibited a significant increase in responding for sufentanil when given the preferential μ-opioid receptor inverse agonist naloxone, suggesting the participation of μ-opioid receptors in the reinforcing properties of sufentanil vapor. Serum sufentanil concentrations significantly correlated with the number of sufentanil vapor deliveries. Rats that were given long access (LgA; 12 h/day) but not short access (ShA; 1 h/day) to vaporized sufentanil escalated their drug intake over time and exhibited both naloxone-precipitated somatic signs of opioid withdrawal and spontaneous withdrawal-induced mechanical hypersensitivity. After 6 months of forced drug abstinence, LgA rats returned to pre-escalation baseline levels of responding for sufentanil and mechanical sensitivity. Upon subsequent re-escalation (ie, after the return to extended access to sufentanil vapor), LgA rats again developed naloxone-precipitated somatic signs of withdrawal and spontaneous withdrawal-induced mechanical hypersensitivity. These findings demonstrate that the operant sufentanil vapor self-administration model has both face and construct validity and therefore will be useful for investigating the neurobiological basis of opioid addiction.

摘要

在美国,阿片类药物滥用处于历史高位,其中吸入(即吸烟和蒸气吸入)是最常见的使用途径之一。我们开发并验证了一种新的阿片类药物自我给药的临床前模型,该模型不需要手术,并且可靠地产生躯体和动机依赖的迹象。大鼠接受训练,通过操作反应(鼻触)在 2 小时的每日时段内接受 10 秒的 vaporized 舒芬太尼,这是一种有效的阿片类药物。大鼠容易且浓度依赖性地自我给予 vaporized 舒芬太尼。当给予选择性 μ-阿片受体反向激动剂纳洛酮时,大鼠对舒芬太尼的反应显著增加,这表明 μ-阿片受体参与了舒芬太尼蒸气的强化特性。血清舒芬太尼浓度与舒芬太尼蒸气输送的数量显著相关。给予大鼠长时间(12 小时/天)而不是短时间(1 小时/天)接触 vaporized 舒芬太尼,它们的药物摄入量随时间增加,并表现出纳洛酮引发的躯体戒断症状和自发性戒断引起的机械性超敏反应。在 6 个月的强制药物戒断后,LgA 大鼠恢复到 vaporized 舒芬太尼反应和机械敏感性的预上升基线水平。随后重新上升(即在返回延长接触舒芬太尼蒸气后),LgA 大鼠再次出现纳洛酮引发的躯体戒断症状和自发性戒断引起的机械性超敏反应。这些发现表明,操作性舒芬太尼蒸气自我给药模型具有表象和结构有效性,因此将有助于研究阿片类药物成瘾的神经生物学基础。

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