The antidepressant agomelatine attenuates morphine-induced reinstatement but not self-administration or precipitated withdrawal

IF 3.3 3区 心理学 Q1 BEHAVIORAL SCIENCES Pharmacology Biochemistry and Behavior Pub Date : 2023-02-01 DOI:10.1016/j.pbb.2023.173525
Alok De , Ken W. Grasing
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Abstract

Background

Exogenous melatonin appears to have anti-addictive properties and was recently shown to improve mental health and metabolic measures in patients receiving chronic opioid maintenance therapy. Agomelatine is a marketed antidepressant which acts as a melatonin agonist. We evaluated its effects using a rat model of morphine-reinforced behavior.

Methods

After pretreatment with noncontingent morphine, male Wistar rats were trained to self-administer intravenous morphine (1.0 mg/kg-injection) under a progressive-ratio schedule. Rats were pretreated with vehicle or agomelatine during extinction, reinstatement, and reacquisition of morphine-reinforced behavior.

Results

Daily treatment with 10 mg/kg-day of agomelatine decreased the number of ratios completed and prolonged latency during morphine-induced reinstatement. There were no significant effects on cue-induced reinstatement, morphine self-administration, or naloxone-precipitated withdrawal. Treatment with 32 mg/kg-day of agomelatine caused postural changes. That dose prolonged withdrawal-induced loss of body weight and caused delayed reductions in food reinforcement.

Summary

In addition to postural effects, high-dose agomelatine worsened the course of spontaneous withdrawal and produced nonspecific effects on food-reinforced behavior. When administered at a selective dose, agomelatine did not modify morphine self-administration or precipitated withdrawal, but decreased morphine-induced reinstatement. Our findings show potential detrimental effects of high-dose agomelatine, with reductions in opioid-seeking behavior after a lower, more selective dose.

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抗抑郁药阿戈美拉汀减轻吗啡诱导的恢复,但不自我给药或沉淀戒断
背景外源性褪黑素似乎具有抗成瘾特性,最近被证明可以改善接受慢性阿片类药物维持治疗的患者的心理健康和代谢指标。阿戈美拉汀是一种市场上销售的抗抑郁药,作为褪黑激素激动剂。我们使用吗啡强化行为的大鼠模型来评估其效果。方法雄性Wistar大鼠经非接触吗啡预处理后,按递增比例训练自行静脉注射吗啡(1.0mg/kg)。在吗啡强化行为的消退、恢复和再获得过程中,用载体或阿戈美拉汀对大鼠进行预处理。结果阿戈美拉汀每日10mg/kg治疗可减少吗啡诱导的恢复过程中完成比率的数量,延长潜伏期。提示诱导的恢复、吗啡自身给药或纳洛酮诱导的戒断没有显著影响。阿戈美拉汀32 mg/kg日治疗引起体位变化。该剂量延长了戒断时间,导致体重下降,并导致食物强化的延迟减少。摘要除了体位性影响外,高剂量阿戈美拉汀还会恶化自发戒断过程,并对食物强化行为产生非特异性影响。当以选择性剂量给药时,阿戈美拉汀不会改变吗啡的自我给药或促使戒断,但会减少吗啡诱导的恢复。我们的研究结果显示,高剂量阿戈美拉汀具有潜在的有害影响,在较低、更具选择性的剂量后,阿片类药物的寻求行为会减少。
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来源期刊
CiteScore
6.40
自引率
2.80%
发文量
122
审稿时长
38 days
期刊介绍: Pharmacology Biochemistry & Behavior publishes original reports in the areas of pharmacology and biochemistry in which the primary emphasis and theoretical context are behavioral. Contributions may involve clinical, preclinical, or basic research. Purely biochemical or toxicology studies will not be published. Papers describing the behavioral effects of novel drugs in models of psychiatric, neurological and cognitive disorders, and central pain must include a positive control unless the paper is on a disease where such a drug is not available yet. Papers focusing on physiological processes (e.g., peripheral pain mechanisms, body temperature regulation, seizure activity) are not accepted as we would like to retain the focus of Pharmacology Biochemistry & Behavior on behavior and its interaction with the biochemistry and neurochemistry of the central nervous system. Papers describing the effects of plant materials are generally not considered, unless the active ingredients are studied, the extraction method is well described, the doses tested are known, and clear and definite experimental evidence on the mechanism of action of the active ingredients is provided.
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