Obestatin prevents analgesic tolerance to morphine and reverses the effects of mild morphine withdrawal in mice

Nándor Lipták, Roberta Dochnal , Krisztina Csabafi, Júlia Szakács, Gyula Szabó
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引用次数: 11

Abstract

Obestatin is a 23-amino acid gut-derived neuropeptide, encoded by the same gene with ghrelin. The goal of this study was to examine the effects of obestatin on the acute and chronic analgesic actions of morphine and on mild morphine withdrawal. Open-field (OF) and elevated plus maze (EPM) tests were used to assess mild morphine withdrawal-induced behavior changes and the heat-radiant tail-flick assay was used to investigate analgesic actions of morphine. CFLP male mice were treated twice a day with graded doses of morphine in EPM and OF experiments and once a day in tail-flick studies. Obestatin (1.5 μg/2 μl) was administrated once a day in all experiments. Furthermore, 0.2 mg/kg naloxone or saline was administered after the final injection of morphine at a dose of 20 mg/kg in EPM and OF. These behavioral parameters were monitored in the OF: the percentage of center ambulation time and distance; whereas in the EPM: the time spent in open arms and the entries into open arms compared to the total time (%OAT) and entries (%OAE). In the OF, obestatin significantly decreased the percentage of time spent in the center in mice undergoing naloxone-precipitated mild morphine withdrawal. EPM results were similar to open field, but obestatin had no significant effect on parameters mentioned above. Besides, obestatin maintained the analgesic effect of morphine 90 and 120 min after morphine injection in mice treated with morphine receiving obestatin compared to mice treated with morphine. In tolerance studies, obestatin diminished the analgesic tolerance to morphine on the 5th day. In this study we confirmed that obestatin reversed the effect of mild morphine withdrawal and enhances the analgesic effect of morphine. These data suggest that obestatin may have a role in opioid-induced analgesia and in behavioral responses induced by opioid withdrawal.

肥胖抑制素阻止小鼠对吗啡的镇痛耐受,并逆转轻度吗啡戒断的效果
肥胖抑制素是一种由23个氨基酸组成的肠源神经肽,与胃饥饿素由同一基因编码。本研究的目的是研究肥胖抑制素对吗啡的急性和慢性镇痛作用以及对吗啡轻度戒断的影响。采用开放野区(OF)和升高+迷宫(EPM)试验评估吗啡戒断引起的轻度行为改变,采用热辐射甩尾试验研究吗啡的镇痛作用。在EPM和of实验中,CFLP雄性小鼠每天使用两次吗啡,在甩尾实验中每天使用一次吗啡。所有实验均给予Obestatin (1.5 μg/2 μl),每天1次。此外,EPM和of最后注射吗啡20 mg/kg后,再注射0.2 mg/kg纳洛酮或生理盐水。监测这些行为参数:中心行走时间和距离的百分比;而在EPM中:张开双臂的时间和张开双臂的条目与总时间(%OAT)和条目(%OAE)的比较。在实验中,肥胖抑制素显著降低了纳洛酮引起的轻度吗啡戒断小鼠在中心停留的时间百分比。EPM结果与野外相似,但肥胖抑制素对上述参数无显著影响。此外,在吗啡注射后90和120分钟,接受肥胖抑制素治疗的吗啡小鼠与接受吗啡治疗的小鼠相比,肥胖抑制素能维持吗啡的镇痛作用。在耐受性研究中,肥胖抑制素在第5天降低了对吗啡的镇痛耐受性。在这项研究中,我们证实了肥胖抑制素逆转了轻度吗啡戒断的作用,并增强了吗啡的镇痛作用。这些数据表明,肥胖抑制素可能在阿片类药物诱导的镇痛和阿片类药物戒断引起的行为反应中发挥作用。
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来源期刊
Regulatory Peptides
Regulatory Peptides 医学-内分泌学与代谢
自引率
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审稿时长
2 months
期刊介绍: Regulatory Peptides provides a medium for the rapid publication of interdisciplinary studies on the physiology and pathology of peptides of the gut, endocrine and nervous systems which regulate cell or tissue function. Articles emphasizing these objectives may be based on either fundamental or clinical observations obtained through the disciplines of morphology, cytochemistry, biochemistry, physiology, pathology, pharmacology or psychology.
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