Reduction of opioid withdrawal symptoms and opioid-induced hyperalgesia by subcutaneous sumatriptan reveals central neuromodulation

IF 4 2区 医学 Q1 CLINICAL NEUROLOGY
Alessandra Pistolesi , Francesco De Cesaris , Daniela Buonvicino , Alberto Chiarugi
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引用次数: 0

Abstract

Triptans are efficacious, largely prescribed antimigraine drugs but where and how they exert their therapeutic effect is debated. Because of the presumed impermeability of the blood brain barrier to triptans, a peripheral antimigraine effect of these drugs have been repeatedly proposed. Recent findings, however, indicate that triptans cross the blood brain barrier, and counteract central nociception in models of pronociceptive sensitization. Here, we investigated the effects of subcutaneous (s.c.) sumatriptan in models of opioid withdrawal and opioid-induced hyperalgesia, two conditions sustained by deranged descending facilitation by the rostral ventromedial medulla (RVM). We found that s.c. sumatriptan injection in morphine-dependent rats 30 min before naloxone-precipitated withdrawal reduced severity of withdrawal symptoms. We also found that at the time of naloxone injection sumatriptan reached contents of 294±19 and 371±30 pg/mg of tissue in the RVM and locus coeruleus, respectively. In keeping with data on morphine withdrawal, s.c. sumatriptan injections suppressed thermal hyperalgesia in rats undergoing repeated dosing of morphine. Sumatriptan affected neither behavioral signs in morphine-dependent rats unexposed to naloxone, nor the extent of the initial antinociceptive response to morphine. Overall, data suggest that peripherally injected sumatriptan reaches CNS concentrations sufficient to exert functional neuromodulation of brainstem regions involved in pronociceptive sensitization and nociplasticity.

Perspective

This article reports that sumatriptan reduces symptoms of morphine withdrawal and morphine-induced hyperalgesia. Data suggests that triptans exert their antinociceptive effects through central mechanisms.
皮下舒马匹坦减轻阿片类戒断症状和阿片类药物引起的痛觉过敏显示中枢神经调节。
曲坦类药物是一种有效的抗偏头痛处方药,但在哪里以及如何发挥其治疗效果仍存在争议。由于假定血脑屏障对曲坦类药物具有不渗透性,这些药物的外周抗偏头痛作用已被反复提出。然而,最近的研究结果表明,曲坦类药物穿过血脑屏障,并在前觉性致敏模型中抵消中枢伤害感觉。在这里,我们研究了皮下(s.c)舒马曲坦对阿片戒断和阿片诱导的痛觉过敏模型的影响,这两种情况由吻侧腹内侧髓质(RVM)的紊乱下行促进维持。我们发现吗啡依赖大鼠在纳洛酮沉淀戒断前30分钟注射舒马曲坦可减轻戒断症状的严重程度。我们还发现,注射纳洛酮时,RVM和蓝斑组织中舒马曲坦的含量分别达到294±19和371±30 pg/mg。与吗啡戒断数据一致,s.c.舒马曲坦注射抑制了反复给药吗啡大鼠的热痛觉过敏。对于未暴露于纳洛酮的吗啡依赖大鼠,舒马曲坦既不影响行为体征,也不影响吗啡初始抗感觉反应的程度。总的来说,数据表明外周注射舒马匹坦达到足够的中枢神经系统浓度,可以对参与前感觉敏化和伤害可塑性的脑干区域进行功能性神经调节。观点:这篇文章报道了舒马曲坦减轻吗啡戒断和吗啡引起的痛觉过敏的症状。数据表明曲坦类药物通过中枢机制发挥其抗感觉作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Journal of Pain
Journal of Pain 医学-临床神经学
CiteScore
6.30
自引率
7.50%
发文量
441
审稿时长
42 days
期刊介绍: The Journal of Pain publishes original articles related to all aspects of pain, including clinical and basic research, patient care, education, and health policy. Articles selected for publication in the Journal are most commonly reports of original clinical research or reports of original basic research. In addition, invited critical reviews, including meta analyses of drugs for pain management, invited commentaries on reviews, and exceptional case studies are published in the Journal. The mission of the Journal is to improve the care of patients in pain by providing a forum for clinical researchers, basic scientists, clinicians, and other health professionals to publish original research.
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