Effects of oral morphine on experimentally evoked itch and pain: a randomized, double-blind, placebo-controlled trial.

IF 1.5 Q4 CLINICAL NEUROLOGY Scandinavian Journal of Pain Pub Date : 2023-09-15 Print Date: 2023-10-26 DOI:10.1515/sjpain-2023-0034
Hiroai Okutani, Silvia Lo Vecchio, Nadia Ammitzbøll, Asbjørn Mohr Drewes, Lars Arendt-Nielsen
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Abstract

Objectives: Pain and itch share similar neuronal networks; hence, it is difficult to explain why opioids can relieve pain but provoke itching. The present human volunteer study aimed to investigate the similarities and differences in responses to experimentally provoked pain and itching to explore the underlying fundamental mechanisms.

Methods: Twenty-four healthy volunteers were enrolled in this single-center, randomized, double-blind, placebo-controlled, parallel-group trial. Three volar forearms and two mandibular areas were marked, and participants randomly received morphine (20 mg) or identical placebo tablets. Heat, cold, and pressure pain thresholds, and vasomotor responses were assessed at baseline and after oral morphine administration. Itch provocations were induced by intradermal application of 1 % histamine or a topical cowhage (non-histaminergic itch) to a marked area of the skin. The participants were subsequently asked to rate their itching and pain intensities. The assessments were repeated for all marked areas.

Results: Morphine caused analgesia, as assessed by the significant modulation of cold and pressure pain thresholds (p<0.05). There were no significant differences in histaminergic or non-histaminergic itch or pain intensity between the morphine and placebo groups. Superficial blood perfusion (vasomotor response) following histamine provocation was significantly increased by morphine (p<0.05) in both areas. No correlation was found between the provoked itch intensity and analgesic efficacy in any area or group.

Conclusions: Oral administration of morphine caused analgesia without modulating itch intensities but increased neurogenic inflammation in response to histamine, suggesting that different opioid mechanisms in histaminergic and non-histaminergic neurons evoke neurogenic inflammation.

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口服吗啡对实验诱发的瘙痒和疼痛的影响:一项随机、双盲、安慰剂对照试验。
目的:疼痛和瘙痒共享相似的神经元网络;因此,很难解释为什么阿片类药物可以缓解疼痛,但会引起瘙痒。目前的人类志愿者研究旨在调查对实验引发的疼痛和瘙痒反应的异同,以探索潜在的基本机制。方法:24名健康志愿者参加这项单中心、随机、双盲、安慰剂对照、平行组试验。标记三个掌侧前臂和两个下颌区域,参与者随机接受吗啡(20 mg)或相同的安慰剂片剂。在基线和口服吗啡后评估热、冷、压痛阈值和血管舒缩反应。皮内施用1 % 组胺或局部牛瘟(非组胺能瘙痒)。随后,参与者被要求对他们的瘙痒和疼痛强度进行评分。对所有标记区域重复进行评估。结果:吗啡引起镇痛,通过对冷痛和压痛阈值的显著调节来评估(P结论:口服吗啡在不调节瘙痒强度的情况下引起镇痛,但增加了对组胺反应的神经源性炎症,这表明组胺能和非组胺能神经元中的不同阿片机制引起神经源性炎性。
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来源期刊
Scandinavian Journal of Pain
Scandinavian Journal of Pain CLINICAL NEUROLOGY-
CiteScore
3.30
自引率
6.20%
发文量
73
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