Hui Li, Bin Zhou, Jing Wu, Yuqing Zhang, Weiya Zhang, Michael Doherty, Xinjia Deng, Ning Wang, Dongxing Xie, Yilun Wang, Hui Xie, Changjun Li, Jie Wei, Guanghua Lei, Chao Zeng
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引用次数: 0
摘要
褪黑素具有缓解疼痛的潜力和长期安全性。我们研究了口服褪黑素对骨关节炎(OA)的镇痛效果,并调查了其潜在机制。我们利用英国初级保健数据库中的数据,对患有 OA 的患者进行了一项队列研究,分别使用量子回归模型和 Cox 比例危险模型,比较了褪黑素启动者和催眠药苯二氮卓类药物(即活性比较药)启动者的口服镇痛处方数量和膝关节/髋关节置换风险。为了阐明因果关系,我们研究了褪黑素对疼痛行为的影响,并探讨了在单碘乙酸大鼠 OA 模型中可能作为褪黑素潜在调节剂的几种代谢物。利用另一项基于社区的队列研究(即湘雅 OA 研究)的数据,我们验证了关键血清代谢物与有症状膝关节 OA 事件之间的关联。与苯二氮卓类催眠药队列(n = 8135)相比,褪黑素队列(n = 813)的后续口服镇痛药处方明显较少(第50百分位数:5 vs. 7,第75百分位数:19 vs. 29,第99百分位数:140 vs. 162),并且在随访期间进行膝关节/髋关节置换的风险较低(危险比 = 0.47,95% Cl:0.30-0.73)。在大鼠身上,口服褪黑素可减轻疼痛行为并提高血清中甘氨酸的水平。在人类(n = 760)中,基线血清甘氨酸水平与发生无症状膝关节退行性关节炎的风险成反比。总之,我们的研究结果表明,口服褪黑素具有治疗 OA 疼痛的巨大潜力。甘氨酸在其镇痛机制中的潜在作用值得进一步研究。
Melatonin is a potential novel analgesic agent for osteoarthritis: Evidence from cohort studies in humans and preclinical research in rats
Melatonin exhibits potential for pain relief and long-term safety profile. We examined the analgesic effects of oral melatonin on osteoarthritis (OA) and investigated the underlying mechanism. Using data from a UK primary care database, we conducted a cohort study in individuals with OA to compare the number of oral analgesic prescriptions and the risk of knee/hip replacement between melatonin initiators and hypnotic benzodiazepines (i.e., active comparator) initiators using quantile regression models and Cox-proportional hazard models, respectively. To elucidate causation, we examined the effects of melatonin on pain behaviors and explored several metabolites that may serve as potential regulatory agents of melatonin in the monoiodoacetate rat model of OA. Using data from another community-based cohort study, that is, the Xiangya OA Study, we verified the association between the key serum metabolite and incident symptomatic knee OA. Compared with the hypnotic benzodiazepines cohort (n = 8135), the melatonin cohort (n = 813) had significantly fewer subsequent prescriptions of oral analgesics (50th percentile: 5 vs. 7, 75th percentile: 19 vs. 29, and 99th percentile: 140 vs. 162) and experienced a lower risk of knee/hip replacement (hazard ratio = 0.47, 95% Cl: 0.30–0.73) during the follow-up period. In rats, oral melatonin alleviated pain behaviors and increased serum levels of glycine. There was an inverse association between baseline serum glycine levels and the risk of incident symptomatic knee OA in humans (n = 760). In conclusion, our findings indicate that oral melatonin shows significant potential to be a novel treatment for OA pain. The potential role of glycine in its analgesic mechanism warrants further investigation.
期刊介绍:
The Journal of Pineal Research welcomes original scientific research on the pineal gland and melatonin in vertebrates, as well as the biological functions of melatonin in non-vertebrates, plants, and microorganisms. Criteria for publication include scientific importance, novelty, timeliness, and clarity of presentation. The journal considers experimental data that challenge current thinking and welcomes case reports contributing to understanding the pineal gland and melatonin research. Its aim is to serve researchers in all disciplines related to the pineal gland and melatonin.