Melatonin is a potential novel analgesic agent for osteoarthritis: Evidence from cohort studies in humans and preclinical research in rats

Author:

Li Hui123,Zhou Bin23,Wu Jing23,Zhang Yuqing45,Zhang Weiya67,Doherty Michael67,Deng Xinjia1,Wang Ning123,Xie Dongxing123,Wang Yilun123,Xie Hui2389,Li Changjun23910,Wei Jie12311,Lei Guanghua1239ORCID,Zeng Chao1239

Affiliation:

1. Department of Orthopaedics, Xiangya Hospital Central South University Changsha China

2. Key Laboratory of Aging‐related Bone and Joint Diseases Prevention and Treatment, Ministry of Education, Xiangya Hospital Central South University Changsha China

3. Hunan Key Laboratory of Joint Degeneration and Injury, Xiangya Hospital Central South University Changsha China

4. Department of Medicine, Division of Rheumatology, Allergy, and Immunology, Massachusetts General Hospital Harvard Medical School Boston Massachusetts USA

5. The Mongan Institute, Massachusetts General Hospital Harvard Medical School Boston Massachusetts USA

6. Academic Rheumatology, School of Medicine University of Nottingham Nottingham UK

7. Pain Centre Versus Arthritis University of Nottingham Nottingham UK

8. Movement System Injury and Repair Research Center, Xiangya Hospital Central South University Changsha China

9. National Clinical Research Center for Geriatric Disorders, Xiangya Hospital Central South University Changsha China

10. Department of Endocrinology, Endocrinology Research Center, Xiangya Hospital Central South University Changsha China

11. Department of Epidemiology and Health Statistics, Xiangya School of Public Health Central South University Changsha China

Abstract

AbstractMelatonin 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.

Funder

National Natural Science Foundation of China

Publisher

Wiley

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