The expression levels of TNF-α and IL-6 in the culture supernatant were measured using commercial enzyme-linked immunosorbent assay ELISA kits, as indicated by the manufacturer BioLegend, San Diego, CA, USA. The absorbance was measured at nm. The concentration of cytokines in the culture supernatant was determined from their respective standard curves.

Male ICR mice at the age of 4—5 weeks were purchased from Nomura Siam International Co. Animals were allowed to acclimatize to laboratory conditions for at least one week before the test procedures. Ethical approval was obtained from the Institutional Animal Care and Use Committee, Faculty of Pharmaceutical Sciences, Chulalongkorn University, Bangkok, Thailand, before the commencement of the study Protocol No.

All the tests were conducted in compliance with the ARRIVE guidelines Animal Research: Reporting of In Vivo Experiments. All treatments were suspended in 0.

Before the nociceptive induction, mice were orally administered different treatments 8 mice per group and placed in acrylic chambers for 1 h for acclimatization to the experimental setup. Behind each acrylic chamber, two mirrors were placed at a 45° angle to facilitate the behavioral observations.

Immediately after formalin administration, mice were placed back in the acrylic chambers, and pain-like behaviors were recorded for 40 min.

Then the recorded videos were analyzed using the Behavioral Observation Research Interactive Software BORIS 71 , and the duration of hind paw licking in each 5 min was determined. Hind paw licking in 0—5 min was considered early phase I, wherein 10—40 min period was considered later phase II.

The percentage of antinociception in either phase was calculated using the following formula:. where D treatment is the duration of hind paw licking for each treated mouse, and D control is the average time of hind paw licking in the vehicle-treated group.

The interaction between two compounds was determined according to the method described by Tallarida et al. The theoretical ED 50 for curcumin-metformin combination was calculated by assuming the occurrence of additive interaction between compounds by using the following equation:. where ED 50 add is the theoretical ED 50 ; ED 50 cur and ED 50 met are experimental ED 50 of curcumin and metformin, respectively; and f is the fixed ratio of each compound 0.

Then the theoretical and experimental ED 50 ED 50 mix values for the combination were compared using the t-test. The interaction was interpreted as additive if the ED 50 add and ED 50 mix were not significantly different.

If the ED 50 mix was significantly lower or higher than the ED 50 add , the interaction was defined as synergistic or antagonistic, respectively. Moreover, the type of interaction between two compounds was also demonstrated by calculating combination index CI and isobologram analysis. The CI was calculated using the following equation:.

Moreover, the type of interaction was also demonstrated by an isobologram as described by Tallarida et al. Briefly, the ED 50 doses of curcumin and metformin were plotted as axial points in a Cartesian plot, and then the ED 50 add and ED 50 mix.

Then a straight-line connecting ED 50 met and ED 50 cur was plotted additive line. The type of interaction was determined by the location of the ED 50 mix relative to the additive line.

cn 73 , and Similarity ensemble approach SEA Search Server bkslab. org These databases can predict the targets of curcumin and metformin at the cellular and mechanistic levels.

Furthermore, inflammatory pain-related targets were used to identify the potential targets in inflammatory pain. Homo sapiens was selected as the target species. The intersection between the target genes of curcumin, metformin, and curcumin and metformin combination and inflammatory pain-related targets was assessed using Venny 2.

The intersection of genes of curcumin-metformin combination and genes of target diseases were further used as a potential target of curcumin-metformin combination on inflammatory pain. The protein—protein interaction was performed and constructed using the STRING database and exported into Cytoscape software 3.

The cytoHubba v. To illustrate the potential mechanism of action and pathways, enrichment analysis was performed using Gene Ontology GO and Kyoto Encyclopedia of Genes and Genomes KEGG pathway enrichment analyses. The KEGG analysis was performed as previously described Three days before the test, mice were trained to remain on a rotating rod at a constant speed 18 rpm for s every day On the experiment day, mice were tested before drug administration, and mice capable of remaining on the rod for on three successive trials were used for the subsequent experiment.

Four independent animal groups 6 mice per group were examined for motor coordination after oral administration of either vehicle, the highest dose of curcumin, metformin or curcumin-metformin combination. The latency to fall was recorded at , , , , and min post-treatment with the cut-off value of s.

The effect of test compounds on the short-term locomotive behaviors was assessed using an automated home-cage monitoring system, LABORAS Metris, Hoofddorp, Netherlands. LABORAS system picks up vibrations generated by the movements of the rodent and converts those to the behavioral classifications, including climbing, rearing, locomotion, and immobility One hour after, mice were placed in the LABORAS cage, and locomotive behavior was recorded for 30 min.

The effect of each compound on short-term locomotive behavior was determined separately for each behavioral measure and presented as a cumulative value of both behavioral duration and frequency. Behavioral measurements were started at Behavioral analysis was subsequently divided into 2 h intervals.

The data analysis was performed using GraphPad Prism 9. All the collected data were summarized with counts and percentages for categorical variables.

The difference between groups was determined by the One-way analysis of variance ANOVA followed by the post hoc test. All the animal protocols were approved by the Institutional Animal Care and Use Committee IACUC of the Faculty of Pharmaceutical Sciences, Chulalongkorn University Protocol No.

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Download references. The authors would also like to thank the th Anniversary Chulalongkorn University Fund for Doctoral Scholarship and Scholarship for International Graduate Students supported by Graduate School, Chulalongkorn University P.

We also thank the Second Century Fund C2F Postdoctoral Fellowship, Chulalongkorn University H. The authors thank Mr. Iksen, Department of Pharmacology and Physiology, Faculty of Pharmaceutical Sciences, Chulalongkorn University for guiding the authors through the network pharmacology analysis. Pharmaceutical Sciences and Technology Program, Faculty of Pharmaceutical Sciences, Chulalongkorn University, Bangkok, , Thailand.

Department of Pharmacology and Physiology, Faculty of Pharmaceutical Sciences, Chulalongkorn University, Bangkok, , Thailand. Institute of Nutrition, Mahidol University, Salaya, Nakhon Pathom, , Thailand. Molecular Probes for Imaging Research Network, Faculty of Pharmaceutical Sciences, Chulalongkorn University, Bangkok, , Thailand.

Metallurgy and Materials Science Research Institute, Chulalongkorn University, Bangkok, , Thailand. Center of Excellence in Natural Products for Ageing and Chronic Diseases, Chulalongkorn University, Bangkok, , Thailand.

Department of Food and Pharmaceutical Chemistry, Faculty of Pharmaceutical Sciences, Chulalongkorn University, Bangkok, , Thailand. You can also search for this author in PubMed Google Scholar. conceptualized and designed the study, performed in vitro and in vivo experiments, analyzed and interpreted data, and wrote the first draft of the manuscript.

conceptualized and designed the study, performed in vitro, and in vivo experiments, and wrote the manuscript. conceptualized and designed the in vitro study.

and P. advised, interpreted, and commented on the manuscript. conceived, designed, drafted, and supervised the study.

The manuscript was written through the contributions of all authors. All authors reviewed and approved the final version of the manuscript. Correspondence to Pasarapa Towiwat. Springer Nature remains neutral with regard to jurisdictional claims in published maps and institutional affiliations.

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Reprints and permissions. Dasuni Wasana, P. Curcumin and metformin synergistically modulate peripheral and central immune mechanisms of pain. Sci Rep 12 , Download citation. Received : 24 November Accepted : 26 May Published : 11 June Anyone you share the following link with will be able to read this content:.

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nature scientific reports articles article. Download PDF. Subjects Drug discovery Pain. Abstract Metformin is a well-tolerated antidiabetic drug and has recently been repurposed for numerous diseases, including pain.

Figure 1. Chemical structures of metformin hydrochloride A and curcumin B. Full size image. Results and discussion Curcumin, in combination with metformin, synergistically inhibited the NO production of LPS-stimulated RAW Figure 2.

Figure 3. Figure 4. Figure 5. Figure 6. Full size table. Figure 7. Figure 8. Figure 9. Figure Conclusion In summary, this study suggests for the first time that curcumin combined with metformin exerts synergistic anti-inflammatory effects in both in vitro and in vivo conditions.

Methods Cell culture RAW Cytotoxicity assay Twenty-four hours after preconditioning of seeded cells, the medium was replaced with µL of serum-free DMEM media containing different concentrations of curcumin 1.

NO assay The nitrite production in the culture supernatant was determined by the Griess reaction. Median-effect analysis: computerized simulation by CompuSyn The type of interaction between curcumin and metformin on RAW Data availability Data will be made available upon request.

Contact pasarapa. c chula. References IASP. Article PubMed PubMed Central Google Scholar Baral, P. Article CAS PubMed PubMed Central Google Scholar Ji, R. Article CAS PubMed PubMed Central Google Scholar Prescott, S.

Chapter Google Scholar Augusto, P. Article CAS PubMed Google Scholar Weng, W. Article CAS PubMed Google Scholar Ge, A.

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