A systematic literature search on PubMed, Embase, the Cochrane Library, China National Knowledge Infrastructure and WanFang databases (with entries up to August 12, 2019 considered) was performed without any restrictions regarding the region, publication date or language. Titles/abstracts were searched using logic combinations of the following terms: (‘ankylosing spondylitis’ OR ‘spondyloarthritis’) AND (‘non-steroidal anti-inflammatory drugs’ OR ‘etoricoxib’ OR ‘celecoxib’ OR ‘meloxicam’ OR ‘diclofenac’ OR ‘naproxen’) AND ‘randomized controlled trial’. The web-based search was supplemented with manual searches of references of relevant reviews on AS. When multiple studies describing the same population were published, the most complete study was used.

All double-blinded RCTs that enrolled patients fulfilling the modified 1984 AS New York criteria (23) were included and comparisons between different NSAIDs or of an NSAID with placebo were performed. The outcomes reported within 12 weeks were used. Studies were excluded if none of the quantitative outcomes of interest (see below) was reported. Studies on patients with concomitant treatment with prednisone >10 mg/d or biologics were excluded, while those using sulfasalazine for patients who had been using them with stable doses prior to the study were considered.

Two researchers (MDF and JL) independently screened the studies retrieved for eligibility and extracted data from the trials included. The following data were extracted for each eligible RCT: First author, publication year, interventions, study duration, endpoints and patients' characteristics. Disagreements were resolved through discussion. Mean differences (MDs) and standard deviations were used to describe continuous outcomes and the number of events was used for dichotomous outcomes. When the values were not provided in the published article, the data were extracted from graphs. For trials that assessed more than one dose of an NSAID, the effects of different doses were pooled together. The present analysis was based on the intent-to-treat principle, which included all patients receiving at least one dose of the studied drug (20,22,24-27).

Evaluations of methodological quality of the RCTs included were performed independently by two reviewers (MDF and JL) according to the standard criteria of The Cochrane Collaboration (28), which consists of seven items: Random sequence generation, allocation concealment, blinding of participants, blinding of outcome assessment, incomplete outcome data, selective reporting and other bias. Regarding each of the above items, each study received a rating as low, high or unclear and two reviewers assessed each trial. The studies were then divided into three categories: i) Low risk of bias: Low risk of bias for all key domains; ii) moderate risk of bias: Unclear risk of bias for one or more key domains; iii) high risk of bias: High risk of bias for one or more key domains.

The primary efficacy endpoints included the mean change in total pain score, patients' global assessment of disease activity (PGA) (29) and the Bath Ankylosing Spondylitis Functional Index (BASFI) (30). Pain and PGA scores were assessed using a 0-100 mm visual analog scale (VAS). BASFI assessment was performed using a series of 10 specific questions, each answered on a 0-100 mm VAS where 0 indicated ‘easy’ and 100 indicated ‘impossible’ (30). The secondary efficacy endpoints were the proportions of patients reaching the Assessment in Ankylosing Spondylitis 20 improvement criteria (ASAS20) (29), which were defined as an improvement of ≥20% and absolute improvement of ≥10 units (0-100 mm VAS) from baseline in at least 3 of the following 4 domains: PGA, total back pain, BASFI and inflammation/morning stiffness, without any worsening of ≥20% and 10 units in the remaining domain.

The safety endpoints included total AEs, GI events, withdrawals due to AEs and serious AEs during the study. The GI events were defined as any abdominal complaints, including nausea, vomiting, dyspepsia, heartburn, diarrhea, constipation and abdominal pain.

Indirect comparisons were performed using a random-effects Bayesian network meta-analysis with WinBUGS version 1.4.3 (MRC Biostatistics Unit). Bayesian network meta-analysis incorporates direct and indirect comparisons of treatments, so as to derive estimates of effect of one treatment against another and perform a ranking of treatments (31-34).

For continuous data, the MDs were reported from the median of the posterior distribution with the accompanying 95% credible intervals (CrIs). For dichotomous data, the odds ratios (ORs) with the 95% CrIs were presented. Furthermore, the probability of being the best (P_best) for each treatment was estimated (35). The goodness of model fit was assessed using the residual deviance to examine the validity of the network models, which should be close to the data points. To assess the robustness of the results, a sensitivity analysis was performed by including only trials with full daily doses of NSAIDs, i.e. etoricoxib 90 mg/d, celecoxib 400 mg/d, meloxicam 15 mg/d, diclofenac 150 mg/d, naproxen 1,000 mg/d and beta-D-mannuronic acid (M2000) 1,000 mg/d (36).

A traditional meta-analysis was also performed using RevMan version 5.3.3 (Cochrane Collaboration) for the outcomes of withdrawals due to AEs and serious AEs. As these outcomes were rare events (<10%), the Peto ORs with corresponding 95% confidence intervals (CIs) were calculated.

The selection process of trials for inclusion in the present study is summarized in Fig. 1. The literature research identified 1,806 records in total, 1,714 of which were excluded after screening their titles and abstracts. The full text of the 92 remaining, potentially eligible articles was reviewed. Finally, 9 RCTs (18-22,24-27) comprising 3,647 patients focusing on 6 NSAIDs, including etoricoxib, celecoxib, meloxicam, diclofenac, naproxen and M2000, were selected for analysis. All studies compared an NSAID with placebo or a different NSAID. A network diagram of treatment comparisons among these trials is provided in Fig. 2.

The major characteristics of the RCTs included are summarized in Table I. While all of the patients included were diagnosed with AS, there were certain differences, e.g. in terms of the pain score, PGA and BASFI at baseline. The treatment duration varied from 6 to 12 weeks. All of the included studies were double-blinded RCTs. The results of the risk of bias assessment of the included trials are presented in Fig. 3. There was a moderate risk of bias in all trials, mostly due to lack of blinding of outcome assessment or allocation concealment.

All of the 9 trials reported the mean change of the pain score (18-22,24-27). A total of 7 trials reported the PGA (19,20,22,24-27), 7 reported the BASFI (18-20,22,24,25,27) and 6 reported the ASAS20 (18-20,22,24,27).

Compared with placebo, all NSAIDs were significantly more efficacious in reducing pain severity (MDs between -17.49 and -25.99 with a lower value indicating higher efficacy; Fig. 4A). Etoricoxib was significantly more effective than celecoxib in terms of pain alleviation (MD=-8.39, 95% CrI: -16.55 to -0.79). Analysis of ranking probabilities indicated that etoricoxib had the highest probability of being the best treatment in decreasing pain severity (P_best, 73.8%) (Table II).

Similarly, significant improvements in PGA and BASFI were determined in patients receiving NSAIDs compared to placebo (Figs. 4B and 5A). Etoricoxib was superior to celecoxib in reducing the PGA score with statistical significance (MD=-9.51, 95% CrI: -17.34 to -1.45). However, there were no significant differences among the NSAIDs in decreasing the BASFI. All NSAIDs had a significantly higher rate of ASAS20 compared with placebo (ORs between 2.71 and 7.54; Fig. 5B). But celecoxib was significantly less efficacious in reaching ASAS20 than etoricoxib (OR=0.36, 95% CrI: 0.15-0.85). The probability analysis suggested that etoricoxib remained the most effective option for the outcomes of PGA, BASFI and ASAS20 (P_best of 67.2, 76.1 and 71.8%, respectively; Table II).

The test for goodness of model fit suggested that the models of efficacy outcomes were appropriate. In the sensitivity analysis of full-dose NSAIDs trials, all NSAIDs were highly effective in improving pain, PGA, BASFI and achieving the ASAS20, except that diclofenac had an inconclusive higher rate of ASAS20 than placebo (data not shown). Etoricoxib remained the best therapy regarding the outcomes of pain, PGA, BASFI and ASAS20 (P_best of 77.8, 65.6, 66.5 and 67.1%, respectively). However, no significant differences were obtained between etoricoxib and celecoxib in improving pain, PGA scores and ASAS20.

A total of 8 RCTs reported on the occurrence of total AEs, GI events, withdrawals due to AEs and serious AEs (18-22,24,25,27). Meloxicam was not included in the analysis due to a lack of data.

Network meta-analysis demonstrated no statistically significant differences among NSAIDs and placebo regarding the risk of total AEs (Fig. 6A). Additionally, no significant differences were identified in AEs of the M2000 and placebo (OR=0.39, 95% CrI: 0.10-1.43). The probability analysis indicated that M2000 had the greatest probability of being the safest treatment (P_best, 90.5%). Furthermore, M2000 was associated with a lower incidence of AEs than celecoxib and diclofenac (OR=0.26, 95% CrI: 0.06-1.00 and OR=0.23, 95% CrI: 0.05-0.99, respectively).

Regarding the risk of GI events, patients treated with diclofenac and naproxen had a significantly higher risk than those taking placebo (OR=2.87, 95% CrI: 1.06-7.67 and OR=2.38, 95% CrI: 1.08-4.93, respectively; Fig. 6B). No significant differences in terms of GI events were determined among the different NSAIDs. However, M2000 had a considerable probability of being ranked as the safest drug for decreasing GI events (62.2%). Regarding withdrawals due to AEs and serious AEs, there were no statistically significant differences among NSAIDs and placebo (Fig. 7A and B).

The test for goodness of model fit suggested that the models of safety endpoints were appropriate. In the sensitivity analysis of full-dose trials, no significant differences in total AEs were identified among NSAIDs and placebo groups. Additionally, no significant differences were identified in the GI events for diclofenac and naproxen when compared with the placebo. M2000 remained the safest therapy for the outcomes of AEs and GI events (P_best of 87.3 and 61.4%, respectively). The results of withdrawals due to AEs and serious AEs remained stable during sensitivity analysis.