Research ArticleArticle
Open Access

Continuation of Methotrexate Resulted in Better Clinical and Radiographic Outcomes Than Discontinuation upon Starting Etanercept in Patients with Rheumatoid Arthritis: 52-week Results from the JESMR Study

HIDETO KAMEDA, KATSUAKI KANBE, ERI SATO, YUKITAKA UEKI, KAZUYOSHI SAITO, SHOUHEI NAGAOKA, TOSHIHIKO HIDAKA, TATSUYA ATSUMI, MICHISHI TSUKANO, TSUYOSHI KASAMA, SHUNICHI SHIOZAWA, YOSHIYA TANAKA, HISASHI YAMANAKA and TSUTOMU TAKEUCHI
The Journal of Rheumatology August 2011, 38 (8) 1585-1592; DOI: https://doi.org/10.3899/jrheum.110014

Abstract

Objective. The aim of the Efficacy and Safety of Etanercept on Active Rheumatoid Arthritis Despite Methotrexate Therapy in Japan (JESMR) study is to compare the efficacy of continuation versus discontinuation of methotrexate (MTX) when starting etanercept (ETN) in patients with active rheumatoid arthritis (RA).

Methods. In total, 151 patients with active RA who had been taking MTX were randomized to either ETN 25 mg twice a week with 6–8 mg/week MTX (the E+M group), or ETN alone (the E group). The primary endpoint at Week 52 was the radiographic progression assessed by van der Heijde-modified Sharp score.

Results. The mean progression in total score at Week 52 was not significantly different, statistically, between the E+M group and the E group (0.8 vs 3.6, respectively; p = 0.06). However, a significant difference was observed in radiographic progression between Weeks 24 and 52 (0.3 vs 2.5; p = 0.03), and the mean progression of the erosion score was negative in the E+M group, which was significantly better than the E group at Week 52 (–0.2 vs 1.8; p = 0.02). Clinically, the cumulative probability plot of the American College of Rheumatology (ACR)-N values at Week 52 clearly demonstrated a superior response in the E+M group than in the E group. ACR20, 50, and 70 response rates at Week 52 in the E+M group (86.3%, 76.7%, and 50.7%) were significantly greater than those in the E group (63.8%; p = 0.003, 43.5%; p < 0.0001 and 29.0%; p = 0.01, respectively).

Conclusion. MTX should be continued when starting ETN in patients with active RA. (ClinicalTrials.gov: NCT00688103)

Key Indexing Terms:

The introduction of biological agents such as tumor necrosis factor-α (TNF-α) inhibitors into the therapeutic strategy for rheumatoid arthritis (RA) resulted in a shift characterized by the sufficient inhibition of arthritic signs and symptoms, radio graphic progression, and functional disability1,2. However, the optimal use of those agents remains to be determined. For example, etanercept (ETN) has been shown to be effective for RA both as a monotherapy and as combination therapy with methotrexate (MTX), and the latter has proved its superiority to the former in MTX-naive patients. Because MTX is the first-line drug for most patients with RA, and ETN is much more expensive than MTX, ETN tends to be started for MTX-refractory, but not MTX-naive, patients in actual clinical practice3,4.

The Add Enbrel or Replace Methotrexate (ADORE) trial was the first to consider whether adding ETN to MTX is better than replacing MTX with ETN. The trial failed to demonstrate the superiority of continuing MTX rather than discontinuing it upon starting ETN therapy5. Because the ADORE trial was only 16 weeks, with a regimen of MTX tapering over the initial 4 weeks, there could be no marked difference between continuation versus discontinuation of MTX, if any difference at all. Longterm efficacy and safety was not compared between the 2 groups.

Therefore, we conducted the Efficacy and Safety of Etanercept on Active Rheumatoid Arthritis Despite Methotrexate Therapy in Japan (JESMR) study to address the differences in clinical activity, radiographic progression, and functional disability over 2 years. The 24-week results from the JESMR study demonstrated that continuation of MTX after the start of ETN was better than discontinuation of MTX, in terms of European League Against Rheumatism (EULAR) response and American College of Rheumatology (ACR20) response rates6. We report the 52-week results, focusing on the radiographic progression measured by van der Heijde-modified Sharp (vdH-Sharp) score (which had been included in the co-primary endpoint), the ACR response7, and functional disability evaluated by the Health Assessment Questionnaire-Disability Index (HAQ-DI)8.

MATERIALS AND METHODS

Patients

Our prospective, randomized, open-label study was conducted at 45 institutions in Japan between June 2005 and January 2007. The study protocol (ClinicalTrials.gov: NCT00688103) was approved by an institutional ethics committee of each participating institute. All patients provided written informed consent in accord with the Declaration of Helsinki.

Patients had to be at least 18 years of age, had to fulfill the ACR 1987 revised classification criteria for RA, and had to meet the guidelines for the proper use of ETN in Japan [having at least 6 tender joints and 6 swollen joints, and either a serum C-reactive protein level of > 2 mg/dl or erythrocyte sedimentation rate (ESR) ≥ 28 mm at 1 h, with adequate safety profiles]9. Precise inclusion and exclusion criteria have been reported6.

Baseline characteristics of the patients were comparable between the ETN group (E group) and the ETN + MTX group (E+M group)6. More than 80% of the patients were women, at an average age of around 57 years, and with a disease duration of around 9 years (Table 1).

View this table:
Table 1.

Demographic features of the patients. Except where indicated otherwise, values are mean ± SD.

The rheumatoid factor was positive in about 90% of patients. The mean MTX dose at enrollment was 7 mg/week, with supplementary folic acid in 38%–52% of patients6. The baseline total vdH-Sharp score and its estimated yearly progression at study entry were very high in both groups, indicating the severity of disease of our patients (Table 1).

Procedures

Patients who had agreed to receive ETN for active RA were randomly assigned to continue MTX (6–8 mg/wk, an approved dose in Japan during the study period), that is, MTX + ETN combination therapy, or to discontinue MTX and switch to ETN monotherapy. Enrollment and randomization were performed on the University Hospital Medical Information Network Website (Tokyo, Japan) on the day of obtaining informed consent. Between June 2005 and January 2007, a total of 151 patients from 34 institutes in Japan were enrolled in the JESMR study. All patients enrolled were treated with ETN 25 mg as a subcutaneous injection twice weekly.

The co-primary endpoints of the JESMR study showed a good response according to the EULAR criteria, as based on a 28-joint Disease Activity Score (DAS28) and the ACR50 response rate at Week 24, as reported6, and the radiographic progression assessed by vdH-Sharp score ranged from 0 to 448 over 52 weeks10. Two trained readers independently scored each radiograph of hands and feet at baseline and at Weeks 24 and 52. Patient identities and treatment groups were blinded to the readers, although the chronological sequence of the radiographs in sets was unmasked. The smallest detectable difference between readers at baseline was 9.9 (standard deviation of the per-patient difference between the readers divided by the square root of 2), and the smallest detectable change over 52 weeks was 1.9.

Statistical analysis

A sample size of 150 patients per treatment group was first calculated to provide > 90% power (α = 0.05, ß = 0.1) with 15% non-completion rate during 24 weeks. This calculation assumed that the ACR50 response rate would be 40% in the E group and 60% in the E+M group. However, because of the delay in patient recruitment, we completed the patient enrollment in January 2005 at a total of 151 patients (74 in the E group and 77 in the E+M group). This decision was based on the calculation that a sample size of 64 per treatment group was needed to provide more than 90% power (α = 0.05, ß = 0.1), assuming that the mean radiographic progression by vdH-Sharp score at 52 weeks would be 1.50 in the E group and −0.80 in the E+M group.

Efficacy analyses included all patients who took the study drugs and had a valid baseline and ≥ 1 on-therapy value for each endpoint. The last observation carried forward (LOCF) and linear imputation were used for the analysis of clinical and radiographic efficacy, respectively, for missing data. All analyses were performed by the CMIC Co. Ltd. Data Center (Osaka, Japan). The proportions of participants who met given criteria were compared with Fisher’s exact test, while the mean values between the groups were compared with the Mann-Whitney U test.

RESULTS

Primary endpoint: radiographic efficacy

Efficacy analysis was performed in 69 patients of the E group and 73 of the E+M group (Figure 1). The rate of per-protocol patients was smaller in the E group than in the E+M group, chiefly because of a lack of efficacy after 24 weeks.

Figure 1.
Figure 1.

Disposition of patients during 52 weeks of the Efficacy and Safety of Etanercept on Active Rheumatoid Arthritis Despite Methotrexate Therapy in Japan (JESMR) study. A total of 151 patients were enrolled, 74 in the etanercept (ETN) group and 77 in the etanercept and methotrexate (MTX) group, and 108 patients (71.5%) completed 52 weeks per protocol.

The baseline vdH-Sharp score was 114.5 ± 85.7 in the E group and 113.1 ± 85.6 in the E+M group (p = 0.99). Cumulative probability plot analysis suggested less overall radiographic progression in the E+M group than in the E group during the 52 weeks (Figure 2A). However, the primary endpoint at 52 weeks was not met because the numerical superiority of the E+M group over the E group in the change in vdH-Sharp score over 52 weeks did not reach a statistically significant difference (0.8 vs 3.6, respectively; p = 0.06), as shown in Figure 2B. Nonetheless, the mean progression in the erosion score was negative exclusively in the E+M group, at both 24 weeks and 52 weeks (−0.1 and −0.2, respectively), and it was significantly better than that in the E group at 52 weeks (1.8; p = 0.02). Moreover, a significant difference was observed in the total score progression between Weeks 24 and 52 (2.5 in the E group and 0.3 in the E+M group; p = 0.03), suggesting the carrying-over effect of MTX for the initial few months.

Figure 2.
Figure 2.

Change in van der Heijde-modified Sharp (vdH-Sharp) total score represented by cumulative probability plot (A) and the mean change of total score as well as erosion and joint space narrowing scores (B) over 52 weeks. Values are mean ± SEM, compared by Mann-Whitney U test (*p = 0.03; **p = 0.02) between groups. ETN: etanercept group; ETN+MTX: etanercept plus methotrexate group.

The proportion of patients showing no radiographic progression over 52 weeks (change in vdH-Sharp score ≤ 0.5) was 39.6% in the E group and 57.4% in the E+M group (p = 0.07), and the proportion showing no clinically significant radiographic progression (change in vdH-Sharp score ≤ smallest detectable change) was 58.5% in the E group and 67.6% in the E+M group (p = 0.34).

Clinical efficacy

Next we performed for the first time a cumulative probability plot analysis of ACR-N values at 52 weeks for both treatment groups (Figure 3). This analysis clearly demonstrated the superior clinical response in the E+M group compared to the E group, and implied that the continuation of MTX would be beneficial, at least to some extent, in nearly 80% of patients upon the commencement of ETN. Indeed, the mean ± SD of ACR-N was 60.9 ± 29.3 for the E+M group, which was significantly greater than that of the E group (31.1 ± 50.8; p = 0.0003). In addition, the area under the curve of the ACR-N throughout 52 weeks was also significantly different between the groups (26.8 ± 13.0 in the E+M group and 18.4 ± 19.0 in the E group; p = 0.008). At the same time, we could easily see the superior ACR response rates in the E+M group compared to the E group, as shown in Figure 3: 86.3% vs 63.8% in ACR20 (p = 0.003), 76.7% vs 43.5% in ACR50 (p < 0.0001), and 50.7% vs 29.0% in ACR70 (p = 0.01), respectively (Table 2). Except for patient global assessment, all important clinical measures, including HAQ-DI, favored the continuation of MTX at Week 52, as shown in Table 2.

Figure 3.
Figure 3.

American College of Rheumatology (ACR) values at 52 weeks; 69 patients in the etanercept group (ETN) and 73 in the etanercept plus methotrexate group (ETN+MTX) were analyzed. Broken lines indicate ACR20, ACR50, and ACR70 values.

View this table:
Table 2.

Comparison of the clinical responses between treatment groups. Except where indicated otherwise, values are mean ± SD.

Safety analyses

Safety profiles between the 2 treatment groups were comparable (Table 3). Similar overall adverse events were observed between the treatment groups. The frequency of general disorders and administration site conditions, mostly injection site reaction (13 in the E group and 7 in the E+M group), tended to be higher in the E group than the E+M group, as well as skin and subcutaneous tissue disorders including eczema and erythema developed at sites unrelated to ETN injection. In contrast, the frequency of hepatobiliary disorders, mostly liver dysfunction, tended to be higher in the E+M group than in the E group. The result was the same between the groups with metabolism and nutrition disorders such as hyperlipidemia, diabetes mellitus, and hyperuricemia. Serious adverse events in the E group were bone fractures in 2 patients (humeral bone and osteoporotic vertebrae). Serious adverse events in the E+M group were bone fractures in 3 (femoral bone in 2, cranial bone in 1), and in 1 patient each, congestive heart failure, cellulitis, herpes zoster, brain hemorrhage, and mammary carcinoma. Cranial bone fracture from a traffic accident and cellulitis developed in the same patient. Treatment was withdrawn because of injection site reaction in 4 patients in the E group and mammary carcinoma in 1 patient in the E+M group. Thus, the safety profile was comparable between 2 groups.

View this table:
Table 3.

Adverse events. Values are numbers of patients who developed (serious) adverse events.

DISCUSSION

In a previous report on the 24-week results of the JESMR study, the superiority of a continuation of MTX over its discontinuation when starting ETN in terms of controlling clinical disease activity (the rates of EULAR good response, remission, and ACR20 response, but not ACR50 and 70 responses) was indicated6. Our 52-week results not only confirmed the previous ones but also proved, for the first time, that the combination of ETN and MTX resulted in a better outcome in radiographic progression determined by vdH-Sharp score, especially in erosions, even in patients who had shown an incomplete response to MTX. The mean progression in total score at Week 52 was not significantly different, statistically, between the E+M group and the E group (0.8 vs 3.6, respectively; p = 0.06). The chief reason for failure to achieve the primary endpoint seemed to be the reduction in sample size due to delayed recruitment of patients. However, a significant difference was observed in radiographic progression between Weeks 24 and 52 (0.3 vs 2.5, respectively; p = 0.03), and the mean progression of the erosion score was negative in the E+M group, which was significantly better than the E group at Week 52 (–0.2 vs 1.8, respectively; p = 0.02). Further, all important clinical measures, including ACR responses, EULAR responses, and HAQ-DI, favored the continuation of MTX at Week 52.

Infliximab was the first biological agent to have demonstrated complete inhibition of radiographic progression in combination with MTX in MTX-refractory patients with active RA11. ETN and adalimumab showed similar efficacy in halting joint destruction in combination with MTX. Both agents proved their superior clinical and radiographic efficacy with MTX combination over monotherapy in MTX-naive patients with early RA (the PREMIER study12) or established RA (the TEMPO study13). Our results led to the conclusion that anti-TNF biological agents should be used in combination with MTX as far as possible, whether the patients are MTX-naive or MTX-refractory, and they strongly support the recent recommendations of the ACR3 and EULAR4.

The reason that the continuation of MTX, which had only shown an inadequate response in the enrolled patients, demonstrated a significant effect with ETN treatment may be as follows: (1) the efficacy of MTX was insufficient but not negligible even as a monotherapy; and (2) the targets of MTX, including activated T cells14, are not identical to those of ETN, resulting in additive or synergistic effects between MTX and ETN. A recent report from the GO-FORWARD study also demonstrated a better clinical response to golimumab with MTX continuation than with its discontinuation in MTX-refractory patients with RA15. The fact that many clinical (ACR50 and 70 response rates and HAQ-DI score) and radiographic (erosion score progression) measures showed statistically significant differences at Week 52 but not at Week 246 may explain why the ADORE study did not show a difference between MTX continuation and discontinuation5,16. The usefulness of MTX continuation seems to be true with all biological agents targeting TNF.

The average disease duration of about 9 years significantly affected the radiographic and HAQ-DI results in the JESMR study. Despite a long disease duration, our patients showed a rapid progression in vdH-Sharp scores with a mean estimated yearly progression of 18–21 (Table 1). This result was close to that of patients with early active RA who were enrolled in the PREMIER study (26–27)12 and was much higher than that in the TEMPO study (8–11)13. This fact may explain, at least in part, the similarities and differences in the radiographic progression results among those clinical trials. In addition, the radiographic progression in our patients could be more aggressive in the initial few years after disease onset. Therefore, whether our results are also true for patients with early RA of < 6 months’ duration should be examined in the near future.

Most of the adverse events, including infections and skin disorders other than injection site reactions, were observed throughout 52 weeks. However, as expected, injection site reaction was less frequent after 24 weeks when compared to our previous report6. In contrast, most of the bone fractures, which were the predominant serious adverse events in our study, developed after 24 weeks. This could be attributed at least in part to the improved activity of daily life of our patients treated with ETN as demonstrated by the HAQ-DI improvement (Table 2).

Our study has several limitations. First, it was not double-blinded. Therefore, one may assume there was an awareness of the treatment effect evaluations by physicians and by patients. However, the changes in acute-phase reactants (Table 2) and radiographic results (Figures 2A and 2B) make that unlikely. Further, there were considerable withdrawal rates in the E group (Figure 1), mostly because of a lack of efficacy after 24 weeks. Since this had been expected, because this study was not double-blinded, we applied the LOCF methods for clinical efficacy analyses instead of intention-to-treat analyses. In addition, the sample size of the JESMR study limited the power of detection of differences between the 2 treatment groups. Actual ACR50 response rates and the radiographic progression were greater than our expectations in both treatment groups. Finally, the dose of MTX approved by the Japanese Ministry of Health, Labor and Welfare had been only 6–8 mg/week throughout this study17,18 although, concordantly, the use of supplementary folic acid was also limited to about half of the patients receiving MTX. In February 2011, the Ministry approved MTX use up to 16 mg/week for patients with RA. Nonetheless, overall clinical and radiographic outcomes of infliximab added to MTX 7–9 mg/week in Japan19,20,21,22,23 were comparable to those in the ATTRACT11 and ASPIRE studies24.

Future studies may also include the prediction of patient outcome after the start of ETN therapy, addressing the question of who can be sufficiently controlled by simply switching from MTX to ETN, and who can be sufficiently controlled by the addition of ETN to MTX but not by switching from MTX to ETN. These subanalyses are now under investigation in the Japan Biological Agent Integrated Consortium (JBASIC) study group.

Our results demonstrated for the first time that the continuation of MTX resulted in a better clinical and radiographic outcome, at least in some aspects, than its discontinuation after the start of ETN in patients with active RA despite MTX therapy. We also showed the usefulness of cumulative probability plot presentation not only for radiographic progression but also for clinical responses such as ACR-N, which may be included in future clinical trials.

Acknowledgment

We acknowledge the following investigators, their staff and all institutions, affiliated and otherwise: K. Shiozawa (Konan Kakogawa Hospital); S. Kobayashi (Juntendo University School of Medicine, Koshigaya Hospital); N. Tamura (Juntendo University School of Medicine, Juntendo Hospital); T. Sawada (The University of Tokyo Hospital); S. Yamana (Higashihiroshima Memorial Hospital); Y. Honda (Kurume University Hospital); T. Kojima (Nagoya University Hospital); H. Takahashi (Sapporo Medical University Hospital); T. Sugiyama (Shimoshizu National Hospital); A. Taniguchi (Tokyo Women’s Medical University, Institute of Rheumatology); T. Nanki (Tokyo Medical and Dental University Hospital, Faculty of Medicine); M. Yamamura (Aichi Medical University Hospital); K. Kurasawa (Dokkyo Medical University Hospital); K. Chiba (Fukushima Daiichi Hospital); K. Kato (Fujita Health University Hospital); K. Ezawa (Kurashiki Kousai Hospital); T. Fujii (Kyoto University Hospital); S. Nakata (Matsuyama Red Cross Hospital); S. Tamachi (Mie Chuo Medical Center); Y. Kawabe (National Hospital Organization Ureshino Medical Center); R. Yano (Okayama University Hospital); T. Kuroiwa (The Hospital of Hyogo College of Medicine); A. Kubota (Toho University Omori Medical Center); Hyogo Prefectural General Rehabilitation Center; Rokko Island Hospital; Kurume University Medical Center; Nagasaki University Hospital of Medicine and Dentistry; Nihon University Itabashi Hospital; Niigata University Medical and Dental Hospital; Osaki Citizens’ Hospital; Saiseikai Takaoka Hospital; St. Marianna University School of Medicine Hospital; Taihakusakura Hospital; Tohoku Kosei Nenkin Hospital; Tohoku University Hospital; and Tsukuba University Hospital.

Footnotes

  • Supported by the Advanced Clinical Research Organization (Japan) and by research grants from the Japanese Ministry of Health, Labor and Welfare.

  • Full Release Article. For details see Reprints/Permissions at jrheum.org

  • Accepted for publication March 15, 2011.

Free online via JRheum Full Release option

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