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We read with interest the recently published recommendations for the use of biosimilars in rheumatology practice.1 However, we have some concerns regarding recommendation 6 on the efficacy and safety of switching from the originator biologic to the respective biosimilar. Considering the strong impact of the European League Against Rheumatism recommendations on real-life clinical decisions, such recommendation seems not sufficiently supported by the evidence because available data do not allow to draw definitive conclusion on the switching strategy. To date, the efficacy and safety of infliximab and etanercept biosimilars in substitution of the bio-originators have been assessed in four long-term extension reports following the blinded phase of the respective randomised controlled trials (RCTs),2–5 but the transposition of these results to the real-life practice seems rather questionable. Indeed, patients treated in the setting of real-world practice greatly differ from those enrolled in clinical trials, as suggested by an analysis from the German Rheumatoid Arthritis: Observation of Biologic Therapy (RABBIT) registry showing that only 21%–33% of the included patients would have been eligible for RCTs.6 Also the results of the Norwegian Switch study (NOR-SWITCH) trial do not adequately support the switching strategy from infliximab originator (re-IFX) to infliximab biosimilar (bio-IFX) in patients with inflammatory rheumatic diseases because only 198 (41%) out of 481 enrolled patients had a rheumatic disorder, including 91 (18.9%) spondyloarthritis (SpA), 77 (16%) rheumatoid arthritis (RA) and 30 (6.2%) psoriatic arthritis (PsA).7 Consequently, the study lacks of statistical power with important repercussion on the clinical significance of the results in patients with SpA, RA and PsA. The Danish Nationwide Biologic (DANBIO) registry reported data from a large series of 802 patients with RA, SpA and PsA who were switched from re-IFX to bio-IFX.8 No negative impact of bio-IFX on the disease activity was recorded, but the retention rate was significantly lower as compared with a historical cohort of patients receiving re-IFX (86.8% vs 83.4%; P: 0.03). Similar findings have been recently observed in other clinical series from Turkey.9
Data from the DANBIO registry on the switching from originator etanercept (re-ETN) to biosimilar etanercept (bio-ETN) were recently presented.10 At the end of the follow-up period, bio-ETN was withdrawn in 129 (8.3%) out of 1548 patients who were in clinical remission prior to the switching. Confirming the different clinical characteristics of patients treated in real-life practice, despite a shorter follow-up duration of 5 months, the percentage of withdrawals was higher than in the study of Emery and colleagues4 (5% over 48 weeks). In this sense, the paucity of data from real life and the absence of controlled trials suggest that also recommendation 7 (evidence level 5 and degree of recommendation D)1 may be misleading for clinicians, who may be driven by health authorities to choices made only on an economic basis.
To conclude, in our opinion, available data from real-world clinical practice, somewhat conflicting with those of RCTs, seem to suggest that it is premature to formulate recommendations on the switching strategy from the bio-originator to its biosimilar.
Handling editor Josef S Smolen
Contributors FC and MB equally contributed to writing the manuscript.
Competing interests None declared.
Provenance and peer review Not commissioned; internally peer reviewed.
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