Abstract

ObjectiveTo compare the efficacy, serum drug concentrations, immunogenicity, and safety of FKB327 with the adalimumab reference product (RP) in combination with methotrexate in patients with moderate-to-severe, active rheumatoid arthritis (RA).MethodsPatients were randomized 1:1 in a double-blind study (NCT02260791), received 40 mg of FKB327 or RP by subcutaneous injection every other week for 24 weeks (Period I), then re-randomized 2:1, remaining on the same study drug or switching to the other up to week 54 in an open-label extension (Period II, NCT02405780). Efficacy was evaluated using American College of Rheumatology (ACR20) response rate difference at week 24 with equivalence margins of ± 13% and − 12% to + 15% using 95% and 90% confidence intervals (CIs), respectively. Efficacy, serum drug concentrations, immunogenicity, and safety were compared at week 54.ResultsA total of 730 patients were randomized in Period I (n = 367 FKB327, n = 363 RP), and 645 transitioned to Period II (n = 216 FKB327–FKB327, n = 108 FKB327–RP, n = 108 RP–FKB327, n = 213 RP–RP). At week 24, ACR20 response rates were 74.1% with FKB327 versus 75.7% with RP. 95% and 90% CI of the response rate difference were − 7.9 to 4.7% and − 7.3 to 3.6%, respectively, meeting predefined equivalence margins. The ACR20 response rate remained over 70% of patients to week 54 with all treatment sequences. In Period I, mean trough serum drug concentrations were slightly higher for patients receiving FKB327 than those receiving RP. Mean concentrations were stable over time and reflected steady state in Period II. The proportions of patients with samples positive for neutralizing antidrug antibodies (ADAs) were comparable (57.7% with FKB327 vs. 55.5% with RP) at week 24, and no consistent difference in ADA were seen between continuous and switched treatments in Period II. Efficacy was slightly reduced in the small proportion of patients with high ADA titers in all treatment groups. No clinically significant differences were observed in the incidence of commonly reported treatment-emergent adverse events between the treatments across Periods I and II.ConclusionFKB327 was equivalent to RP in clinical efficacy and demonstrated comparable safety and immunogenicity in patients with moderate-to-severe RA. No effect of switching between FKB327 and RP was observed.Trial registrationClinicalTrials.gov, NCT02260791, Registered 29 July 2014.ClinicalTrials.gov, NCT02405780, Registered 17 July 2015.

Highlights

  • Rheumatoid arthritis (RA) is a chronic autoimmune disease characterized by joint pain, stiffness, swelling, and loss of function

  • FKB327 is being developed as a proposed biosimilar product that contains adalimumab but has different excipients to those in reference product (RP), all of which are commonly used in biologic treatments

  • In the safety analysis set (SAS), 216 patients had received FKB327 in Period I and Period II, 108 patients received FKB327 followed by RP, 108 patients received RP followed by FKB327, and 213 patients received RP for both periods

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Summary

Introduction

Rheumatoid arthritis (RA) is a chronic autoimmune disease characterized by joint pain, stiffness, swelling, and loss of function. The TNF-α inhibitor adalimumab (Humira®; AbbVie), hereafter referred to as the reference product (RP), is a biological diseasemodifying anti-rheumatic drug (bDMARD) that has been approved for the treatment of patients with moderate-to-severe, active RA [3,4,5]. RP is licensed for use in combination with the conventional synthetic disease-modifying anti-rheumatic drug (DMARD) methotrexate (MTX) or as monotherapy in many other indications [5]. As existing licensed therapies are approaching or have passed their patent expiration, increasing numbers of TNFα inhibitor biosimilars for RA therapy are currently in clinical development [6,7,8,9,10,11]. FKB327 is being developed as a proposed biosimilar product that contains adalimumab but has different excipients to those in RP, all of which are commonly used in biologic treatments. A subsequent Phase I clinical study of FKB327 and RP has demonstrated comparable pharmacokinetic, safety, and immunogenicity profiles [13]

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