Randomised study of PF-06410293, an adalimumab (ADL) biosimilar, compared with reference ADL for the treatment of active rheumatoid arthritis: results from weeks 26–52, including a treatment switch from reference ADL to PF-06410293

Rieke Alten; Carol Cronenberger; Daniel F Alvarez; Amy E Bock; Ivana Vranic; Wuyan Zhang

doi:10.1136/rmdopen-2021-001578

RMD Open (Aug 2021)

Randomised study of PF-06410293, an adalimumab (ADL) biosimilar, compared with reference ADL for the treatment of active rheumatoid arthritis: results from weeks 26–52, including a treatment switch from reference ADL to PF-06410293

Rieke Alten,
Carol Cronenberger,
Daniel F Alvarez,
Amy E Bock,
Ivana Vranic,
Wuyan Zhang

Affiliations

Rieke Alten: 6 University Medicine, Schlosspark Klinik, Berlin, Germany
Carol Cronenberger: 2 Global Product Development, Inflammation and Immunology, Pfizer Inc, Collegeville, Pennsylvania, USA
Daniel F Alvarez: 2 Global Product Development, Inflammation and Immunology, Pfizer Inc, Collegeville, Pennsylvania, USA
Amy E Bock: 3 Global Product Development, Clinical Development and Operations, Pfizer Inc, Cambridge, Massachusetts, USA
Ivana Vranic: 4 Worldwide R&D, Safety Surveillance Risk Management, Pfizer Inc, Tadworth, UK
Wuyan Zhang: 5 Global Product Development, Biometrics and Data Management, Pfizer Inc, Lake Forest, Illinois, USA

DOI: https://doi.org/10.1136/rmdopen-2021-001578
Journal volume & issue: Vol. 7, no. 2

Abstract

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Objective To investigate the efficacy, safety, immunogenicity and pharmacokinetics of biosimilar adalimumab (ADL) PF-06410293 (ADL-PF; adalimumab-afzb) versus EU-sourced reference ADL (ADL-EU) in patients with active rheumatoid arthritis (RA) on longer-term treatment and after being switched from ADL-EU to ADL-PF.Methods In this multinational, double-blind study, patients with active RA were initially randomised to ADL-PF or ADL-EU for 26 weeks (treatment period (TP) 1). At the start of TP2 (weeks 26–52), patients in the ADL-EU arm were blindly re-randomised 1:1 to remain on ADL-EU (ADL-EU/ADL-EU; n=135) or switched to ADL-PF (ADL-EU/ADL-PF; n=134); patients receiving ADL-PF continued blinded treatment (ADL-PF/ADL-PF; n=283).Results The American College of Rheumatology 20% improvement (ACR20) response rates were comparable between treatment groups at all visits during TP2. At week 52, ACR20 response rates were 82.7% (ADL-PF/ADL-PF), 79.3% (ADL-EU/ADL-EU) and 84.3% (ADL-EU/ADL-PF). Other measures of deep response (ACR50/70, ACR/EULAR-defined remission, EULAR good response, and Disease Activity Score in 28 Joints Based on High-Sensitivity C-Reactive Protein <2.6) and Health Assessment Questionnaire−Disability Index were maintained over TP2 and comparable between groups. Treatment-emergent adverse events were reported in 43.5% (ADL-PF/ADL-PF), 44.4% (ADL-EU/ADL-EU) and 38.3% (ADL-EU/ADL-PF) of patients; there were no clinically meaningful differences in the safety profiles between groups. The percentage of patients who were antidrug antibody positive was comparable overall among ADL-PF/ADL-PF (47.3%), ADL-EU/ADL-EU (54.1%) and ADL-EU/ADL-PF (45.9%).Conclusions The similar efficacy, safety, immunogenicity and pharmacokinetics of ADL-PF and ADL-EU, maintained up to week 52, were unaffected by blinded treatment switch from ADL-EU to ADL-PF at week 26.Trial registration number ClinicalTrials.gov identifier: NCT02480153; EudraCT number: 2014-000352-29.

Published in RMD Open

ISSN: 2056-5933 (Online)
Publisher: BMJ Publishing Group
Country of publisher: United Kingdom
LCC subjects: Medicine
Website: https://rmdopen.bmj.com

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