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Cited 15 time in webofscience Cited 12 time in scopus
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Efficacy and safety of switching from rituximab to biosimilar CT-P10 in rheumatoid arthritis: 72-week data from a randomized Phase 3 trialopen access

Authors
Shim, Seung CheolBožić-Majstorović, LjubinkaKasay, Alfredo BerrocalEl-Khouri, Elias ChalouhiIrazoque-Palazuelos, FedraMolina, Francisco Fidencio ConsMedina-Rodriguez, Francisco G.Miranda, PedroShesternya, PavelChavez-Corrales, JoseWiland, PiotrJeka, SlawomirGarmish, OlenaHrycaj, PawelFomina, NataliaPark, WonSuh, Chang-HeeLee, Sang JoonLee, Sung YoungBae, Yun JuYoo, Dae Hyun
Issue Date
Dec-2019
Publisher
OXFORD UNIV PRESS
Keywords
rituximab; CT-P10; rheumatoid arthritis; B cells; DMARDs (biologic); disease activity; anti-TNF; switch; biosimilar
Citation
RHEUMATOLOGY, v.58, no.12, pp.2193 - 2202
Indexed
SCIE
SCOPUS
Journal Title
RHEUMATOLOGY
Volume
58
Number
12
Start Page
2193
End Page
2202
URI
https://scholarworks.bwise.kr/hanyang/handle/2021.sw.hanyang/11610
DOI
10.1093/rheumatology/kez152
ISSN
1462-0324
Abstract
Objective To evaluate the efficacy and safety of CT-P10, a rituximab biosimilar after a single switch, during a multinational, randomized, double-blind Phase 3 trial involving patients with RA. Methods Patients received 48 weeks’ treatment with CT-P10 or United States- or European Union-sourced reference rituximab (US-RTX and EU-RTX, respectively). Patients entering the extension period (weeks 48–72) remained on CT-P10 (CT-P10/CT-P10; n = 122) or US-RTX (US-RTX/US-RTX; n = 64), or switched to CT-P10 from US-RTX (US-RTX/CT-P10; n = 62) or EU-RTX (EU-RTX/CT-P10; n = 47) for an additional course. Efficacy endpoints included Disease Activity Score using 28 joints (DAS28), American College of Rheumatology (ACR) response rates, and quality of life-related parameters. Pharmacodynamics, immunogenicity and safety were also assessed. Results At week 72, similar improvements were observed by disease activity parameters including DAS28 and ACR response rate in the four extension period treatment groups. Quality of life improvements at week 72 vs baseline were similarly shown during the extension period in all groups. Newly developed anti-drug antibodies were detected in two patients following study drug infusion in the extension period. Similar pharmacodynamic and safety profiles were observed across groups. Conclusion Long-term use of CT-P10 up to 72 weeks was effective and well tolerated. Furthermore, switching from reference rituximab to CT-P10 in RA was well tolerated and did not result in any clinically meaningful differences in terms of efficacy, pharmacodynamics, immunogenicity and safety.
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