J 2023

Biosimilar SB11 versus reference ranibizumab in neovascular age-related macular degeneration: 1-year phase III randomised clinical trial outcomes

BRESSLER, N. M., M. VEITH, Jan HAMOUZ, Jan ERNEST, D. ZALEWSKI et. al.

Basic information

Original name

Biosimilar SB11 versus reference ranibizumab in neovascular age-related macular degeneration: 1-year phase III randomised clinical trial outcomes

Authors

BRESSLER, N. M., M. VEITH, Jan HAMOUZ (203 Czech Republic), Jan ERNEST (203 Czech Republic), D. ZALEWSKI, Jan STUDNICKA (203 Czech Republic), A. VAJAS, A. PAPP, G. VOGT, J. LUU, Veronika MATUŠKOVÁ (203 Czech Republic, belonging to the institution), Y. H. YOON, T. PREGUN, T. KIM, D. SHIN, I. OH, H. JEONG, M. Y. KIM and S. J. WOO (guarantor)

Edition

The British journal of ophthalmology : incorporating the Royal London ophthalmic hospital reports, the Ophthalmic review and the Ophthalmoscope, London, British Journal of Ophthalmology, 2023, 0007-1161

Other information

Language

English

Type of outcome

Článek v odborném periodiku

Field of Study

30207 Ophthalmology

Country of publisher

United Kingdom of Great Britain and Northern Ireland

Confidentiality degree

není předmětem státního či obchodního tajemství

References:

Impact factor

Impact factor: 4.100 in 2022

RIV identification code

RIV/00216224:14110/23:00129940

Organization unit

Faculty of Medicine

UT WoS

000723337800001

Keywords in English

retina; neovascularisation; macula; degeneration

Tags

Tags

International impact, Reviewed
Změněno: 26/1/2024 09:44, Mgr. Tereza Miškechová

Abstract

V originále

Background/Aims To provide longer-term data on efficacy, safety, immunogenicity and pharmacokinetics (PK) of ranibizumab biosimilar SB11 compared with the reference ranibizumab (RBZ) in patients with neovascular age-related macular degeneration (nAMD). Methods Setting: Multicentre. Design: Randomised, double-masked, parallel-group, phase III equivalence study. Patient population: >= 50 years old participants with nAMD (n=705), one 'study eye'. Intervention: 1:1 randomisation to monthly intravitreal injection of 0.5 mg SB11 or RBZ. Main outcome measures: Visual efficacy endpoints, safety, immunogenicity and PK up to 52 weeks. Results Baseline and disease characteristics were comparable between treatment groups. Of 705 randomised participants (SB11: n=351; RBZ: n=354), 634 participants (89.9%; SB11: n=307; RBZ: n=327) completed the study until week 52. Previously reported equivalence in primary efficacy remained stable up to week 52 and were comparable between SB11 and RBZ. The adjusted treatment difference between SB11 and RBZ in full analysis set at week 52 of change from baseline in best-corrected visual acuity was -0.6 letters (90% CI -2.1 to 0.9) and of change from baseline in central subfield thickness was -14.9 mu m (95% CI -25.3 to -4.5). The incidence of ocular treatment-emergent adverse events (TEAEs) (SB11: 32.0% vs RBZ: 29.7%) and serious ocular TEAE (SB11: 2.9% vs RBZ: 2.3%) appeared comparable between treatment groups, and no new safety concerns were observed. The PK and immunogenicity profiles were comparable, with a 4.2% and 5.5% cumulative incidence of antidrug antibodies up to week 52 for SB11 and RBZ, respectively. Conclusions Longer-term results of this study further support the biosimilarity established between SB11 and RBZ.