THU0150 Long-Term Safety and Efficacy of SB4 (Etanercept Biosimilar) in Patients with Rheumatoid Arthritis: Comparison between Continuing SB4 and Switching from Etanercept Reference Product To SB4

Emery, Paul; Vencovský, Jiří; Sylwestrzak, Anna; Leszczyński, Piotr; Porawska, Wieslawa; Stasiuk, Barbara; Hilt, Joanna; Mosterova, Zdenka; Cheong, Soo Yeon; Ghil, Jeehoon

doi:10.1136/annrheumdis-2016-eular.3137

Cited by 15 publications

(17 citation statements)

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“…The NOR-SWITCH infliximab trial was conducted across six indications and used a non-inferiority margin of 15% (adapted from rheumatoid arthritis studies), with results suggesting no loss of efficacy and no unexpected treatment-emergent adverse events (TEAEs) [53]. Eight studies reported similar outcomes between groups, but failed to provide a formal statistical analysis of between-group comparisons [55, 56, 69, 70, 75, 98, 102–104]. …”

Section: Resultsmentioning

confidence: 99%

“…Percentage achieving good or moderate EULAR-ESR and EULAR-CRP responses similar between groups for each time point (week 8, 16 and 24)CT-P10/CT-P10 vs rituximab/CT-P10, AE: 24 vs 20%; SAE: 3 vs 5%; infusion-related reaction: 3 vs 5%; infection: 8 vs 10%CT-P10/CT-P10 vs rituximab/CT-P10: 13 vs 15% (all since pre-switch). nADAs, n = 1Emery et al 2016 (abstract) [101, 102]With rheumatoid arthritis ( N = 245)119ETN RP, 52 weeks (study also included patients on SB4 throughout, with no switch)SB4, 48 weeksWeeks 52–100, ETN RP/SB4 vs SB4/SB4, ACR20: 79 vs 78%; ACR50: 61 vs 60%; ACR70: 42 vs 43% (statistical analysis NR)Weeks 52–100, ETN RP/SB4: ≥ 1 TEAE, n = 58 (49%); ≥ 1 SAE, n = 2 (2%); serious infections, n = 1 (1%); death, n = 0 (0%); SB4/SB4: ≥ 1 TEAE, n = 60 (48%); ≥ 1 SAE, n = 6 (5%); serious infections, n = 1 (1%); death (from hepatic cancer), n = 1 (1%)Weeks 52–100, ETN RP/SB4: n = 1 (1%); SB4/SB4: n = 1 (1%)Griffiths et al 2017 [103]With chronic plaque psoriasis ( N = 531)196GP2015 or ETN, 12 weeks (study also included patients re-randomised to same treatment, with different dosing schedule, with no switch)Patients with PASI improvement ≥ 50% re-randomised to series of 3 treatment switches to week 30, then continuation on last assigned treatment to week 52Baseline to week 52, mean scores and percentage changes in PASI score at all time points similar between continued GP2015 and ETN groups, and between pooled continued and pooled switched groups. Response rates increased over time in all treatment groups until week 30 and then remained stable to week 52≥1 TEAE up to week 52, continued GP2015 vs continued ETN switched GP2015 vs switched ETN: 60 vs 57 vs 61 vs 59%.…”

Section: Introductionmentioning

confidence: 99%

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Biosimilarity and Interchangeability: Principles and Evidence: A Systematic Review

et al. 2018

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Background The efficacy, safety and immunogenicity risk of switching between an originator biologic and a biosimilar or from one biosimilar to another are of potential concern.Objectives The aim was to conduct a systematic literature review of the outcomes of switching between biologics and their biosimilars and identify any evidence gaps.Methods A systematic literature search was conducted in PubMed, EMBASE and Cochrane Library from inception to June 2017. Relevant societal meetings were also checked. Peer-reviewed studies reporting efficacy and/or safety data on switching between originator and biosimilar products or from one biosimilar to another were selected. Studies with fewer than 20 switched patients were excluded. Data were extracted on interventions, study population, reason for treatment switching, efficacy outcomes, safety and anti-drug antibodies.ResultsThe systematic literature search identified 63 primary publications covering 57 switching studies. The reason for switching was reported as non-medical in 50 studies (23 clinical, 27 observational). Seven studies (all observational) did not report whether the reasons for switching were medical or non-medical. In 38 of the 57 studies, fewer than 100 patients were switched. Follow-up after switching went beyond 1 year in eight of the 57 studies. Of the 57 studies, 33 included statistical analysis of disease activity or patient outcomes; the majority of these studies found no statistically significant differences between groups for main efficacy parameters (based on P < 0.05 or predefined acceptance ranges), although some studies observed changes for some parameters. Most studies reported similar safety profiles between groups.Conclusions There are important evidence gaps around the safety of switching between biologics and their biosimilars. Sufficiently powered and appropriately statistically analysed clinical trials and pharmacovigilance studies, with long-term follow-ups and multiple switches, are needed to support decision-making around biosimilar switching.Electronic supplementary materialThe online version of this article (10.1007/s40259-017-0256-z) contains supplementary material, which is available to authorized users.

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Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Biosimilarity and Interchangeability: Principles and Evidence: A Systematic Review

et al. 2018

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“…Of these, 119 patients in the maintenance group and 113 switched patients continued to week 100. Efficacy and radiographic progression were sustained and comparable between groups, with response rates of 77.9% in maintained patients and 79.1% in switched patients for ACR20; 59.8% and 60.9%, respectively, for ACR50; and 42.6% and 41.7%, respectively for ACR70 10. The safety profiles between weeks 52 and 100 were also similar, with at least one TEAE reported in 47.8% of patients in the SB4 arm and 48.7% of those in the Enbrel arm.…”

Section: Considering Extension Studies and Switchingmentioning

confidence: 87%

“…This was a typical example of a biosimilar study, with a 52 week randomised double blind period followed by an open label extension period up to week 100 in which all patients received SB4 and methotrexate allowing evaluation of a single switch from a bio-originator to the biosimilar 9. The double blind period included 596 patients, but the extension period was carried out only in Poland and the Czech Republic and included 245 patients 10. The primary endpoint was American College of Rheumatology 20 (ACR20) response rate at week 24.…”

Section: Considering Clinical Data For Approved Biosimilarsmentioning

confidence: 99%

Biosimilars already approved and in development

et al. 2017

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As of mid-2017, 10 tumour necrosis factor inhibitors (four for etanercept and three each for adalimumab and infliximab) and a first rituximab biosimilar are on the market, and a considerable number more are in various stages of development. The clinical trials of biosimilars, which have included long term extensions, have used various designs to look at switching between originator and biosimilar products, with reassuring results for clinical practice. For the infliximab biosimilar CT-P13 in particular, several studies have examined non-medical switching in real world practice. The results suggest that switching does not compromise safety, efficacy, or immunogenicity. However, additional data from clinical and real world switching studies, especially of switching between two or more biosimilars, are needed, as is continuing pharmacovigilance with larger databases to fill remaining gaps in the evidence. As biosimilar development continues, innovations in formulation and drug delivery technology may become of increasing interest.

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“…The results showed no loss of efficacy for up to 100 weeks, with a similar efficacy observed in the switching and maintenance groups (table 2). 33 Furthermore, switching did not result in any treatment emergent problems or an increase in adverse events or immunogenicity (table 2). 33 Overall, SB4 was well tolerated and effective over 2 years in patients with rheumatoid arthritis 33…”

Section: Considering Patient Managementmentioning

confidence: 94%

Biosimilars: considerations for clinical practice

et al. 2017

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With the projected expansion of the biosimilars market, there will be an increased propensity for the substitution of reference biological products with cheaper biosimilars for economic reasons (ie, non-medical switching). This will lower the cost per patient and should provide the benefit of wider access to biological therapies. However, it is essential that patients and clinicians fully understand the rationale for non-medical switching and its potential implications in terms of efficacy, safety, and immunogenicity. To date, clinical experience supports the use of biosimilars and a growing body of evidence from clinical trials and real world observational studies specifically supports clinical decision making around non-medical switching. Equally, as non-medical switching becomes more common, it is essential that pharmacovigilance systems adapt to handle the increasing volumes of data needed to effectively monitor the use of biosimilars and detect new signals. This will require a reduced reliance on registries, as well as streamlining and integration of existing systems to allow a frequent cycle of online reporting of adverse events by healthcare professionals, analysis by national authorities, and feedback to treating clinicians. This article considers the current use and future uptake of biosimilars from a clinical perspective.

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THU0150 Long-Term Safety and Efficacy of SB4 (Etanercept Biosimilar) in Patients with Rheumatoid Arthritis: Comparison between Continuing SB4 and Switching from Etanercept Reference Product To SB4

Cited by 15 publications

References 0 publications

Biosimilarity and Interchangeability: Principles and Evidence: A Systematic Review

Biosimilarity and Interchangeability: Principles and Evidence: A Systematic Review

Biosimilars already approved and in development

Biosimilars: considerations for clinical practice

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