P417 Frequent Early Nocebo Complaints but Maintained Clinical Efficacy, Biomarker and Therapeutic drug levels following mandatory Biosimilar Switch in Patients with Inflammatory Bowel disease: Preliminary data from a Prospective Observational Cohort Study

Wetwittayakhlang, Panu; Karkout, K; Tselekouni, Paraskevi; Al-Jabri, Reem; Bessissow, Talat; Afif, Waqqas; Wild, Gary; Bitton, Alain; Lakatos, Péter L.

doi:10.1093/ecco-jcc/jjac190.0547

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“…Nocebo effects are psychological, physiological, and neurobiological phenomena associated with actual or perceived harms that occur because of patients' negative expectations, and not due to the known pharmacologic actions of treatment [24][25][26][27]. A prospective observational study reported frequent early nocebo complaints following non-medical biosimilar switch (including infliximab and ADA RP to biosimilar switches) in Canadian patients with inflammatory bowel disease, although biomarker levels and their clinical efficacy were well maintained [28]. Unfortunately, reasons for switching and patient clinical status were unknown in our current study as they were not documented in the LRx claims databases.…”

Section: Patterns Of Switching From Abp 501mentioning

confidence: 99%

Treatment Persistence and Switching Patterns of Adalimumab Biosimilar ABP 501 in European Patients with Rheumatologic Diseases

Jin,

Kruppert,

Scholz

et al. 2024

Rheumatol Ther

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Introduction ABP 501 was an adalimumab (ADA) biosimilar approved for treating immune-mediated inflammatory diseases (IMIDs) including rheumatoid arthritis (RA), psoriatic arthritis (PsA), and ankylosing spondylitis (AS). In this retrospective study, we aimed to examine the treatment patterns of ABP 501 among patients with these IMIDs using German and French pharmacy claims databases. Methods Patients with RA, PsA, or AS who initiated ABP 501 between October 2018 and March 2020 and were observed continuously for ≥ 365 days both before and after ABP 501 initiation were included. Descriptive analyses of persistence and switch after ABP 501 discontinuation were conducted and reported for each disease cohort by prior use of ADA products (patients naïve to ADA or patients experienced with ADA). Results Median (95% confidence interval) persistence on ABP 501 was 9.4 (8.6–10.3), 10.2 (9.0–11.7), and 12.1 (11.0–13.1) months in German patients, and 11.7 (9.9–13.3), 7.1 (5.8–8.4), and 10.8 (9.6–11.9) months in French patients for RA, PsA, and AS, respectively. For patients who switched from ABP 501 to another targeted therapy during the first 12 months of follow-up, switching patterns varied between patients naïve to ADA and patients experienced with ADA in both Germany and France, with patients naïve to ADA switching most frequently to other targeted therapies including non-ADA tumor necrosis factor inhibitor (TNFi), non-TNFi biologic, or Janus Kinase inhibitor (JAKi) and patients experienced with ADA switching most frequently back to ADA reference product (RP). Conclusions Across three rheumatologic diseases, about half of patients persisted on ABP 501 at the end of 12 months after treatment initiation in both Germany and France. Patients experienced with ADA were more likely to switch back to ADA RP, regardless of indication and country, suggesting a possible nocebo effect. Future studies are warranted to understand reasons of discontinuation and switching. Supplementary Information The online version contains supplementary material available at 10.1007/s40744-024-00647-4.

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