Comparative Effectiveness of Bimekizumab and Risankizumab in Patients with Psoriatic Arthritis at 52 Weeks Assessed Using a Matching-Adjusted Indirect Comparison

Philip J. Mease; Richard B. Warren; Peter Nash; Jean-Marie Grouin; Nikos Lyris; Damon Willems; Vanessa Taieb; Jason Eells; Iain B. McInnes

doi:10.1007/s40744-024-00706-w

Rheumatology and Therapy (Aug 2024)

Comparative Effectiveness of Bimekizumab and Risankizumab in Patients with Psoriatic Arthritis at 52 Weeks Assessed Using a Matching-Adjusted Indirect Comparison

Philip J. Mease,
Richard B. Warren,
Peter Nash,
Jean-Marie Grouin,
Nikos Lyris,
Damon Willems,
Vanessa Taieb,
Jason Eells,
Iain B. McInnes

Affiliations

Philip J. Mease: Swedish Medical Center/Providence St. Joseph Health and University of Washington
Richard B. Warren: Dermatology Centre, Northern Care Alliance NHS Foundation Trust, Manchester Academic Health Science Centre, NIHR Manchester Biomedical Research Centre, The University of Manchester
Peter Nash: School of Medicine, Griffith University School of Medicine
Jean-Marie Grouin: University of Rouen
Nikos Lyris: UCB Pharma
Damon Willems: UCB Pharma
Vanessa Taieb: UCB Pharma
Jason Eells: UCB Pharma
Iain B. McInnes: College of Medical Veterinary and Life Sciences, University of Glasgow

DOI: https://doi.org/10.1007/s40744-024-00706-w
Journal volume & issue: Vol. 11, no. 5
pp. 1403 – 1412

Abstract

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Abstract Introduction The relative efficacy of bimekizumab and risankizumab in patients with PsA who were biologic disease-modifying anti-rheumatic drug naïve (bDMARD naïve) or with previous inadequate response or intolerance to tumor necrosis factor inhibitors (TNFi-IR) was assessed at 52 weeks (Wk52) using matching-adjusted indirect comparisons (MAIC). Methods Relevant trials were systematically identified. For patients who were bDMARD naïve, individual patient data (IPD) from BE OPTIMAL (NCT03895203; N = 431) were matched with summary data from KEEPsAKE-1 (NCT03675308; N = 483). For patients who were TNFi-IR, IPD from BE COMPLETE (NCT03896581; N = 267) were matched with summary data from the TNFi-IR patient subgroup in KEEPsAKE-2 (NCT03671148; N = 106). To adjust for cross-trial differences, patients from the bimekizumab trials were re-weighted to match the baseline characteristics of patients in the risankizumab trials. Adjustment variables were selected based on expert consensus (n = 5) and adherence to established MAIC guidelines. Recalculated bimekizumab Wk52 outcomes for American College of Rheumatology (ACR) 20/50/70 response criteria and minimal disease activity (MDA) index (non-responder imputation) were compared with risankizumab outcomes via non-placebo-adjusted comparisons. Results In patients who were bDMARD naïve, bimekizumab had a significantly greater likelihood of response than risankizumab at Wk52 for ACR50 (odds ratio [95% confidence interval]: 1.52 [1.11, 2.09]) and ACR70 (1.80 [1.29, 2.51]). In patients who were TNFi-IR, bimekizumab had a significantly greater likelihood of response than risankizumab at Wk52 for ACR20 (1.78 [1.08, 2.96]), ACR50 (3.05 [1.74, 5.32]), ACR70 (3.69 [1.82, 7.46]), and MDA (2.43 [1.37, 4.32]). Conclusions Using MAIC, bimekizumab demonstrated a greater likelihood of efficacy in most ACR and MDA outcomes than risankizumab in patients with PsA who were bDMARD naïve and TNFi-IR at Wk52. Trial Registration NCT03895203, NCT03896581, NCT03675308, NCT03671148.

Published in Rheumatology and Therapy

ISSN: 2198-6576 (Print); 2198-6584 (Online)
Publisher: Adis, Springer Healthcare
Country of publisher: United Kingdom
LCC subjects: Medicine: Internal medicine: Specialties of internal medicine: Diseases of the musculoskeletal system
Website: https://www.springer.com/journal/40744

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