Rituximab versus tocilizumab in anti-TNF inadequate responder patients with rheumatoid arthritis (R4RA): 16-week outcomes of a stratified, biopsy-driven, multicentre, open-label, phase 4 randomised controlled trial

Frances Humby,Giovanni Giorli,Ernest Choy,Stephen Kelly,Alberto Cauli,Alessandra Nerviani,Bernard Lauwerys,Christopher J Edwards,Costantino Pitzalis,Liliane Fossati-Jimack,Hasan Rizvi,Raquel Celis,Bhaskar Dasgupta,Joanna Peel,Pier Paolo Sainaghi,Felice Rivellese,Louise Warren,Georgina Thorborn,Mattia Bellan,Pauline Ho,Patrick Verschueren,Christopher Holroyd,Mattia Congia,Gaye Hadfield,Charlotte Thompson,Nagui Gendi,Carlomaurizio Montecucco,Peter Sasieni,Piero Reynolds,Nora Ng,Patrick Durez,Maya H Buch,Laura White,Rebecca Hands,Arti Mahto,Vasco C Romão,Arthur G Pratt ,Julio Ramírez ,Myles Lewis ,Peter Taylor ,John D Isaacs ,João Eurico Fonseca ,Robert J Moots ,Silvia Bugatti ,Michèle Bombardieri ,Juan D Cañete

doi:10.1016/s0140-6736(20)32341-2

Abstract

SummaryBackgroundAlthough targeted biological treatments have transformed the outlook for patients with rheumatoid arthritis, 40% of patients show poor clinical response, which is mechanistically still unexplained. Because more than 50% of patients with rheumatoid arthritis have low or absent CD20 B cells—the target for rituximab—in the main disease tissue (joint synovium), we hypothesised that, in these patients, the IL-6 receptor inhibitor tocilizumab would be more effective. The aim of this trial was to compare the effect of tocilizumab with rituximab in patients with rheumatoid arthritis who had an inadequate response to anti-tumour necrosis factor (TNF) stratified for synovial B-cell status.MethodsThis study was a 48-week, biopsy-driven, multicentre, open-label, phase 4 randomised controlled trial (rituximab vs tocilizumab in anti-TNF inadequate responder patients with rheumatoid arthritis; R4RA) done in 19 centres across five European countries (the UK, Belgium, Italy, Portugal, and Spain). Patients aged 18 years or older who fulfilled the 2010 American College of Rheumatology and European League Against Rheumatism classification criteria for rheumatoid arthritis and were eligible for treatment with rituximab therapy according to UK National Institute for Health and Care Excellence guidelines were eligible for inclusion in the trial. To inform balanced stratification, following a baseline synovial biopsy, patients were classified histologically as B-cell poor or rich. Patients were then randomly assigned (1:1) centrally in block sizes of six and four to receive two 1000 mg rituximab infusions at an interval of 2 weeks (rituximab group) or 8 mg/kg tocilizumab infusions at 4-week intervals (tocilizumab group). To enhance the accuracy of the stratification of B-cell poor and B-cell rich patients, baseline synovial biopsies from all participants were subjected to RNA sequencing and reclassified by B-cell molecular signature. The study was powered to test the superiority of tocilizumab over rituximab in the B-cell poor population at 16 weeks. The primary endpoint was defined as a 50% improvement in Clinical Disease Activity Index (CDAI50%) from baseline. The trial is registered on the ISRCTN database, ISRCTN97443826, and EudraCT, 2012-002535-28.FindingsBetween Feb 28, 2013, and Jan 17, 2019, 164 patients were classified histologically and were randomly assigned to the rituximab group (83 [51%]) or the tocilizumab group (81 [49%]). In patients histologically classified as B-cell poor, there was no statistically significant difference in CDAI50% between the rituximab group (17 [45%] of 38 patients) and the tocilizumab group (23 [56%] of 41 patients; difference 11% [95% CI −11 to 33], p=0·31). However, in the synovial biopsies classified as B-cell poor with RNA sequencing the tocilizumab group had a significantly higher response rate compared with the rituximab group for CDAI50% (rituximab group 12 [36%] of 33 patients vs tocilizumab group 20 [63%] of 32 patients; difference 26% [2 to 50], p=0·035). Occurrence of adverse events (rituximab group 76 [70%] of 108 patients vs tocilizumab group 94 [80%] of 117 patients; difference 10% [–1 to 21) and serious adverse events (rituximab group 8 [7%] of 108 vs tocilizumab group 12 [10%] of 117; difference 3% [–5 to 10]) were not significantly different between treatment groups.InterpretationThe results suggest that RNA sequencing-based stratification of rheumatoid arthritis synovial tissue showed stronger associations with clinical responses compared with histopathological classification. Additionally, for patients with low or absent B-cell lineage expression signature in synovial tissue tocilizumab is more effective than rituximab. Replication of the results and validation of the RNA sequencing-based classification in independent cohorts is required before making treatment recommendations for clinical practice.FundingEfficacy and Mechanism Evaluation programme from the UK National Institute for Health Research.

Highlights

There was no significant difference between the rituximab and the tocilizumab groups using histological B-cell classification for Rheumatoid arthritis is a chronic immune mediated inflammatory disease characterised by synovitis and joint damage that results in considerable morbidity and increased mortality.[1]
Given the mechanism of the primary endpoint, the study showed a significant difference in favour of tocilizumab in the number of patients with an improvement in Clinical Disease Activity Index (CDAI) by 50% or more and CDAI less than 10·1
Patients aged 18 years or older who fulfilled the 2010 ACR and European League Against Rheumatism (EULAR) classification criteria for rheumatoid arthritis[16] and were eligible for treatment with rituximab therapy according to UK National Institute for Health and Care Excellence (NICE) guidelines[17] were eligible for inclusion in the study

Summary

Introduction

Rheumatoid arthritis is a chronic immune mediated inflammatory disease characterised by synovitis and joint damage that results in considerable morbidity and increased mortality.[1]. The important role of B cells is supported by the efficacy of the specific CD20 B-cell depleting drug, rituximab.[5] Rituximab is licensed for use in rheumatoid arthritis after unsuccessful conventional synthetic DMARDs and tumour necrosis factor (TNF) inhibitor therapy In this more therapy-resistant patient cohort, clinical response to rituximab is heterogeneous, with only 30% of patients reported to have a 50% improvement in the American College of Rheumatology response criteria (ACR50) at 6 months.[6] Given the mechanism of the primary endpoint, the study showed a significant difference in favour of tocilizumab in the number of patients with an improvement in Clinical Disease Activity Index (CDAI) by 50% or more and CDAI less than 10·1 (ie, low disease activity, defined as major treatment response; CDAI-MTR). In patients who were classified as B-cell poor, tocilizumab was superior to rituximab for most secondary outcomes

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Results

Discussion

Conclusion