Rituximab versus intravenous cyclophosphamide in patients with connective tissue disease-associated interstitial lung disease in the UK (RECITAL): a double-blind, double-dummy, randomised, controlled, phase 2b trial
Rituximab versus intravenous cyclophosphamide in patients with connective tissue disease-associated interstitial lung disease in the UK (RECITAL): a double-blind, double-dummy, randomised, controlled, phase 2b trial
Background: rituximab is often used as rescue therapy in interstitial lung disease (ILD) associated with connective tissue disease (CTD), but has not been studied in clinical trials. This study aimed to assess whether rituximab is superior to cyclophosphamide as a treatment for severe or progressive CTD associated ILD.
Methods: we conducted a randomised, double-blind, double-dummy, phase 2b trial to assess the superiority of rituximab compared with cyclophosphamide. Patients aged 18-80 years with severe or progressive ILD related to scleroderma, idiopathic inflammatory myositis, or mixed CTD, recruited across 11 specialist ILD or rheumatology centres in the UK, were randomly assigned (1:1) to receive rituximab (1000 mg at weeks 0 and 2 intravenously) or cyclophosphamide (600 mg/m2 body surface area every 4 weeks intravenously for six doses). The primary endpoint was rate of change in forced vital capacity (FVC) at 24 weeks compared with baseline, analysed using a mixed-effects model with random intercepts, adjusted for baseline FVC and CTD type. Prespecified secondary endpoints reported in this Article were change in FVC at 48 weeks versus baseline; changes from baseline in 6 min walk distance, diffusing capacity of the lung for carbon monoxide (DLCO), physician-assessed global disease activity (GDA) score, and quality-of-life scores on the St George's Respiratory Questionnaire (SGRQ), King's Brief Interstitial Lung Disease (KBILD) questionnaire, and European Quality of Life Five-Dimension (EQ-5D) questionnaire at 24 and 48 weeks; overall survival, progression-free survival, and time to treatment failure; and corticosteroid use. All endpoints were analysed in the modified intention-to-treat population, which comprised all patients who received at least one dose of study drug. This trial is registered with ClinicalTrials.gov (NCT01862926).
Findings: between Dec 1, 2014, and March 31, 2020, we screened 145 participants, of whom 101 participants were randomly allocated: 50 (50%) to receive cyclophosphamide and 51 (50%) to receive rituximab. 48 (96%) participants in the cyclophosphamide group and 49 (96%) in the rituximab group received at least one dose of treatment and were included in analyses; 43 (86%) participants in the cyclophosphamide group and 42 (82%) participants in the rituximab group completed 24 weeks of treatment and follow-up. At 24 weeks, FVC was improved from baseline in both the cyclophosphamide group (unadjusted mean increase 99 mL [SD 329]) and the rituximab group (97 mL [234]); in the adjusted mixed-effects model, the difference in the primary endpoint at 24 weeks was -40 mL (95% CI -153 to 74; p=0·49) between the rituximab group and the cyclophosphamide group. KBILD quality-of-life scores were improved at 24 weeks by a mean 9·4 points (SD 20·8) in the cyclophosphamide group and 8·8 points (17·0) in the rituximab group. No significant differences in secondary endpoints were identified between the treatment groups, with the exception of change in GDA score at week 48, which favoured cyclophosphamide (difference 0·90 [95% CI 0·11 to 1·68]). Improvements in lung function and respiratory-related quality-of-life measures were observed in both treatment groups. Lower corticosteroid exposure over 48 weeks of follow-up was recorded in the rituximab group. Two (4%) of 48 participants who received cyclophosphamide and three (6%) of 49 who received rituximab died during the study, all due to complications of CTD or ILD. Overall survival, progression-free survival, and time to treatment failure did not significantly differ between the two groups. All participants reported at least one adverse event during the study. Numerically fewer adverse events were reported by participants receiving rituximab (445 events) than those receiving cyclophosphamide (646 events). Gastrointestinal and respiratory disorders were the most commonly reported adverse events in both groups. There were 62 serious adverse events of which 33 occurred in the cyclophosphamide group and 29 in the rituximab group.
Interpretation: rituximab was not superior to cyclophosphamide to treat patients with CTD-ILD, although participants in both treatment groups had increased FVC at 24 weeks, in addition to clinically important improvements in patient-reported quality of life. Rituximab was associated with fewer adverse events. Rituximab should be considered as a therapeutic alternative to cyclophosphamide in individuals with CTD-ILD requiring intravenous therapy.
Funding: efficacy and Mechanism Evaluation Programme (Medical Research Council and National Institute for Health Research, UK).
humans, rtituximab/therapeutic use, quality of life, lung diseases, interstitial/drug therapy, cyclophosphamide/adverse effects, connective tissue diseases/complications, adrenal cortex hormones/therapeutic use, double-blind method, United Kingdom, treatment outcome
45-54
Maher, Toby M.
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Tudor, Veronica A.
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Saunders, Peter
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Gibbons, Michael A.
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Fletcher, Sophie V.
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Denton, Christopher P.
ca542734-bcd7-4e95-9f51-8b0dd580700e
Hoyles, Rachel K.
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Parfrey, Helen
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Renzoni, Elisabetta A.
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Kokosi, Maria
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Wells, Athol U
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Ashby, Deborah
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Szigeti, Matyas
71717ecf-a611-427e-aecb-0071e570614b
Molyneaux, Philip L.
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22 December 2022
Maher, Toby M.
6c166764-7a4e-4d20-b528-381a7218ea0b
Tudor, Veronica A.
6d192b8f-7b16-4919-a762-79eef979b805
Saunders, Peter
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Gibbons, Michael A.
e5231df8-d0bc-4cb6-9a8e-a1bf5882ae9e
Fletcher, Sophie V.
d05721e8-8943-4f13-a1f5-4ba183741c89
Denton, Christopher P.
ca542734-bcd7-4e95-9f51-8b0dd580700e
Hoyles, Rachel K.
0cc27739-be35-4907-ac26-a604500d98d5
Parfrey, Helen
8755bb45-8fd1-4a8f-85e5-58992812d9af
Renzoni, Elisabetta A.
9671c0cb-707e-405b-bc00-b9987b01e638
Kokosi, Maria
d690f1da-4f73-4802-8d2b-2448ca27ef17
Wells, Athol U
47bba0f1-7cf9-4e3d-97b3-2be719a87357
Ashby, Deborah
12a12757-6283-4323-a4b8-7f32b475847b
Szigeti, Matyas
71717ecf-a611-427e-aecb-0071e570614b
Molyneaux, Philip L.
9761b4a9-5539-4683-a023-af7e351365ee
Maher, Toby M., Tudor, Veronica A., Saunders, Peter, Gibbons, Michael A., Fletcher, Sophie V., Denton, Christopher P., Hoyles, Rachel K., Parfrey, Helen, Renzoni, Elisabetta A., Kokosi, Maria, Wells, Athol U, Ashby, Deborah, Szigeti, Matyas and Molyneaux, Philip L.
,
RECITAL Investigators
(2022)
Rituximab versus intravenous cyclophosphamide in patients with connective tissue disease-associated interstitial lung disease in the UK (RECITAL): a double-blind, double-dummy, randomised, controlled, phase 2b trial.
The Lancet Respiratory Medicine, 11 (1), .
(doi:10.1016/S2213-2600(22)00359-9).
Abstract
Background: rituximab is often used as rescue therapy in interstitial lung disease (ILD) associated with connective tissue disease (CTD), but has not been studied in clinical trials. This study aimed to assess whether rituximab is superior to cyclophosphamide as a treatment for severe or progressive CTD associated ILD.
Methods: we conducted a randomised, double-blind, double-dummy, phase 2b trial to assess the superiority of rituximab compared with cyclophosphamide. Patients aged 18-80 years with severe or progressive ILD related to scleroderma, idiopathic inflammatory myositis, or mixed CTD, recruited across 11 specialist ILD or rheumatology centres in the UK, were randomly assigned (1:1) to receive rituximab (1000 mg at weeks 0 and 2 intravenously) or cyclophosphamide (600 mg/m2 body surface area every 4 weeks intravenously for six doses). The primary endpoint was rate of change in forced vital capacity (FVC) at 24 weeks compared with baseline, analysed using a mixed-effects model with random intercepts, adjusted for baseline FVC and CTD type. Prespecified secondary endpoints reported in this Article were change in FVC at 48 weeks versus baseline; changes from baseline in 6 min walk distance, diffusing capacity of the lung for carbon monoxide (DLCO), physician-assessed global disease activity (GDA) score, and quality-of-life scores on the St George's Respiratory Questionnaire (SGRQ), King's Brief Interstitial Lung Disease (KBILD) questionnaire, and European Quality of Life Five-Dimension (EQ-5D) questionnaire at 24 and 48 weeks; overall survival, progression-free survival, and time to treatment failure; and corticosteroid use. All endpoints were analysed in the modified intention-to-treat population, which comprised all patients who received at least one dose of study drug. This trial is registered with ClinicalTrials.gov (NCT01862926).
Findings: between Dec 1, 2014, and March 31, 2020, we screened 145 participants, of whom 101 participants were randomly allocated: 50 (50%) to receive cyclophosphamide and 51 (50%) to receive rituximab. 48 (96%) participants in the cyclophosphamide group and 49 (96%) in the rituximab group received at least one dose of treatment and were included in analyses; 43 (86%) participants in the cyclophosphamide group and 42 (82%) participants in the rituximab group completed 24 weeks of treatment and follow-up. At 24 weeks, FVC was improved from baseline in both the cyclophosphamide group (unadjusted mean increase 99 mL [SD 329]) and the rituximab group (97 mL [234]); in the adjusted mixed-effects model, the difference in the primary endpoint at 24 weeks was -40 mL (95% CI -153 to 74; p=0·49) between the rituximab group and the cyclophosphamide group. KBILD quality-of-life scores were improved at 24 weeks by a mean 9·4 points (SD 20·8) in the cyclophosphamide group and 8·8 points (17·0) in the rituximab group. No significant differences in secondary endpoints were identified between the treatment groups, with the exception of change in GDA score at week 48, which favoured cyclophosphamide (difference 0·90 [95% CI 0·11 to 1·68]). Improvements in lung function and respiratory-related quality-of-life measures were observed in both treatment groups. Lower corticosteroid exposure over 48 weeks of follow-up was recorded in the rituximab group. Two (4%) of 48 participants who received cyclophosphamide and three (6%) of 49 who received rituximab died during the study, all due to complications of CTD or ILD. Overall survival, progression-free survival, and time to treatment failure did not significantly differ between the two groups. All participants reported at least one adverse event during the study. Numerically fewer adverse events were reported by participants receiving rituximab (445 events) than those receiving cyclophosphamide (646 events). Gastrointestinal and respiratory disorders were the most commonly reported adverse events in both groups. There were 62 serious adverse events of which 33 occurred in the cyclophosphamide group and 29 in the rituximab group.
Interpretation: rituximab was not superior to cyclophosphamide to treat patients with CTD-ILD, although participants in both treatment groups had increased FVC at 24 weeks, in addition to clinically important improvements in patient-reported quality of life. Rituximab was associated with fewer adverse events. Rituximab should be considered as a therapeutic alternative to cyclophosphamide in individuals with CTD-ILD requiring intravenous therapy.
Funding: efficacy and Mechanism Evaluation Programme (Medical Research Council and National Institute for Health Research, UK).
Text
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e-pub ahead of print date: 11 November 2022
Published date: 22 December 2022
Keywords:
humans, rtituximab/therapeutic use, quality of life, lung diseases, interstitial/drug therapy, cyclophosphamide/adverse effects, connective tissue diseases/complications, adrenal cortex hormones/therapeutic use, double-blind method, United Kingdom, treatment outcome
Identifiers
Local EPrints ID: 478229
URI: http://eprints.soton.ac.uk/id/eprint/478229
ISSN: 2213-2600
PURE UUID: 7ba67d43-b944-41b0-8b52-8d4758c4edf3
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Date deposited: 26 Jun 2023 16:34
Last modified: 17 Mar 2024 02:19
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Contributors
Author:
Toby M. Maher
Author:
Veronica A. Tudor
Author:
Peter Saunders
Author:
Michael A. Gibbons
Author:
Sophie V. Fletcher
Author:
Christopher P. Denton
Author:
Rachel K. Hoyles
Author:
Helen Parfrey
Author:
Elisabetta A. Renzoni
Author:
Maria Kokosi
Author:
Athol U Wells
Author:
Deborah Ashby
Author:
Matyas Szigeti
Author:
Philip L. Molyneaux
Corporate Author: RECITAL Investigators
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