Early initiation of treatment for Rheumatoid arthritis (RA) can prevent several of the long term problems associated with the condition. However, many RA patients develop lung inflammation and scarring, called 'interstitial lung disease' (RA-ILD), contributing to early death in 1 in 5 people. There is no proven treatment for these patients and some medications for RA can in fact worsen their lung disease. There is a need therefore to find safe medications that can not only control RA joint disease, but also prevent progression of RA-ILD. Abatacept is an approved drug for treating RA and is used widely. It is a newer RA medication, with a unique mechanism of action, and it has been shown to prevent progression of joint damage and improve physical function. The investigators aim to assess the safety of this medication in patients with RA-ILD and improve our understanding of the mechanism of lung damage in rheumatoid disease. The investigators will perform a small clinical trial to assess the feasibility of performing a larger randomized controlled trial. A total of 30 patients with RA-ILD will be treated with abatacept infusions fortnightly for the first month, then every 4 weeks for a total of 20 weeks. In order to be eligible for the study, a patient must be able to provide written informed consent, be aged ≥18 years, and have interstitial lung disease that has not responded to or progressed over 6 months despite conventional immunosuppression. Change in lung function (forced vital capacity) at 24 weeks will be evaluated. To assess the mechanisms that may be involved with the development of ILD, the investigators will assess the effects of abatacept on biomarkers obtained from the blood and the lung (bronchoalveolar lavage), including markers of infection (the lung microbiome).
Study Type
INTERVENTIONAL
Allocation
NA
Purpose
TREATMENT
Masking
NONE
Enrollment
30
The IV dose varies according to weight: \<60kg=500mg ≥60 but≤100kg=750mg \>100kg=1g This equates to approximately 10mg/kg.
Addenbrookes Hospital
Cambridge, United Kingdom
RECRUITINGPapworth Hospital
Cambridge, United Kingdom
RECRUITINGForced Vital Capacity (FVC)
Assessing the change of Forced Vital Capacity (FVC) across screening, baseline V2 (prior to abatacept), V6 and V9.
Time frame: 28 weeks (Screening-V9)
Transfer factor of the lung for carbon monoxide (TLCO)
Assessing the change of Transfer factor of the lung for carbon monoxide (TLCO) at screening (prior to abatacept), V6 and V9.
Time frame: 28 weeks (Screening-V9)
MRC dyspnoea score
Assessing the change of MRC dyspnoea score completed at Baseline V2 (prior to abatacept), V6, V9
Time frame: 24 weeks (Baseline-V9)
Kings Brief Interstitial Lung Disease score (K-BILD)
Assessing the change of Kings Brief Interstitial Lung Disease score (K-BILD) questionnaire completed at Baseline V2 (prior to abatacept), V6, V9
Time frame: 24 weeks (Baseline-V9)
Semi-quantitative radiological scoring of the ILD
Assessing the change of HRCT chest scans performed at screening (prior to abatacept and V9 (end of trial)
Time frame: 28 weeks (Screening-V9)
Resting oxygen saturation
Resting oxygen saturation recorded at all visits
Time frame: 28 weeks
DAS28
DAS28 recorded at all visits
Time frame: 28 weeks
Leicester Cough Questionnaire score
Assessing the change of Leicester Cough Questionnaire completed at Baseline V2 (prior to abatacept), V6, V9
Time frame: 24 weeks (Baseline-V9)
EQ-5D
Assessing the change of EQ-5D Questionnaire completed at Baseline V2 (prior to abatacept), V6, V9
Time frame: 24 weeks (Baseline-V9)
Respiratory tract infection
Assessing the number of Respiratory tract infections recorded following IMP dosing between V2-V9
Time frame: 24 weeks (Baseline-V9)
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