Diagnosis of myositis-associated interstitial lung disease: Utility of the myositis autoantibody line immunoassay - 19/10/21
, Matthew J.S. Parker b, c, d , Jane F. Bleasel b, d , Lauren K. Troy a, b , Edmund M. Lau a, b , Helen E. Jo a, b, c , Alan K.Y. Teoh a, b, c , Susanne Webster a , Stephen Adelstein b, e, f , Tamera J. Corte a, b, c Abstract |
Objectives |
The detection of myositis autoantibodies (MA) in patients with interstitial lung disease (ILD) has major implications for diagnosis and management, especially amyopathic and forme frustes of idiopathic inflammatory myositis-associated ILD (IIM-ILD). Use of the MA line immunoblot assay (MA-LIA) in non-rheumatological cohorts remains unvalidated. We assessed the diagnostic performance of the MA-LIA and explored combined models with clinical variables to improve identification of patients with IIM-ILD.
Methods |
Consecutive patients referred to a specialist ILD clinic, with ILD-diagnosis confirmed at multidisciplinary meeting, and MA-LIA performed within six months of baseline were included. Pre-specified MA-LIA thresholds were evaluated for IIM-ILD diagnosis.
Results |
A total 247 ILD patients were included (IIM-ILD n = 12, non-IIM connective tissue disease-associated ILD [CTD-ILD] n = 52, idiopathic interstitial pneumonia [IIP] n = 115, other-ILD n = 68). Mean age was 64.8 years, with 45.3% female, mean FVC 75.5% and DLCO 59.2% predicted. MA were present in 13.8% overall and 83.3% of IIM-ILD patients. The most common MA in IIM-ILD and non-IIM ILD patients were anti-Jo-1 (prevalence 40%) and anti-PMScl (29.2%) autoantibodies respectively. The pre-specified low-positive threshold (>10 signal intensity) had the highest discriminative capacity for IIM-ILD (AUC 0.86). Combining MA-LIA with age, gender, clinical CTD-manifestations and an overlap non-specific interstitial pneumonia/organising pneumonia pattern on HRCT improved discrimination for IIM-ILD (AUC 0.96).
Conclusion |
The MA-LIA is useful to support a diagnosis of IIM-ILD as a complement to multi-disciplinary ILD assessment. Clinical interpretation is optimised by consideration of the strength of the MA-LIA result together with clinical and radiological features of IIM-ILD.
Le texte complet de cet article est disponible en PDF.Highlights |
• | Use of the myositis autoantibody line-immunoassay (MA-LIA) in ILD cohorts is unvalidated. |
• | MA-LIA thresholds strongly influence test performance. |
• | Combining the MA-LIA with clinical variables enhances myositis-ILD identification. |
• | Validation of ILD-specific MA-LIA reference intervals is required. |
• | Positive MA in non-myositis patients require prospective, long-term characterisation. |
Keywords : Interstitial lung disease, Myositis autoantibody, Connective tissue disease, Autoimmune disease, Immunoblot
Plan
Vol 187
Article 106581- octobre 2021 Retour au numéro
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