A Clinically and Biologically Based Subclassification of the Idiopathic Inflammatory Myopathies Using Machine Learning

Simon W. M. Eng; Jeannette M. Olazagasti; Anna Goldenberg; Cynthia S. Crowson; Chester V. Oddis; Timothy B. Niewold; Rae S. M. Yeung; Ann M. Reed

doi:10.1002/acr2.11115

ACR Open Rheumatology (Mar 2020)

A Clinically and Biologically Based Subclassification of the Idiopathic Inflammatory Myopathies Using Machine Learning

Simon W. M. Eng,
Jeannette M. Olazagasti,
Anna Goldenberg,
Cynthia S. Crowson,
Chester V. Oddis,
Timothy B. Niewold,
Rae S. M. Yeung,
Ann M. Reed

Affiliations

Simon W. M. Eng: Hospital for Sick Children (SickKids), University of Toronto Toronto Ontario Canada
Jeannette M. Olazagasti: Mayo Clinic Rochester Minnesota
Anna Goldenberg: Hospital for Sick Children (SickKids), Vector Institute, University of Toronto Toronto Ontario Canada
Cynthia S. Crowson: Mayo Clinic Rochester Minnesota
Chester V. Oddis: University of Pittsburgh Pittsburgh Pennsylvania
Timothy B. Niewold: Mayo Clinic Rochester Minnesota
Rae S. M. Yeung: Hospital for Sick Children (SickKids), University of Toronto Toronto Ontario Canada
Ann M. Reed: Duke University School of Medicine Durham North Carolina

DOI: https://doi.org/10.1002/acr2.11115
Journal volume & issue: Vol. 2, no. 3
pp. 158 – 166

Abstract

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Objective Published predictive models of disease outcomes in idiopathic inflammatory myopathies (IIMs) are sparse and of limited accuracy due to disease heterogeneity. Computational methods may address this heterogeneity by partitioning patients based on clinical and biological phenotype. Methods To identify new patient groups, we applied similarity network fusion (SNF) to clinical and biological data from 168 patients with myositis (64 adult polymyositis [PM], 65 adult dermatomyositis [DM], and 39 juvenile DM [JDM]) in the Rituximab in Myositis trial. We generated a sparse proof‐of‐concept bedside classifier using multinomial regression and identified characteristics that distinguished these groups. We conducted χ2 tests to link new patient groups with the myositis subtypes. Results SNF identified five patient groups in the discovery cohort that subdivided the myositis subtypes. The sparse multinomial regressor to predict patient group assignments (areas under the receiver operating characteristic curve = [0.78, 0.97]; areas under the precision‐recall curve = [0.55, 0.96]) found that autoantibody enrichment defined four of these groups: anti–Mi‐2, anti–signal recognition peptide (SRP), anti–nuclear matrix protein 2 (NXP2), and anti‐synthetase (Syn). Depletion of immunoglobulin M (IgM) defined the fifth group. Each group was associated with one subtype, with adult DM being associated with anti–Mi‐2 and anti‐Syn autoantibodies, JDM being associated with anti‐NXP2 autoantibodies, and adult PM being associated with IgM depletion and anti‐SRP autoantibodies. These associations enabled us to further resolve the current myositis subtypes. Conclusion Using unsupervised machine learning, we identified clinically and biologically homogeneous groups of patients with IIMs, forming the basis of an integrated disease classification based on both clinical and biological phenotype, thus validating other approaches and what has been previously described.

Published in ACR Open Rheumatology

ISSN: 2578-5745 (Online)
Publisher: Wiley
Country of publisher: United States
LCC subjects: Medicine: Internal medicine: Specialties of internal medicine: Diseases of the musculoskeletal system
Website: https://onlinelibrary.wiley.com/journal/25785745

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