ACR Meeting Abstracts

ACR Meeting Abstracts

Abstract Number: 760

Cluster Analysis To Explore Clinical Subclassification Of Eosinophilic Granulomatosis With Polyangiitis (Churg–Strauss)

Thomas Neumann1, Frank Moosig2, Augusto Vaglio3, Jochen Zwerina4, Renato Alberto Sinico5, Wojciech Szczeklik6, Paolo Bottero7, Phillip Bremer8, Andrea Gioffredi9, Barbara Sokolowska6, Luca Di Toma5, Federica Maritati9, Julian Großkreutz10, Claus Kroegel11, Matthieu Resche-Rigon12 and Alfred Mahr13, 1Jena University Hospital, Internal Medicine III, Jena, Germany, 2Vasculitis Clinic, Klinikum Bad Bramstedt & University Hospital of Schleswig Holstein, Bad Bramstedt, Germany, 3Unit of Nephrology, University Hospital of Parma, Parma, Italy, 4Ludwig Bolzmann institut of osteology at the 4th medical departmen, Hanusch Hospital, Vienna, Austria, 5Clinical Immunology Unit and Renal Unit, Department of Medicine, Azienda Ospedaliera Ospedale San Carlo Borromeo, Milan, Italy, 6Department of Medicine, Jagiellonian University Medical College, Krakow, Poland, 7llergy and Clinical Immunology Unit, Magenta Hospital, Magenta, Italy, 8University Hospital Schleswig Holstein and Klinikum Bad Bramstedt, Bad Bramstedt, Germany, 9Department of Clinical Medicine, Nephrology and Health Sciences, University of Parma, Parma, Italy, 10Department of Neurology, Jena University-Hospital, Jena, Germany, 11Jena University Hospital, Internal Medicine I, Jena, Germany, 12Biostatistics, Hopital Saint-Louis, Paris, France, 13Department of Internal Medicine, Hospital Saint-Louis, Paris, France

Meeting: 2013 ACR/ARHP Annual Meeting

Keywords: ,

Session Information

Title: Vasculitis I

Session Type: Abstract Submissions (ACR)

Background/Purpose: Results from descriptive studies of eosinophilic granulomatosis with polyangiitis (EGPA) suggest distinct clinical subclasses that may be determined by anti-neutrophil cytoplasmic antibody (ANCA) status. We used hierarchical cluster analysis to explore whether EGPA could be subclassified.

Methods: The study was based on patients with clinically diagnosed EGPA followed in 6 tertiary referral centers for vasculitis in Germany, Italy and Poland. Clinical data and ANCA results were collected retrospectively on a standardized case report form. A hierarchical cluster analysis (Ward’s method) was performed using the following 12 input variables assessed at diagnosis or at relapse including the main symptoms and organ involvements (general symptoms, arthromuscular, mucocutaneous, ophthalmological, ENT, cardiovascular, gastrointestinal, renal and central nervous system involvement, peripheral neuropathy, non-fixed lung infiltrates) and ANCA positivity. The resulting clusters were described by their most prominent summary characteristics. The distribution of clinical variables was analyzed by ANCA status with chi-square test.

Results: The analyzed dataset included 362 EGPA cases diagnosed between 1984 and 2013. Median age at diagnosis was 50 years and 48% were males; ANCA were detected in 35%. The cluster analysis produced 3 clusters of respectively 158 (cluster 1), 74 (cluster 2) and 130 subjects (cluster 3). They were characterized as follows: cluster 1 by high proportion of renal involvement (43%) and positive ANCA serology (73%); cluster 2 by virtually absent renal involvement (4%) and no ANCA (0%); and cluster 3 by an intermediate phenotype with renal involvement (15%), positive ANCA (9%) and more frequent cardiovascular (57% vs. 33% and 38% for clusters 1 and 2, respectively) and gastrointestinal involvement (44% vs. 22% and 15%). Stratification of the 11 clinical input variables by ANCA status found that ANCA positivity was associated with more frequent arthromuscular involvement (= 0.045), renal involvement (< 0.0001), peripheral neuropathy (= 0.011), constitutional symptoms (= 0.006) while absence of ANCA was associated with more frequent cardiovascular involvement (= 0.005).

Conclusion: Cluster analysis of EGPA, although reinforcing the link between ANCA status and renal, peripheral nervous system and cardiovascular involvement, does not suggest that this disease is composed of clearly separated and mutually exclusive subclasses.

Disclosure:

T. Neumann,
None;

F. Moosig,
None;

A. Vaglio,
None;

J. Zwerina,
None;

R. A. Sinico,
None;

W. Szczeklik,
None;

P. Bottero,
None;

P. Bremer,
None;

A. Gioffredi,
None;

B. Sokolowska,
None;

L. Di Toma,
None;

F. Maritati,
None;

J. Großkreutz,
None;

C. Kroegel,
None;

M. Resche-Rigon,
None;

A. Mahr,
None.

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