Quantification of Antifibrillarin (anti-U3 RNP) Antibodies: A New Insight for Patients with Systemic Sclerosis

Audrey Benyamine; Daniel Bertin; Noémie Resseguier; Xavier Heim; Julien Bermudez; David Launay; Sylvain Dubucquoi; Adrian Hij; Dominique Farge; Alain Lescoat; Isabelle Bahon-Riedinger; Nouria Benmostefa; Luc Mouthon; Jean-Robert Harlé; Gilles Kaplanski; Pascal Rossi; Nathalie Bardin; Brigitte Granel

doi:10.3390/diagnostics11061064

Diagnostics (Jun 2021)

Quantification of Antifibrillarin (anti-U3 RNP) Antibodies: A New Insight for Patients with Systemic Sclerosis

Audrey Benyamine,
Daniel Bertin,
Noémie Resseguier,
Xavier Heim,
Julien Bermudez,
David Launay,
Sylvain Dubucquoi,
Adrian Hij,
Dominique Farge,
Alain Lescoat,
Isabelle Bahon-Riedinger,
Nouria Benmostefa,
Luc Mouthon,
Jean-Robert Harlé,
Gilles Kaplanski,
Pascal Rossi,
Nathalie Bardin,
Brigitte Granel

Affiliations

Audrey Benyamine: Internal Medicine Department, North Hospital of Marseilles, Public Assistance Hospital of Marseilles (AP-HM), 13015 Marseilles, France
Daniel Bertin: Immunology Laboratory, La Conception Hospital, Public Assistance Hospital of Marseilles (AP-HM), 13005 Marseilles, France
Noémie Resseguier: Epidemiology and Health Economics, La Timone Hospital, AP-HM, Aix Marseilles University (AMU), 13005 Marseilles, France
Xavier Heim: Aix Marseilles University (AMU), INSERM, INRA, C2VN, 13005 Marseilles, France
Julien Bermudez: Aix Marseilles University (AMU), INSERM, INRA, C2VN, 13005 Marseilles, France
David Launay: Univ. Lille, U1286-INFINITE—Institute for Translational Research in Inflammation, F-59000 Lille, France
Sylvain Dubucquoi: Immunology Institute, Hospital University Center of Lille, 59037 Lille, France
Adrian Hij: Public Assistance Hospital of Paris, Saint-Louis Hospital, Autoimmune and Vascular Disease Unit, Internal Medicine (UF04), Center of reference for rare systemic autoimmune diseases (FAI2R), Université de Paris, EA 3518, Paris, France
Dominique Farge: Public Assistance Hospital of Paris, Saint-Louis Hospital, Autoimmune and Vascular Disease Unit, Internal Medicine (UF04), Center of reference for rare systemic autoimmune diseases (FAI2R), Université de Paris, EA 3518, Paris, France
Alain Lescoat: Internal Medicine and Clinical Immunology Department, Hospital University Center of Rennes, 35000 Rennes, France
Isabelle Bahon-Riedinger: Immunology Laboratory, Hospital University Center of Rennes, 35033 Rennes, France
Nouria Benmostefa: Internal Medicine Department, Center of reference for rare systemic autoimmune diseases of Ile de France, Cochin Hospital, Public Assistance Hospital of Paris (AP-HP), 75014 Paris, France
Luc Mouthon: Internal Medicine Department, Center of reference for rare systemic autoimmune diseases of Ile de France, Cochin Hospital, Public Assistance Hospital of Paris (AP-HP), 75014 Paris, France
Jean-Robert Harlé: Internal Medicine Department, La Timone Hospital, Public Assistance Hospital of Marseilles (AP-HM), 13005 Marseilles, France
Gilles Kaplanski: Aix Marseilles University (AMU), INSERM, INRA, C2VN, 13005 Marseilles, France
Pascal Rossi: Internal Medicine Department, North Hospital of Marseilles, Public Assistance Hospital of Marseilles (AP-HM), 13015 Marseilles, France
Nathalie Bardin: Aix Marseilles University (AMU), INSERM, INRA, C2VN, 13005 Marseilles, France
Brigitte Granel: Internal Medicine Department, North Hospital of Marseilles, Public Assistance Hospital of Marseilles (AP-HM), 13015 Marseilles, France

DOI: https://doi.org/10.3390/diagnostics11061064
Journal volume & issue: Vol. 11, no. 6
p. 1064

Abstract

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Background: The detection of additional autoantibodies is of great concern in systemic sclerosis (SSc) when those included in the ACR/EULAR classification are negative. In this context, the interest of antifibrillarin (anti-U3RNP) autoantibodies (AFAs) in the routine evaluation of SSc remains unclear. We aimed to assess the relevance of AFAs and their clinical association in SSc patients. Methods: In a multicenter observational retrospective study, we collected immunological and clinical data associated with AFA positivity in SSc (n = 42) and non-SSc patients (n = 13). Patients with SSc negative for AFAs (n = 83) were considered as a control group. AFAs were detected by indirect immunofluorescence (IIF) using HEp-2 cells, EliA or immunoblot techniques. Results: We confirmed a typical nuclear IIF pattern and showed that AFAs are mostly exclusive towards SSc conventional autoantibodies. Although also observed in non-SSc patients, high levels of AFAs with the ELiA technique allowed the diagnosis of SSc. Compared to AFA-negative SSc patients, AFA-positive SSc patients more frequently exhibited visceral involvements. They more frequently suffered from the diffuse cutaneous form and had a higher global severity of the disease. Conclusions: We demonstrate the usefulness of quantifying AFAs in the immunological exploration of SSc, especially when patients are seronegative for SSc conventional autoantibodies and display a typical IIF pattern. AFAs might constitute an interesting marker of SSc severity.

Published in Diagnostics

ISSN: 2075-4418 (Online)
Publisher: MDPI AG
Country of publisher: Switzerland
LCC subjects: Medicine: Medicine (General)
Website: http://www.mdpi.com/journal/diagnostics

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