Clinical Relevance of Anti-C3 and Anti-C4 Autoantibodies in Lupus Nephritis

Vasil Vasilev; Mikel Rezola Artero; Marijana Petkova; Galya Mihaylova; Marie-Agnes Dragon-Durey; Maria Radanova; Lubka T Roumenina

doi:10.1016/j.ekir.2024.01.052

Clinical Relevance of Anti-C3 and Anti-C4 Autoantibodies in Lupus Nephritis

Kidney Int Rep. 2024 Feb 2;9(5):1429-1440. doi: 10.1016/j.ekir.2024.01.052. eCollection 2024 May.

Authors

Vasil Vasilev¹, Mikel Rezola Artero^{2

3}, Marijana Petkova¹, Galya Mihaylova⁴, Marie-Agnes Dragon-Durey^{2

5}, Maria Radanova⁴, Lubka T Roumenina²

Affiliations

¹ Clinic of Nephrology, University Hospital - "Tzaritza Yoanna - ISUL", Medical University of Sofia, Sofia, Bulgaria.
² Centre de Recherche des Cordeliers, INSERM, Sorbonne Université, Université de Paris, Team Inflammation, complement and cancer, Paris, France.
³ Department of Bacteriology and Immunology, Haartman Institute, and Translational Immunology Research Program, University of Helsinki, Helsinki, Finland.
⁴ Department of Biochemistry, Molecular Medicine and Nutrigenomics, Medical University of Varna, Varna, Bulgaria.
⁵ Laboratoire d'Immunologie, Hôpital Européen Georges Pompidou, APHP, Paris, France; Université de Paris, Paris, France.

Abstract

Introduction: Complement system overactivation is pivotal in lupus nephritis (LN) pathophysiology. Considering that anti-C3 autoantibodies play a significant role in LN pathophysiology, we explored them as disease activity biomarkers and compared them to the ones against the homologous protein, C4.

Methods: We investigated the presence of anti-C3 and anti-C4 IgG autoantibodies in a LN cohort (N = 85 patients) and monitored their changes over time. We correlated autoantibody presence with clinical parameters. We conducted cross-sectional and longitudinal analyses (N = 295 samples, 8 years follow-up) to explore associations between autoantibodies and disease progression. Antigen-specific anti-C3 or anti-C4 IgG were purified from plasma by affinity chromatography and their reactivity was tested for cross-reactivity against purified C3 or C4 by enzyme-linked immunosorbent assay (ELISA).

Results: The reactivity against C3 was independent of C4. Our study revealed distinct roles for anti-C3 and anti-C4 in LN. Anti-C3 IgG exhibited stronger clinical correlations than anti-C4, showing associations with hypocomplementemia, anti-dsDNA, class IV LN, and active disease according to British Isles Lupus Assessment Group (BILAG) renal score. In a longitudinal analysis, anti-C3 positivity at initial sampling predicted present and future disease exacerbation alone and even better when combined with anti-dsDNA, as indicated by a transition to BILAG category A.

Conclusion: Our research provides insights into anti-C3/C3b and anti-C4 autoantibodies in LN, revealing that they are often not cross-reactive. Anti-C3 utility as disease activity biomarkers is underscored by its stronger clinical associations and predictive value for future flares. Combining anti-C3 and anti-dsDNA out-performs the 2 factors alone, suggesting that the incorporation of anti-C3/C3b quantification into routine clinical practice could improve LN management.

Keywords: anti-C3 autoantibodies; anti-C3b autoantibodies; anti-C4 autoantibodies; biomarkers; complement; lupus nephritis.