Circulating Anti-GB3 Antibody as a Biomarker of Myocardial Inflammation in Patients with Fabry Disease Cardiomyopathy

Author:

Frustaci Andrea1ORCID,Verardo Romina2,Magnocavallo Michele3ORCID,Scialla Rossella2ORCID,Sansone Luigi14ORCID,Russo Matteo Antonio14ORCID

Affiliation:

1. IRCCS San Raffaele Rome, 00166 Roma, Italy

2. Cellular and Molecular Cardiology Lab, IRCCS L. Spallanzani, 00149 Roma, Italy

3. Arrhythmology Unit, Ospedale Fatebenefratelli Isola Tiberina—Gemelli Isola, 00186 Rome, Italy

4. MEBIC Consortium, San Raffaele Open University, 00166 Rome, Italy

Abstract

Background: Fabry disease cardiomyopathy (FDCM) has manifested some resistance to enzyme replacement therapy (ERT), particularly in its advanced phase. Recently, myocardial inflammation of autoimmune origin has been demonstrated in FDCM. Aims: The objective of this study was the assessment of circulating anti-globotriaosylceramide (GB3) antibodies as potential biomarkers of myocardial inflammation in FDCM, defined by the additional presence of ≥CD3+ 7 T lymphocytes/low-power field associated with focal necrosis of adjacent myocytes. Its sensitivity was based on the evidence of overlapping myocarditis at left ventricular endomyocardial biopsy. Methods and Results: From January 1996 to December 2021, 85 patients received a histological diagnosis of FDCM in our department and 48 (56.5%) of them had an overlapping myocardial inflammation with negative PCR for common cardiotropic viruses, positive antiheart, and antimyosin abs. The presence of anti-GB3 antibodies was evaluated with an in-house ELISA assay (BioGeM scarl Medical Investigational Research, MIR—Ariano Irpino, Italy), along with antiheart and antimyosin abs, in the FDCM patients and compared with control healthy individuals. The correlation between levels of circulating anti-GB3 autoantibody myocardial inflammation and FDCM severity was assessed. Anti-Gb3 antibodies were above the positivity cut-off in 87.5% of FDCM subjects with myocarditis (42 out of 48), while 81.1% of FDCM patients without myocarditis were identified as negative for Gb3 antibodies. Positive anti-Gb3 abs correlated with positive antiheart and antimyosin abs. Conclusions: The present study suggests a potential positive role of anti-GB3 antibodies as a marker of overlapping cardiac inflammation in patients with FDCM.

Funder

Investigator Initiated Research

Italian Health Ministry

Fondazione Roma

Publisher

MDPI AG

Subject

General Medicine

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