Using imlifidase to elucidate the characteristics and importance of anti-GBM antibodies produced after start of treatment

Author:

Tyrberg Linnéa12,Andersson Fanny1,Uhlin Fredrik34,Hellmark Thomas1,Segelmark Mårten15ORCID

Affiliation:

1. Department of Clinical Sciences Lund, Lund University , Lund , Sweden

2. AT-unit, Helsingborg Hospital , Helsingborg , Sweden

3. Department of Nephrology and Department of Health, Medicine and Caring Sciences, Linköping University , Linköping , Sweden

4. Department of Health Technologies, Tallinn University of Technology , Tallinn , Estonia

5. Department of Nephrology, Skåne University Hospital , Lund , Sweden

Abstract

ABSTRACT Background Autoantibodies are common in glomerulonephritis, but the clinical benefit of rapid elimination has not been determined, even in anti-glomerular basement membrane (GBM) disease. Even less is known about the importance of autoantibody characteristics, including epitope specificity and immunoglobulin G (IgG) subclass distribution. We aimed to address this by characterizing the autoantibody profile in anti-GBM patients: we utilized samples from the GOOD-IDES-01 (treating GOODpasture's disease with Imunoglobulin G Degrading Enzyme of Streptococcus pyogenous) (ClinicalTrials.gov identifier: NCT03157037) trial , where imlifidase, which cleaves all IgG in vivo within hours, was given to 15 anti-GBM patients. Methods In the GOOD-IDES-01 trial, plasmapheresis was (re)started if anti-GBM antibodies rebounded. Serum samples were collected prospectively for 6 months and analyzed for anti-GBM epitope specificity using recombinant constructs of the EA and EB epitopes, IgG subclass using monoclonal antibodies, and anti-neutrophil cytoplasmic antibodies (ANCA). The results were correlated with clinical data. Results Patients with a rebound (n = 10) tended to have lower eGFR at 6 months (11 vs 34 mL/min/1.73 m2, P = .055), and patients with dialysis at 6 months had a higher EB/EA ratio at rebound (0.8 vs 0.5, P = .047). Moreover, two patients demonstrated increasing epitope restriction and several patients displayed a shift in subclass distribution at rebound. Six patients were double positive for ANCA. ANCA rebound was seen in 50% of patients; only one patient remained ANCA positive at 6 months. Conclusions In this study, rebound of anti-GBM antibodies, especially if directed against the EB epitope, was associated with a worse outcome. This supports the notion that all means should be used to eliminate anti-GBM antibodies. In this study ANCA was removed early and long-term by imlifidase and cyclophosphamide.

Funder

Skane University Hospital Research Foundations

Region Skåne

Region Östergötland

Ingrid Asp Foundation

Hansa Biopharma

Inga-Britt and Arne Lundberg Foundation

Swedish Research Council

Thelma Zoéga's Fund for Medical Research

Publisher

Oxford University Press (OUP)

Subject

Transplantation,Nephrology

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