Anti-dsDNA B-Cell ELISpot as a Monitoring and Flare Prediction Tool in SLE Patients

Author:

Pérez-Isidro Albert12ORCID,Xipell Marc234,Llobell Arturo12,De Moner Noemí1,Lledó Gema M.256ORCID,Cervera Ricard256ORCID,Prieto-González Sergio256ORCID,Quintana Luis F.234ORCID,Espinosa Gerard256ORCID,García-Ormaechea Mila17,Ruiz-Ortiz Estíbaliz12,Viñas Odette12

Affiliation:

1. Department of Immunology, Centre de Diagnòstic Biomèdic (CDB), Hospital Clínic, 08036 Barcelona, Spain

2. Institut d’Investigacions Biomèdiques August Pi i Sunyer (IDIBAPS), 08036 Barcelona, Spain

3. Department of Nephrology and Renal Transplantation, Hospital Clínic, University of Barcelona, 08036 Barcelona, Spain

4. Reference Centre for Complex Glomerular Disease (CSUR) of the Spanish Health System, 08036 Barcelona, Spain

5. Department of Autoimmune Diseases, Hospital Clínic, University of Barcelona, 08036 Barcelona, Spain

6. Reference Centre for Systemic Autoimmune Diseases (CSUR) of the Spanish Health System, 08036 Barcelona, Spain

7. Lime Tree Surgery NHS, Worthing BN14 0DL, UK

Abstract

Anti-dsDNA autoantibodies quantification and complement levels are widely used to monitor disease activity in systemic lupus erythematosus (SLE). However, better biomarkers are still needed. We hypothesised whether the dsDNA antibody-secreting B-cells could be a complementary biomarker in disease activity and prognosis of SLE patients. Fifty-two SLE patients were enrolled and followed for up to 12 months. Additionally, 39 controls were included. An activity cut-off (comparing active and non-active patients according to clinical SLEDAI-2K) was established for SLE-ELISpot, chemiluminescence and Crithidia luciliae indirect immunofluorescence tests (≥11.24, ≥374.1 and ≥1, respectively). Assays performances together with complement status were compared regarding major organ involvement at the inclusion and flare-up risk prediction after follow-up. SLE-ELISpot showed the best performance in identifying active patients. High SLE-ELISpot results were associated with haematological involvement and, after follow-up, with an increased hazard ratio for disease flare-up (3.4) and especially renal flare (6.5). Additionally, the combination of hypocomplementemia and high SLE-ELISpot results increased those risks up to 5.2 and 32.9, respectively. SLE-ELISpot offers complementary information to anti-dsDNA autoantibodies to evaluate the risk of a flare-up in the following year. In some cases, adding SLE-ELISpot to the current follow-up protocol for SLE patients can improve clinicians’ personalised care decisions.

Funder

Hospital Clínic de Barcelona

Publisher

MDPI AG

Subject

General Medicine

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