Disruption of memory B-cell trafficking by belimumab in patients with systemic lupus erythematosus

Author:

Arends Eline J1ORCID,Zlei Mihaela23ORCID,Tipton Christopher M45,Cotic Jasna6,Osmani Zgjim1,de Bie Fenna J2,Kamerling Sylvia W A1,van Maurik Andre7,Dimelow Richard8,Gregan Yun Irene9,Fox Norma Lynn10,Rabelink Ton J1,Roth David A11,Sanz Ignacio4,van Dongen Jacques J M12,van Kooten Cees1,Teng Y K Onno1ORCID

Affiliation:

1. Expert Center for Lupus-, Vasculitis-, and Complement-Mediated Systemic diseases (LuVaCs), Department of Internal Medicine—Section Nephrology, Leiden University Medical Centre , Leiden, The Netherlands

2. Department of Immunology, Leiden University Medical Centre , Leiden, The Netherlands

3. Medical Laboratory, Department of Flow Cytometry, Regional Institute of Oncology , Iasi, Romania

4. Lowance Centre for Human Immunology, Emory University School of Medicine , Atlanta, GA, USA

5. Department of Medicine, Division of Rheumatology, Emory University , Atlanta, GA, USA

6. Clinical Statistics, GSK , Middlesex, UK

7. Clinical Pharmacology and Experimental Medicine, GSK , Hertfordshire, UK

8. Clinical Pharmacology Modelling and Simulation, GSK , Hertfordshire, UK

9. Clinical Science Immunology, GSK , Collegeville, PA, USA

10. Clinical Development, GSK , Collegeville, PA, USA

11. Research and Development, GSK , Collegeville, PA, USA

12. Centro de Investigación del Cáncer-Instituto de Biología Molecular y Celular del Cáncer (CIC-IBMCC, USAL-CSIC-FICUS) and Department of Medicine, University of Salamanca , Salamanca, Spain

Abstract

Abstract Objectives Autoreactive memory B cells (MBCs) contribute to chronic and progressive courses in autoimmune diseases like SLE. The efficacy of belimumab (BEL), the first approved biologic treatment for SLE and LN, is generally attributed to depletion of activated naïve B cells and inhibition of B-cell activation. BEL’s effect on MBCs is currently unexplained. We performed an in-depth cellular and transcriptomic analysis of BEL’s impact on the blood MBC compartment in patients with SLE. Methods A retrospective meta-analysis was conducted, pooling flow cytometry data from four randomized trials involving 1245 patients with SLE treated with intravenous BEL or placebo. Then, extensive MBC phenotyping was performed using high-sensitivity flow cytometry in patients with mild/moderate SLE and severe SLE/LN treated with subcutaneous BEL. Finally, transcriptomic characterization of surging MBCs was performed by single-cell RNA sequencing. Results In BEL-treated patients, a significant increase in circulating MBCs, in a broad range of MBC subsets, was established at week 2, gradually returning to baseline by week 52. The increase was most prominent in patients with higher SLE disease activity, serologically active patients and patients aged ≤18 years. MBCs had a non-proliferating phenotype with a prominent decrease in activation status and downregulation of numerous migration genes. Conclusion Upon BEL initiation, an increase of MBCs was firmly established. In the small cohort investigated, circulating MBCs were de-activated, non-proliferative and demonstrated characteristics of disrupted lymphocyte trafficking, expanding on our understanding of the therapeutic mechanism of B-cell-activating factor inhibition by BEL. Trial registration ClinicalTrials.gov, http://clinicaltrials.gov, NCT00071487, NCT00410384, NCT01632241, NCT01649765, NCT03312907, NCT03747159.

Funder

GSK

Dutch Kidney Foundation

the Netherlands Organization for Scientific Research

University of Salamanca

Dutch Kidney Foundation and Netherlands Organization for Scientific Research

Aurinia Pharmaceuticals

Novartis and KezarBio

Fishawack Indicia Ltd

Publisher

Oxford University Press (OUP)

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