Pathogenic Citrulline‐Multispecific B Cell Receptor Clades in Rheumatoid Arthritis

Philip J. Titcombe; Gustaf Wigerblad; Natalie Sippl; Na Zhang; Anna Shmagel; Peter Sahlström; Y Zhang; Laura O. Barsness; Yogita Ghodke‐Puranik; Azar Baharpoor; Monika Hansson; Lena Israelsson; Karl Skriner; Timothy B. Niewold; Lars Klareskog; Camilla I. Svensson; Khaled Amara; Vivianne Malmström; Daniel L. Mueller

doi:10.1002/art.40590

Pathogenic Citrulline‐Multispecific B Cell Receptor Clades in Rheumatoid Arthritis

Philip J. Titcombe(University of Minnesota), Gustaf Wigerblad(Karolinska Institutet), Natalie Sippl(Karolinska Institutet), Na Zhang(University of Minnesota Medical Center), Anna Shmagel(University of Minnesota Medical Center), Peter Sahlström(Karolinska Institutet), Y Zhang(University of Minnesota Medical Center), Laura O. Barsness(University of Minnesota Medical Center), Yogita Ghodke‐Puranik(New York University), Azar Baharpoor(Karolinska Institutet), Monika Hansson(Karolinska Institutet), Lena Israelsson(Karolinska Institutet), Karl Skriner(Charité - Universitätsmedizin Berlin), Timothy B. Niewold(New York University), Lars Klareskog(Karolinska Institutet), Camilla I. Svensson(Karolinska Institutet), Khaled Amara(Karolinska Institutet), Vivianne Malmström(Karolinska Institutet), Daniel L. Mueller(University of Minnesota Medical Center)

Arthritis & Rheumatology

June 21, 2018

10.1002/art.40590

Cited by 111

Abstract

OBJECTIVE: Anti-citrullinated protein antibodies (ACPAs) have proven highly useful as biomarkers for rheumatoid arthritis (RA). However, composition and functionality of the associated autoreactive B cell repertoire have not been directly assessed. We aimed to selectively investigate citrullinated autoantigen-specific B cell receptors (BCRs) involved in RA and initiate studies on their pathogenicity. METHODS: Blood samples were obtained from patients in a University of Minnesota cohort with ACPA-positive RA (n = 89). Tetramer sets bearing citrullinated filaggrin peptide cfc1 or citrullinated α-enolase peptide were constructed to specifically capture autoreactive B cells from the unaltered, polyclonal repertoire in RA patients. Citrullinated peptide tetramer-bound B cells were subjected to flow cytometric cell sorting and single-cell IGH, IGK, and IGL gene sequencing for B cell lineage determinations. BCR gene sequences were also expressed as recombinant monoclonal antibodies (mAb) for direct evaluation of citrullinated autoantigen binding and effector functionality. RESULTS: Using citrullinated peptide tetramer enrichment to investigate single autoreactive blood B cells, we identified biased V-region gene usage and conserved junction arrangements in BCRs from RA patients. Parsimonious clustering of related immunoglobulin gene nucleotide sequences revealed clonal expansions of rare individual B cell clades, in parallel with divergent sequence mutations. Correspondingly, recombinant mAb generated from such BCR lineages demonstrated citrulline-dependent cross-reactivity extending beyond the citrullinated peptides used for B cell capture. A pair of citrullinated autoantigen-specific mAb with cross-reactive binding profiles also promoted arthritis in mice. CONCLUSION: Our findings suggest that broad ACPA specificities in RA arise from a restricted repertoire of evolving citrulline-multispecific B cell clades with pathogenic potential.

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