Monoclonal IgG Antibodies Generated from Joint-derived B Cells of RA Patients Have a Strong Bias Toward Citrullinated Autoantigen Recognition

Overview

Journal J Exp Med

Specialties Allergy & Immunology
General Medicine

Date 2013 Feb 27

PMID 23440041

Citations 89

Authors

Khaled Amara

Johanna Steen

Fiona Murray

Henner Morbach

Blanca M Fernandez-Rodriguez

Vijay Joshua

Marianne Engstrom

Omri Snir

Lena Israelsson

Anca I Catrina

Hedda Wardemann

Davide Corti

Eric Meffre

Lars Klareskog

Vivianne Malmstrom

Affiliations

Soon will be listed here.

Abstract

Antibodies targeting citrullinated proteins (ACPAs [anticitrullinated protein antibodies]) are commonly found in patients with rheumatoid arthritis (RA), strongly associate with distinct HLA-DR alleles, and predict a more aggressive disease course as compared with seronegative patients. Still, many features of these antibodies, including their site of production and the extent of MHC class II-driven T cell help, remain unclarified. To address these questions, we have used a single B cell-based cloning technology to isolate and express immunoglobulin (Ig) genes from joint-derived B cells of active RA patients. We found ∼25% of synovial IgG-expressing B cells to be specific for citrullinated autoantigens in the investigated ACPA(+) RA patients, whereas such antibodies were not found in ACPA(-) patients. The citrulline-reactive monoclonal antibodies did not react with the unmodified arginine peptides, yet several reacted with more than one citrullinated antigen. A role for active antigen selection of the citrulline-reactive synovial B cells was supported by the strong bias toward amino acid replacement mutations in ACPA(+) antibodies and by their loss of reactivity to citrullinated autoantigens when somatic mutations were reverted to the corresponding germline sequences.

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