B Lymphocyte Autoimmunity in Rheumatoid Synovitis is Independent of Ectopic Lymphoid Neogenesis

Overview

Journal J Immunol

Specialty Allergy & Immunology

Date 2008 Jun 21

PMID 18566445

Citations 57

Authors

Tineke Cantaert

Johanna Kolln

Trieneke Timmer

Tineke C van der Pouw Kraan

Bernard Vandooren

Rogier M Thurlings

Juan D Canete

Anca I Catrina

Theo Out

Cor L Verweij

Yiping Zhang

Paul P Tak

Dominique Baeten

Affiliations

Soon will be listed here.

Abstract

B lymphocyte autoimmunity plays a crucial role in the pathogenesis of rheumatoid arthritis. The local production of autoantibodies and the presence of ectopic lymphoid neogenesis in the rheumatoid synovium suggest that these dedicated microenvironments resembling canonical lymphoid follicles may regulate the initiation and maturation of B cell autoimmunity. In this study, we assessed experimentally the relevance of ectopic lymphoid neogenesis for B cell autoimmunity by a detailed structural, molecular, and serological analysis of seropositive and seronegative human synovitis. We demonstrate that synovial lymphoid neogenesis is a reversible process associated with inflammation which is neither restricted to nor preferentially associated with autoantibody positive rheumatic conditions. Despite the abundant expression of key chemokines and cytokines required for full differentiation toward germinal center reactions, synovial lymphoid neogenesis in rheumatoid arthritis only occasionally progresses toward fully differentiated follicles. In agreement with that observation, we could not detect Ag-driven clonal expansion and affinity maturation of B lymphocytes. Furthermore, ectopic lymphoid neogenesis is not directly associated with local production of anti-citrullinated protein Abs and rheumatoid factor in the rheumatoid joint. Therefore, we conclude that synovial lymphoid neogenesis is not a major determinant of these rheumatoid arthritis-specific autoantibody responses.

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