Molecular analysis of rheumatoid factor (RF)-negative B cell hybridomas from rheumatoid synovial tissue: evidence for an antigen-induced stimulation with selection of high mutated IgVH and low mutated IgVL/λ genes

Abstract

The mutational pattern of IgV_H and IgV_L genes from synovial tissue B cell hybridomas (n = 8) of patients (n = 4) with rheumatoid arthritis (RA) was analysed, which had been produced by the electrofusion technique without prior in vitro stimulation. The molecular data were correlated with immunohistopathological data and parameters of local disease activity. The IgV_H genes of the B cell hybridomas belonged to the V_H3 family (DP42; DP47, n = 2; DP53), the V_H1 family (DP75), the V_H4 family (DP71) and the V_H5 family (DP73); 7/7 IgV_H genes showed somatic mutations, the R/S ratio (CDR) was > 3 in 4/7 IgV_H genes and the mean R/S ratio of all IgV_H genes was 9.3 (CDR) and 1.0 (FR), suggesting an antigen-dependent selection. The IgV_L/λ genes belonged to the Vλ1 family (DPL2, DPL5, DPL8nf), the Vλ2 family (DPL11, n = 2) and to the Vλ6 family (IGLV6S1); 6/6 IgV_L genes showed somatic mutations, the R/S ratio (CDR) was > 3 in 3/6 IgV_L genes and the mean R/S ratio of all IgV_L was 3.0 (CDR) and 2.3 (FR), suggesting an antigen-dependent selection. The synovial tissue exhibited germinal centres in the follicles (3/4), with the unique distribution of Ki-M4⁺ follicular dendritic cells and Ki-67⁺ proliferating cells and a dominance of IgA⁺ plasma cells (3/3). All patients were positive for RF in serum and exhibited severe local symptoms (swelling 4/4; warmth 4/4; effusion 2/4), whereas the hybridomas were negative for RF. Since B cell hybridomas showed hypermutation and affinity selection for IgV_H and IgV_L/λ genes and the patients exhibited severe local symptoms with germinal centres in synovial tissue, this study indicates that an antigen-driven process is behind the B cell expansion in the synovial tissue of clinically affected joints. These mutated B hybridomas were negative for RF, thus suggesting that antigens different from RF are also involved in the local B cell expansion and in the chronic synovitis of RA.