Immunoglobulin VH gene sequence analysis of spontaneous murine immunoglobulin‐secreting B‐cell tumours with clinical features of human disease

Abstract

The 5T series of multiple myelomas (MM) and Waldenstrsöm’s macroglobulinaemia-like lymphomas (WM), which developed spontaneously in ageing mice of the C57BL/KaLwRij strain, shows clinical and biological features that closely resemble their corresponding human diseases. In order to compare the patterns of somatic mutation in V_H genes of mouse tumours with those of human counterparts, we have determined and analysed sequences of immunoglobulin V_H genes in five cases of murine MM, two of WM and one of biclonal benign monoclonal gammopathy (BMG). Four of five MM and 2/2 WM cases used V_H genes of the large J558 family; one MM used a gene of the VGAM3.8 family, and both clones of the BMG used genes of the 36-60 family. N-region insertions were observed in all cases, but D-segment genes were only identified in 6/9 cases, which were all from the D-SP family and translated in reading frame 3. Compared with human MM, in which the V_H genes have been found to be consistently hypermutated (mean%±SD=8·8±3·2), the degree of somatic mutation in the murine tumours was significantly lower (mean%±SD=2·9±2·3). There was no significant evidence of clustering of replacement mutations in complementarity determining regions (CDR), a feature considered to be characteristic of antigen-selected sequences. However, one clone of the biclonal BMG case showed intraclonal variation, a feature described in some cases of human BMG. These results indicate that murine V_H genes in mature tumours differ from human counterparts in the level and distribution of somatic mutations, but support the concept that BMG may be distinct from MM.