Evidence that multiple myeloma Ig heavy chain VDJ genes contain somatic mutations but show no intraclonal variation

MH Bakkus, C Heirman, I Van Riet, B Van Camp… - 1992 - ashpublications.org
MH Bakkus, C Heirman, I Van Riet, B Van Camp, K Thielemans
1992ashpublications.org
To investigate whether somatic hypermutation occurs in multiple myeloma (MM) Ig VH
region genes, we have cloned and sequenced the expressed VH genes from five cases of
MM. The sequences were obtained after polymerase chain reaction (PCR) on total RNA
isolated from the bone marrow, using 5′ VH family-specific leader and 3′ C gamma-or C
alpha-specific primers. MM-specific CDR3 oligonucleotides were produced to isolate VH
genes expressed by the malignant plasma cells. In all five cases, the productive Ig gene …
Abstract
To investigate whether somatic hypermutation occurs in multiple myeloma (MM) Ig VH region genes, we have cloned and sequenced the expressed VH genes from five cases of MM. The sequences were obtained after polymerase chain reaction (PCR) on total RNA isolated from the bone marrow, using 5′ VH family-specific leader and 3′ C gamma- or C alpha- specific primers. MM-specific CDR3 oligonucleotides were produced to isolate VH genes expressed by the malignant plasma cells. In all five cases, the productive Ig gene used the VH3 family. Extensive sequence analysis of multiple independent M13 clones showed no intraclonal variation with no evidence for ongoing somatic hypermutation in MM VH region genes. We were able to identify possible germline counterparts of the expressed VH genes in two cases. Comparison of these genes shows that the MM VH region genes have somatic mutations characteristic for an antigen-driven process. In the other three cases, no close homology could be found with published VH3 sequences. These findings implicate that, in MM, clonal proliferation takes place in a cell type that has already passed through the phase of somatic hypermutation.
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