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To analyze the immunoglobulin repertoire of human IgM B cells and the CD5 and CD5 sup -subsets, individual CD19 /IgM /CD5 or CD5 (-) B cells were sorted and non-productive as well as productive VH gene rearrangements were amplified from genomic DNA and sequenced. In both subsets, the VH 3 family was overrepresented largely as a result of preferential usage of a small number of specific individual family members. In the CD5 B cell subset, all other VH families were found at a frequency expected from random usage, whereas in the CD5 (-) population, VH 4 appeared to be overrepresented in the nonproductive repertoire, and also negatively selected since it was found significantly less often in the productive compared to the nonproductive repertoire; the VH 1 family was significantly diminished in the productive rearrangements of CD5- B cells. 3-23/DP-47 was the most frequently used VH gene segment and was found significantly more often than expected from random usage in productive rearrangements of both CD5 and CD5- B cells. Evidence for selection based on the D segment and the JH gene usage was noted in CD5 B cells. No differences were found between the B cell subsets in CDR3 length, the number of N-nucleotides or evidence of exonuclease activity. Somatically hypermutated VH DJH rearrangements were significantly more frequent and extensive in CD5- compared to CD5 IgM B cells, indicating that IgM memory B cells were more frequent in the CD5- B cell population. Of note, the frequency of specific VH genes in the mutated population differed from that in the nonmutated population, suggesting that antigen stimulation imposed additional biases on the repertoire of IgM B cells. These results indicate that the expressed repertoire of IgM B cell subsets is shaped by recombinational bias, as well as selection before and after antigen exposure. Moreover, the influences on the repertoires of CD5 and CD5- B cells are significantly different, suggesting that human peripheral blood CD5 and CD5- B cells represent different B cell lineages, with similarities to murine B-1a and B-2 subsets, respectively. (J. Clin. Invest. 1997. 99:2488-2501.)

Copyright (C) 1997 The American Society for Clinical Investigation, Inc.