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VH replacement rescues progenitor B cells with two nonproductive VDJ alleles

    Research output: Contribution to journalArticlepeer-review

    Abstract

    Inaccurate VDJ rearrangements generate a large number of progenitor (pro)-B cells with two nonproductive IgH alleles. Such cells lack essential survival signals mediated by surface IgM heavy chain (μH chain) expression and are normally eliminated. However, secondary rearrangements of upstream VH gene segments into assembled VDJ exons have been described in mice transgenic for productive μH chains, a process known as VH replacement. If VH replacement was independent of chain signals, it could also modify nonproductive VDJ exons and thus rescue pro-B cells with unsuccessful rearrangements on both alleles. To test this hypothesis, we homologously replaced the JH cluster of a mouse with a nonproductive VDJ exon. Surprisingly, B cell development in IgHVDJ-/VDJ- mice was only slightly impaired and significant numbers of IgM-positive B cells were produced. DNA sequencing confirmed that all VDJ sequences from μH chain-positive B lymphoid cells were generated by VH replacement in a RAG-dependent manner. Another unique feature of our transgenic mice was the presence of IgH chains with unusually long CDR3-H regions. Such IgH chains were functional and only modestly counter-selected, arguing against a strict length constraint for CDR3-H regions. In conclusion, VH replacement can occur in the absence of a μH chain signal and provides a potential rescue mechanism for pro-B cells with two nonproductive IgH alleles. Copyright © 2006 by The American Association of Immunologists, Inc.
    Original languageEnglish
    Pages (from-to)7007-7014
    Number of pages7
    JournalJournal of Immunology
    Volume177
    Issue number10
    Publication statusPublished - 15 Nov 2006

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