Direct Reduction of Antigen Receptor Expression in Polyclonal B Cell Populations Developing In Vivo Results in Light Chain Receptor Editing

  • Shen S
  • Manser T
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Abstract

Secondary Ab V region gene segment rearrangement, termed receptor editing, is a major mechanism contributing to B lymphocyte self-tolerance. However, the parameters that determine whether a B cell undergoes editing are a current subject of debate. We tested the role that the level of BCR expression plays in the regulation of receptor editing in a polyclonal population of B cells differentiating in vivo. Expression of a short hairpin RNA for κ L chain RNA in B cells resulted in reduction in levels of this RNA and surface BCRs. Strikingly, fully mature and functional B cells that developed in vivo and efficiently expressed the short hairpin RNA predominantly expressed BCRs containing λ light chains. This shift in L chain repertoire was accompanied by inhibition of development, increased Rag gene expression, and increased λ V gene segment-cleavage events at the immature B cell stage. These data demonstrated that reducing the translation of BCRs that are members of the natural repertoire at the immature B cell stage is sufficient to promote editing.

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Shen, S., & Manser, T. (2012). Direct Reduction of Antigen Receptor Expression in Polyclonal B Cell Populations Developing In Vivo Results in Light Chain Receptor Editing. The Journal of Immunology, 188(1), 47–56. https://doi.org/10.4049/jimmunol.1102109

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