IL-7R signaling activates widespread VH and DH gene usage to drive antibody diversity in bone marrow B cells

IL-7R 信号激活广泛的 VH 和 DH 基因使用,从而驱动骨髓 B 细胞中的抗体多样性

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作者:Amanda Baizan-Edge, Bryony A Stubbs, Michael J T Stubbington, Daniel J Bolland, Kristina Tabbada, Simon Andrews, Anne E Corcoran

Abstract

Generation of the primary antibody repertoire requires V(D)J recombination of hundreds of gene segments in the immunoglobulin heavy chain (Igh) locus. The role of interleukin-7 receptor (IL-7R) signaling in Igh recombination has been difficult to partition from its role in B cell survival and proliferation. With a detailed description of the Igh repertoire in murine IL-7Rα-/- bone marrow B cells, we demonstrate that IL-7R signaling profoundly influences VH gene selection during VH-to-DJH recombination. We find skewing toward 3' VH genes during de novo VH-to-DJH recombination more severe than the fetal liver (FL) repertoire and uncover a role for IL-7R signaling in DH-to-JH recombination. Transcriptome and accessibility analyses suggest reduced expression of B lineage transcription factors (TFs) and targets and loss of DH and VH antisense transcription in IL-7Rα-/- B cells. Thus, in addition to its roles in survival and proliferation, IL-7R signaling shapes the Igh repertoire by activating underpinning mechanisms.

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