Open Biology (Jul 2018)

Loss of runx1 function results in B cell immunodeficiency but not T cell in adult zebrafish

  • Yali Chi,
  • Zhibin Huang,
  • Qi Chen,
  • Xiaojie Xiong,
  • Kemin Chen,
  • Jin Xu,
  • Yiyue Zhang,
  • Wenqing Zhang

DOI
https://doi.org/10.1098/rsob.180043
Journal volume & issue
Vol. 8, no. 7

Abstract

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Transcription factor RUNX1 holds an integral role in multiple-lineage haematopoiesis and is implicated as a cofactor in V(D)J rearrangements during lymphocyte development. Runx1 deficiencies resulted in immaturity and reduction of lymphocytes in mice. In this study, we found that runx1W84X/W84X mutation led to the reduction and disordering of B cells, as well as the failure of V(D)J rearrangements in B cells but not T cells, resulting in antibody-inadequate-mediated immunodeficiency in adult zebrafish. By contrast, T cell development was not affected. The decreased number of B cells mainly results from excessive apoptosis in immature B cells. Disrupted B cell development results in runx1W84X/W84X mutants displaying a similar phenotype to common variable immunodeficiency—a primary immunodeficiency disease primarily characterized by frequent susceptibility to infection and deficient immune response, with marked reduction of antibody production of IgG, IgA and/or IgM. Our studies demonstrated an evolutionarily conserved function of runx1 in maturation and differentiation of B cells in adult zebrafish, which will serve as a valuable model for the study of immune deficiency diseases and their treatments.

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