Cell Reports (Jan 2018)

Age-Associated Decline in Thymic B Cell Expression of Aire and Aire-Dependent Self-Antigens

  • Sergio Cepeda,
  • Carolina Cantu,
  • Stephanie Orozco,
  • Yangming Xiao,
  • Zoe Brown,
  • Manpreet K. Semwal,
  • Thomas Venables,
  • Mark S. Anderson,
  • Ann V. Griffith

Journal volume & issue
Vol. 22, no. 5
pp. 1276 – 1287

Abstract

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Summary: Although autoimmune disorders are a significant source of morbidity and mortality in older individuals, the mechanisms governing age-associated increases in susceptibility remain incompletely understood. Central T cell tolerance is mediated through presentation of self-antigens by cells constituting the thymic microenvironment, including epithelial cells, dendritic cells, and B cells. Medullary thymic epithelial cells (mTECs) and B cells express distinct cohorts of self-antigens, including tissue-restricted self-antigens (TRAs), such that developing T cells are tolerized to antigens from peripheral tissues. We find that expression of the TRA transcriptional regulator Aire, as well as Aire-dependent genes, declines with age in thymic B cells in mice and humans and that cell-intrinsic and cell-extrinsic mechanisms contribute to the diminished capacity of peripheral B cells to express Aire within the thymus. Our findings indicate that aging may diminish the ability of thymic B cells to tolerize T cells, revealing a potential mechanistic link between aging and autoimmunity. : Mechanisms governing age-associated increases in autoimmunity remain elusive. Expression of Aire and downstream self-antigens by thymic B cells helps tolerize developing T cells. Cepeda et al. report age-associated declines in expression of Aire and self-antigen genes in thymic B cells concomitant with increases in T-bet and IgG2a expression. Keywords: thymus, B cell, aging, Aire