Thymocytes trigger self-antigen-controlling pathways in immature medullary thymic epithelial stages

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Self-reactive CD4+ thymocytes induce self-antigen expression and other key molecules in immature medullary thymic epithelial cells, influencing their transcriptional regulators and subset composition, including Aire+ mTEChi precursors.

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Abstract

Interactions of developing T cells with Aire + medullary thymic epithelial cells expressing high levels of MHCII molecules (mTEC hi ) are critical for the induction of central tolerance. In turn, thymocytes regulate the cellularity of Aire + mTEC hi . However, it remains unknown whether thymocytes control Aire + mTEC hi -precursors that are contained in mTEC lo cells or other mTEC lo subsets that have recently been delineated or identified by single-cell transcriptomic analyses. Here, using three distinct transgenic mouse models, in which antigen-presentation between mTECs and CD4 + thymocytes is perturbed, we show by high-throughput RNA-seq that self-reactive CD4 + thymocytes induce in mTEC lo the expression of tissue-restricted self-antigens, cytokines, chemokines and adhesion molecules important for T-cell development. This gene activation program is combined with a global increase of the active H3K4me3 histone mark. Finally, we show that these interactions induce key mTEC transcriptional regulators and govern mTEC lo subset composition, including Aire + mTEC hi -precursors, post-Aire and tuft-like mTECs. Our genome-wide study thus reveals that self-reactive CD4 + thymocytes control multiple unsuspected facets from immature stages of mTECs, which determines their heterogeneity.

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europepmc
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