Opposing peripheral fates of tissue-restricted self antigen-specific conventional and regulatory CD4+ T cells.

The development of self antigen-specific T cells is influenced by how the self antigen is expressed. Here, we created a mouse in which a model self antigen is conditionally expressed in different tissue environments. Using peptide:MHCII tetramer-based cell enrichment methods, we examined the development of corresponding endogenous self antigen-specific CD4+ T cell populations. While ubiquitous self antigen expression resulted in efficient deletion of self antigen-specific T cells in the thymus, some tissue-restricted expression patterns resulted in partial deletion of the population in peripheral lymphoid organs. Deletion specifically affected Foxp3- conventional T cells (Tconv) with a bias towards high avidity TCR expressing cells in the case of thymic, but not peripheral deletion. In contrast, Foxp3+ Treg exhibited elevated frequencies with increased TCR avidity. T cells surviving deletion were functionally impaired, with Tconv cells exhibiting more impairment than Tregs. Collectively, our results illustrate how postthymic recognition of tissue-restricted self antigens results in opposing developmental fates for Tconv and Treg cell subsets. © 2019 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim.

Citation

Zimeng Zhang, Francois P Legoux, Spencer W Vaughan, James J Moon. Opposing peripheral fates of tissue-restricted self antigen-specific conventional and regulatory CD4+ T cells. European journal of immunology. 2020 Jan;50(1):63-72

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PMID: 31580477

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