Literature DB >> 23980163

Overlapping gene coexpression patterns in human medullary thymic epithelial cells generate self-antigen diversity.

Sheena Pinto1, Chloé Michel, Hannah Schmidt-Glenewinkel, Nathalie Harder, Karl Rohr, Stefan Wild, Benedikt Brors, Bruno Kyewski.   

Abstract

Promiscuous expression of numerous tissue-restricted self-antigens (TRAs) in medullary thymic epithelial cells (mTECs) is essential to safeguard self-tolerance. A distinct feature of promiscuous gene expression is its mosaic pattern (i.e., at a given time, each self-antigen is expressed only in 1-3% of mTECs). How this mosaic pattern is generated at the single-cell level is currently not understood. Here, we show that subsets of human mTECs expressing a particular TRA coexpress distinct sets of genes. We identified three coexpression groups comprising overlapping and complementary gene sets, which preferentially mapped to certain chromosomes and intrachromosomal gene clusters. Coexpressed gene loci tended to colocalize to the same nuclear subdomain. The TRA subsets aligned along progressive differentiation stages within the mature mTEC subset and, in vitro, interconverted along this sequence. Our data suggest that single mTECs shift through distinct gene pools, thus scanning a sizeable fraction of the overall repertoire of promiscuously expressed self-antigens. These findings have implications for the temporal and spatial (re)presentation of self-antigens in the medulla in the context of tolerance induction.

Entities:  

Keywords:  central tolerance; human thymic epithelial cells; promiscuous gene expression

Mesh:

Substances:

Year:  2013        PMID: 23980163      PMCID: PMC3773787          DOI: 10.1073/pnas.1308311110

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


  38 in total

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2.  Chromosomal clustering of genes controlled by the aire transcription factor.

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3.  Transient colocalization of X-inactivation centres accompanies the initiation of X inactivation.

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Review 4.  A central role for central tolerance.

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5.  Interchromosomal interactions and olfactory receptor choice.

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7.  Loss of Aire-dependent thymic expression of a peripheral tissue antigen renders it a target of autoimmunity.

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8.  Expression of tumor-associated differentiation antigens, MUC1 glycoforms and CEA, in human thymic epithelial cells: implications for self-tolerance and tumor therapy.

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9.  Promiscuous gene expression in thymic epithelial cells is regulated at multiple levels.

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10.  Spontaneous autoimmunity prevented by thymic expression of a single self-antigen.

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  36 in total

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Review 2.  Lymphocyte repertoire selection and intracellular self/non-self-discrimination: historical overview.

Authors:  Donald R Forsdyke
Journal:  Immunol Cell Biol       Date:  2014-11-11       Impact factor: 5.126

Review 3.  Thymic tolerance as a key brake on autoimmunity.

Authors:  Mickie Cheng; Mark S Anderson
Journal:  Nat Immunol       Date:  2018-06-20       Impact factor: 25.606

Review 4.  Thymic epithelial cell heterogeneity: TEC by TEC.

Authors:  Noam Kadouri; Shir Nevo; Yael Goldfarb; Jakub Abramson
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5.  DNA breaks and chromatin structural changes enhance the transcription of autoimmune regulator target genes.

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Journal:  J Biol Chem       Date:  2017-02-27       Impact factor: 5.157

Review 6.  Update on Aire and thymic negative selection.

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Review 7.  AIRE expands: new roles in immune tolerance and beyond.

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Review 8.  Alopecia areata: Animal models illuminate autoimmune pathogenesis and novel immunotherapeutic strategies.

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Review 9.  Positive and negative selection of the T cell repertoire: what thymocytes see (and don't see).

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Review 10.  Generation of diversity in thymic epithelial cells.

Authors:  Yousuke Takahama; Izumi Ohigashi; Song Baik; Graham Anderson
Journal:  Nat Rev Immunol       Date:  2017-03-20       Impact factor: 53.106

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