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A landscape of X-inactivation during human T cell development

Author

Listed:
  • Björn Gylemo

    (Linköping University)

  • Maike Bensberg

    (Linköping University)

  • Viktoria Hennings

    (University of Gothenburg
    University of Gothenburg)

  • Christina Lundqvist

    (University of Gothenburg)

  • Alessandro Camponeschi

    (University of Gothenburg)

  • Dóra Goldmann

    (Linköping University)

  • Huan Zhang

    (Linköping University)

  • Aida Selimović-Pašić

    (Linköping University)

  • Antonio Lentini

    (Linköping University)

  • Olov Ekwall

    (University of Gothenburg
    University of Gothenburg)

  • Colm E. Nestor

    (Linköping University)

Abstract

Females exhibit a more robust immune response to both self-antigens and non-self-antigens than males, resulting in a higher prevalence of autoimmune diseases but more effective responses against infection. Increased expression of X-linked immune genes in female T cells is thought to underlie this enhanced response. Here we isolate thymocytes from pediatric thymi of healthy males (46, XY), females (46, XX), a female with completely skewed X-chromosome inactivation (46, XX, cXCI) and a female with Turner syndrome (45, X0). Using whole exome sequencing, RNA sequencing and DNA methylation data, we present a sex-aware expression profile of T cell development and generate a high-resolution map of escape from X-chromosome inactivation (XCI). Unexpectedly, XCI is transcriptionally and epigenetically stable throughout T cell development, and is independent of expression of XIST, the lncRNA responsible for XCI initiation during early embryonic development. In thymocytes, several genes known to escape XCI are expressed from only one X-chromosome. Additionally, we further reveal that a second X-chromosome is dispensable for T cell development. Our study thus provides a high-resolution map of XCI during human development and suggests a re-evaluation of XCI in sex differences in T cell function.

Suggested Citation

  • Björn Gylemo & Maike Bensberg & Viktoria Hennings & Christina Lundqvist & Alessandro Camponeschi & Dóra Goldmann & Huan Zhang & Aida Selimović-Pašić & Antonio Lentini & Olov Ekwall & Colm E. Nestor, 2024. "A landscape of X-inactivation during human T cell development," Nature Communications, Nature, vol. 15(1), pages 1-14, December.
  • Handle: RePEc:nat:natcom:v:15:y:2024:i:1:d:10.1038_s41467-024-54110-7
    DOI: 10.1038/s41467-024-54110-7
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    References listed on IDEAS

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    1. Takehiro Takahashi & Mallory K. Ellingson & Patrick Wong & Benjamin Israelow & Carolina Lucas & Jon Klein & Julio Silva & Tianyang Mao & Ji Eun Oh & Maria Tokuyama & Peiwen Lu & Arvind Venkataraman & , 2020. "Sex differences in immune responses that underlie COVID-19 disease outcomes," Nature, Nature, vol. 588(7837), pages 315-320, December.
    2. Taru Tukiainen & Alexandra-Chloé Villani & Angela Yen & Manuel A. Rivas & Jamie L. Marshall & Rahul Satija & Matt Aguirre & Laura Gauthier & Mark Fleharty & Andrew Kirby & Beryl B. Cummings & Stephane, 2017. "Landscape of X chromosome inactivation across human tissues," Nature, Nature, vol. 550(7675), pages 244-248, October.
    3. Antonio Lentini & Huaitao Cheng & J. C. Noble & Natali Papanicolaou & Christos Coucoravas & Nathanael Andrews & Qiaolin Deng & Martin Enge & Björn Reinius, 2022. "Elastic dosage compensation by X-chromosome upregulation," Nature Communications, Nature, vol. 13(1), pages 1-12, December.
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