Characterisation of the dual roles of senescent-like T cells that arise during healthy and unhealthy ageing

  1. Conor Garrod-Ketchely
  2. Lauren A Callender
  3. Johannes Schroth
  4. Katie Littlewood
  5. Elizabeth C Carroll
  6. Dina Tamsan
  7. Victoria SK Tsang
  8. Isabell Nessel
  9. Natalie E Riddell
  10. Benny Chain
  11. Daniel Harding
  12. Federica M Marelli-Berg
  13. Jonas Bystrom
  14. Melissa Pereira Da Costa
  15. Amaia Carrascal-Miniño
  16. George P Keeling
  17. Truc T Pham
  18. Kavitha Sunassee
  19. Rafael TM de Rosales
  20. Samantha YA Terry
  21. Melanie Pattrick
  22. Caroline Sutcliffe
  23. Anne Worthington
  24. Gill Hood
  25. Sarah Finer
  26. Sian M Henson
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Abstract

Ageing is associated with significant immune changes, with unhealthy ageing characterised by chronic inflammation and immune dysregulation. Here we identify a population of CD8⁺ TEMRAcells during unhealthy ageing, which exhibit features of premature senescence and are regulated in part by TGFβ. These cells show impaired cytotoxic function and altered migratory behaviour, including an increased presence in tissues. TGFβ plays a pivotal role in modulating their phenotype by inducing CD103 expression and downregulating KLRG1, causing these cells to resemble tissue-resident memory cells. This disruption to receptor recycling leads to defective degranulation potentially altering the capacity of these cells to mount an effective immune response. Overall, these findings suggest that TEMRAcells in the context of unhealthy ageing are a pathogenic T cell subset that accumulate in tissues where they are unable to exert an effector function.

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