Are immunosenescent T cells really senescent?

Helena Slaets, Naomi Veeningen, Peter L.J. de Keizer, Niels Hellings*, Sven Hendrix

*Corresponding author for this work

Research output: Contribution to journalReview articlepeer-review

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Abstract

Loss of proper T-cell functioning is a feature of aging that increases the risk of developing chronic diseases. In aged individuals, highly differentiated T cells arise with a reduced expression of CD28 and CD27 and an increased expression of KLRG-1 or CD57. These cells are often referred to as immunosenescent T cells but may still be highly active and contribute to autoimmunity. Another population of T cells known as exhausted T cells arises after chronic antigen stimulation and loses its effector functions, leading to a failure to combat malignancies and viral infections. A process called cellular senescence also increases during aging, and targeting this process has proven to be fruitful against a range of age-related pathologies in animal models. Cellular senescence occurs in cells that are irreparably damaged, limiting their proliferation and typically leading to chronic secretion of pro-inflammatory factors. To develop therapies against pathologies caused by defective T-cell function, it is important to understand the differences and similarities between immunosenescence and cellular senescence. Here, we review the hallmarks of cellular senescence versus senescent and exhausted T cells and provide considerations for the development of specific therapies against age-related diseases.

Original languageEnglish
Article numbere14300
JournalAging Cell
Volume23
Issue number10
Early online date7 Aug 2024
DOIs
Publication statusPublished - Oct 2024

Keywords

  • exhaustion-T-lymphocytes
  • immunosenescence-aging
  • senescence
  • T-cells

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