Are immunosenescent T cells really senescent?

Author:

Slaets Helena12ORCID,Veeningen Naomi12,de Keizer Peter L. J.3ORCID,Hellings Niels12,Hendrix Sven4

Affiliation:

1. Neuro‐Immune Connections and Repair Lab, Department of Immunology and Infection Biomedical Research Institute, Hasselt University Diepenbeek Belgium

2. UMSC–University MS Center, Campus Diepenbeek Diepenbeek Belgium

3. Center for Molecular Medicine University Medical Center Utrecht Utrecht The Netherlands

4. Institute of Translational Medicine, Medical School Hamburg Hamburg Germany

Abstract

AbstractLoss 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.

Funder

Fonds Wetenschappelijk Onderzoek

Publisher

Wiley

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