Abstract

Abstract In studies of immune aging, naive T cells frequently take center stage. Describing the complexity of the human naive T cell repertoire remains a daunting task; however, emerging data suggest that homeostatic mechanisms are robust enough to maintain a large and diverse CD4 T cell repertoire with age. Compartment shrinkage and clonal expansions are challenges for naive CD8 T cells. In addition to population aspects, identification of potentially targetable cellular defects is receiving renewed interest. The last decade has seen remarkable progress in identifying genetic and biochemical pathways that are pertinent for aging in general and that are instructive to understand naive T cell dysfunction. One hallmark sets naive T cell aging apart from most other tissues except stem cells: they initiate but do not complete differentiation programs toward memory cells. Maintaining quiescence and avoiding differentiation may be the ultimate challenge to maintain the functions unique for naive T cells.

Keywords

BiologyRepertoireNaive T cellPopulationT cellCD8Stem cellImmune systemCompartment (ship)ImmunologyNeuroscienceCell biologyT-cell receptorMedicineHistory

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Publication Info

Year
2015
Type
review
Volume
194
Issue
9
Pages
4073-4080
Citations
351
Access
Closed

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Jörg J. Goronzy, Fengqin Fang, Mary Cavanagh et al. (2015). Naive T Cell Maintenance and Function in Human Aging. The Journal of Immunology , 194 (9) , 4073-4080. https://doi.org/10.4049/jimmunol.1500046

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DOI
10.4049/jimmunol.1500046