Abstract
Insight into the maintenance of naive T cells is essential to understand defective immune responses in the context of aging and other immune compromised states. In humans, naive CD4+ T cells, in contrast to CD8+ T cells, are remarkably well retained with aging. Here, we show that low-affinity TCR engagement is the main driving force behind the emergence and accumulation of naive-like CD4+ T cells with enhanced sensitivity to IL-2 in aged humans. In vitro, we show that these CD45RA(+)CD25(dim)CD4(+) T cells can develop from conventional naive CD25(-)CD4+ T cells upon CD3 cross-linking alone, in the absence of costimulation, rather than via stimulation by the homeostatic cytokines IL-2, IL-7, or IL-15. In vivo, TCR engagement likely occurs in secondary lymphoid organs as these cells were detected in lymph nodes and spleen where they showed signs of recent activation. CD45RA(+)CD25(dim)CD4+ T cells expressed a broad TCRV repertoire and could readily differentiate into functional T helper cells. Strikingly, no expansion of CD45RA(+)CD25(dim)CD8+ T cells was detected with aging, thereby implying that maintenance of naive CD4+ T cells is uniquely regulated. Our data provide novel insight into the homeostasis of naive T cells and may guide the development of therapies to preserve or restore immunity in the elderly.
Original language | English |
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Pages (from-to) | 744-753 |
Number of pages | 10 |
Journal | Aging Cell |
Volume | 14 |
Issue number | 5 |
DOIs | |
Publication status | Published - Oct-2015 |
Keywords
- aging
- homeostasis
- interleukin-2
- interleukin-7
- TCR engagement
- T lymphocytes
- CD4(+) T-CELLS
- IN-VIVO
- HIV-INFECTION
- REPERTOIRE DIVERSITY
- LYMPHOID ORGANS
- HELPER-CELLS
- OLD-AGE
- MEMORY
- EXPRESSION
- PROLIFERATION