Inflammation directs memory precursor and short-lived effector CD8+ T cell fates via the graded expression of T-bet transcription factor
As acute infections resolve, effector CD8(+) T cells differentiate into interleukin-7 receptor(lo) (IL-7R(lo)) short-lived effector cells (SLECs) and IL-7R(hi) memory precursor effector cells (MPECs) capable of generating long-lived memory CD8(+) T cells. By using another SLEC marker, KLRG1, we found that KLRG1(hi) effector cells began appearing early during infection and were committed to downregulating IL-7R. Unlike IL-7R(hi) MPECs, KLRG1(hi) IL-7R(lo) SLECs relied on IL-15, but I L-15 could not sustain their long-term maintenance or homeostatic turnover. The decision between SLEC and MPEC fates was regulated by the amount of inflammatory cytokines (i.e., IL-12) present during T cell priming. According to the amount of inflammation, a gradient of T-bet was created in which high T-bet expression induced SLECs and low expression promoted MPECs. These results elucidate a mechanism by which the innate immune system sets the relative amounts of a lineage-determining transcription factor in activated CD8(+) T cells and, correspondingly, regulates their memory cell potential.
- Publisher
- CELL PRESS
- Issue Date
- 2007-08
- Language
- English
- Article Type
- Article
- Keywords
CUTTING EDGE; SELECTIVE EXPRESSION; PROTECTIVE IMMUNITY; VIRAL-INFECTIONS; IL-7 RECEPTOR; IN-VIVO; ANTIGEN; RESPONSES; DIFFERENTIATION; HOMEOSTASIS
- Citation
IMMUNITY, v.27, no.2, pp.281 - 295
- ISSN
- 1074-7613
- Appears in Collection
- MSE-Journal Papers(저널논문)
- Files in This Item
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