Differential IL-2 expression defines developmental fates of follicular versus nonfollicular helper T cells

In response to infection, naïve CD4 T cells differentiate into two subpopulations: T follicular helper (T ) cells, which support B cell antibody production, and non-T cells, which enhance innate immune cell functions. Interleukin-2 (IL-2), the major cytokine produced by naïve T cells, plays an impor...

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Veröffentlicht in:Science (American Association for the Advancement of Science) 2018-09, Vol.361 (6407)
Hauptverfasser: DiToro, Daniel, Winstead, Colleen J, Pham, Duy, Witte, Steven, Andargachew, Rakieb, Singer, Jeffrey R, Wilson, C Garrett, Zindl, Carlene L, Luther, Rita J, Silberger, Daniel J, Weaver, Benjamin T, Kolawole, E Motunrayo, Martinez, Ryan J, Turner, Henrietta, Hatton, Robin D, Moon, James J, Way, Sing Sing, Evavold, Brian D, Weaver, Casey T
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Sprache:eng
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Zusammenfassung:In response to infection, naïve CD4 T cells differentiate into two subpopulations: T follicular helper (T ) cells, which support B cell antibody production, and non-T cells, which enhance innate immune cell functions. Interleukin-2 (IL-2), the major cytokine produced by naïve T cells, plays an important role in the developmental divergence of these populations. However, the relationship between IL-2 production and fate determination remains unclear. Using reporter mice, we found that differential production of IL-2 by naïve CD4 T cells defined precursors fated for different immune functions. IL-2 producers, which were fated to become T cells, delivered IL-2 to nonproducers destined to become non-T cells. Because IL-2 production was limited to cells receiving the strongest T cell receptor (TCR) signals, a direct link between TCR-signal strength, IL-2 production, and T cell fate determination has been established.
ISSN:0036-8075
1095-9203
DOI:10.1126/science.aao2933