The Potency of TCR Signaling Differentially Regulates NFATc/p Activity and Early IL-4 Transcription in Naive CD4 super(+) T Cells

The Potency of TCR Signaling Differentially Regulates NFATc/p Activity and Early IL-4 Transcription in Naive CD4 super(+) T Cells

The potency of TCR signaling can regulate the differentiation of naive CD4 super(+) T cells into Th1 and Th2 subsets. In this work we demonstrate that TCR signaling by low-affinity, but not high-affinity, peptide ligands selectively induces IL-4 transcription within 48 h of priming naive CD4 super(+...

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Veröffentlicht in:The Journal of immunology (1950) 2002-04, Vol.168 (8), p.3825-3832
Hauptverfasser: Brogdon, J L, Leitenberg, D, Bottomly, K
Format: Artikel
Sprache:eng
Schlagworte:
CD4 antigen
NF-ATc protein
NF-ATp protein
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Zusammenfassung:The potency of TCR signaling can regulate the differentiation of naive CD4 super(+) T cells into Th1 and Th2 subsets. In this work we demonstrate that TCR signaling by low-affinity, but not high-affinity, peptide ligands selectively induces IL-4 transcription within 48 h of priming naive CD4 super(+) T cells. This early IL-4 transcription is STAT6 independent and occurs before an increase in GATA-3. Furthermore, the strength of the TCR signal differentially affects the balance of NFATp and NFATc DNA binding activity, thereby regulating IL-4 transcription. Low-potency TCR signals result in high levels of nuclear NFATc and low levels of NFATp, which are permissive for IL-4 transcription. These data provide a model for how the strength of TCR signaling can influence the generation of Th1 and Th2 cells.
ISSN:0022-1767