Epigenetic Thpok silencing limits the time window to choose CD4 super(+) helper-lineage fate in the thymus

CD4 super(+) helper and CD8 super(+) cytotoxic T cells differentiate from common precursors in the thymus after T-cell receptor (TCR)-mediated selection. Commitment to the helper lineage depends on persistent TCR signals and expression of the ThPOK transcription factor, whereas a ThPOK cis-regulator...

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Veröffentlicht in:The EMBO journal 2013-04, Vol.32 (8), p.1183-1194
Hauptverfasser: Tanaka, Hirokazu, Naito, Taku, Muroi, Sawako, Seo, Wooseok, Chihara, Risa, Miyamoto, Chizuko, Kominami, Ryo, Taniuchi, Ichiro
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Sprache:eng
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Zusammenfassung:CD4 super(+) helper and CD8 super(+) cytotoxic T cells differentiate from common precursors in the thymus after T-cell receptor (TCR)-mediated selection. Commitment to the helper lineage depends on persistent TCR signals and expression of the ThPOK transcription factor, whereas a ThPOK cis-regulatory element, ThPOK silencer, represses Thpok gene expression during commitment to the cytotoxic lineage. Here, we show that silencer-mediated alterations of chromatin structures in cytotoxic-lineage thymocytes establish a repressive state that is epigenetically inherited in peripheral CD8 super(+) T cells even after removal of the silencer. When silencer activity is enhanced in helper-lineage cells, by increasing its copy number, a similar heritable Thpok silencing occurs. Epigenetic locking of the Thpok locus may therefore be an independent event from commitment to the cytotoxic lineage. These findings imply that long-lasting TCR signals are needed to establish stable Thpok expression activity to commit to helper T-cell fate and that full commitment to the helper lineage requires persistent reversal of silencer activity during a particular time window.
ISSN:0261-4189
DOI:10.1038/emboj.2013.47