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Interleukin 2 modulates thymic-derived regulatory T cell epigenetic landscape.


ABSTRACT: Foxp3+CD4+ regulatory T (Treg) cells are essential for preventing fatal autoimmunity and safeguard immune homeostasis in vivo. While expression of the transcription factor Foxp3 and IL-2 signals are both required for the development and function of Treg cells, the commitment to the Treg cell lineage occurs during thymic selection upon T cell receptor (TCR) triggering, and precedes the expression of Foxp3. Whether signals beside TCR contribute to establish Treg cell epigenetic and functional identity is still unknown. Here, using a mouse model with reduced IL-2 signaling, we show that IL-2 regulates the positioning of the pioneer factor SATB1 in CD4+ thymocytes and controls genome wide chromatin accessibility of thymic-derived Treg cells. We also show that Treg cells receiving only low IL-2 signals can suppress endogenous but not WT autoreactive T cell responses in vitro and in vivo. Our findings have broad implications for potential therapeutic strategies to reprogram Treg cells in vivo.

SUBMITTER: Chorro L 

PROVIDER: S-EPMC6299086 | biostudies-literature | 2018 Dec

REPOSITORIES: biostudies-literature

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Interleukin 2 modulates thymic-derived regulatory T cell epigenetic landscape.

Chorro Laurent L   Suzuki Masako M   Chin Shu Shien SS   Williams Tere M TM   Snapp Erik L EL   Odagiu Livia L   Labrecque Nathalie N   Lauvau Grégoire G  

Nature communications 20181218 1


Foxp3<sup>+</sup>CD4<sup>+</sup> regulatory T (T<sub>reg</sub>) cells are essential for preventing fatal autoimmunity and safeguard immune homeostasis in vivo. While expression of the transcription factor Foxp3 and IL-2 signals are both required for the development and function of T<sub>reg</sub> cells, the commitment to the T<sub>reg</sub> cell lineage occurs during thymic selection upon T cell receptor (TCR) triggering, and precedes the expression of Foxp3. Whether signals beside TCR contribut  ...[more]

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