A ThPOK-LRF transcriptional node maintains the integrity and effector potential of post-thymic CD4+ T cells

ThPOK-LRF转录节点维持胸腺后CD4+T细胞的完整性和效应潜能

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作者:Melanie S Vacchio, Lie Wang, Nicolas Bouladoux, Andrea C Carpenter, Yumei Xiong, Linus C Williams, Elizabeth Wohlfert, Ki-Duk Song, Yasmine Belkaid, Paul E Love, Rémy Bosselut

Abstract

The transcription factor ThPOK promotes CD4(+) T cell differentiation in the thymus. Here, using a mouse strain that allows post-thymic gene deletion, we show that ThPOK maintains CD4(+) T lineage integrity and couples effector differentiation to environmental cues after antigenic stimulation. ThPOK preserved the integrity and amplitude of effector responses and was required for proper differentiation of types 1 and 2 helper T cells in vivo by restraining the expression and function of Runx3, a nuclear factor crucial for cytotoxic T cell differentiation. The transcription factor LRF acts redundantly with ThPOK to prevent the transdifferentiation of mature CD4(+) T cells into CD8(+) T cells. As such, the ThPOK-LRF transcriptional module was essential for CD4(+) T cell integrity and responses.

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