The Th17 immune response is controlled by the Rel–RORγ

Artigo Acesso aberto Revisado por pares

The Th17 immune response is controlled by the Rel–RORγ–RORγT transcriptional axis

2011; Rockefeller University Press; Volume: 208; Issue: 11 Linguagem: Inglês

10.1084/jem.20110462

ISSN

1540-9538

Autores

Qingguo Ruan, Vasumathi Kameswaran, Yan Zhang, Shijun J. Zheng, Jing Sun, Junmei Wang, Jennifer DeVirgiliis, Hsiou‐Chi Liou, Amer A. Beg, Youhai H. Chen,

Tópico(s)

Retinoids in leukemia and cellular processes

Resumo

The Th17 cells use the retinoid-related orphan receptor-γ (Rorg or Rorc) to specify their differentiation and lineage-specific function. However, how Rorg is switched on during Th17 differentiation is unknown. We report here that c-Rel and RelA/p65 transcription factors drive Th17 differentiation by binding to and activating two distinct Rorg promoters that control RORγT and RORγ expression, respectively. Similar to RORγT, RORγ is selectively expressed in Th17 cells and is effective in specifying the Th17 phenotype. T cells deficient in c-Rel or RelA are significantly compromised in Th17 differentiation, and c-Rel–deficient mice are defective in Th17 responses. Thus, Th17 immunity is controlled by a Rel–RORγ–RORγT axis, and strategies targeting Rel/NF-κB can be effective for controlling Th17 cell–mediated diseases.

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The Th17 immune response is controlled by the Rel–RORγ–RORγT transcriptional axis