Diverse Targets of the Transcription Factor STAT3 Contribute to T Cell Pathogenicity and Homeostasis

Durant, Lydia; Watford, Wendy T.; Ramos, Haydeé L.; Laurence, Arian; Vahedi, Golnaz; Wei, Lai; Takahashi, Hayato; Sun, Hongwei; Kanno, Yuka; Powrie, Fiona; O’Shea, John J.

doi:10.1016/j.immuni.2010.05.003

Cited by 601 publications

(596 citation statements)

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“…In the case of the Il17a and Rorc gene loci, STAT3 directly binds the promoter and also intergenic regions and induces alterations to the epigenetic signature of these genes. Consistent with these studies (37,38), loss of STAT3 resulted in the disappearance of IL-17A-producing cells (Fig. S5A).…”

Section: Menin Does Not Control the Expression Of Other Key Transcripsupporting

confidence: 88%

“…STAT3 directly regulates not only gene expression but also epigenetic modifications of numerous genes involved in Th17 cell differentiation (37,38). In the case of the Il17a and Rorc gene loci, STAT3 directly binds the promoter and also intergenic regions and induces alterations to the epigenetic signature of these genes.…”

Section: Menin Does Not Control the Expression Of Other Key Transcripmentioning

confidence: 99%

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Trithorax complex component Menin controls differentiation and maintenance of T helper 17 cells

Watanabe¹,

Onodera²,

Kanai³

et al. 2014

Proc. Natl. Acad. Sci. U.S.A.

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Epigenetic modifications, such as posttranslational modifications of histones, play an important role in gene expression and regulation. These modifications are in part mediated by the Trithorax group (TrxG) complex and the Polycomb group (PcG) complex, which activate and repress transcription, respectively. We herein investigate the role of Menin, a component of the TrxG complex in T helper (Th) cell differentiation and show a critical role for Menin in differentiation and maintenance of Th17 cells. Menin −/− T cells do not efficiently differentiate into Th17 cells, leaving Th1 and Th2 cell differentiation intact in in vitro cultures. Menin deficiency resulted in the attenuation of Th17-induced airway inflammation. In differentiating Th17 cells, Menin directly bound to the Il17a gene locus and was required for the deposition of permissive histone modifications and recruitment of the RNA polymerase II transcriptional complex. Interestingly, although Menin bound to the Rorc locus, Menin was dispensable for the induction of Rorc expression and permissive histone modifications in differentiating Th17 cells. In contrast, Menin was required to maintain expression of Rorc in differentiated Th17 cells, indicating that Menin is essential to stabilize expression of the Rorc gene. Thus, Menin orchestrates Th17 cell differentiation and function by regulating both the induction and maintenance of target gene expression.

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Section: Menin Does Not Control the Expression Of Other Key Transcripsupporting

confidence: 88%

Section: Menin Does Not Control the Expression Of Other Key Transcripmentioning

confidence: 99%

Trithorax complex component Menin controls differentiation and maintenance of T helper 17 cells

Watanabe¹,

Onodera²,

Kanai³

et al. 2014

Proc. Natl. Acad. Sci. U.S.A.

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show abstract

“…HIC1 has been shown to interact with and inhibit DNA binding of transcription factors such as T-cell factor-4, b-catenin, and STAT3. [38][39][40] As HIC1-deficient T H 17 cells produce heightened levels of the STAT3 target gene IL-17A, 41 we hypothesized that increased STAT3 activity was associated with HIC1 deficiency. We first examined the levels of IL-6-induced active phosphorylated STAT3 in HIC1-sufficient and -deficient T H 17 cells by flow cytometry.…”

Section: Hic1 Is Required To Limit Stat3 Signaling In T H 17 Cellsmentioning

confidence: 99%

“…Consistent with this hypothesis, we found increased STAT3 binding to the Il17a promoter in the absence of HIC1 (Figure 8d), whereas there was no difference in binding at an irrelevant site (Il5 promoter). Examination of mRNA expression for other known STAT3 target genes associated with TH17-cell differentiation 41 revealed slight but insignificant increases in gene expression of Rorc, Socs3, Irf4, Ahr, or Il23r (Figure 8e). Thus, HIC1 does not appear to directly regulate the molecular machinery that Our results suggest that the micronutrient RA regulates HIC1 expression in immune cells in the intestine.…”

Section: Hic1 Is Required To Limit Stat3 Signaling In T H 17 Cellsmentioning

confidence: 99%

“…54 Further, STAT3 was shown to be required to drive both colitis and systemic inflammation not only by modulating T H 17-cell differentiation but also by promoting T-cell activation and survival. 41 However, targeted therapies against IL-17A in Crohn's disease have been proven ineffective 55,56 and recent studies have shown that IL-17A is important for maintaining intestinal barrier integrity and has a protective role in regard to the development of colitis. 57,58 Further, it is becoming more apparent that the T H 17-cell lineage has a degree of heterogeneity with regards to pathogenicity.…”

Section: Hic1 Is Required To Limit Stat3 Signaling In T H 17 Cellsmentioning

confidence: 99%

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