A Critical Role for Transcription Factor Smad4 in T Cell Function that Is Independent of Transforming Growth Factor β Receptor Signaling

Gu, Ai Di; Zhang, Song; Wang, Yunqi; Xiong, Hui; Curtis, Thomas A.; Wan, Yisong Y.

doi:10.1016/j.immuni.2014.12.019

Cited by 43 publications

(45 citation statements)

References 47 publications

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“…Cre + Smad2-fl/fl Smad3-fl/fl mice were always used before 6 wk of age, a time point at which in our hands mice exhibited no signs of disease. No such disease was ever noted in mice with Smad4 deleted in T cells, consistent with previous reports (22,23). Mice of both sexes were used throughout these experiments, and no differences between sexes were noted.…”

Section: Micesupporting

confidence: 89%

Functions of Smad Transcription Factors in TGF-β1–Induced Selectin Ligand Expression on Murine CD4 Th Cells

Ebel

Kansas

2016

The Journal of Immunology

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Selectins are carbohydrate-binding adhesion molecules that control leukocyte traffic. Induction of selectin ligands on T cells is controlled primarily by cytokines, including TGF-β1, and requires p38α MAPK, but transcriptional mechanisms that underlie cytokine-driven selectin ligand expression are poorly understood. In this study, we show, using mice with conditional deletions of the TGF-β1–responsive transcription factors Smad2, Smad3, or Smad4, that induction of selectin ligands on CD4 cells in response to TGF-β1 requires Smad4 plus either Smad2 or Smad3. Analysis of CD4 cells from mice with only one functional Smad4 allele revealed a sharp gene dosage effect, suggesting the existence of a threshold of TGF-β1 signal strength required for selectin ligand induction. Both Smad4 plus either Smad2 or Smad3 were selectively required for induction of Fut7 and Gcnt1, glycosyltransferases critical for selectin ligand biosynthesis, but they were not required for St3gal4 or St3gal6 induction. Smad4 plus either Smad2 or Smad3 were also required for induction of Runx transcription factors by TGF-β1. Enforced expression of Runx2, but not Runx1 or Runx3, in Smad2/Smad3 doubly deficient CD4 cells restored selectin ligand expression to wild-type levels. In contrast, enforced expression of Runx1, Runx2, or Runx3 failed to restore differentiation of TGF-β1–dependent Th cell lineages, including Th17, Th9, and induced regulatory T cells. These results show that Smads are directly required for Th cell differentiation independent of Runx induction but only indirectly required via Runx2 for TGF-β1–induced selectin ligand induction on murine CD4 T cells.

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Section: Micesupporting

confidence: 89%

Functions of Smad Transcription Factors in TGF-β1–Induced Selectin Ligand Expression on Murine CD4 Th Cells

Ebel

Kansas

2016

The Journal of Immunology

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“…Moreover, absence of TGF-β signaling did not greatly impact antiviral cytokine secretion by D b :GP 33-41 LCMV-specific CD8 T cells upon cognate peptide stimulation (Supplemental Figure 1D). We also found that TGF-β signaling only minimally suppressed the effector markers KLRG and Ly6C on virus-specific CD8 T cells, or granzyme B on IFN-γ-producing cells, after GP [33][34][35][36][37][38][39][40][41] peptide stimulation (Supplemental Figure 1, E-G). Overall, these data show that deletion of Tgfbr2 prior to infection only minimally affected CD8 T cell antiviral responses early after chronic LCMV infection.…”

Section: Cellmentioning

confidence: 74%

“…A recent study demonstrated that CD4 T cellspecific deletion of SMAD4 during development using Cd4-Cre mice reduces accumulation of activated CD4 and CD8 T cells due to reduced c-myc induction and compromises transgenic OT-II CD4 T cell-based B16-OVA melanoma rejection (35). In addition, KLRG + effector CD8 T cell differentiation, but not cell numbers, was defective in SMAD4-deficient OT-1 transgenic T cells after lung influenza-OVA infection (58).…”

Section: Cd49dmentioning

confidence: 99%

TGF-β receptor maintains CD4 T helper cell identity during chronic viral infections

Lewis¹,

Wehrens²,

Labarta-Bajo³

et al. 2016

Journal of Clinical Investigation

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“…As a pleiotropic cytokine, TGF-β regulates various immune cell types including natural killer cells, myeloid cells, CD4+ and CD8+ T cells, promotes generation of T-regulatory cells. These properties are essential for the maintenance of tissue homeostasis and self-tolerance, but are also involved in tumor immune evasion mechanisms [13]. Surgical trauma, pain and blood loss were shown to induce the increase of systemic levels of TGF-β [8].…”

Section: Resultsmentioning

confidence: 99%

The effect of perioperative analgesic drugs omnopon and dexketoprofen on the functional activity of immune cells in murine model of tumor surgery

Sydor¹,

Khranovska²,

Skachkova³

et al. 2016

Ukr.Biochem.J.

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A Critical Role for Transcription Factor Smad4 in T Cell Function that Is Independent of Transforming Growth Factor β Receptor Signaling

Cited by 43 publications

References 47 publications

Functions of Smad Transcription Factors in TGF-β1–Induced Selectin Ligand Expression on Murine CD4 Th Cells

Functions of Smad Transcription Factors in TGF-β1–Induced Selectin Ligand Expression on Murine CD4 Th Cells

TGF-β receptor maintains CD4 T helper cell identity during chronic viral infections

The effect of perioperative analgesic drugs omnopon and dexketoprofen on the functional activity of immune cells in murine model of tumor surgery

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