Eos Mediates Foxp3-Dependent Gene Silencing in CD4
            <sup>+</sup>
            Regulatory T Cells

Fan, Ping; Yu, Hong‐Ren; Dang, Eric V.; Barbi, Joseph; Pan, Xiaoyu; Grosso, Joseph F.; Jinasena, Dinili; Sharma, Sudarshana M.; McCadden, Erin; Getnet, Derese; Drake, Charles G.; Liu, Jun O.; Ostrowski, Michael C.; Pardoll, Drew M.

doi:10.1126/science.1176077

Cited by 304 publications

(317 citation statements)

References 32 publications

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“…Recently, Pardoll and colleagues (Pan et al, 2009) demonstrated that FOXP3-dependent gene silencing involved in downregulation of IL-2 and IFNg in mouse Treg is related to FOXP3 interaction with Eos, a zincfinger transcription factor of the Ikaros family. Direct interaction of Eos and FOXP3 induces epigenetic chromatin modifications that result in gene silencing in Treg.…”

Section: Foxp3 Controls Gene Expression In Tregmentioning

confidence: 99%

Human FOXP3 and cancer

et al. 2010

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FOXP3 is a transcription factor necessary and sufficient for induction of the immunosuppressive functions in regulatory T lymphocytes. Its expression was first considered as specific of this cell type, but FOXP3 can also be transiently expressed in T-cell antigen receptoractivated human nonregulatory T cells. Recent data indicate that FOXP3 is also expressed by some nonlymphoid cells, in which it can repress various oncogenes that are restored following FOXP3 deletion or mutation. This review summarizes major advances in (1) the understanding of Foxp3 functions in human regulatory T cells, (2) the prognostic significance of Foxp3-expressing T cells in human malignancies and (3) the significance of Foxp3 expression in human tumor cells.

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Section: Foxp3 Controls Gene Expression In Tregmentioning

confidence: 99%

Human FOXP3 and cancer

et al. 2010

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“…The mechanism by which Eos is involved in Foxp3-dependent gene silencing may be through its corepressors such as C-terminal binding protein 1, which affects histone modification and promoter methylation involved in selective gene silencing. 168 Finally, FOXP3 has also been found to directly interact with c-Rel through its N-terminal region to repress the NF-kB pathway in mature Treg cells. 169 It is highly likely that FOXP3 has many other binding partners.…”

Section: Dynamic Regulation Of the Foxp3 Complexmentioning

confidence: 99%

“…The knockdown of Eos reverses Foxp3-mediated suppression of IL-2 expression, but has little effect on CD25, CTLA-4 and GITR expression. 168 Therefore, Eos is necessary for gene silencing but not for the expression of Foxp3-activated genes. The mechanism by which Eos is involved in Foxp3-dependent gene silencing may be through its corepressors such as C-terminal binding protein 1, which affects histone modification and promoter methylation involved in selective gene silencing.…”

Section: Dynamic Regulation Of the Foxp3 Complexmentioning

confidence: 99%

“…Eos is a zinc-finger transcription factor that belongs to the Ikaros family, and a recently identified functional component of the Foxp3 complex that acts specifically to promote Foxp3-mediated target gene repression. 168 Eos is highly expressed in Treg cells, especially in activated Treg cells (CD4 þ CD25 hi CD62L lo ) and can bind to the proline-rich domain of Foxp3. The knockdown of Eos reverses Foxp3-mediated suppression of IL-2 expression, but has little effect on CD25, CTLA-4 and GITR expression.…”

Section: Dynamic Regulation Of the Foxp3 Complexmentioning

confidence: 99%

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Molecular mechanisms underlying the regulation and functional plasticity of FOXP3+ regulatory T cells

et al. 2011

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CD4þ CD25 þ regulatory T (Treg) cells engage in the maintenance of immunological self-tolerance and homeostasis by limiting aberrant or excessive inflammation. The transcription factor forkhead box P3 (FOXP3) is critical for the development and function of Treg cells. The differentiation of the Treg cell lineage is not terminal, as developmental and functional plasticity occur through the sensing of inflammatory signals in the periphery. Here, we review the recent progress in our understanding of the molecular mechanisms underlying the regulation and functional plasticity of CD4 þ CD25 þ FOXP3 þ Treg cells, through the perturbation of FOXP3 and its complex at a transcriptional, translational and post-translational level.

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“…It also revealed a number of other transcriptional regulators of the Treg signature, including Eos, Helios, Lef1 and GATA-1, some were shown previously to be associated with Treg cell function. 5,6 The actual contributions of four transcription factors, Eos, GATA-1, Xbp1 and Helios, were then verified by direct expression profiling of Treg cells from the knockout mice of these genes. Surprisingly, the Treg signatures in each of these mutated mice were not altered significantly compared to wild-type cells.…”

Section: 2mentioning

confidence: 99%

One way to pathogenesis, many ways to homeostasis

Wang

2012

Cell Mol Immunol

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Eos Mediates Foxp3-Dependent Gene Silencing in CD4 ⁺ Regulatory T Cells

Cited by 304 publications

References 32 publications

Human FOXP3 and cancer

Human FOXP3 and cancer

Molecular mechanisms underlying the regulation and functional plasticity of FOXP3+ regulatory T cells

One way to pathogenesis, many ways to homeostasis

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Eos Mediates Foxp3-Dependent Gene Silencing in CD4 + Regulatory T Cells

Cited by 304 publications

References 32 publications

Human FOXP3 and cancer

Human FOXP3 and cancer

Molecular mechanisms underlying the regulation and functional plasticity of FOXP3+ regulatory T cells

One way to pathogenesis, many ways to homeostasis

Contact Info

Product

Resources

About

Eos Mediates Foxp3-Dependent Gene Silencing in CD4 ⁺ Regulatory T Cells