IKKα controls canonical TGFβ–SMAD signaling to regulate genes expressing SNAIL and SLUG during EMT in Panc1 cells

Brandl, Martina; Seidler, Barbara; Haller, Ferdinand; Adamski, Jerzy; Schmid, Roland M.; Saur, Dieter; Schneider, Günter

doi:10.1242/jcs.071100

Cited by 115 publications

(66 citation statements)

References 51 publications

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“…HaCaT cells transition into a mesenchymal phenotype in response to TGF-β, with increased expression of Slug, a Snail-related transcription factor that drives EMT, dispersion of E-cadherin from junctions, decreased epithelial and increased mesenchymal gene expression, and changes in actin organization and cell shape (Lamouille and Derynck, 2007; Thuault et al, 2006). TGF-β-activated Smad3 directly controls Slug and several other EMT-regulated genes (Brandl et al, 2010; Xu et al, 2009). In contrast to many cell lines, HaCaT cells do not repress E-cadherin expression during EMT (data not shown).…”

Section: Resultsmentioning

confidence: 99%

Innate Antiviral Host Defense Attenuates TGF-β Function through IRF3-Mediated Suppression of Smad Signaling

Bailey-Bucktrout

et al. 2014

Molecular Cell

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Summary TGF-β signaling is essential in many processes, including immune surveillance, and its dysregulation controls various diseases, including cancer, fibrosis, and inflammation. Studying the innate host defense, which functions in most cell types, we found that RLR signaling represses TGF-β responses. This regulation is mediated by activated IRF3, using a dual mechanism of IRF3-directed suppression. Activated IRF3 interacts with Smad3, thus inhibiting TGF-β-induced Smad3 activation, and, in the nucleus, disrupts functional Smad3 transcription complexes by competing with co-regulators. Consequently, IRF3 activation by innate antiviral signaling represses TGF-β-induced growth inhibition, gene regulation and epithelial-mesenchymal transition, and the generation of Treg effector lymphocytes from naïve CD4+ lymphocytes. Conversely, silencing IRF3 expression enhances epithelial-mesenchymal transition, TGF-β-induced Treg cell differentiation upon virus infection, and Treg cell generation in vivo. We present a novel mode of regulation of TGF-β signaling by the antiviral defense, with evidence for its role in immune tolerance and cancer cell behavior.

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Section: Resultsmentioning

confidence: 99%

Innate Antiviral Host Defense Attenuates TGF-β Function through IRF3-Mediated Suppression of Smad Signaling

Bailey-Bucktrout

et al. 2014

Molecular Cell

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“…Furthermore, all of these pathways are necessary for promoting increased expression of the EndMT-inducing transcription factor Snail, which suppresses cell adhesion and promotes EndMT [13]. Smad proteins have been shown to bind directly to the promoter of the Snail gene to regulate its transcription [31–34]. Transcription factors induced by Smad-independent signaling that regulate Snail transcription remain unclear, but we show that these pathways have a critical role in controlling Snail gene expression.…”

Section: Discussionmentioning

confidence: 97%

Transforming growth factor-β2 promotes Snail-mediated endothelial–mesenchymal transition through convergence of Smad-dependent and Smad-independent signalling

Medici

Potenta

Kalluri

2011

Biochemical Journal

275

257

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SYNOPSIS Endothelial-mesenchymal transition (EndMT) is a critical process of cardiac development and disease progression. However, little is know about the signaling mechanisms that cause endothelial cells to transform into mesenchymal cells. Here we show that transforming growth factor-beta2 (TGF-β2) stimulates EndMT through Smad, MEK, PI3K, and p38 MAPK signaling pathways. Inhibitors of these pathways prevent TGF-β2-induced EndMT. Furthermore, we show that all of these pathways are essential for increasing expression of the cell adhesion suppressing transcription factor Snail. Inhibition of Snail with siRNA prevents TGF-β2-induced EndMT. However, over-expression of Snail is not sufficient to cause EndMT. Chemical inhibition of GSK-3β allows EndMT to be induced by Snail over-expression. Expression of a mutant Snail protein that is resistant to GSK-3β-dependent inactivation also promotes EndMT. These data provide the foundation for understanding the roles of specific signaling pathways in mediating EndMT.

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“…Whole cell lysates and nuclear extracts were prepared and western blots were carried out as described (9,24). A formaldehyde-based cross-linking protocol was used for immunoprecipitations as described by Klockenbusch and Kast (25).…”

Section: Methodsmentioning

confidence: 99%

“…Antibodies are shown in Supplementary Table S1. Avidin-Biotin-Complex DNA-(ABCD) assay was done as described (24). Sequences of the 5′ biotinylated oligonucleotides are listed in Supplementary Table S1.…”

Section: Methodsmentioning

confidence: 99%

MYC and EGR1 synergize to trigger tumor cell death by controlling NOXA and BIM transcription upon treatment with the proteasome inhibitor bortezomib

Wirth

Stojanović

Christian

et al. 2014

Nucleic Acids Research

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The c-MYC (MYC afterward) oncogene is well known for driving numerous oncogenic programs. However, MYC can also induce apoptosis and this function of MYC warrants further clarification. We report here that a clinically relevant proteasome inhibitor significantly increases MYC protein levels and that endogenous MYC is necessary for the induction of apoptosis. This kind of MYC-induced cell death is mediated by enhanced expression of the pro-apoptotic BCL2 family members NOXA and BIM. Quantitative promoter-scanning chromatin immunoprecipitations (qChIP) further revealed binding of MYC to the promoters of NOXA and BIM upon proteasome inhibition, correlating with increased transcription. Both promoters are further characterized by the presence of tri-methylated lysine 4 of histone H3, marking active chromatin. We provide evidence that in our apoptosis models cell death occurs independently of p53 or ARF. Furthermore, we demonstrate that recruitment of MYC to the NOXA as well as to the BIM gene promoters depends on MYC's interaction with the zinc finger transcription factor EGR1 and an EGR1-binding site in both promoters. Our study uncovers a novel molecular mechanism by showing that the functional cooperation of MYC with EGR1 is required for bortezomib-induced cell death. This observation may be important for novel therapeutic strategies engaging the inherent pro-death function of MYC.

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IKKα controls canonical TGFβ–SMAD signaling to regulate genes expressing SNAIL and SLUG during EMT in Panc1 cells

Cited by 115 publications

References 51 publications

Innate Antiviral Host Defense Attenuates TGF-β Function through IRF3-Mediated Suppression of Smad Signaling

Innate Antiviral Host Defense Attenuates TGF-β Function through IRF3-Mediated Suppression of Smad Signaling

Transforming growth factor-β2 promotes Snail-mediated endothelial–mesenchymal transition through convergence of Smad-dependent and Smad-independent signalling

MYC and EGR1 synergize to trigger tumor cell death by controlling NOXA and BIM transcription upon treatment with the proteasome inhibitor bortezomib

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