Smad3 Is a Key Nonredundant Mediator of Transforming Growth Factor β Signaling in Nme Mouse Mammary Epithelial Cells

Dzwonek, Joanna; Preobrazhenska, Olena; Cazzola, Silvia; Conidi, Andrea; Schellens, Ann; Dinther, Maarten van; Stubbs, Andrew; Klippel, Anke; Huylebroeck, Danny; Dijke, Peter ten; Verschueren, Kristin

doi:10.1158/1541-7786.mcr-08-0558

Cited by 28 publications

(29 citation statements)

References 38 publications

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“…Furthermore, in vitro studies have shown that Smad2 and Smad3 have unique functions in mammary epithelium and oncogenesis, in which Smad3 and not Smad2 is critical to inducing TGFβ-mediated apoptosis, cell cycle arrest and EMT. 18,19 …”

Section: Tgfβ and Smad Signalingmentioning

confidence: 99%

“…As stated, TGFβ can stimulate tumor progression and metastasis by inducing EMT 72,73 in a process that is Smad3-dependent. 19 During EMT, cells lose their epithelial characteristics, including cell adhesion and polarity, and acquire a mesenchymal morphology and the ability to migrate. During this process, cells downregulate the expression of epithelial markers and upregulate the expression of mesenchymal markers.…”

Section: Role Of Smad3 In Pro-metastatic Eventsmentioning

confidence: 99%

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Phospho-specific Smad3 signaling

Tarasewicz

Jeruss²

2012

Cell Cycle

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Section: Tgfβ and Smad Signalingmentioning

confidence: 99%

Section: Role Of Smad3 In Pro-metastatic Eventsmentioning

confidence: 99%

Phospho-specific Smad3 signaling

Tarasewicz

Jeruss²

2012

Cell Cycle

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“…In the 4T1 and the MDA-MB-231 tumor models, systemic administration of a soluble TbRII protein or dominant negative TbRII overexpression, respectively, displayed anti-metastatic effects (Yin et al, 1999;Muraoka et al, 2002). Several studies have provided evidence that Smad2 and Smad3 have different transcriptional functions and profiling studies have revealed distinct target genes for Smad2 and Smad3 (Kretschmer et al, 2003;LaGamba et al, 2005;Dzwonek et al, 2009). In addition, although mice deficient in Smad2 are embryonic lethal, Smad3-deficient mice are viable (Weinstein et al, 1998;Ashcroft et al, 1999;Yang et al, 1999).…”

Section: Introductionmentioning

confidence: 99%

Smad2 and Smad3 have opposing roles in breast cancer bone metastasis by differentially affecting tumor angiogenesis

et al. 2009

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Transforming growth factor (TGF)-b can suppress and promote breast cancer progression. How TGF-b elicits these dichotomous functions and which roles the principle intracellular effector proteins Smad2 and Smad3 have therein, is unclear. Here, we investigated the specific functions of Smad2 and Smad3 in TGF-b-induced responses in breast cancer cells in vitro and in a mouse model for breast cancer metastasis. We stably knocked down Smad2 or Smad3 expression in MDA-MB-231 breast cancer cells. The TGF-b-induced Smad3-mediated transcriptional response was mitigated and enhanced by Smad3 and Smad2 knockdown, respectively. This response was also seen for TGF-b-induced vascular endothelial growth factor (VEGF) expression. TGF-b induction of key target genes involved in bone metastasis, were found to be dependent on Smad3 but not Smad2. Strikingly, whereas knockdown of Smad3 in MDA-MB-231 resulted in prolonged latency and delayed growth of bone metastasis, Smad2 knockdown resulted in a more aggressive phenotype compared with control MDA-MB-231 cells. Consistent with differential effects of Smad knockdown on TGF-b-induced VEGF expression, these opposing effects of Smad2 versus Smad3 could be directly correlated with divergence in the regulation of tumor angiogenesis in vivo. Thus, Smad2 and Smad3 differentially affect breast cancer bone metastasis formation in vivo.

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“…The procedure was performed in hippocampal or cortical extracts from rats that were sacrificed on E18 or P3-P60, or extracts from cell cultures as described previously (Dzwonek et al, 2009). The following antibodies were used: sheep anti-CD44 (R&D Systems), rabbit anti-GFP (MBL International), chicken anti-b-galactosidase (Abcam), mouse anti-GAPDH (Millipore) and anti-Src (Cell Signaling).…”

Section: Western Blottingmentioning

confidence: 99%

CD44 regulates dendrite morphogenesis through Src tyrosine kinase-dependent positioning of the Golgi

Skupien¹,

Konopka²,

Trzaskoma³

et al. 2014

Development

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The acquisition of proper dendrite morphology is a crucial aspect of neuronal development towards the formation of a functional network. The role of the extracellular matrix and its cellular receptors in this process has remained enigmatic. We report that the CD44 adhesion molecule, the main hyaluronan receptor, is localized in dendrites and plays a crucial inhibitory role in dendritic tree arborization in vitro and in vivo. This novel function is exerted by the activation of Src tyrosine kinase, leading to the alteration of Golgi morphology. The mechanism operates during normal brain development, but its inhibition might have a protective influence on dendritic trees under toxic conditions, during which the silencing of CD44 expression prevents dendritic shortening induced by glutamate exposure. Overall, our results indicate a novel role for CD44 as an essential regulator of dendritic arbor complexity in both health and disease.

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Smad3 Is a Key Nonredundant Mediator of Transforming Growth Factor β Signaling in Nme Mouse Mammary Epithelial Cells

Cited by 28 publications

References 38 publications

Phospho-specific Smad3 signaling

Phospho-specific Smad3 signaling

Smad2 and Smad3 have opposing roles in breast cancer bone metastasis by differentially affecting tumor angiogenesis

CD44 regulates dendrite morphogenesis through Src tyrosine kinase-dependent positioning of the Golgi

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