Loss of Singleminded-2s in the Mouse Mammary Gland Induces an Epithelial-Mesenchymal Transition Associated with Up-Regulation of Slug and Matrix Metalloprotease 2

Laffin, Brian; Wellberg, Elizabeth A.; Kwak, Hyeong Il; Burghardt, Robert C.; Metz, Richard P.; Gustafson, Tanya L.; Schedin, Pepper; Porter, Weston W.

doi:10.1128/mcb.01701-07

Cited by 78 publications

(110 citation statements)

References 39 publications

(43 reference statements)

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“…In support of the former, loss of sINGLEMINdEd-2s in the mouse mammary gland induces sNAIL2-mediated EMT, indicating how gene inactivation may circumvent EMT dormancy in the adult mammary gland (219). In support of the latter, there is evidence for the heterogeneous expression and nuclear translocation of sNAIL (220) and sNAIL2 (221) following exposure to hypoxia at the invasive front, highlighting the importance of the microenvironment in providing extracellular signals for initiation of EMT at metastasis.…”

Section: Epithelial To Mesenchymal Transitionmentioning

confidence: 75%

Signalling pathways involved in endocrine resistance in breast cancer and associations with epithelial to mesenchymal transition (Review)

Saleh

Sharaf²,

Luqmani

2011

Int J Oncol

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Abstract. Both de novo and acquired endocrine resistance constitute a major therapeutic problem for treatment of hormone-positive breast cancer. Multiple explanatory mechanisms have been proposed through the study of cellular models which focus principally on receptor tyrosine kinase mediated signalling pathways utilizing sRC, PI3K, MAPK and sMAds. Many of the transducing molecules, particularly nuclear transcription factors such as sNAIL, TwIsT, sNAIL2, ZEB, FOXC2, TCF/LEF and GOOsECOId are participants in proliferation as well as invasion and metastasis, involving a process of orchestrated cellular remodeling which is being likened to the process of epithelial to mesenchymal transition that takes place during embryonic development. we review the accumulating evidence that points towards the occurrence of this phenomenon as a consequence of the loss of endocrine control, with both processes being similarly characterized by depletion of cell adhesion proteins, E-cadherin, catenins and cytokeratins, increased association with the extracellular matrix through induction of metalloproteinases, fibronectin and collagen, and a switch to a mobile vimentin-based cytoskeletal structure with loss of apical basal polarity. IntroductionEndocrine therapy represents the most effective form of treatment for the majority of breast cancer patients whose tumours over-express the estrogen receptor (ER). In addition to ablative procedures (ovariectomy) and administration of antiendocrine agents to inhibit ovarian function, treatment is reliant predominantly upon anti-hormonal agents termed selective estrogen modulators (sERMs). Until recent introduction of agents such as toremifene and raloxifene, tamoxifen has been the mainstay of treatment (1) inducing objective response or disease stabilization in over half of previously untreated metastatic breast cancer patients with ER + tumours (2). Further options include the use of pure anti-estrogens such as fulvestrant (Faslodex) which achieves its effects through receptor degradation, and application of aromatase inhibitors that reduce extra-gonadal peripheral estrogen synthesis from the adrenals and adipose tissue, including the breast. Both types of agents improve relapse-free survival and reduce incidence of contralateral breast cancers in women with early-stage cancer and increase overall survival in patients with advanced disease (3,4). Unfortunately, following initial response to sERMs and second line therapy with aromatase inhibitors, most patients subsequently develop resistance to both classes of drugs and become refractive to further attempts at endocrine manipulation. Added to the de novo resistance in patients whose tumours express levels of ER <10 fmol/mg protein, this presents a serious therapeutic problem, particularly in view of the increased aggressiveness of hormone insensitive breast cancers. Estrogen receptor actionThe classical mode of action of ER is related to the regulation of expression of genes with estrogen response elements (ERE) in their promoters through t...

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Section: Epithelial To Mesenchymal Transitionmentioning

confidence: 75%

Signalling pathways involved in endocrine resistance in breast cancer and associations with epithelial to mesenchymal transition (Review)

Saleh

Sharaf²,

Luqmani

2011

Int J Oncol

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“…Mechanistic roles for SIM2s and BNIP3 in cancer remain to be fully defined; however, deregulation of both factors are emerging as select solid tumour markers and are associated with poor prognostic outcomes (DeYoung et al, 2002;Halvorsen et al, 2007;Laffin et al, 2008;Burton and Gibson, 2009). As discussed previously, decreased BNIP3 levels and poor prognosis (Okami et al, 2004;Erkan et al, 2005;Mahon et al, 2007) clearly correlate with elevated SIM2s expression (DeYoung et al, 2002(DeYoung et al, , 2003b in pancreatic cancer.…”

Section: Sim2s Attenuates Hypoxic Induction Of Bnip3 Via Activities Wmentioning

confidence: 94%

“…Conversely, however, SIM2s has recently been found to be repressed in breast cancer tumours (Kwak et al, 2007). In contrast to the colon and pancreatic tumour-derived cell lines tested, loss of SIM2s in MCF-7 breast cancer cells correlates to cell survival through the activation of SLUG-mediated EMT (epithelial-mesenchymal transition) (Kwak et al, 2007;Laffin et al, 2008). Whether changes in SIM2s expression levels are required for tumour growth and/or tumour maintenance, and how SIM2s expression and transcriptional activities fit into the molecular profile of disease progression, is in need of further investigation.…”

Section: Introductionmentioning

confidence: 99%

“…Cell-based reporter gene assays have shown the murine long isoform to mediate repression of transcription via carboxy-terminal repression domains (Ema et al, 1996b;Moffett et al, 1997;Woods and Whitelaw, 2002). Recently, hSIM2s-mediated repression of the SLUG gene in breast cancer cells has been reported (Laffin et al, 2008). Another repressive mode of SIM2 is by sequestration of ARNT from other bHLH/PAS transcription factors, a mechanism by which SIM2 can interfere with the function of the hypoxia-inducible factor 1a (HIF1a) (Woods and Whitelaw, 2002).…”

Section: Introductionmentioning

confidence: 99%

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The HIF1α-inducible pro-cell death gene BNIP3 is a novel target of SIM2s repression through cross-talk on the hypoxia response element

Farrall

Whitelaw

2009

Oncogene

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The short isoform of single-minded 2 (SIM2s), a basic helix-loop-helix/PAS (bHLH/PAS) transcription factor, is upregulated in pancreatic and prostate tumours; however, a mechanistic role for SIM2s in these cancers is unknown. Microarray studies in prostate DU145 cells identified the pro-cell death gene, BNIP3 (Bcl-2/adenovirus E1B 19 kDa interacting protein 3), as a novel putative target of SIM2s repression. Further validation showed BNIP3 repression in several prostate and pancreatic carcinoma-derived cell lines with ectopic expression of human SIM2s. BNIP3 levels are enhanced in prostate carcinoma cells upon short interfering (si)RNA-mediated knockdown of endogenous SIM2s. Chromatin immunoprecipitation and promoter studies show that SIM2s represses BNIP3 through its activities at the proximal promoter hypoxia response element (HRE), the site through which the bHLH/PAS family member, hypoxia-inducible factor 1a (HIF1a), induces BNIP3. SIM2s attenuates BNIP3 hypoxic induction via the HRE, and increased hypoxic induction of BNIP3 occurs with siRNA knockdown of endogenous SIM2s in prostate PC3AR þ cells. BNIP3 is implicated in hypoxia-induced cell death processes. Prolonged treatment of PC3AR þ cells with hypoxia mimetics, DP and DMOG, confers hypoxia-induced autophagy, measured by enhanced LC3-II levels and SQSTM1/p62 turnover. We show that PC3AR þ cells expressing ectopic SIM2s have enhanced survival in these conditions. Induction of LC3-II and turnover of SQSTM1/p62 are attenuated in PC3AR þ / SIM2s DMOG and hypoxia-treated cells, suggesting that SIM2s may attenuate autophagic cell death processes, perhaps through BNIP3 repression. These data show, for the first time, SIM2s cross-talk on an endogenous HRE. SIM2s' functional interference with HIF1a activities on BNIP3 may indicate a novel role for SIM2s in promoting tumourigenesis.

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“…TGF can also phosphorylate certain cytoplasmic proteins regulating cell polarity and tight junction formation. These include RAS/MAPK (Xue et al, 2003), integrin -1 (Blanco et al, 2002), integrin-linked kinase (Hartwell et al, 2006), p38 MAPK (Mani et al, 2007), RHOA kinase (ROCK) (Moody et al, 2005), PI3K , JAGGED1/NOTCH (Come et al, 2006), SARA (Laffin et al, 2008), NFKB (Lester et al, 2007), PAR6 (Berx et al, 2001;Storci et al, 2008), pAR66A and ERK (Wu et al, 2009). Furthermore, EMT induced by the oncogenic stimulation by RAS and/or RAF activation in mammary, kidney and skin epithelial tissue was found to depend almost completely on TGF-signaling (Moustakas and Heldin, 2009).…”

Section: Transforming Growth Factor βmentioning

confidence: 99%

Endocrine Resistance and Epithelial Mesenchymal Transition in Breast Cancer

Saleh¹,

Luqmani²

2011

Breast Cancer - Focusing Tumor Microenvironment, Stem Cells and Metastasis

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Loss of Singleminded-2s in the Mouse Mammary Gland Induces an Epithelial-Mesenchymal Transition Associated with Up-Regulation of Slug and Matrix Metalloprotease 2

Cited by 78 publications

References 39 publications

Signalling pathways involved in endocrine resistance in breast cancer and associations with epithelial to mesenchymal transition (Review)

Signalling pathways involved in endocrine resistance in breast cancer and associations with epithelial to mesenchymal transition (Review)

The HIF1α-inducible pro-cell death gene BNIP3 is a novel target of SIM2s repression through cross-talk on the hypoxia response element

Endocrine Resistance and Epithelial Mesenchymal Transition in Breast Cancer

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