Downregulation of Sef, an inhibitor of receptor tyrosine kinase signaling, is common to a variety of human carcinomas

Zisman‐Rozen, Simona; Fink, Dorit; Ben‐Izhak, Ofer; Fuchs, Yaron; Brodski, A.; Kraus, Manfred; Bejar, Jacob; Ron, Dina

doi:10.1038/sj.onc.1210424

Cited by 41 publications

(56 citation statements)

References 21 publications

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“…The loss of hSef, therefore, is not in itself an oncogenic event but has an important permissive role in enhancing growth factor stimulation in prostate cancer. This hypothesis is supported by others who have similarly found that the loss of hSef can augment receptor tyrosine kinase signalling in cancer cells (Zisman-Rozen et al, 2007).…”

Section: Discussionsupporting

confidence: 75%

“…hSef has been reported to interact with both nerve growth factor (NGF) and epidermal growth factor (EGF) signalling (Xiong et al, 2003;Torii et al, 2004;Ziv et al, 2006). Silencing of hSef has further been shown to accelerate EGF-stimulated proliferation of cervical carcinoma cells in vitro (Zisman-Rozen et al, 2007). More recently, Ren et al (2008) reported evidence that hSef interacts and co-localises with the EGF receptor.…”

Section: Discussionmentioning

confidence: 98%

“…These act as feedback inhibitory checkpoints at key steps in the intracellular signalling cascade (Thisse and Thisse, 2005;Mason et al, 2006;Bundschu et al, 2007). The role of these regulators in malignancies has attracted much attention with reports of loss of expression in different tumour types (McKie et al, 2005;Fong et al, 2006;Yoshida et al, 2006;Zisman-Rozen et al, 2007).…”

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confidence: 99%

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Similar expression to FGF (Sef) inhibits fibroblast growth factor-induced tumourigenic behaviour in prostate cancer cells and is downregulated in aggressive clinical disease

et al. 2009

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The fibroblast growth factor (FGF) axis is an important mitogenic stimulus in prostate carcinogenesis. We have previously reported that transcript level of human similar expression to FGF (hSef), a key regulator of this pathway, is downregulated in clinical prostate cancer. In this study we further analysed the role of hSef in prostate cancer. METHODS: hSef function was studied in in vitro and in vivo prostate cancer models using stable over-expression clones. Protein expression of hSef was studied in a comprehensive tissue microarray. RESULTS: Stable over-expression of hSef resulted in reduced in vitro cancer cell proliferation, migration and invasive potential. In an in vivo xenograft model, the expression of hSef significantly retarded prostate tumour growth as compared with empty vector (P ¼ 0.03) and non-transfected (P ¼ 0.0001) controls. Histological examination further showed a less invasive tumour phenotype and reduced numbers of proliferating cells (P ¼ 0.0002). In signalling studies, hSef inhibited FGF-induced ERK phosphorylation, migration to the nucleus and activation of a reporter gene. Constitutively active Ras, however, was able to reverse these effects, suggesting that hSef exerts an effect either above or at the level of Ras in prostate cancer cells. In a large tissue microarray, we observed a significant loss of hSef protein in high-grade (Po0.0001) and metastatic (Po0.0001) prostate cancer. CONCLUSION: Considered together, the role of hSef in attenuating FGF signalling and evidence of downregulation in advanced tumours argue strongly for a tumour suppressor function in human prostate cancer.

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Section: Discussionsupporting

confidence: 75%

Section: Discussionmentioning

confidence: 98%

mentioning

confidence: 99%

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Similar expression to FGF (Sef) inhibits fibroblast growth factor-induced tumourigenic behaviour in prostate cancer cells and is downregulated in aggressive clinical disease

et al. 2009

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“…Within the human reproductive system, SEF transcripts were detected in testes, ovarian surface epithelium (OSE), and mammary and prostate epithelium (Preger et al 2004, Zisman-Rozen et al 2007. SEF expression is downregulated in ovarian, breast and prostate carcinomas in a manner that correlates with tumor aggressiveness and poor prognosis, underscoring its role as a tumor suppressor (Darby et al 2006, Zisman-Rozen et al 2007, Murphy et al 2010.…”

Section: Introductionmentioning

confidence: 99%

“…SEF expression is downregulated in ovarian, breast and prostate carcinomas in a manner that correlates with tumor aggressiveness and poor prognosis, underscoring its role as a tumor suppressor (Darby et al 2006, Zisman-Rozen et al 2007, Murphy et al 2010. SEF inhibits FGF signaling also in cervical carcinoma and endometrial carcinoma cell lines (Torii et al 2004, Ziv et al 2006, Zisman-Rozen et al 2007, Zhang et al 2011. Thus far, SEF regulation in mammals was only demonstrated during wound healing in the model of rat nervous system (Grothe et al 2008), and nothing is known regarding SEF regulation in the reproductive system.…”

Section: Introductionmentioning

confidence: 99%

Expression and regulation of the tumor suppressor, SEF, during folliculogenesis in humans and mice

et al. 2014

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Similar expression to FGF (SEF or IL17RD), is a tumor suppressor and an inhibitor of growth factors as well as of pro-inflammatory cytokine signaling. In this study, we examined the regulation of Sef expression by gonadotropins during ovarian folliculogenesis. In sexually immature mice, in situ hybridization (ISH) localized Sef gene expression to early developing oocytes and granulosa cells (GC) but not to theca cells. Sef was also expressed in mouse ovarian endothelial cells, in the fallopian tube epithelium as well as in adipose tissue venules. SEF protein expression, determined by immunohistochemistry (IHC), correlated well with Sef mRNA expression in GC, while differential expression was noticed in oocytes. High Sef mRNA but undetectable SEF protein levels were observed in the oocytes of primary/secondary follicles, while an inverse correlation was found in the oocytes of preantral and small antral follicles. Sef mRNA expression dropped after pregnant mare's serum gonadotropin (PMSG) administration, peaked at 6-8 h after human chorionic gonadotropin (hCG) treatment, and declined by 12 h after this treatment. ISH and IHC localized the changes to oocytes and mural GC following PMSG treatment, whereas Sef expression increased in mural GC and declined in granulosa-lutein cells upon hCG treatment. The ovarian expression of SEF was confirmed using human samples. ISH localized SEF transcripts to human GC of antral follicles but not to corpora lutea. Furthermore, SEF mRNA was detected in human GC recovered from preovulatory follicles. These results are the first to demonstrate Sef expression in a healthy ovary during folliculogenesis. Hormonal regulation of its expression suggests that Sef may be an important factor involved in intra-ovarian control mechanisms.

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Expression and functional role of negative signalling regulators in tumour development and progression

Murphy

Hori

Sewell

et al. 2010

Intl Journal of Cancer

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Alterations in intracellular signalling pathways such as the mitogen-activated protein kinases (MAPKs) are key common mechanisms of tumour development and progression. As such, there has been intense research into developing drugs that can inhibit or attenuate intracellular signalling. In recent years, there has been increasing recognition that the cell already has innate negative regulatory proteins that achieve this in normal homeostasis. These regulators provide a feedback inhibitory mechanism that controls the intensity and duration of activated signalling by exogenous stimuli. Members of this group include Raf kinase inhibitor protein 1, the MAPK phosphatases, the SPROUTY and SPRED families and similar expression to FGF. A number of studies have now demonstrated significant alterations in expression of negative regulators in malignant tissue in different cancer types. In functional studies, manipulated expression of these regulators has been shown to significantly influence tumour cell behaviour and phenotype. Here, we summarise the evidence for the functional expression of negative signalling regulators in tumour growth and progression and discuss their potential role as cancer biomarkers and targets for novel drug therapy.Aberrant activation of intracellular signalling by growth factors or other exogenous stimuli is a key mechanism contributing to cancer development and progression. This activation, particularly through the mitogen-activated protein kinase (MAPK) pathway results in diverse mitogenic and pro-survival stimuli promoting tumourigenic behaviour. Intracellular signalling however is subject to different levels of regulation that serve to modulate and attenuate the eventual impact of stimulation. The role of negative signalling regulators has attracted particular interest. Negative signalling regulators are feedback induced mechanisms that are innate to the cell. There is now emerging evidence that negative signalling regulators are themselves altered in the transition from benign to malignant cells. These regulators have been implicated in cancer genesis, growth, metastasis and chemotherapy resistance across diverse tumour types. Thus, negative signalling regulators may have a key role to play in both cancer development and progression. In this context, these regulators may prove important biomarkers of disease progression and may be themselves potential novel therapy targets. In this minireview, we discuss the evidence for the role of key negative regulators implicated in cancer and their potential utility as biomarkers and in therapy. Raf Kinase Inhibitor Protein/ Phosphatidylethanolamine-Binding Protein 1Raf kinase inhibitor protein 1 (RKIP1) is one the best studied negative signalling regulators in tumours because of its putative role as a metastasis suppressor. RKIP is a member of the phosphatidylethanolamine-binding protein (PEBP) family. RKIP was identified in a yeast 2 hybrid screen as a Raf interacting protein by Yeung et al.1 RKIP inhibits Raf activation of MEK but is itself not a subs...

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Downregulation of Sef, an inhibitor of receptor tyrosine kinase signaling, is common to a variety of human carcinomas

Cited by 41 publications

References 21 publications

Similar expression to FGF (Sef) inhibits fibroblast growth factor-induced tumourigenic behaviour in prostate cancer cells and is downregulated in aggressive clinical disease

Similar expression to FGF (Sef) inhibits fibroblast growth factor-induced tumourigenic behaviour in prostate cancer cells and is downregulated in aggressive clinical disease

Expression and regulation of the tumor suppressor, SEF, during folliculogenesis in humans and mice

Expression and functional role of negative signalling regulators in tumour development and progression

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