Expression of SOCS1 and SOCS3 genes is differentially regulated in breast cancer cells in response to proinflammatory cytokine and growth factor signals

Evans, Michele K.; Yu, Cheng‐Rong; Lohani, Althaf; Rm, Mahdi; Liu, Xiaoyu; Ar, Trzeciak; Egwuagu, C.E.

doi:10.1038/sj.onc.1209993

Cited by 66 publications

(56 citation statements)

References 33 publications

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“…43 SOCS5 has been shown to be decreased in prostate cancer cell lines compared to a non-malignant prostate cell line. 44 Collectively, these data support the notion that elevation of hsa-miR-141 and hsa-miR-375 in prostate tumors alters gene expression programs, and that identification of their target genes could yield information regarding prostate cancer biology. We are currently undertaking functional studies to investigate whether these miRNAs contribute to disease development and/or progression.…”

Section: Early Detection and Diagnosissupporting

confidence: 61%

Discovery of circulating microRNAs associated with human prostate cancer using a mouse model of disease

Selth

Townley

Gillis

et al. 2011

Intl Journal of Cancer

176

155

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Circulating microRNAs (miRNAs) are emerging as useful non-invasive markers of disease. The objective of this study was to use a mouse model of prostate cancer as a tool to discover serum miRNAs that could be assessed in a clinical setting. Global miRNA profiling identified 46 miRNAs at significantly altered levels (p 0.05) in the serum of TRansgenic Adenocarcinoma of Mouse Prostate (TRAMP) mice with advanced prostate cancer compared to healthy controls. A subset of these miRNAs with known human homologues were validated in an independent cohort of mice and then measured in serum from men with metastatic castration-resistant prostate cancer (mCRPC; n 5 25) or healthy men (n 5 25). Four miRNAs altered in mice, mmumiR-141, mmu-miR-298, mmu-miR-346 and mmu-miR-375, were also found to be at differential levels in the serum of men with mCRPC. Three of these (hsa-miR-141, hsa-miR-298 and hsa-miR-375) were upregulated in prostate tumors compared with normal prostate tissue, suggesting that they are released into the blood as disease progresses. Moreover, the intra-tumoral expression of hsa-miR-141 and hsa-miR-375 were predictors of biochemical relapse after surgery. This study is the first to demonstrate that specific serum miRNAs are common between human prostate cancer and a mouse model of the disease, highlighting the potential of such models for the discovery of novel biomarkers.Prostate cancer is the most commonly diagnosed non-skin malignancy in men in Western countries, constituting up to 25% of all male cancer diagnoses and 9% of cancer deaths among men in the USA and Europe. 1,2 The widespread use of serum prostate specific antigen (PSA) testing along with increasing public awareness of prostate cancer has resulted in a significant increase in the proportion of patients with clinically localized tumors at the time of diagnosis who likely will not die of the disease. 3 Localized prostate cancers exhibit high levels of genetic, biological and clinical heterogeneity, 4,5 and current prognostic tools (based upon clinicopathologic parameters) are imperfect predictors of disease course. New molecular markers are urgently required to better predict the likely outcome and behavior of individual cancers. microRNAs (miRNAs) are small RNA molecules of 21-23nt that bind with imperfect complementarity to sequences in specific mRNA targets and typically silence their expression by translational inhibition or mRNA decay. miRNAs are estimated to regulate the expression of greater than 60% of all protein-coding genes 6 and, as such, play vital roles in all aspects of normal physiology. Given their biological importance, it is not surprising that miRNA expression is frequently dysregulated in human cancer. 7 Accumulating evidence suggests that miRNAs can contribute to tumorigenesis either by directly modulating oncogenic or tumor suppressor pathways (oncomirs and tumor suppressor miRNAs, respectively) and/or being regulated by oncogenes or tumor suppressor genes. 8 Several characteristics of miRNAs make them ideal biomarkers for...

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Section: Early Detection and Diagnosissupporting

confidence: 61%

Discovery of circulating microRNAs associated with human prostate cancer using a mouse model of disease

Selth

Townley

Gillis

et al. 2011

Intl Journal of Cancer

176

155

View full text Add to dashboard Cite

show abstract

“…Indeed, reports describing SOCS-3 hypermethylation and subsequent loss of expression in a variety of cancers support the idea that SOCS-3 may have a tumor-suppressing function (94)(95)(96)(97). In contrast, elevated SOCS-3 expression was reported in human breast cancer and melanoma tissues, as well as in a subset of classic Hodgkin's lymphoma cell lines and primary lymphoma cells (98)(99)(100)(101)(102)(103)(104). In several studies, SOCS-3 promoted cell growth and proliferation in a number of cancers (100,103,105), and elevated levels of SOCS-3 were reported to confer a growth advantage to a melanoma cell line (103).…”

Section: Involvement Of Socs-3 In Gliomasmentioning

confidence: 87%

Signal Transducer and Activator of Transcription-3: A Molecular Hub for Signaling Pathways in Gliomas

Brantley

Benveniste

2008

Molecular Cancer Research

208

159

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“…Interestingly, a good correlation between constitutive SOCS 3 expression, lack of its inducibility and IFN cell resistance was obtained in additional melanoma cell lines (Table 1). The strong upregulation of SOCS 3 following IFN-g could be a specific feature of melanoma lineages because epithelial breast cancer cells showed its downregulation (Evans et al, 2007) or variable expression (Souckova, unpublished data). However, in breast cancer cells SOCS 1 was strongly activated while its induction was rather weak in melanoma lines used.…”

Section: Expression Profiles Of Socss In Melanoma Cellsmentioning

confidence: 99%

“…In support, three IFN-insensitive WM 1158R, WM 9 and 1205 Lu melanoma lines had high basal expression of SOCS 3 compared to sensitive cells. Furthermore, breast cancer (Evans et al, 2007) and leukaemia cells (Sakai et al, 2002) showed elevated constitutive expression of SOCS 1 and SOCS 3 and the resistance to proinflammatory cytokines including IFN-g. Perhaps IFN sensitivity of a SOCS 3 promoter is reduced due to aberrant expression of an activatory transcription factor(s). In this context, aberrant activation of tissue-specific promoters has been observed in cancers (Kovarik et al, 1993).…”

Section: Expression Profiles Of Socss In Melanoma Cellsmentioning

confidence: 99%

“…These studies indicated that aberrant silencing could be a cause for constitutive activation of JAK/STAT pathway in cancer cells. However, other studies also indicated that malignant cells compared to their normal counterparts express SOCS genes constitutively (Sakai et al, 2002;Li et al, 2004;Evans et al, 2007) and forced expression of SOCS transgene often conferred resistance to IFN. Constitutive expression can potentially hamper immunotherapy by inactivating cytokine signals.…”

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confidence: 99%

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Development of IFN-γ resistance is associated with attenuation of SOCS genes induction and constitutive expression of SOCS 3 in melanoma cells

et al. 2007

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The resistance to interferons (IFNs) limits their anticancer therapeutic efficacy. Here we studied the evolution of an IFN-resistant state in vitro using melanoma cell lines. We found that the cells became less sensitive to antiproliferative effect of IFN-g after prolonged cultivation enabling us to isolate sensitive and resistant subclones of the parental line. We investigated transcription of signal transducer and activator of transcription (STAT) 1 -6 and suppressor of cytokine signalling (SOCS) 1 -3 genes, and phosphorylation of STAT 1 protein. The resistant subline (termed WM 1158R) differed from the sensitive subline (WM 1158S) by a constitutive expression of SOCS 3, lack or weak SOCS 1 -3 activation following IFN-g, and short duration of cytokine activatory signal. Similar correlations were observed in additional melanoma lines differing in IFN sensitivities. At the protein level, IFN-g induced strong and prolonged STAT 1 activation at serine 727 (S727) in WM 1158R while in WM 1158S cells phosphorylation of this amino acid was much less pronounced. On the other hand, phosphorylation of tyrosine 701 (Y701) was stimulated regardless of the sensitivity phenotype. In conclusion, constitutive expression of SOCS 3 is correlated with attenuation of its induction following IFN treatment. These results suggest that progression of melanoma cells from IFN sensitivity to IFN insensitivity associates with changes in SOCS expression.

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Expression of SOCS1 and SOCS3 genes is differentially regulated in breast cancer cells in response to proinflammatory cytokine and growth factor signals

Cited by 66 publications

References 33 publications

Discovery of circulating microRNAs associated with human prostate cancer using a mouse model of disease

Discovery of circulating microRNAs associated with human prostate cancer using a mouse model of disease

Signal Transducer and Activator of Transcription-3: A Molecular Hub for Signaling Pathways in Gliomas

Development of IFN-γ resistance is associated with attenuation of SOCS genes induction and constitutive expression of SOCS 3 in melanoma cells

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