Expression profiling of Ral-depleted bladder cancer cells identifies RREB-1 as a novel transcriptional Ral effector

Oxford, Gary; Smith, Steven C.; Theodorescu, Dan

doi:10.1038/sj.onc.1210521

Cited by 25 publications

(22 citation statements)

References 31 publications

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“…RREB1 is a transcription factor that has been reported to be either an activator, [22][23][24] or a repressor 25-28 of gene expression, the action of which is dependent upon the gene and cell type. 29 Our results reveal that REEB-1 is a positive regulator of ZIP3 gene expression. Consequently, the existence of downregulated RREB1 in PanIN and early malignancy must be accompanied by preceding upstream events that promote the downregulation of RREB1.…”

Section: Discussionmentioning

confidence: 87%

The cytotoxic role of RREB1, ZIP3 zinc transporter, and zinc in human pancreatic adenocarcinoma

Franklin

Zou

Costello

2014

Cancer Biology & Therapy

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Pancreatic cancer (ductal adenocarcinoma) remains a deadly cancer with ~85% mortality, and a 5-year survival rate of ~6% or less for the past 30 years. The factors and events associated with the development of pancreatic cancer are poorly identified. As such, effective biomarkers for early detection of malignancy are lacking. Efficacious chemotherapy once the cancer is identified does not exist. Recent clinical studies have revealed that the zinc levels are consistently and markedly decreased in adenocarcinoma as compared with normal/benign pancreatic tissue. The decreased zinc is exhibited in well-differentiated malignancy and in progressing malignancy, and also exists throughout the development of PanIN. Concurrent with the decrease in zinc, RREB1 transcription factor and ZIP3 zinc uptake transporter are downregulated. Thus, a RREB1/ZIP3/Zinc transformation appears to be an early event in the development of pancreatic cancer. We propose that this transformation is necessary to prevent the accumulation of high cellular zinc levels, which result in cytotoxic effects on the developing malignant cells. This report now demonstrates that exposure of Panc1 cells to physiological concentrations of zinc that result in increased zinc uptake and accumulation also inhibits cell proliferation. The study further shows that ZIP3 is the important transporter required for the accumulation of zinc and its inhibition of proliferation. RREB1 is identified as the positive regulator of ZIP3 expression. Therefore, the pathway of RREB1/ZIP3/Zinc and its downregulation during oncogenesis exist to prevent the accumulation of cytotoxic levels of zinc during the development and progression of the malignant cells in pancreatic adenocarcinoma.

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Section: Discussionmentioning

confidence: 87%

The cytotoxic role of RREB1, ZIP3 zinc transporter, and zinc in human pancreatic adenocarcinoma

Franklin

Zou

Costello

2014

Cancer Biology & Therapy

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“…Despite its implication in Ras, Ral, p16, p53, and androgen receptor 10,11,14,19,20 signaling pathways, sparse data exist regarding the nature, expression, or function of RREB1 mRNA and protein in cancer cells. This is the first study to address this gap by describing RREB1 expression in human cancers, as well as the first to examine isoform expression in human tissues and cell lines.…”

Section: Discussionmentioning

confidence: 99%

“…8,9 Notably, the RREB1 (Rasresponsive element binding protein 1) transcription factor was identified as a putative Ral-regulated gene through batch analysis of promoter sequences in Ral target genes. 10 Experiments confirmed that Ral manipulation affects RREB1 reporter activity in bladder cancer cells. 10 The significance of RREB1 continues to be elucidated as studies have found it to function in either the induction or repression of gene expression.…”

mentioning

confidence: 80%

“…10 Experiments confirmed that Ral manipulation affects RREB1 reporter activity in bladder cancer cells. 10 The significance of RREB1 continues to be elucidated as studies have found it to function in either the induction or repression of gene expression. Genes induced by RREB1 include those encoding calcitonin, 11 FSH, 12 MT-IIA, 13 p53, 14 and secretin 15 ; genes repressed by RREB1 include those encoding angiotensinogen, 16 HLA-G, 17 hZIP1, 18 p16, 19 and PSA.…”

mentioning

confidence: 80%

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RREB1 Transcription Factor Splice Variants in Urologic Cancer

Nitz

Harding

Smith

et al. 2011

The American Journal of Pathology

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RREB1 is an alternatively spliced transcription factor implicated in Ras signaling and cancer. Little is known about the expression of RREB1 isoforms in cell lines or human tumors, or about the clinical relevance of the latter. We have developed tools for IHC of RREB1 protein isoform-specific amplification of RREB1 mRNA and selective knockdown of RREB1 isoforms and use these to provide new information by characterizing RREB1 expression in bladder and prostate cancer cell lines and human tissue samples. Previously described splice variants RREB1␣, RREB1␤, RREB1␥, and RREB1␦ were identified, as well as the novel variant RREB1 . Total and isoform-specific mRNA expression was lower in most but not all tumors, compared with normal tissues. RREB1 IHC performed on a bladder cancer TMA did not indicate a relationship between total RREB1 expression and overall survival after radical cystectomy for invasive bladder cancer. In contrast, in vitro proliferation studies using the UMUC-3 bladder cancer cell line after selective isoform-specific knockdown of expression indicate that RREB1␣ is not necessary for proliferation, but that RREB1␤ may be required. These contributions should accelerate progress in the nascent RREB1 field by providing new reagents while also providing clues to the role of RREB1 isoforms in human cancer and raising the possibility of isoform-specific roles in human carcinogenesis and progression.

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“…Neither study implicated RALB in the generation of primary tumours; however, the Counter group found that chronic RALB depletion severely impaired or eliminated the capacity of several pancreatic cancer lines to generate lymph-node metastases following tail vein injection 10 . Interestingly, Ral-dependent gene-expression patterns that might contribute to metastatic behaviour have recently been uncovered by genomic expression profiling 25,26 . Although these studies clearly convict Ral proteins as key offenders in the maintenance of tumorigenicity, further work is needed to determine whether the biological consequences observed reflect distinct contributions of Ral signalling to tumorigenicity in diverse cell types, and/ or distinct sensitivities to the tissue microenvironment, and/or differences in phenotypic penetrance as a consequence of residual RALA or RALB protein expression.…”

Section: Box 1 | the G-protein Cyclementioning

confidence: 99%

Harnessing Functional Genomics to Reverse Chemoresistance in Breast Cancer

Bodemann¹

2008

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Expression profiling of Ral-depleted bladder cancer cells identifies RREB-1 as a novel transcriptional Ral effector

Cited by 25 publications

References 31 publications

The cytotoxic role of RREB1, ZIP3 zinc transporter, and zinc in human pancreatic adenocarcinoma

The cytotoxic role of RREB1, ZIP3 zinc transporter, and zinc in human pancreatic adenocarcinoma

RREB1 Transcription Factor Splice Variants in Urologic Cancer

Harnessing Functional Genomics to Reverse Chemoresistance in Breast Cancer

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