<i>OCT4</i> spliced variant <i>OCT4B1</i> is expressed in human colorectal cancer

Gazouli, Maria; Roubelakis, Maria G.; Theodoropoulos, George; Papailiou, Joanna; Vaiopoulou, Anna; Pappa, Kalliopi I.; Nikiteas, Nikolaos; Anagnou, Nicholas P.

doi:10.1002/mc.20773

Cited by 51 publications

(48 citation statements)

References 36 publications

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“…Notably, the BMP4 pathway is involved in mammalian palatogenesis [71], and mutations in BMP4 have been associated with human NSCL/P [12], [58], [59]. Research has shown that OCT4 is overexpressed in cancer cell lines and in diverse cancer entities [24], [37], [67], suggesting that aberrant transcriptional regulation of OCT4 might be a mechanism in cancer susceptibility. Thus, a plausible hypothesis is that rs6457327 regulates OCT4 expression, and that this regulation is a possible common process in oncogenesis and the development of NSCL/P.…”

Section: Discussionmentioning

confidence: 99%

Nonsyndromic cleft lip with or without cleft palate and cancer: Evaluation of a possible common genetic background through the analysis of GWAS data

et al. 2016

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Previous research suggests a genetic overlap between nonsyndromic cleft lip with or without cleft palate (NSCL/P) and cancer. The aim of the present study was to identify common genetic risk loci for NSCL/P and cancer entities that have been reported to co-occur with orofacial clefting. This was achieved through the investigation of large genome-wide association study datasets. Investigations of 12 NSCL/P single nucleotide polymorphisms (SNPs) in 32 cancer datasets, and 204 cancer SNPs in two NSCL/P datasets, were performed. The SNPs rs13041247 (20q12) and rs6457327 (6p21.33) showed suggestive evidence for an association with both NSCL/P and a specific cancer entity. These loci harbor genes of biological relevance to oncogenesis (MAFB and OCT4, respectively). This study is the first to characterize possible pleiotropic risk loci for NSCL/P and cancer in a systematic manner. The data represent a starting point for future research by identifying a genetic link between NSCL/P and cancer.

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Section: Discussionmentioning

confidence: 99%

Nonsyndromic cleft lip with or without cleft palate and cancer: Evaluation of a possible common genetic background through the analysis of GWAS data

et al. 2016

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“…Overexpression of OCT4B1 has been related to poor prognosis in cancer in several studies. Expression of OCT4B1 was upregulated in CRC tissues, compared to adjacent non-cancerous tissues, which suggested OCT4B1 to represent a potential biomarker for the initiation, progression and differentiation of CRC (26). Like OCT4B1, SOX2 is reported to act as an oncogene, being upregulated in CRC, and in esophageal squamous cell carcinoma, where it correlated to poor clinical outcome (27,28).…”

Section: Discussionmentioning

confidence: 99%

Preoperative low dose NSAID treatment influences the genes for stemness, growth, invasion and metastasis in colorectal cancer

Lönnroth

Andersson

Asting

et al. 2014

International Journal of Oncology

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Preclinical data, and an increasing list of clinical investigations, show anti-inflammatory agents to favourably influence the biology of colorectal tumor. We have earlier reported on re-expression of activated immune cells after three days preoperative treatment of patients with colorectal carcinoma, randomized to receive oral NSAID (indomethacin or celebrex). Antisecretory prophylaxis (esomeprasol) was provided to all patients and served as sham treatment. Concomittant to MHC locus activation, Prominin1/CD133, a marker associated with stemness and poor prognosis in several solid tumors, was downregulated. The aim of the present study was to evaluate expression of additional regulators belonging to the stem cell niche, OCT4, SOX2 and BMP7, as well as some microRNAs, reported to act as tumor suppressors or oncomiRs. Peroperative tumor biopsies were analyzed by microarrays, quantitative real-time PCR and immunohistochemistry (IHC). The stem cell master regulator SOX2 was increased by NSAIDs (p<0.01), as well as the tumor suppressor miR-630 (p<0.01), while BMP7, a marker for poor prognosis in CRC, was downregulated by NSAID (indomethacin, p<0.02). The upregulation of SOX2, but not of its heterodimer binding partner OCT4, could imply a negative feed-back loop, with a switch-off for stemness preservation of tumor cells. This is supported by the overall evaluation of gene expression profiles with subsequent events, indicating less aggressive tumors following NSAID treatment.

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“…A large amount of data has showed up-regulation of key stemness factors, like Sox2 and Nanog in several types of cancer cells and the importance of targeting these regulators in cancer therapy (2)(3)(4)(5)(6)(7)(8). Sox2 and Nanog are transcription factors that are essential for maintaining self-renewal or pluripotency of undifferentiated embryonic stem cells (17).…”

Section: Discussionmentioning

confidence: 99%

Suppressive Effect of Crocin and Cisplatin on Pluripotency Genes Expression in Human Cervical Cancer Cells

2017

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Background: Cervical cancer is the fourth most common cancer in women. Since pluripotency genes are one of the main contributors of cancer, designing novel combinational therapies that target them would be helpful. Methods: In this study we assayed the anticancer effects of crocin and cisplatin on cervical cancer cells through suppression of Sox2 and Nanog. OV2008 cells were treated with crocin and cisplatin, and the viability and apoptosis were assessed by the MTT and Flowcytometery respectively. The expression levels of mRNA of pluripotency genes were detected by Real-Time PCR analysis. Results: Our data showed that treatment of OV2008 cells with crocin and cisplatin decrease cell viability in a dose-and timedependent manner. Also cell cycle analysis indicated that the percentage of apoptotic cells significantly increased after treatment. Moreover, this treatment led to down-regulation of Sox2 and Nanog genes. Conclusions: So it would be proposed that crocin in combination with cisplatin could induce cytotoxicity in cervical cancer cells through inhibition of pluripotency genes.

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OCT4 spliced variant OCT4B1 is expressed in human colorectal cancer

Cited by 51 publications

References 36 publications

Nonsyndromic cleft lip with or without cleft palate and cancer: Evaluation of a possible common genetic background through the analysis of GWAS data

Nonsyndromic cleft lip with or without cleft palate and cancer: Evaluation of a possible common genetic background through the analysis of GWAS data

Preoperative low dose NSAID treatment influences the genes for stemness, growth, invasion and metastasis in colorectal cancer

Suppressive Effect of Crocin and Cisplatin on Pluripotency Genes Expression in Human Cervical Cancer Cells

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