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R results concerning Cyclin D1 and Bcl-2 were consistent with some of these publications [35,36,37,38,39]. Variation in the prognostic significance of Cyclin D1 and Bcl-2 in previous studies may be attributable to differences in sample size, definitions of positive expression, the inclusion of tumors from different subsites of the oral cavity, and the diversity of treatments. More importantly, our data showed that the expression of Cyclin D1 and Bcl-2 in TSCC tissues is inversely correlated with miR-195 levels. These important observations not only support previous findings that Cyclin D1 and Bcl-2 are target genes silenced by miR-195 but also demonstrate that the expression of miR-195 is potentially a more accurate prognostic tumor marker than Cyclin D1 or Bcl-2 levels alone in TSCC patients. The anti-tumor effect of miR-195 in TSCC could be at least partially via inhibition of Cyclin D1 and Bcl-2 expression. We performed a series of experiments using two TSCC cell lines (SCC-15 and CAL27) to investigate the function of miR-195. Ourresults demonstrate that ectopic overexpression of miR-195 reduces cell viability, inhibits cell cycle progression, and promotes cell apoptosis. Moreover, Cyclin D1 and Bcl-2 were shown to be direct targets of miR-195 by a dual-luciferase reporter assay and western blots, and their inhibition may account for the antitumor effect of miR-195 in TSCC. However, because TargetScan predicts hundreds of potential targets of miR-195 (http://www. targetscan.org), we cannot exclude the possibility that other potential targets of miR-195 may govern additional cancer pathways that promote TSCC cancer development and that miR-195 may also target different molecules in different types of cancer. Our study focused on a large series of patients who satisfied stringent recruitment criteria: (1) tumor location at the anterior body of the tongue, (2) squamous cell carcinoma, and (3) surgery as the primary treatment. We hope that this study will provide more accurate and clinically useful information on the prognostic significance of miR-195 expression. Several papers have described the involvement of miRNAs in head and neck squamous cell carcinoma [42,43,44,45]. In these publications, which generally have included comparisons of 256373-96-3 site normal and tumor samples, miRNA profiling was used to associate the expression of miRNAs with malignant progression and prognosis. Although these initial data have already suggested that miRNAs are involved in squamous cell carcinogenesis, the studies have always included heterogenous groups of patients with cancers from different subsites of oral cavity, and gene expression patterns from squamous cell carcinomas at different subsites of oral cavity may not be equally associated with cancer prognosis. For example, squamous cell carcinomas of the tongue have been shown to be different from those of the cheek in previous studies [46,47], perhaps because different molecular genetic pathways are involved. In conclusion, our study has confirmed in a large and homogeneous patient population that miR-195 expression was decreased in 80.2 of TSCC tumor samples compared with adjacent nonmalignant tissues and has provided 1081537 evidence that miR-195 may be an get Calcitonin (salmon) independent biomarker of clinical prognosis among TSCC patients. Moreover, the anti-tumor effects of miR195 in TSCC may be partially mediated by its inhibition of Cyclin D1 and Bcl-2 expression. Because miR-195 appears to have an anti-tumor effect in TSCC cell li.R results concerning Cyclin D1 and Bcl-2 were consistent with some of these publications [35,36,37,38,39]. Variation in the prognostic significance of Cyclin D1 and Bcl-2 in previous studies may be attributable to differences in sample size, definitions of positive expression, the inclusion of tumors from different subsites of the oral cavity, and the diversity of treatments. More importantly, our data showed that the expression of Cyclin D1 and Bcl-2 in TSCC tissues is inversely correlated with miR-195 levels. These important observations not only support previous findings that Cyclin D1 and Bcl-2 are target genes silenced by miR-195 but also demonstrate that the expression of miR-195 is potentially a more accurate prognostic tumor marker than Cyclin D1 or Bcl-2 levels alone in TSCC patients. The anti-tumor effect of miR-195 in TSCC could be at least partially via inhibition of Cyclin D1 and Bcl-2 expression. We performed a series of experiments using two TSCC cell lines (SCC-15 and CAL27) to investigate the function of miR-195. Ourresults demonstrate that ectopic overexpression of miR-195 reduces cell viability, inhibits cell cycle progression, and promotes cell apoptosis. Moreover, Cyclin D1 and Bcl-2 were shown to be direct targets of miR-195 by a dual-luciferase reporter assay and western blots, and their inhibition may account for the antitumor effect of miR-195 in TSCC. However, because TargetScan predicts hundreds of potential targets of miR-195 (http://www. targetscan.org), we cannot exclude the possibility that other potential targets of miR-195 may govern additional cancer pathways that promote TSCC cancer development and that miR-195 may also target different molecules in different types of cancer. Our study focused on a large series of patients who satisfied stringent recruitment criteria: (1) tumor location at the anterior body of the tongue, (2) squamous cell carcinoma, and (3) surgery as the primary treatment. We hope that this study will provide more accurate and clinically useful information on the prognostic significance of miR-195 expression. Several papers have described the involvement of miRNAs in head and neck squamous cell carcinoma [42,43,44,45]. In these publications, which generally have included comparisons of normal and tumor samples, miRNA profiling was used to associate the expression of miRNAs with malignant progression and prognosis. Although these initial data have already suggested that miRNAs are involved in squamous cell carcinogenesis, the studies have always included heterogenous groups of patients with cancers from different subsites of oral cavity, and gene expression patterns from squamous cell carcinomas at different subsites of oral cavity may not be equally associated with cancer prognosis. For example, squamous cell carcinomas of the tongue have been shown to be different from those of the cheek in previous studies [46,47], perhaps because different molecular genetic pathways are involved. In conclusion, our study has confirmed in a large and homogeneous patient population that miR-195 expression was decreased in 80.2 of TSCC tumor samples compared with adjacent nonmalignant tissues and has provided 1081537 evidence that miR-195 may be an independent biomarker of clinical prognosis among TSCC patients. Moreover, the anti-tumor effects of miR195 in TSCC may be partially mediated by its inhibition of Cyclin D1 and Bcl-2 expression. Because miR-195 appears to have an anti-tumor effect in TSCC cell li.

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Author: heme -oxygenase