首页> 外文期刊>Cellular Oncology: Analytical Cellular Pathology >GTSE1, CDC20, PCNA, and MCM6 Synergistically Affect Regulations in Cell Cycle and Indicate Poor Prognosis in Liver Cancer
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GTSE1, CDC20, PCNA, and MCM6 Synergistically Affect Regulations in Cell Cycle and Indicate Poor Prognosis in Liver Cancer

机译:GTSe1,CDC20,PCNA和MCM6协同影响细胞周期中的法规,表明肝癌预后差

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GTSE1 is well correlated with tumor progression; however, little is known regarding its role in liver cancer prognosis. By analyzing the hepatocellular carcinoma (HCC) datasets in GEO and TCGA databases, we showed that high expression of GTSE1 was correlated with advanced pathologic stage and poor prognosis of HCC patients. To investigate underlying molecular mechanism, we generated GTSE1 knockdown HCC cell line and explored the effects of GTSE1 deficiency in cell growth. Between GTSE1 knockdown and wild-type HCC cells, we identified 979 differentially expressed genes (520 downregulated and 459 upregulated genes) in the analysis of microarray-based gene expression profiling. Functional enrichment analysis of DEGs suggested that S phase was dysregulated without GTSE1 expression, which was further verified from flow cytometry analysis. Moreover, three other DEGs: CDC20, PCNA, and MCM6, were also found contributing to GTSE1-related cell cycle arrest and to be associated with poor overall survival of HCC patients. In conclusion, GTSE1, together with CDC20, PCNA, and MCM6, may synergistically promote adverse prognosis in HCC by activating cell cycle. Genes like GTSE1, CDC20, PCNA, and MCM6 may be promising prognostic molecular biomarkers in liver cancer.
机译:Gtse1与肿瘤进展相关;然而,对其在肝癌预后的作用很少令人着重。通过分析Geo和TCGA数据库中的肝细胞癌(HCC)数据集,我们表明GTSe1的高表达与晚期病理阶段和HCC患者的预后不良。为了研究潜在的分子机制,我们产生了GTSe1敲低HCC细胞系,并探讨了GTSe1缺乏对细胞生长的影响。在GTSe1敲低和野生型HCC细胞之间,我们鉴定了979个差异表达的基因(520下调和459个上调基因)在分析微阵列的基因表达分析中。 Degs的功能性富集分析表明,没有GTSe1表达的不测定S期,从流式细胞术分析进一步验证。此外,还发现三种其他参数:CDC20,PCNA和MCM6有助于GTSe1相关的细胞周期停滞,并且与HCC患者的整体存活差有关。总之,GTSe1与CDC20,PCNA和MCM6一起可以通过激活细胞周期来协同促进HCC的不良预后。 GTSe1,CDC20,PCNA和MCM6等基因可能是肝癌中预后的预后分子生物标志物。

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