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A novel mRNA-miRNA-lncRNA competing endogenous RNA triple sub-network associated with prognosis of pancreatic cancer

机译:一种新型的mRNA-miRNA-lncRNA竞争内源性RNA三重亚网络与胰腺癌的预后相关

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摘要

Background: Recently, increasing evidence has uncovered the roles of mRNA-miRNA-lncRNA network in multiple human cancers. However, a systematic mRNA-miRNA-lncRNA network linked to pancreatic cancer prognosis is still absent. Methods: Differentially expressed genes (DEGs) were first identified by mining and datasets. DAVID database was utilized to conduct functional enrichment analysis. Protein-protein interaction (PPI) network was built using STRING database, and hub genes were identified by Cytoscape plug-in CytoHubba. Upstream miRNAs and lncRNAs of mRNAs were predicted by miRTarBase and miRNet, respectively. Expression, survival and correlation analysis for genes, miRNAs and lncRNAs were performed via GEPIA, Kaplan-Meier plotter and starBase. Results: 734 and 180 upregulated and downregulated significant DEGs were identified, respectively. Functional enrichment analysis revealed that they were significantly enriched in focal adhesion, pathways in cancer and metabolic pathways. According to node degree, hub genes in the PPI networks were screened, such as TGFB1 and ALB. Among the top 20 hub genes, 7 upregulated genes and 2 downregulated hub genes had significant prognostic values in pancreatic cancer. 33 miRNAs were predicted to target the 9 key genes. But only high expression of 8 miRNAs indicated favorable prognosis in pancreatic cancer. Then, 90 lncRNAs were predicted to potentially bind to the 8 miRNAs. SCAMP1, HCP5, MAL2 and LINC00511 were finally identified as key lncRNAs. By combination of results from expression, survival and correlation analysis demonstrated that MMP9/ITGB1-miR-29b-3p-HCP5 competing endogenous RNA (ceRNA) sub-network was linked to prognosis of pancreatic cancer. Conclusions: In a word, we established a novel mRNA-miRNA-lncRNA sub-network, among which each RNA may be utilized as a prognostic biomarker of pancreatic cancer.
机译:背景:最近,越来越多的证据揭示了mRNA-miRNA-lncRNA网络在多种人类癌症中的作用。但是,仍然缺乏与胰腺癌预后相关的系统性mRNA-miRNA-lncRNA网络。方法:首先通过挖掘和数据集鉴定差异表达基因(DEG)。利用DAVID数据库进行功能富集分析。使用STRING数据库构建了蛋白质-蛋白质相互作用(PPI)网络,并通过Cytoscape插件CytoHubba鉴定了轮毂基因。 miRTarBase和miRNet分别预测了上游的miRNA和mRNA的lncRNA。通过GEPIA,Kaplan-Meier绘图仪和starBase对基因,miRNA和lncRNA进行表达,存活和相关性分析。结果:分别确定了734个和180个上调和下调的重要DEG。功能富集分析显示,它们在粘着斑,癌症途径和代谢途径中显着丰富。根据节点的程度,筛选了PPI网络中的集线器基因,例如TGFB1和ALB。在排名前20位的Hub基因中,有7个上调基因和2个下调的Hub基因在胰腺癌中具有重要的预后价值。预测有33个miRNA靶向9个关键基因。但是只有高表达的8个miRNA提示胰腺癌预后良好。然后,预测有90个lncRNA可能与8个miRNA结合。最终将SCAMP1,HCP5,MAL2和LINC00511鉴定为关键的lncRNA。通过表达结果的组合,存活和相关性分析表明,MMP9 / ITGB1-miR-29b-3p-HCP5竞争内源性RNA(ceRNA)子网与胰腺癌的预后相关。结论:总之,我们建立了一个新的mRNA-miRNA-lncRNA子网,其中每个RNA均可作为胰腺癌的预后生物标志物。

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