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miRNA‐194 predicts favorable prognosis in gastric cancer and inhibits gastric cancer cell growth by targeting CCND1

机译:MiRNA-194预测胃癌中有利预后并通过靶向CCND1来抑制胃癌细胞生长

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摘要

MicroRNAs (MiRNAs) play critical roles in regulating target gene expression and multiple cellular processes in human cancer malignant progression. However, the function of miR‐194 in gastric cancer (GC) remains unclear and controversial. In this study, we identified a series of miRNAs that can serve as prognostic biomarkers for GC by analysis of miRNA expression using The Cancer Genome Atlas data. Among them, miR‐100, miR‐125b, miR‐199a, and miR‐194 were the four most promising prognostic biomarkers in GC due to their significant associations with various clinical characteristics of patients. miR‐100, miR‐125b, and miR‐199a predicted poor prognosis in GC, while miR‐194 predicted favorable prognosis in GC. We also provide the first comprehensive transcriptome analysis of miR‐194 in GC. Our data suggest that miR‐194 tends to regulate target genes by binding to their 3′ UTRs in a 7‐mer‐A1, 7‐mer‐m8, or 8‐mer manner. KEGG pathway analysis showed that the cell cycle was one of the pathways most affected by miR‐194 in GC. Moreover, CCND1 was shown to be a novel target gene of miR‐194 in GC. Additionally, downregulation of CCND1 by miR‐194 in GC further led to cell growth inhibition and cell cycle arrest. In conclusion, miR‐100, miR‐125b, miR‐199a, and miR‐194 may have potential as prognostic and diagnostic biomarkers for GC. miR‐194 suppresses GC cell growth mainly through targeting CCND1 and induction of cell cycle arrest.
机译:MicroRNA(miRNA)在调节靶基因表达和人类癌症恶性进展中的多种细胞过程中起重要作用。然而,MIR-194在胃癌(GC)中的功能仍然不清楚和争议。在这项研究中,我们鉴定了一系列MiRNA,其可以通过使用癌症基因组ATLAS数据分析miRNA表达来作为GC的预后生物标志物。其中,由于其具有各种临床特征的患者的各种临床特征,MIR-100,MIR-125B,MIR-199A和MIR-194是GC中最有前途的预后生物标志物。的miR-100,的miR-125B,和miR-199a的预测GC预后较差,而的miR-194预测GC预后良好。我们还提供了MIR-194在GC的第一个全面的转录体分析。我们的数据表明miR-194倾向于通过以7-MER-A1,7-MER-M8或8-MEL方式结合其3'UTR来调节靶基因。 Kegg途径分析表明,细胞周期是GC中MiR-194受影响最大的途径之一。此外,CCND1被证明是GC中miR-194的新靶基因。另外,在GC中通过MIR-194的CCND1的下调进一步导致细胞生长抑制和细胞周期停滞。总之,MIR-100,MIR-125B,MIR-199A和MIR-194可以具有潜在的GC预后和诊断生物标志物。 MIR-194主要通过靶向CCND1和诱导细胞周期骤停抑制GC细胞生长。

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