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Diagnostic significance and potential function of miR-338-5p in hepatocellular carcinoma: A bioinformatics study with microarray and RNA sequencing data

机译:MiR-338-5P在肝细胞癌中的诊断意义和潜在功能:微阵列和RNA测序数据的生物信息学研究

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摘要

MicroRNA (miR)-338-5p has been studied in hepatocellular carcinoma (HCC); however, the diagnostic value and molecular mechanism underlying its actions remains to be elucidated. The present study aimed to validate the diagnostic ability of miR-338-5p and further explore the underlying molecular mechanism. Data from eligible studies, Gene Expression Omnibus (GEO) chips and The Cancer Genome Atlas (TCGA) datasets were gathered in the data mining and the integrated meta-analysis, to evaluate the significance of miR-338-5p in diagnosing HCC comprehensively. The potential target genes of miR-338-5p were achieved from the intersection of the deregulated targets of miR-338-5p from GEO and TCGA in addition to the predicted target genes from 12 online software. A protein-protein-interaction (PPI) network was drawn to illustrate the interaction between target genes and to define the hub genes. Gene Ontology (GO) and Kyoto Encyclopedia of Genes and Genomes (KEGG) pathway enrichment analyses were performed to investigate the function of the target genes. From the results, miR-338-5p exhibited favorable value in diagnosing HCC. Types of sample and experiment were defined as the possible sources of heterogeneity in meta-analysis. A total of 423 genes were selected as the potential target genes of miR-338-5p, and five genes were defined as the hub genes from the PPI network. The GO and KEGG analyses indicated that the target genes were significantly assembled in the pathways of metabolic process and cell cycle. miR-338-5p may function as a novel diagnostic target for HCC through regulating certain target genes and signaling pathways.
机译:MicroRNA(MIR)-338-5P已在肝细胞癌(HCC)中研究;然而,其行为的诊断价值和分子机制仍有待阐明。本研究旨在验证miR-338-5p的诊断能力,进一步探索潜在的分子机制。来自符合条件的研究的数据,在数据挖掘和集成的荟萃分析中收集了基因表达综合征(Geo)芯片和癌症基因组地图集(​​TCGA)数据集,以评估miR-338-5p综合诊断HCC的重要性。除了来自12个在线软件的预测的目标基因外,MiR-338-5P的潜在靶基因是从Geo和TCGA的解除衰减靶标的因解毒靶点。绘制蛋白质 - 蛋白质相互作用(PPI)网络以说明靶基因之间的相互作用并限定轮毂基因。进行基因本体(GO)和京都基因组(Kegg)途径富集分析以研究靶基因的功能。结果,MIR-338-5P在诊断HCC方面表现出良好的价值。样品和实验类型被定义为Meta分析中的可能的异质性源。选择共423个基因作为miR-338-5p的潜在靶基因,并且将五个基因定义为来自PPI网络的集线器。 Go和Kegg分析表明,在代谢过程和细胞周期的途径中显着地组装了靶基因。 MiR-338-5P可以通过调节某些靶基因和信号通路来用作HCC的新型诊断靶标。

著录项

  • 来源
    《Molecular medicine reports》 |2018年第1期|共16页
  • 作者单位

    Guangxi Med Univ Dept Gen Surg Affiliated Hosp 2 166 Daxue Rd East Nanning 530007 Guangxi;

    Guangxi Med Univ Dept Gen Surg Affiliated Hosp 2 166 Daxue Rd East Nanning 530007 Guangxi;

    Guangxi Med Univ Dept Pathol Affiliated Hosp 1 Nanning 530021 Guangxi Peoples R China;

    Guangxi Med Univ Dept Pathol Affiliated Hosp 1 Nanning 530021 Guangxi Peoples R China;

    Guangxi Med Univ Dept Pathol Affiliated Hosp 1 Nanning 530021 Guangxi Peoples R China;

    Guangxi Med Univ Dept Gen Surg Affiliated Hosp 2 166 Daxue Rd East Nanning 530007 Guangxi;

    Guangxi Med Univ Dept Gen Surg Affiliated Hosp 2 166 Daxue Rd East Nanning 530007 Guangxi;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 基础医学;
  • 关键词

    miR-338-5p; HCC; GEO; meta-analysis; target genes;

    机译:mir-338-5p;hcc;geo;meta分析;靶基因;

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