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Identification of ceRNA network based on a RNA-seq shows prognostic lncRNA biomarkers in human lung adenocarcinoma

机译:基于RNA-SEQ的Cerna网络的鉴定显示人肺腺癌中的预后LNCRNA生物标志物

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Previous studies have emphasized the significant functions of long non-coding RNAs (lncRNAs) as competing endogenous RNAs (ceRNAs) in tumor biology. However, the functions of certain cancer lncRNAs in the lncRNA-related ceRNA network in lung adenocarcinoma (LUAD) are unknown. A systematic and integrative survey of RNA-seq data from The Cancer Genome Atlas (TCGA) was performed to identify candidate lncRNAs for the prognosis of LUAD. In total, 20,502 genes that contain 181 lncRNAs were evaluated in a cohort of 570 LUAD cases. Initially, 6,280 differentially expressed genes (fold-change 2, P0.05) were obtained using R package, which includes 75 lncRNAs. Next, by univariate regression and multivariate Cox proportional hazards analysis, 32 genes were associated with survival in LUAD. Using these 29 mRNAs and 3 lncRNAs, a prognosis index (PI) was calculated to accurately estimate the survival in LUAD: PI=Sigma exp(risk gene) x HRrisk (gene). Furthermore, the 32-gene signature was an independent prognostic indicator for LUAD (HR 1; P0.05, by multivariate analysis). Weighted gene co-expression network analysis (WGCNA) of three risk lncRNAs-FAM138B, NHEG1 and TLX1NB-was performed, based on the P-values of the associated genes, and the top 27 miRNAs that bound to these lncRNAs were predicted by Miranda as target miRNAs. Next, these target miRNAs were transferred to the TarBase, miRTarBase, miRecards and starBase v2.0 databases to obtain their target genes. According to the previous miRNA-mRNA and miRNA-lncRNA data, three lncRNA-miRNA-mRNA ceRNA networks were established, based on the 29 prognostic mRNAs, forming a regulatory network in LUAD. The present study provided insight into the lncRNA-related ceRNA network in LUAD and has identified potential diagnostic and prognostic biomarkers.
机译:以前的研究强调了长期非编码RNA(LNCRNA)作为肿瘤生物学竞争内源性RNA(Cernas)的重要功能。然而,某些癌症LNCRNA在肺腺癌(Luad)中的某些癌症LNCRNA的功能是未知的。进行来自癌症基因组Atlas(TCGA)的RNA-SEQ数据的系统和综合调查,以鉴定候选LNCRNA用于管道预后。总共含有181例LNCRNA的20,502个基因,在570例水道病例的队列中评价。最初,使用R包装获得6,280个差异表达基因(折叠变化& 2,p <0.05),其包括75℃。接下来,通过单变量的回归和多元COX比例危害分析,32个基因与管道生存有关。使用这些29 mRNA和3 LNCRNA,计算预后指数(PI),以准确估计LUAD中的存活:PI = Sigma EXP(风险基因)X HRRRISK(基因)。此外,32-基因签名是管道(HR& 1; P <0.05,通过多变量分析)的独立预后指示剂。基于相关基因的p值,对三种风险LNCRNA-FAM138B,NHEG1和TLX1NB-and的加权基因共表达网络分析(WGCNA),并通过Miranda预测与这些LNCRNA结合的前27个miRNA。目标mirnas。接下来,将这些靶MiRNA转移到Tarbase,Mirtarbase,Mirecards和Starbase V2.0数据库中以获得其靶基因。根据先前的miRNA-mRNA和miRNA-LNCRNA数据,基于29个预后MRNA建立了三种LNCRNA-miRNA-mRNA Cerna网络,在拉德形成了监管网络。本研究提供了对拉德的LNCRNA相关的Cerna网络的洞察力,并确定了潜在的诊断和预后生物标志物。

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