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首页> 外文期刊>Oncology letters >Identification of candidate RNA signatures in triple-negative breast cancer by the construction of a competing endogenous RNA network with integrative analyses of Gene Expression Omnibus and The Cancer Genome Atlas data
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Identification of candidate RNA signatures in triple-negative breast cancer by the construction of a competing endogenous RNA network with integrative analyses of Gene Expression Omnibus and The Cancer Genome Atlas data

机译:鉴别基因表达综合分析竞争内源性RNA网络鉴定三阴性乳腺癌中的候选RNA签名及癌症基因组ATLAS数据

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摘要

Triple-negative breast cancer (TNBC) is a subtype of breast cancer that is characterized by aggressive and metastatic clinical characteristics and generally leads to earlier distant recurrence and poorer prognosis than other molecular subtypes. Accumulating evidence has demonstrated that long non-coding RNAs (lncRNAs) serve a crucial role in a wide variety of biological processes by interacting with microRNAs (miRNAs) as competing endogenous RNAs (ceRNAs) and, thus, affect the expression of target genes in multiple types of cancer. Seven datasets from the Gene Expression Omnibus (GEO) database, including 444 tumor and 88 healthy tissue samples, were utilized to investigate the underlying mechanisms of TNBC and identify prognostic biomarkers. Differentially expressed genes (DEGs) were further validated in The Cancer Genome Atlas database and the associations between their expression levels and clinical information were analyzed to identify prognostic values. A potential lncRNA-miRNA-mRNA ceRNA network was also constructed. Finally, 69 mRNAs from the integrated Gene Expression Omnibus datasets were identified as DEGs using the robust rank aggregation method with |log2FC|>1 and adjusted P<0.01 set as the significance cut-off levels. In addition, 29 lncRNAs, 21 miRNAs and 27 mRNAs were included in the construction of the ceRNA network. The present study elucidated the mechanisms underlying the progression of TNBC and identified novel prognostic biomarkers for TNBC.
机译:三重阴性乳腺癌(TNBC)是乳腺癌的亚型,其特征在于侵袭性和转移性临床特征,并且通常导致早期的远程复发和预后的预后多于其他分子亚型。累积证据表明,长期非编码RNA(LNCRNA)通过与竞争内源RNA(CERNAS)相互作用,通过与MicroRNAs(MiRNA)相互作用,为多种生物过程中的一种至关重要的作用,从而影响多个靶基因的表达癌症的类型。来自基因表达的七种数据集(Geo)数据库(包括444个肿瘤和88个健康组织样品,用于研究TNBC的潜在机制并鉴定预后生物标志物。在癌症基因组Atlas数据库中进一步验证了差异表达的基因(DEGS),分析了它们的表达水平与临床信息之间的关联以鉴定预后值。还构建了潜在的LNCRNA-miRNA-mRNA Cerna网络。最后,使用稳健的级别聚集方法与综合基因表达综合基因表达的69mRNA使用稳健的级别聚集方法用| LOG2FC |> 1和调整的P <0.01设定为显着的截止水平。此外,29个LNCRNA,21 miRNA和27 mRNA被列入Cerna网络的建设中。本研究阐明了TNBC进展的基础,并确定了TNBC的新型预后生物标志物。

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