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Microarray data analysis reveals gene expression changes in response to ionizing radiation in MCF7 human breast cancer cells

机译:微阵列数据分析揭示了基因表达响应于MCF7人乳腺癌细胞中的电离辐射而变化

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The aim of this study was to identify potential therapeutic target genes for breast cancer (BC) by the investigation of gene expression changes after ionizing radiation (IR) in BC cells. Gene expression profile GSE21748, including BC cell line MCF-7 samples at different time points after IR treatment, were downloaded from Gene Expression Omnibus. Differentially expressed genes (DEGs) were identified in different time points following IR compared with cell samples before IR, respectively. Gene ontology functions and The Kyoto Encyclopedia of Genes and Genomes pathways of the overlapping DEGs were enriched using DAVID. Transcription factor (TFs)-encoding genes were identified from the overlapping DEGs, followed by construction of transcriptional regulatory network and co-expression network. A total of 864 overlapping DEGs were identified, which were significantly enriched in regulation of cell proliferation and apoptosis, and cell cycle process. We found that FOXD1, STAT6, XBP1, STAT2, LMO2, TFAP4, STAT3, STAT1 were hub nodes in the transcriptional regulatory network of the overlapping DEGs. The co-expression network of target genes regulated by STAT3, STAT1, STAT6 and STAT2 included some key genes such as BCL2L1. STAT1, STAT2, STAT3, STAT6, XBP1, BCL2L1, CYB5D2, ESCO2, and PARP2 were significantly affected by IR and they may be used as therapeutic gene targets in the treatment of BC.
机译:本研究的目的是通过在BC细胞中电离辐射(IR)之后的基因表达变化来确定乳腺癌(BC)的潜在治疗靶基因。基因表达谱GSE21748,包括在IR治疗后不同时间点的BC细胞系MCF-7样品,从基因表达Omnibus下载。在IR之后的不同时间点分别与IR之前的细胞样品相比,在不同的时间点中鉴定了差异表达的基因(DEGS)。基因本体功能和基因的京都植物和基因组的基因组富集的富集使用大卫富集。转录因子(TFS) - 从重叠的DEG鉴定出转录因子(TFS)基因,然后施加转录调节网络和共表达网络。鉴定了总共864个重叠的次数,这在细胞增殖和细胞凋亡的调节和细胞周期过程中显着富集。我们发现Foxd1,STAT6,XBP1,STAT2,LMO2,TFAP4,STAT3,Stat1是重叠段的转录调节网络中的集线器节点。 STAT3,STAT1,STAT6和Stat2调节的靶基因的共表达网络包括一些关键基因,例如BCL2L1。 STAT1,STAT2,STAT3,STAT6,XBP1,BCL2L1,CYB5D2,ESCO2和PARP2受IR的显着影响,并且它们可以用作治疗BC的治疗基因靶标。

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