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首页> 外文期刊>Cancer biology & therapy >Co-expression network analysis of long noncoding RNAs (IncRNAs) and cancer genes revealsSFTTWP and CASC2abnormalities in lung squamous cell carcinoma
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Co-expression network analysis of long noncoding RNAs (IncRNAs) and cancer genes revealsSFTTWP and CASC2abnormalities in lung squamous cell carcinoma

机译:长不用RNA(Incrnas)和癌症基因的共表达网络分析显示肺鳞状细胞癌中的术略量和Casc2

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摘要

ABSTRACT. Lung squamous cell carcinoma(LSCC) is the most common and aggressive lung tumor with poor clinical outcome. Previously studies showed that deregulation of long noncoding RNAs (IncRNAs) were involved in LSCC. We intended to figure out the role of IncRNAs in the regulation process of cancer-related genes and pathways they are involved. Data of 552 samples, including 501 cancer samples and 51 normal ones, were extracted from The Cancer Genome Atlas (TCGA). Differentially expressed IncRNAs (DEIs) were screened out (FDR<0.05, |logFC|>1) and then followed by GO ontology and KEGG annotation analysis. Oncogenes from COSMIC data set and Tumor suppressor genes (TSGs) from TSGene data set were collected and analyzed by gene Set Enrichment Analysis (GSEA) . The differentially expressed oncogenes and tumor supressor gene (TSGs) were obtained and co-expression analysis was conducted to generate co-expression IncRNA-gene pairs, which can be helpful in figuring out the role of IncRNA in the regulation of oncogenes and tumor suppressor genes. A total of 31 IncRNAs with low expression levels and 37 IncRNAs with high expression levels were screened out and most of them were enriched in pathways such as meiosis, male gamete generation, defensins. Of note, SFTA1P and CASC2 were found to be related with most of the oncogenes and TSGs by co-expression analysis. We suggested SFTA1P and CASC2 played important role in the regulation of both oncogene and TSGs during the carcinogenesis of LSCC and have the potential to be applied in future diagnosis, prognostic process and target therapy of LSCC
机译:抽象的。肺鳞状细胞癌(LSCC)是最常见而激进的肺肿瘤,临床结果不佳。以前的研究表明,LONCC的LONCOD NNAS(Incrnas)的放松管制参与LSCC。我们打算弄清楚Incrnas在癌症相关基因和途径的调节过程中的作用。从癌症基因组地图集(​​TCGA)中提取552个样品的数据,包括501个癌症样品和51个正常情况。筛选差异表达的Incrnas(DEI)(FDR <0.05,| logfc |> 1),然后用GO本体和KEGG注释分析。收集来自来自Tsgene数据集的宇宙数据集和肿瘤抑制基因(TSG)的癌肠化合物,并通过基因设定富集分析(GSEA)分析。得到差异表达的癌素和肿瘤的癌基因(TSG),并进行共表达分析以产生共表达IncRNA-基因对,这有助于图解IncRNA在调节癌肠和肿瘤抑制基因中的作用。筛选出总共31例具有低表达水平和37个Incrnas的Incrnas,并且其中大部分富含Meiosis,男性配子生成,防御素等途径。注意,发现SFTA1P和CASC2通过共表达分析与大多数癌基因和TSG相关。我们建议SFTA1P和Casc2在LSCC的致癌过程中调节癌基因和TSG的调节中发挥着重要作用,并具有在未来诊断,预后过程和LSCC的靶治疗中应用的可能性

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