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MicroRNA induction by copy number gain is associated with poor outcome in squamous cell carcinoma of the lung

机译:拷贝数增加引起的MicroRNA诱导与肺鳞状细胞癌预后不良有关

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摘要

Copy number gains in cancer genomes have been shown to induce oncogene expression and promote carcinogenesis; however, their role in regulating oncogenic microRNAs (onco-miRNAs) remains largely unknown. Our aim was to identify onco-miRNAs induced by copy number gains in human squamous cell carcinoma (Sq) of the lung. We performed a genome-wide screen of onco-miRNAs from 245 Sqs using data sets from RNA-sequencing, comparative genomic hybridization, and the corresponding clinical information from The Cancer Genome Atlas. Among 1001 miRNAs expressed in the samples, 231 were correlated with copy number alternations, with only 11 of these being highly expressed in Sq compared to adenocarcinoma and normal tissues. Notably, miR-296-5p, miR-324-3p, and miR-3928-3p expression was significantly associated with poor prognosis. Multivariate analysis using the Cox proportional hazards model showed that miRNA expression and smoking were independent prognostic factors and were associated with poor prognosis. Furthermore, the three onco-miRNAs inhibited FAM46C to induce MYC expression, promoting proliferation of Sq cells. We found that copy number gains in Sq of the lung induce onco-miRNA expression that is associated with poor prognosis.
机译:已经显示,癌症基因组中拷贝数的增加可诱导癌基因表达并促进癌变。然而,它们在调控致癌微RNA(onco-miRNA)中的作用仍然未知。我们的目的是鉴定人肺鳞状细胞癌(Sq)中拷贝数增加引起的癌基因miRNA。我们使用来自RNA测序,比较基因组杂交的数据集以及来自The Cancer Genome Atlas的相应临床信息,对245 Sqs上的onco-miRNA进行了全基因组筛选。在样品中表达的1001个miRNA中,有231个与拷贝数变化相关,与腺癌和正常组织相比,其中只有11个在Sq中高表达。值得注意的是,miR-296-5p,miR-324-3p和miR-3928-3p表达与不良预后显着相关。使用Cox比例风险模型进行的多变量分析显示,miRNA表达和吸烟是独立的预后因素,并与不良预后相关。此外,这三种癌基因-miRNA抑制FAM46C诱导MYC表达,促进Sq细胞增殖。我们发现,肺Sq中拷贝数的增加会诱导与不良预后相关的癌基因-miRNA表达。

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