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首页> 外文期刊>Frontiers in Cell and Developmental Biology >Genome-Wide Analysis of the Expression of Circular RNA Full-Length Transcripts and Construction of the circRNA-miRNA-mRNA Network in Cervical Cancer
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Genome-Wide Analysis of the Expression of Circular RNA Full-Length Transcripts and Construction of the circRNA-miRNA-mRNA Network in Cervical Cancer

机译:基因组分析宫颈癌循环RNA全长转录物的表达及Circrna-miRNA-mRNA网络的构建

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Increasing evidence suggests that circular RNA (circRNA) plays an important role in tumorigenesis by regulating gene expression at the transcriptional and post-transcriptional levels. Alternative splicing events permit multiple transcript isoforms of circRNA to be produced; however, changes in the expression of circRNA full-length transcripts in cervical cancer remain unclear. Here, we systematically explored the dysregulation circRNA full-length transcripts and constructed an improved circRNA-miRNA-mRNA regulatory network to provide potential biomarkers and possible treatment targets in cervical cancer. We identified 9359 circular full-length transcripts from RNase R-treated RNA-seq data in cervical cancer, of which 353 circular full-length transcripts were significantly differentially expressed (DE) between the tumor and normal group. A total of 881 DE mRNA transcript isoforms were also identified from total RNA-seq data in cervical cancer, of which 421 (47.8%) transcript isoforms were up-regulated, and 460 (52.2%) transcript isoforms were down-regulated in tumor samples. A circRNA-miRNA-mRNA competitively regulated network, including 33 circRNA transcripts, 2 miRNAs, and 189 mRNA transcripts was constructed. Three genes (COPE, RAB3B, and TFPI) in the network were significantly associated with overall survival (P 0.05), which indicated that these genes could act as prognostic biomarkers for patients with cervical cancer. Our study revealed genome-wide differential expression of full-length circRNA transcripts and constructed a more accurate circRNA-miRNA-mRNA network at the full-length transcript expression level in cervical cancer. CircRNA may thus be involved in the development of cervical cancer by regulating the expression of COPE, RAB3B, and TFPI. However, the specific regulatory mechanism in cervical cancer requires further study.
机译:越来越多的证据表明,通过调节转录和转录后水平的基因表达,圆形RNA(CircrNA)在肿瘤内发挥着重要作用。替代剪接事件允许生产多种转录同种型卷发;然而,宫颈癌中CircrNA全长转录物表达的变化仍然不清楚。在这里,我们系统地探索了呼吸困难CircrNA全长转录物,并构建了一种改进的CircrNA-miRNA-mRNA调节网络,以提供潜在的生物标志物和宫颈癌中可能的治疗靶标。我们确定了来自宫颈癌的RNase r治疗的RNA-SEQ数据的9359个圆形全长转录物,其中353个圆形全长转录物在肿瘤和正常组之间显着表达(DE)。还从宫颈癌中的总RNA-SEQ数据中鉴定了总共881℃转录同种型,其中421(47.8%)转录同种型是上调的,460(52.2%)转录同种型在肿瘤样品中下调。 Circrna-miRNA-mRNA竞争性调节网络,包括33种CircRNA转录物,2 miRNA和189例mRNA转录物。网络中的三个基因(应对,Rab3b和TFPI)与总存活率显着相关(P <0.05),表明这些基因可作为宫颈癌患者的预后生物标志物。我们的研究揭示了全长CircrNA转录物的基因组差异表达,并在宫颈癌的全长转录表达水平下构建了更准确的CircRNA-miRNA-mRNA网络。因此,CircRNA可以通过调节COPE,RAB3B和TFPI的表达,参与宫颈癌的发育。然而,宫颈癌的特定调节机制需要进一步研究。

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