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Comprehensive analysis of the whole coding and non-coding RNA transcriptome expression profiles and construction of the circRNA-lncRNA co-regulated ceRNA network in laryngeal squamous cell carcinoma

机译:综合分析整个编码和非编码RNA转录组表达谱和喉鳞状细胞癌中Circrna-lncrNA共调节Cerna网络的构建

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Recently, accumulating evidence has demonstrated that non-coding RNAs (ncRNAs) play a vital role in oncogenicity. Nevertheless, the regulatory mechanisms and functions remain poorly understood, especially for lncRNAs and circRNAs. In this study, we simultaneously detected, for the first time, the expression profiles of the whole transcriptome, including miRNA, circRNA and lncRNA + mRNA, in five pairs of laryngeal squamous cell carcinoma (LSCC) and matched non-carcinoma tissues by microarrays. Five miRNAs, four circRNAs, three lncRNAs and five mRNAs that were dysregulated were selected to confirm the verification of the microarray data by quantitative real-time PCR (qRT-PCR) in 20 pairs of LSCC samples. We constructed LSCC-related competing endogenous RNA (ceRNA) networks of lncRNAs and circRNAs (circRNA or lncRNA-miRNA-mRNA) respectively. Functional annotation revealed the lncRNA-mediated ceRNA network were enriched for genes involved in the tumor-associated pathways. Hsa_circ_0033988 with the highest degree in the circRNA-mediated ceRNA network was associated with fatty acid degradation, which was responsible for the depletion of fat in tumor-associated cachexia. Finally, to clarify the ncRNA co-regulation mechanism, we constructed a circRNA-lncRNA co-regulated network by integrating the above two networks and identified 9 modules for further study. A subnetwork of module 2 with the most dysregulated microRNAs was extracted to establish the ncRNA-involved TGF--associated pathway. In conclusion, our findings provide a high-throughput microarray data of the coding and non-coding RNAs and establish the foundation for further functional research on the ceRNA regulatory mechanism of non-coding RNAs in LSCC.
机译:最近,累积证据表明,非编码RNA(NCRNA)在雌性发生性中发挥着至关重要的作用。尽管如此,监管机制和功能仍然明显,特别是对于LNCRNA和Circrnas。在这项研究中,我们同时检测到整个转录组的表达谱,包括MiRNA,CircRNA和LNCrNA + mRNA,其中五对喉鳞状细胞癌(LSCC)和通过微阵列匹配的非癌组织。选择了五种miRNA,四个CircrNA,三个LNCRNA和五个MRNA,以确认通过数量实时PCR(QRT-PCR)在20对LSCC样品中通过定量实时PCR(QRT-PCR)验证。我们分别构建了LNCRNA和Circrnas(Circrna或Lncrna-mRNA)的LSCC相关的竞争内源性RNA(Cerna)网络。功能注释显示出富含LNCRNA介导的Cerna网络,富集涉及肿瘤相关途径的基因。 HSA_CIRC_0033988具有最高程度的CircrNA介导的Cerna网络与脂肪酸降解有关,这是肿瘤相关的恶病症中脂肪的枯竭。最后,为了阐明NCRNA共调控机制,通过将上述两个网络集成并识别出9个模块进行进一步研究,我们构建了CircRNA-lncrNA共调控网络。提取模块2的模块2的子网,提取具有最多的微小RORNA,以建立NCRNA涉及的TGF相关途径。总之,我们的研究结果提供了编码和非编码RNA的高通量微阵列数据,并建立了对LSCC中非编码RNA的CERNA调节机制进一步功能研究的基础。

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