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Identification of genes and pathways involved in malignant pleural mesothelioma using bioinformatics methods

机译:使用生物信息学方法鉴定涉及恶性胸膜间皮瘤的基因和途径

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Malignant pleural mesothelioma (MPM) is a rare tumor in the?pleura. This study was carried out to identify key genes and pathways that may be involved in MPM. Microarray datasets GSE51024 and GSE2549 were analyzed for differentially expressed genes (DEGs) between normal and MPM tissues. The identified DEGs were subjected to functional analyses using bioinformatics tools. A total of 276 DEGs were identified, consisting of 187 downregulated and 79 upregulated genes. Gene ontology and Kyoto encyclopedia of genes and genomes pathway enrichment analysis indicated that the DEGs were enriched in extracellular structure organization, extracellular matrix, and ECM?receptor interaction. Due to high degree of connectivity among 24 hub genes, EZH2 and HMMR are likely to play roles in the carcinogenesis and progression of MPM. The two genes were found over-expressed in MPM tissues. Patients with elevated EZH2 and HMMR expressions had poor overall survival. EZH2 and HMMR are identified to be the hub genes for MPM and they may be further characterized to better understand the molecular mechanisms underlying the carcinogenesis of MPM.
机译:恶性胸膜间皮瘤(MPM)是葡萄牙膜的罕见肿瘤。进行该研究以鉴定可能参与MPM的关键基因和途径。分析微阵列数据集GSE51024和GSE2549在正常和MPM组织之间进行差异表达基因(DEGS)。使用生物信息学工具对已鉴定的可进行功能分析。鉴定了总共276℃,由187个下调和79个上调基因组成。基因本体和京都基因型途径途径浓缩分析表明,富含细胞外结构组织,细胞外基质和ECM的富集蛋白酶相互作用。由于24个枢纽基因之间的高连接性,EZH2和HMMR可能在致癌物中发挥作用和MPM的进展。发现两种基因在MPM组织中过度表达。 EZH2和HMMR表达升高的患者总体存活差。 EZH2和HMMR被鉴定为MPM的轮毂基因,并且它们可以进一步表征以更好地了解MPM的致癌物质下面的分子机制。

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