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首页> 外文期刊>DNA and Cell Biology >Identification of Key Genes in Association with Progression and Prognosis in Cervical Squamous Cell Carcinoma
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Identification of Key Genes in Association with Progression and Prognosis in Cervical Squamous Cell Carcinoma

机译:宫颈鳞状细胞癌进展和预后关联基因的鉴定

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摘要

Cervical cancer remains a primary cause of female death in developing countries, but its prognosis can be greatly improved if patients are diagnosed earlier. In the present study, we screened the common differentially expressed genes (DEGs) of cervical squamous cell carcinoma (CESC) from dataset GSE7803, Gene Expression Omnibus, and The Cancer Genome Atlas databases. An integrated bioinformatics analysis was performed based on these DEGs for their enrichment in functions and pathways, interaction network, prognostic signature, and candidate molecular drugs. As a result, 164 (114 upregulated and 47 downregulated) DEGs of CESC were identified for further investigation. We then conducted the gene ontology term enrichment and Kyoto Encyclopedia of Genes and Genomes Pathway analyses to reveal the underlying functions and pathways of these DEGs. In the protein-protein interaction network, hub module and hub genes were identified. Five genes of significant prognostic value-DSG2, ITM2A, CENPM, RIBC2, and MEIS2-were identified by prognostic signature analysis and used to construct a risk linear model. Further validation and investigation suggested DSG2 might be a key gene in CESC prognosis. We then identified two candidate small molecules (trichostatin A and tanespimycin) against CESC. Further validation and exploration of these hub genes are warranted for future prospect in clinical applications.
机译:宫颈癌仍然是发展中国家女性死亡的主要原因,但如果患者之前诊断,可以大大提高其预后。在本研究中,从数据集GSE7803,基因表达综合征和癌症基因组Atlas数据库中筛选颈鳞状细胞癌(CESC)的常见差异表达基因(CESC)。基于这些DEG来进行整合的生物信息学分析,用于其富集功能和途径,相互作用网络,预后签名和候选分子药物。结果,确定了164(114个上调和47个下调的CESC以进一步调查。然后,我们进行了基因本体论富集和京都的基因和基因组途径分析,揭示了这些DEG的潜在功能和途径。在蛋白质 - 蛋白质相互作用网络中,鉴定了集线器模块和轮毂基因。通过预后签名分析鉴定出明显预后值-DSG2,ITM2A,CENPM,RIBC2和MEIS2的五个基因,并用于构建风险线性模型。进一步的验证和调查表明DSG2可能是CESC预后的关键基因。然后我们确定了对CESC的两种候选小分子(Trichostatin A和Tanespimycin)。对临床应用的未来前景有必要进一步验证和探索。

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