Network Analysis in the Identification of Genes Conferring Metastatic Potential in Hepatocellular Carcinoma

Yin-Quan Tang
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Abstract

Objectives: Hepatocellular carcinoma (HCC) is a common liver cancer accounting with high mortality rate owing to metastasis. Anti-metastatic treatment is scant while proposed mechanisms are in excess, yet specific molecular drivers of HCC remain at large. Therefore, our study aims to identify drivers of HCC metastasis using protein-protein interaction (PPI) networks to identify key driver genes associated with HCC metastasis. Methods: From differential expression genes (DEGs) analysis using GSE45114 microarray dataset, four main hub genes that correlated with patient survival were identified. The first hub gene, SERPINC1 had the highest centrality parameter in impeding HCC metastasis, implicating thrombin mediation through thrombin-induced tumor growth and angiogenesis. Results: Our study reveals that thrombin was not differentially expressed, hence, suggesting the involvement of other, less-well studied pathways in impeding metastasis, such as KNG1, PAH, AMBP, and TTR. Findings for CD44 were consistent with existing literature. Meanwhile, FGG and APOA5, both less studied genes in the context cancer metastasis studies, were found to be crucial in impeding HCC metastasis. Conclusion: This study identified four potential proteins (SERPINC1, CD44, FGG and APOA5) to be therapeutic targets or biomarkers and demonstrates the use of PPI networks for understanding HCC metastasis at a more profound level.
鉴别肝细胞癌转移潜能基因的网络分析
目的:肝细胞癌(HCC)是一种常见的肝癌,因转移而死亡率高。抗转移治疗缺乏,而提出的机制过多,但HCC的特定分子驱动因素仍然很大。因此,我们的研究旨在通过蛋白-蛋白相互作用(PPI)网络确定HCC转移的驱动因素,以确定与HCC转移相关的关键驱动基因。方法:利用GSE45114微阵列数据集对差异表达基因(DEGs)进行分析,鉴定出与患者生存相关的4个主要枢纽基因。第一个枢纽基因serpin1在阻止HCC转移中具有最高的中心性参数,暗示凝血酶通过凝血酶诱导的肿瘤生长和血管生成介导。结果:我们的研究显示凝血酶没有差异表达,因此,提示其他研究较少的途径参与了阻止转移,如KNG1, PAH, AMBP和TTR。CD44的发现与现有文献一致。同时,FGG和APOA5这两个在癌症转移研究中研究较少的基因在阻止HCC转移中发挥了关键作用。结论:本研究确定了四个潜在的蛋白(serpin1、CD44、FGG和APOA5)作为治疗靶点或生物标志物,并证明了PPI网络在更深入的层面上用于了解HCC转移。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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CiteScore
5.60
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