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inFRank: a ranking-based identification of influential genes in biological networks

机译:inFRank:基于排名的生物网络中有影响力的基因鉴定

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摘要

Capturing the predominant driver genes is critical in the analysis of high-throughput experimental data; however, existing methods scarcely include the unique characters of biological networks. Herein we introduced a ranking-based computational framework (inFRank) to rank the proteins by their influence. Using inFRank, we identified the top 20 influential genes in hepatocellular carcinoma (HCC). Network analysis revealed a prominent community composed of 7 influential genes. Intriguingly, five genes among the community were critical for mitotic spindle assembly checkpoint (SAC), suggesting that dysregulation of SAC could be a distinct feature of HCC and targeting SAC-associated genes might be a promising therapeutic strategy. Cox regression analysis revealed that CDC20 exerted as an independent risk factor for patient survival, indicating that CDC20 could be a novel biomarker for HCC prognosis. inFRank was then used for pan-cancer study, and all of the most influential genes in 18 cancers were achieved. We identified altogether 19 genes that were important in multiple cancers, and observed that cancers originating from the same organ or function-related organs tended to share more influential genes. Collectively, our results demonstrated that the inFRank was a powerful approach for deep interpretation of high-throughput data and better understanding of complex diseases.
机译:捕获主要的驱动基因对于分析高通量实验数据至关重要。然而,现有方法几乎没有包括生物网络的独特特征。在这里,我们介绍了一种基于排名的计算框架(inFRank),可以根据蛋白质的影响对其进行排名。使用inFRank,我们鉴定了肝细胞癌(HCC)的前20个有影响力的基因。网络分析揭示了一个由7个有影响基因组成的杰出社区。有趣的是,群落中的五个基因对于有丝分裂纺锤体装配检查点(SAC)至关重要,这表明SAC失调可能是HCC的独特特征,而靶向SAC相关基因可能是一种有前途的治疗策略。 Cox回归分析显示CDC20成为患者生存的独立危险因素,表明CDC20可能是HCC预后的新生物标志物。然后将inFRank用于泛癌研究,并获得了18种癌症中所有最有影响力的基因。我们共鉴定了19种在多种癌症中重要的基因,并观察到源自同一器官或功能相关器官的癌症倾向于共享更多有影响力的基因。总体而言,我们的结果表明,inFRank是深度解释高通量数据和更好地了解复杂疾病的有力方法。

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