预测肺腺癌的新型厌氧相关基因特征

Mengying Xiao , Yong Li , Yusheng Zhou , Xingyun Liu , Guotao Tang
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引用次数: 0

摘要

方法基于TCGA数据库中的基因表达矩阵,我们通过加权基因共表达网络分析(WGCNA)建立了共表达模块。然后,我们根据 WGCNA 结果、DEGs 和 345 个 ANRGs 确定了 LUAD 与正常样本之间差异表达的 ANRGs(DE-ANGs)。利用GO和KEGG数据库解释了DE-ANRGs的生物功能。使用单变量和多变量回归模型来验证风险模型是否可作为独立的预后因素。结果56个DE-ANRGs在肿瘤组织中的表达存在显著差异。我们建立了一个4-ANRG预后特征。在TCGA队列和外部GSE31210验证队列中,高风险组的OS明显低于低风险组。此外,风险模型的预测性能在 ROC 曲线上得到了很好的验证。此外,单变量 COX 分析和多变量 Cox 分析均表明,风险评分可作为 LUAD 患者的独立预后因素。校准曲线和 C 指数表明,提名图在预测 LUAD 患者的 1 年、3 年和 5 年生存率方面效果令人满意。
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A novel anoikis-related gene signature predicts in lung adenocarcinoma

Objective

To generate a prognostic model prognosis based on anoikis-related genes (ANRGs) expression for Lung adenocarcinoma (LUAD), an exploration of the prognostic value of ANRGs in LUAD was conducted.

Methods

Based on the expression matrix of genes from the TCGA database, we built the co-expressed modules by weighted gene co-expression network analysis (WGCNA). Then we identified the differentially expressed ANRGs (DE-ANGs) between LUAD and normal samples by the WGCNA results, DEGs, and the 345 ANRGs. The biofunction of the DE-ANRGs was interpreted using the GO and KEGG databases. Univariate and multivariate regression models were used to verify whether the risk model could serve as an independent prognostic factor. A nomogram was utilized to predict overall survival (OS) in LUAD.

Results

The expression of 56 DE-ANRGs was significantly different in tumor tissues. We established a 4-ANRG prognostic signature. In the TCGA cohort and the external GSE31210 validation cohort, the OS of the high-risk group was lower than that of the low-risk group significantly. Moreover, the prediction performance of the risk model was excellently verified by the ROC curve. In addition, both univariate COX and multivariate Cox analyses indicated that risk score could act as an independent prognostic factor for LUAD patients. The calibration curve and C-index demonstrated that the nomogram was satisfactory in predicting 1, 3- and 5-year survival in LUAD patients.

Conclusions

Our study developed a novel prognostic signature of 4 ANRGs with Excellent prognostic performance for LUAD patients.

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