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Construction and validation of a TP53-associated immune prognostic model for gastric cancer

机译:胃癌TP53相关免疫预后模型的构建与验证

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Increasing evidence indicates that TP53 mutation impacts the patients prognosis by regulating the gastric cancer (GC) immunophenotype. An immune prognostic signature (IPS) was constructed based on TP53 status. The effects of the IPS on the immune microenvironment of GC were analyzed. We also constructed a nomogram integrating the IPS and other clinical factors. An IPS was constructed in the TCGA cohort and validated in the meta-GEO cohort. TP53 mutation resulted in the downregulation of the immune response in GC. Concretely, high-risk patients were characterized by increased monocyte, macrophage M0 and T cell follicular helper infiltration; increased stromal score, ESTIMATE score and immune score; higher TIM3 and BTLA expression; and decreased dendritic cell and T cell CD4 memory-activated infiltration and tumor purity. The nomogram also showed good predictive performance. These results suggest that the IPS is an effective prognostic indicator for GC patients, which might provide a theoretical foundation for immunotherapy.
机译:越来越多的证据表明TP53突变通过调节胃癌(GC)免疫型型来影响患者预后。根据TP53状态构建免疫预后签名(IPS)。分析了IP对GC免疫微环境的影响。我们还构建了一种集成IP和其他临床因素的载体图。 IPS在TCGA队列中构建并在Meta-Geo Cohort中验证。 TP53突变导致GC中免疫应答的下调。具体而言,高风险的患者的特征是单核细胞,巨噬细胞M0和T细胞毛囊渗透渗透增加;增加基质分数,估计分数和免疫评分;较高的tim3和btla表达;并且降低树突细胞和T细胞CD4记忆激活渗透和肿瘤纯度。 NOM图还显示出良好的预测性能。这些结果表明,IPS是GC患者的有效预后指标,这可能为免疫疗法提供理论基础。

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