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生物信息学分析鉴定出 COL1A1、THBS2 和 SPP1 可作为胃癌患者预后和免疫治疗反应的潜在预测因子。

Bioinformatics analysis identifies COL1A1, THBS2 and SPP1 as potential predictors of patient prognosis and immunotherapy response in gastric cancer.

机构信息

Department of Oncology, Tongji Hospital, Tongji Medical College, Huazhong University of Science and Technology, Wuhan, Hubei, China.

出版信息

Biosci Rep. 2021 Jan 29;41(1). doi: 10.1042/BSR20202564.

Abstract

BACKGROUND

The present study aimed to use bioinformatics tools to explore pivotal genes associated with the occurrence of gastric cancer (GC) and assess their prognostic significance, and link with clinicopathological parameters. We also investigated the predictive role of COL1A1, THBS2, and SPP1 in immunotherapy.

MATERIALS AND METHODS

We identified differential genes (DEGs) that were up- and down-regulated in the three datasets (GSE26942, GSE13911, and GSE118916) and created protein-protein interaction (PPI) networks from the overlapping DEGs. We then investigated the potential functions of the hub genes in cancer prognosis using PPI networks, and explored the influence of such genes in the immune environment.

RESULTS

Overall, 268 overlapping DEGs were identified, of which 230 were up-regulated and 38 were down-regulated. CytoHubba selected the top ten hub genes, which included SPP1, TIMP1, SERPINE1, MMP3, COL1A1, BGN, THBS2, CDH2, CXCL8, and THY1. With the exception of SPP1, survival analysis using the Kaplan-Meier database showed that the levels of expression of these genes were associated with overall survival. Genes in the most dominant module explored by MCODE, COL1A1, THBS2, and SPP1, were primarily enriched for two KEGG pathways. Further analysis showed that all three genes could influence clinicopathological parameters and immune microenvironment, and there was a significant correlation between COL1A1, THBS2, SPP1, and PD-L1 expression, thus indicating a potential predictive role for GC response to immunotherapy.

CONCLUSION

ECM-receptor interactions and focal adhesion pathways are of great significance in the progression of GC. COL1A1, THBS2, and SPP1 may help predict immunotherapy response in GC patients.

摘要

背景

本研究旨在利用生物信息学工具探索与胃癌(GC)发生相关的关键基因,并评估其预后意义,并与临床病理参数相关联。我们还研究了 COL1A1、THBS2 和 SPP1 在免疫治疗中的预测作用。

材料和方法

我们从三个数据集(GSE26942、GSE13911 和 GSE118916)中鉴定出上调和下调的差异基因(DEGs),并从重叠的 DEGs 中创建蛋白质-蛋白质相互作用(PPI)网络。然后,我们使用 PPI 网络研究了核心基因在癌症预后中的潜在功能,并探讨了这些基因在免疫环境中的影响。

结果

总的来说,鉴定出 268 个重叠的 DEG,其中 230 个上调,38 个下调。CytoHubba 选择了前十个核心基因,包括 SPP1、TIMP1、SERPINE1、MMP3、COL1A1、BGN、THBS2、CDH2、CXCL8 和 THY1。除了 SPP1 之外,使用 Kaplan-Meier 数据库的生存分析表明,这些基因的表达水平与总生存率相关。通过 MCODE 探索的最主要模块中的基因,COL1A1、THBS2 和 SPP1,主要富集在两个 KEGG 途径中。进一步分析表明,这三个基因都可以影响临床病理参数和免疫微环境,并且 COL1A1、THBS2、SPP1 和 PD-L1 的表达之间存在显著相关性,因此表明它们可能对 GC 对免疫治疗的反应具有预测作用。

结论

细胞外基质-受体相互作用和焦点粘连途径在 GC 的进展中具有重要意义。COL1A1、THBS2 和 SPP1 可能有助于预测 GC 患者的免疫治疗反应。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f507/7796188/793bcea8e24e/bsr-41-bsr20202564-g1.jpg

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