Identification and Validation of a Novel Prognostic Signature of Gastric Cancer Based on Seven Complement System-Related Genes: An Integrated Analysis.

IF 1.5 4区医学 Q4 BIOTECHNOLOGY & APPLIED MICROBIOLOGY

Critical Reviews in Eukaryotic Gene Expression Pub Date : 2025-01-01 DOI:10.1615/CritRevEukaryotGeneExpr.2024057000

Jiaxing Zhang, Weijing Zhu, Shengrui Yang, Jie Liu, Futian Tang, Yumin Li

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引用次数: 0

Abstract

The complement system (CS) is linked to the progression of gastric cancer (GC), which has a high mortality rate, though its mechanisms in GC remain unclear. This study aims to identify CS-related prognostic genes with causal links to GC, and to investigate their mechanisms. The intersection between differentially expressed genes (DEGs) obtained from the TCGA-STAD dataset and CS-related genes (CRGs) was defined as differentially expressed CRGs (DCRGs). Prognostic genes with a causal association with GC (pCDCRGs) were sequentially identified via Mendelian randomization (MR) analysis and Cox and least absolute shrinkage and selection operator (LASSO) regression analyses, followed by expression analysis. A gene signature and a nomogram were then established based on pCDCRGs and independent prognostic factors. Subsequent analyses focused on functional enrichment, immune relevance, drug sensitivity, gene interactions, and molecular regulatory networks. Eventually, reverse transcription-quantitative PCR (RT-qPCR) was employed to validate expression of pCDCRGs. DCRGs were obtained from the intersection of 8,418 DEGs and 241 CRGs. Among 12 DCRGs with causal association (CDCRGs) with GC, 7 genes were identified as pCDCRGs, including FANCG, FANCF, F2R, C4BPA, SERPINF2, PROC, and CD59. Notably, CD59 was markedly highly expressed in the normal group, whereas the other genes were markedly highly expressed in the GC group. Afterward, an accurate pCDCRG signature was developed. Risk score, age, and stage were recognized as independent risk factors, and the constructed nomogram demonstrated strong predictive accuracy. Additionally, analyses indicated that these 7 pCDCRGs may influence GC by affecting pathways such as complement and coagulation cascades, immune cell infiltration, immune characteristics, immunotherapy responses, and drug sensitivity. These effects may be linked to gene interactions and the regulatory roles of lncRNAs like RMRP and miRNAs such as hsa-mir-613. RT-qPCR showed C4BPA, PROC, F2R, and SERPINF2 were markedly up-regulated, whereas CD59 was markedly down-regulated in GC tissues. This study identified seven complement system-related prognostic genes with causal links to GC, based on which we developed a highly predictive 7-pCDCRG signature, providing valuable insights for clinical prognostic prediction and immunotherapy in GC patients.

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基于7个补体系统相关基因的胃癌新预后特征的鉴定和验证：一项综合分析。

补体系统（CS）与胃癌（GC）的发展有关，胃癌（GC）具有高死亡率，尽管其在胃癌中的机制尚不清楚。本研究旨在鉴定与GC有因果关系的cs相关预后基因，并探讨其机制。从TCGA-STAD数据集中获得的差异表达基因（DEGs）与cs相关基因（CRGs）之间的交集被定义为差异表达的CRGs （DCRGs）。通过孟德尔随机化（MR）分析、Cox和最小绝对收缩和选择算子（LASSO）回归分析，依次确定与GC有因果关系的预后基因（pCDCRGs），然后进行表达分析。然后根据pCDCRGs和独立预后因素建立基因标记和nomogram。随后的分析集中在功能富集、免疫相关性、药物敏感性、基因相互作用和分子调控网络上。最后，采用逆转录定量PCR （RT-qPCR）验证pCDCRGs的表达。从8418个deg和241个crg的交叉点获得dcrg。在12个与GC有因果关系的DCRGs （CDCRGs）中，有7个基因被鉴定为pCDCRGs，包括FANCG、FANCF、F2R、C4BPA、serinf2、PROC和CD59。值得注意的是，CD59在正常组中显著高表达，而其他基因在GC组中显著高表达。随后，开发了准确的pCDCRG信号。风险评分、年龄和分期被认为是独立的危险因素，构建的nomogram具有较强的预测准确性。此外，分析表明，这7种pCDCRGs可能通过影响补体和凝血级联、免疫细胞浸润、免疫特性、免疫治疗反应和药物敏感性等途径影响GC。这些影响可能与基因相互作用和lncrna（如RMRP）和mirna（如hsa-mir-613）的调控作用有关。RT-qPCR结果显示，GC组织中C4BPA、PROC、F2R和serinf2明显上调，而CD59明显下调。本研究确定了7个与胃癌有因果关系的补体系统相关预后基因，在此基础上，我们开发了一个具有高度预测性的7-pCDCRG特征，为胃癌患者的临床预后预测和免疫治疗提供了有价值的见解。

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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来源期刊

Critical Reviews in Eukaryotic Gene Expression 生物-生物工程与应用微生物

CiteScore

2.70

自引率

0.00%

发文量

审稿时长

1 months

期刊介绍： Critical ReviewsTM in Eukaryotic Gene Expression presents timely concepts and experimental approaches that are contributing to rapid advances in our mechanistic understanding of gene regulation, organization, and structure within the contexts of biological control and the diagnosis/treatment of disease. The journal provides in-depth critical reviews, on well-defined topics of immediate interest, written by recognized specialists in the field. Extensive literature citations provide a comprehensive information resource. Reviews are developed from an historical perspective and suggest directions that can be anticipated. Strengths as well as limitations of methodologies and experimental strategies are considered.