GPX3-Mediated Oxidative Stress Affects Pyrimidine Metabolism Levels in Stomach Adenocarcinoma via the AMPK/mTOR Pathway

IF 2.2 4区 医学 Q2 MEDICINE, GENERAL & INTERNAL International Journal of Clinical Practice Pub Date : 2024-01-30 DOI:10.1155/2024/6875417
Yaowen Zhang, Yixin Yang, Shanshan Kuang, Yang Zhang, Hancheng Qin, Jisheng Xie
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Abstract

Background. Amino acid metabolism, including ATP production, nucleotide synthesis, and redox homeostatic processes, are associated with proliferation and differentiation of tumor cells. This study aimed to identify novel prognostic biomarkers and potential therapeutic targets of amino acid metabolism-related genes for stomach adenocarcinoma (STAD). Methods. RNA sequencing transcriptome data in the TCGA-STAD (training set) and GTEx datasets (validation set) were used. The LIMMA R program enabled the differentially expressed amino acid metabolism-related genes (AAMRGs) to be found. A prognostic risk score model based on clinical phenotypic features was built using LASSO regression and step multi-Cox analyses. Gene set enrichment analysis (GSEA) was used to find potential molecular pathways associated with STAD. Hierarchical cluster analysis was used to evaluate pyrimidine metabolism. Cultured STAD cells assessed the proliferation of STAD and upregulation of GPX3 expression by CCK8 and flow cytometry. Transwell and wound healing assays assessed the impact of GPX3 on invasion and migration of STAD cells. Western blot and qRT-PCR were used to measure changes in pyrimidine metabolism-related markers and active molecules involved in the AMPK/mTOR signaling pathway. Results. Three AAMRGs, DNMT1, F2R, and GPX3, could independently predict the course of STAD. Pyrimidine metabolism appeared to be significantly associated with these by GSEA and clustering analyses. Pyrimidine metabolism was negatively correlated with GPX3. Functional studies using an overexpressed GPX3 plasmid showed an enhanced migration and invasion of STAD cells as well as the expression of genes associated with pyrimidine metabolism and the AMPK/mTOR signaling pathway. By using a CAD siRNA, it was found that that GPX3 affected 5-fluorouracil resistance during de novo synthesis of pyrimidine through the CAD-UMPS signaling axis. Conclusions. GPX3 which regulates the level of pyrimidine metabolism through the AMPK/mTOR pathway was found to be closely associated with STAD. Our findings demonstrate GPX3 is a reliable biomarker for the prognosis of amino acid metabolism and a probable target for STAD therapy.

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GPX3 介导的氧化应激通过 AMPK/mTOR 通路影响胃腺癌的嘧啶代谢水平
背景。氨基酸代谢,包括 ATP 生成、核苷酸合成和氧化还原平衡过程,与肿瘤细胞的增殖和分化有关。本研究旨在确定胃腺癌(STAD)氨基酸代谢相关基因的新型预后生物标志物和潜在治疗靶点。研究方法使用 TCGA-STAD 数据集(训练集)和 GTEx 数据集(验证集)中的 RNA 测序转录组数据。利用 LIMMA R 程序找到了差异表达的氨基酸代谢相关基因(AAMRGs)。利用 LASSO 回归和阶跃多 Cox 分析建立了基于临床表型特征的预后风险评分模型。基因组富集分析(GSEA)用于寻找与 STAD 相关的潜在分子通路。层次聚类分析用于评估嘧啶代谢。培养的 STAD 细胞通过 CCK8 和流式细胞术评估了 STAD 的增殖和 GPX3 表达的上调。透孔试验和伤口愈合试验评估了 GPX3 对 STAD 细胞侵袭和迁移的影响。Western 印迹和 qRT-PCR 被用来测量嘧啶代谢相关标记物和参与 AMPK/mTOR 信号通路的活性分子的变化。结果显示三种AAMRGs(DNMT1、F2R和GPX3)可独立预测STAD的病程。通过GSEA和聚类分析,嘧啶代谢似乎与这些因素有显著关联。嘧啶代谢与 GPX3 呈负相关。使用过表达 GPX3 质粒进行的功能研究显示,STAD 细胞的迁移和侵袭能力增强,与嘧啶代谢和 AMPK/mTOR 信号通路相关的基因表达也增强。通过使用 CAD siRNA,研究发现 GPX3 通过 CAD-UMPS 信号轴影响了嘧啶从头合成过程中的 5 氟尿嘧啶耐药性。结论通过 AMPK/mTOR 通路调节嘧啶代谢水平的 GPX3 被发现与 STAD 密切相关。我们的研究结果表明,GPX3 是氨基酸代谢预后的可靠生物标志物,也是 STAD 治疗的可能靶点。
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来源期刊
CiteScore
5.30
自引率
0.00%
发文量
274
审稿时长
3-8 weeks
期刊介绍: IJCP is a general medical journal. IJCP gives special priority to work that has international appeal. IJCP publishes: Editorials. IJCP Editorials are commissioned. [Peer reviewed at the editor''s discretion] Perspectives. Most IJCP Perspectives are commissioned. Example. [Peer reviewed at the editor''s discretion] Study design and interpretation. Example. [Always peer reviewed] Original data from clinical investigations. In particular: Primary research papers from RCTs, observational studies, epidemiological studies; pre-specified sub-analyses; pooled analyses. [Always peer reviewed] Meta-analyses. [Always peer reviewed] Systematic reviews. From October 2009, special priority will be given to systematic reviews. [Always peer reviewed] Non-systematic/narrative reviews. From October 2009, reviews that are not systematic will be considered only if they include a discrete Methods section that must explicitly describe the authors'' approach. Special priority will, however, be given to systematic reviews. [Always peer reviewed] ''How to…'' papers. Example. [Always peer reviewed] Consensus statements. [Always peer reviewed] Short reports. [Always peer reviewed] Letters. [Peer reviewed at the editor''s discretion] International scope IJCP publishes work from investigators globally. Around 30% of IJCP articles list an author from the UK. Around 30% of IJCP articles list an author from the USA or Canada. Around 45% of IJCP articles list an author from a European country that is not the UK. Around 15% of articles published in IJCP list an author from a country in the Asia-Pacific region.
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