Diagnostic and prognostic value of disulfidptosis-related genes in sepsis

Wenlu Zou, Lintao Sai, Wen Sai, Li Song, Gang Wang
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Abstract

Background

Sepsis is a disease associated with high morbidity and mortality rates, especially among the elderly and patients in intensive care units. Disulfidptosis, a newly identified form of cell death triggered by disulfide stress, is emerging as a significant factor in disease progression. This study aimed to explore the diagnostic and prognostic value of disulfidptosis-related genes in sepsis.

Methods

We obtained two datasets from the Gene Expression Omnibus (GEO) database to conduct our analysis. Functional enrichment analysis was performed to identify relevant biological pathways. A protein-protein interaction network was constructed to identify hub genes critical to sepsis. Additionally, we analyzed the immune infiltration status in sepsis patients. The diagnostic value of these hub genes for sepsis was evaluated using nomograms, receiver operating characteristic (ROC) curves, and calibration curves in both training and validation datasets. Finally, a miRNA-immune-related hub genes (miRNA-IHGs) regulatory network was developed to elucidate the synergistic interactions between miRNAs and their target genes.

Results

A total of 3,469 differentially expressed genes (DEGs) were identified, of which seven were related to disulfidptosis (DR-DEGs). Functional enrichment analysis showed that DR-DEGs were significantly enriched in pathways related to actin dynamics. Five hub genes (MYH10, ACTN4, MYH9, FLNA, and IQGAP1) were identified as central to these processes. The analysis of immune infiltration revealed significantly lower levels of 11 immune cell types, while macrophages and regulatory T cells were significantly elevated in sepsis patients. The area under the ROC curves (AUCs) of the IHGs risk prediction model were 0.917 and 0.894 for the training and validation sets, respectively. A miRNA-IHGs regulatory network, comprising 17 nodes and 27 edges, was constructed, with MYH9 being the most frequently regulated by miRNAs.

Conclusion

The pathophysiological process of sepsis appears to involve disulfidptosis, highlighting it as a potential new therapeutic targets for sepsis management.
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败血症中与二硫化硫相关基因的诊断和预后价值
背景败血症是一种发病率和死亡率都很高的疾病,尤其是在老年人和重症监护病房的病人中。二硫化物中毒是一种新发现的由二硫化物应激引发的细胞死亡形式,正在成为疾病进展的一个重要因素。本研究旨在探讨脓毒症中与二硫化物中毒相关基因的诊断和预后价值。我们进行了功能富集分析,以确定相关的生物学通路。我们构建了一个蛋白质-蛋白质相互作用网络,以确定对败血症至关重要的枢纽基因。此外,我们还分析了败血症患者的免疫浸润状态。在训练数据集和验证数据集中,我们使用提名图、接收者操作特征曲线(ROC)和校准曲线评估了这些枢纽基因对败血症的诊断价值。最后,研究人员建立了一个 miRNA-免疫相关枢纽基因(miRNA-IHGs)调控网络,以阐明 miRNA 与其靶基因之间的协同作用。功能富集分析表明,DR-DEGs 在肌动蛋白动力学相关通路中显著富集。五个中心基因(MYH10、ACTN4、MYH9、FLNA 和 IQGAP1)被确定为这些过程的中心基因。对免疫浸润的分析表明,脓毒症患者体内 11 种免疫细胞类型的水平明显降低,而巨噬细胞和调节性 T 细胞则明显升高。IHGs风险预测模型的训练集和验证集的ROC曲线下面积(AUC)分别为0.917和0.894。结论脓毒症的病理生理过程似乎涉及二硫化血症,这突出表明二硫化血症是脓毒症治疗的潜在新靶点。
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