AI Article Synopsis

  • - The study investigates preeclampsia (PE) by analyzing various gene expression datasets to identify novel genes that could serve as diagnostic and therapeutic targets, focusing on the immune mechanisms involved.
  • - Researchers utilized multiple algorithms to refine candidate genes and developed a predictive nomogram and a neural network model (FCNN), achieving strong predictive power for PE diagnosis and highlighting immune cell involvement in the condition.
  • - Five biomarkers were validated, demonstrating significant diagnostic potential with high AUC values, and the analysis revealed a crucial link between these biomarkers and immune responses, further emphasizing the role of the immune system in PE pathogenesis.

Article Abstract

Background: Preeclampsia (PE) poses significant diagnostic and therapeutic challenges. This study aims to identify novel genes for potential diagnostic and therapeutic targets, illuminating the immune mechanisms involved.

Methods: Three GEO datasets were analyzed, merging two for training set, and using the third for external validation. Intersection analysis of differentially expressed genes (DEGs) and WGCNA highlighted candidate genes. These were further refined through LASSO, SVM-RFE, and RF algorithms to identify diagnostic hub genes. Diagnostic efficacy was assessed using ROC curves. A predictive nomogram and fully Connected Neural Network (FCNN) were developed for PE prediction. ssGSEA and correlation analysis were employed to investigate the immune landscape. Further validation was provided by qRT-PCR on human placental samples.

Result: Five biomarkers were identified with validation AUCs: (0.663, 95% CI: 0.577-0.750), (0.850, 95% CI: 0.792-0.908), (0.797, 95% CI: 0.728-0.867), (0.839, 95% CI: 0.775-0.902), and (0.811, 95% CI: 0.742-0.880), all of which are involved in key biological processes. The nomogram showed strong predictive power (C-index 0.873), while FCNN achieved an optimal AUC of 0.911 (95% CI: 0.732-1.000) in five-fold cross-validation. Immune infiltration analysis revealed the importance of T cell subsets, neutrophils, and NK cells in PE, linking these genes to immune mechanisms underlying PE pathogenesis.

Conclusion: , , , , and are validated as key diagnostic biomarkers for PE. Nomogram and FCNN could credibly predict PE. Their association with immune infiltration underscores the crucial role of immune responses in PE pathogenesis.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11560445PMC
http://dx.doi.org/10.3389/fimmu.2024.1416297DOI Listing

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