4.3 Article

Cadherin dysregulation in gastric cancer: insights into gene expression, pathways, and prognosis

Journal

JOURNAL OF GASTROINTESTINAL ONCOLOGY
Volume -, Issue -, Pages -

Publisher

AME PUBLISHING COMPANY
DOI: 10.21037/jgo-23-700

Keywords

Cadherin genes; gastric cancer (GC); gene expression; biomarkers; prognosis

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In this study, the role of Cadherin family genes in gastric cancer (GC) was investigated using bioinformatics analysis. The analysis revealed significant differential expression of Cadherin genes in GC samples and their association with critical cellular processes such as cell adhesion and immune modulation. Lower expression levels of most Cadherin genes were linked to improved prognosis in GC patients, suggesting their potential as valuable prognostic biomarkers.
Background: The Cadherin gene family holds immense significance in maintaining the integrity and functionality of stomach tissues, playing crucial roles in cell-cell adhesion, cell migration and differentiation. Dysregulation of cadherin expression and function has been closely associated with various gastric diseases, particularly gastric cancer (GC). Understanding the regulation and clinical implications of cadherin genes in GC is essential to improve our knowledge and to identify new potential prognostic markers and therapeutic targets. Methods: In this study, we provide an overview on the role of cadherin family genes in GC using bioinformatics analysis. We analyzed the expression, mutational status, and prognostic value of these genes based on available public datasets. Our methodology involved data mining, differential expression analysis, functional enrichment analysis, and survival analysis to explore the association between cadherin gene expression and clinical outcomes in GC patients. Additionally, we investigated the relationship between cadherin expression and immune cell infiltration to gain insights into the tumor microenvironment's role in Results: Our bioinformatics analysis revealed significant differential expression of 16 cadherin genes in GC samples compared to normal tissues. Approximately up to 52% of the analyzed cancer samples exhibited genomic alterations in these cadherins, indicating their potential relevance in GC development. Functional enrichment analysis demonstrated that these differentially expressed cadherins were closely associated with critical cellular processes, including cell adhesion and immune-modulation. Remarkably, lower expression levels of most cadherin genes were linked to improved prognosis in GC patients, suggesting their potential importance as valuable prognostic biomarkers. Conclusions: The findings deriving from our comprehensive study provide important insights into the dysregulation of cadherin genes in GC and their impact on gene expression, molecular pathways, and prognosis. The associations with clinical outcomes and immune cell infiltration highlight the potential role of cadherin genes as prognostic biomarkers and therapeutic targets in GC.

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