Abstract
BackgroundCD4+ memory T cells are an important component of the tumor microenvironment (TME) and affect tumor occurrence and progression. Nevertheless, there has been no systematic analysis of the effect of CD4+ memory T cells in gastric cancer (GC).MethodsThree datasets obtained from microarray and the corresponding clinical data of GC patients were retrieved and downloaded from the Gene Expression Omnibus (GEO) database. We uploaded the normalize gene expression data with standard annotation to the CIBERSORT web portal for evaluating the proportion of immune cells in the GC samples. The WGCNA was performed to identify the modules the CD4+ memory T cell related module (CD4+ MTRM) which was most significantly associated with CD4+ memory T cell. Univariate Cox analysis was used to screen prognostic CD4+ memory T cell-related genes (CD4+ MTRGs) in CD4+ MTRM. LASSO analysis and multivariate Cox analysis were then performed to construct a prognostic gene signature whose effect was evaluated by Kaplan-Meier curves and receiver operating characteristic (ROC), Harrell’s concordance index (C-index), and decision curve analyses (DCA). A prognostic nomogram was finally established based on the CD4+ MTRGs.ResultWe observed that a high abundance of CD4+ memory T cells was associated with better survival in GC patients. CD4+ MTRM was used to stratify GC patients into three clusters by unsupervised clustering analysis and ten CD4+ MTRGs were identified. Overall survival, five immune checkpoint genes and 17 types of immunocytes were observed to be significantly different among the three clusters. A ten-CD4+ MTRG signature was constructed to predict GC patient prognosis. The ten-CD4+ MTRG signature could divide GC patients into high- and low-risk groups with distinct OS rates. Multivariate Cox analysis suggested that the ten-CD4+ MTRG signature was an independent risk factor in GC. A nomogram incorporating this signature and clinical variables was established, and the C-index was 0.73 (95% CI: 0.697–0.763). Calibration curves and DCA presented high credibility for the OS nomogram.ConclusionWe identified three molecule subtypes, ten CD4+ MTRGs, and generated a prognostic nomogram that reliably predicts OS in GC. These findings have implications for precise prognosis prediction and individualized targeted therapy.
Highlights
Gastric cancer (GC) is the fifth most diagnosed malignancy and is the third highest cause of cancer mortality worldwide [1]
These results indicated that high CD4 memory resting T cells, low CD4 memory activated T cells and low M1 macrophages were significantly associated with poorer overall survival (OS), p = 0.002, p < 0.001, p = 0.029, respectively (Figure 2A)
This module was most negatively associated with resting CD4+ memory T cells, while it was most positively associated with activated CD4+ memory T cells and M1 macrophages, as assessed by the heatmap and scatter plot scores (Figure 3A)
Summary
Gastric cancer (GC) is the fifth most diagnosed malignancy and is the third highest cause of cancer mortality worldwide [1]. CD4+ memory T cell has been reported to be an important role in TME In colorectal cancer, it has been suggested in more infiltrated than normal tissue [11]; in triple-negative breast cancer, CD4+ memory T cell enrichment score seem higher in invasive tumors [12]; in lung adenocarcinoma, it seemed relative hypometabolism and favorable prognosis [13], but the relationship is not yet clear in the case of GC. Through the bioinformatics tool of CIBERSORT and Kaplan-Meier survival curves, we explored the relationship between immune infiltration and outcome of patients with gastric cancer according to the gene expression profiles from the GEO database and found that prognosis were closely associated to memory CD4+ T cells. There has been no systematic analysis of the effect of CD4+ memory T cells in gastric cancer (GC)
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