首页> 美国卫生研究院文献>Journal of Cellular and Molecular Medicine >Collagen Type III Alpha 1 chain regulated by GATA‐Binding Protein 6 affects Type II IFN response and propanoate metabolism in the recurrence of lower grade glioma
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Collagen Type III Alpha 1 chain regulated by GATA‐Binding Protein 6 affects Type II IFN response and propanoate metabolism in the recurrence of lower grade glioma

机译:由GATA结合蛋白6调节的III型IIIα1链影响II型IFN响应和丙种代谢在较低级胶质瘤的复发中

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摘要

Some studies suggested the prognosis value of immune gene in lower grade glioma (LGG). Recurrence in LGG is a tough clinical problem for many LGG patients. Therefore, prognosis biomarker is required. Multivariate prognosis Cox model was constructed and then calculated the risk score. And differential expressed transcription factors (TFs) and differential expressed immune genes (DEIGs) were co‐analysed. Besides, significant immune cells/pathways were identified by single sample gene set enrichment analysis (ssGSEA). Moreover, gene set variation analysis (GSVA) and univariate Cox regression were applied to filter prognostic signalling pathways. Additionally, significant DEIG and immune cells/pathways, and significant DEIG and pathways were co‐analysed. Further, differential enriched pathways were identified by GSEA. In sum, a scientific hypothesis for recurrence LGG including TF, immune gene and immune cell/pathway was established. In our study, a total of 536 primary LGG samples, 2,498 immune genes and 318 TFs were acquired. Based on edgeR method, 2,164 DEGs, 2,498 DEIGs and 31 differentials expressed TFs were identified. A total of 106 DEIGs were integrated into multivariate prognostic model. Additionally, the AUC of the ROC curve was 0.860, and P value of Kaplan‐Meier curve < 0.001. GATA6 (TF) and COL3A1 (DEIG) were selected (R = 0.900, P < 0.001, positive) as significant TF‐immune gene links. Type II IFN response (P < 0.001) was the significant immune pathway. Propanoate metabolism (P < 0.001) was the significant KEGG pathway. We proposed that COL3A1 was positively regulated by GATA6, and by effecting type II IFN response and propanoate metabolism, COL3A1 involved in LGG recurrence.
机译:一些研究表明免疫基因在较低级胶质瘤(LGG)中的预后值。 LGG的复发是许多LGG患者的艰难临床问题。因此,需要预后生物标志物。构建多变量预后Cox模型,然后计算风险分数。共同分析差异表达的转录因子(TFS)和差异表达的免疫基因(DEIGS)。此外,通过单样本基因设定富集分析(SSGSEA)鉴定出显着的免疫细胞/途径。此外,施用基因设定变异分析(GSVA)和单变量COX回归以过滤预后信号通路。另外,共同分析了显着的DEIG和免疫细胞/途径和显着的DEIG和途径。此外,通过GSEA鉴定了差异富集的途径。总之,建立了包括TF,免疫基因和免疫细胞/途径的复发LGG的科学假设。在我们的研究中,获得了总共536个初级LGG样品,2,498个免疫基因和318种TFS。基于编辑方法,鉴定了2,164℃,2,498个DEIGS和31种差异表达TFS。共有106个DEIGS被整合到多元预后模型中。另外,ROC曲线的AUC为0.860,Kaplan-Meier曲线的P值<0.001。选择GATA6(TF)和COL3A1(DEIG)(r = 0.900,p <0.001,阳性)作为显着的TF免疫基因链接。 II型IFN响应(P <0.001)是显着的免疫途径。丙种新陈代谢(P <0.001)是重要的KEGG途径。我们提出COL3A1由GATA6积极调节,并通过效应II型IFN反应和丙种代谢,COL3A1参与LGG复发。

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