实用医学杂志2024,Vol.40Issue(1):7-12,6.DOI:10.3969/j.issn.1006-5725.2024.01.002
基于转录组测序探究C-MET表达在非小细胞肺癌中的免疫调控机制
RNA sequencing-based research on the immune regulation mechanism of C-MET in lung cancer
摘要
Abstract
Objective To analyze the immune regulation mechanism of C-MET expression in non-small cell lung cancer by transcriptome sequencing technology.Methods The C-MET expression of lung adenocarci-noma cell line(H1993)and lung squamous cell carcinoma cell line(EBC-1)with high C-MET expression was silenced using siRNA molecular interference technology.The differentially expressed genes(DEGs)before and after C-MET silencing were detected using transcriptome sequencing technology.The signal pathways and related genes of the immune microenvironment in which C-MET may participate in regulation were excavated through bioinformat-ics analysis.Finally,the co-culture technique of human immune cells with H1993 and EBC-1 was used to verify the effect of C-MET on immune factors such as INF-γ,INF-β and CXCL-10.Results We detected 505 DEGs in total using transcriptome sequencing.There were 38 differentially expressed genes in the C-MET regulation group before and after H1993,24 upregulated differentially expressed genes,and 14 downregulated differentially expressed genes,respectively.There are a total of 467 differentially expressed genes in the C-MET regulation group of EBC-1,347 upregulated differentially expressed genes,and 121 downregulated differentially expressed genes,respec-tively.KEGG analysis of differential genes suggested that C-MET expression might participate in the regulation of immune cell regulatory factors through the IL-17 signaling pathway,white blood cell differentiation,cytokine receptor activity,cell cycle,cytokine receptor activity,and cytokine-cytokine receptor interaction.The effect of C-MET on immune factor secretion was verified using the co-culture technique of lung cancer cells and human immune cells,and the results of Rt-qPCR assay suggested,the mRNA transcriptional level of INF-γ in PBMC co-cultured with the C-MET high expression group was 77 times that of the low expression group,and the mRNA transcriptional level of CXCL-10 was 1.6 times that of the low expression group.The mRNA transcriptional level of INF--β was twice as high as that of the low expression group.Conclusion C-MET expression may participate in the regulation of tumor surrounding immune microenvironment through IL-17 signaling pathway,leukocyte differen-tiation,and cytokine receptor activity pathway.关键词
非小细胞肺癌/C-MET/免疫微环境/表达谱测序Key words
non-small cell lung cancer/C-MET/immune microenvironment/expression profile sequencing分类
医药卫生引用本文复制引用
徐越,张言斌,苏珊..基于转录组测序探究C-MET表达在非小细胞肺癌中的免疫调控机制[J].实用医学杂志,2024,40(1):7-12,6.基金项目
国家自然科学青年基金项目(编号:8200113358) (编号:8200113358)
广东省自然科学基金(编号:2022A1515012400) (编号:2022A1515012400)
广州市科技计划项目(编号:202206010134,202002030152) (编号:202206010134,202002030152)
