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首页> 外文期刊>Frontiers in Molecular Biosciences >Identification of Radiotherapy-Associated Genes in Lung Adenocarcinoma by an Integrated Bioinformatics Analysis Approach
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Identification of Radiotherapy-Associated Genes in Lung Adenocarcinoma by an Integrated Bioinformatics Analysis Approach

机译:综合生物信息学分析方法鉴定肺腺癌中的放射疗法相关基因

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Radiotherapy (RT) plays an important role in the prognosis of lung adenocarcinoma (LUAD) patients, but the radioresistance (RR) of LUAD is still a challenge that needs to be overcome. The current study aimed to investigate LUAD patients with RR to illuminate the underlying mechanisms. We utilized gene set variation analysis (GSVA) and The Cancer Immunome Atlas (TCIA) database to characterize the differences in biological functions and neoantigen-coding genes between RR and radiosensitive (RS) patients. Weighted Gene co-expression network analysis (WGCNA) was used to explore the relationship between RT-related traits and hub genes in two modules, i.e., RR and RS; two representative hub genes for RR (MZB1 and DERL3) and two for RS (IFI35 and PSMD3) were found to be related to different RT-related traits. Further analysis of the hub genes with the Lung Cancer Explorer (LCE), PanglaoDB and GSVA resources revealed the differences in gene expression levels, cell types and potential functions. On this basis, the Tumor and Immune System Interaction Database (TISIDB) was used to identify the potential association between RR genes and B cell infiltration. Finally, we used the Computational Analysis of Resistance (CARE) database to identify specific gene-associated drugs for RR patients and found that GSK525762A and nilotinib might be promising candidates for RR treatment. Taken together, these results demonstrate that B cells in TME may have a significant impact on the RT and that these two drug candidates, GSK525762A and nilotinib, might be helpful for the treatment of RR patients.
机译:放射疗法(RT)在肺腺癌(Luad)患者的预后起着重要作用,但拉德的辐射仪(RR)仍然是需要克服的挑战。目前的研究旨在调查鲁拉患者的RR患者照亮潜在机制。我们利用基因设定变异分析(GSVA)和癌症免疫癌症(TCIA)数据库,以表征RR和辐射敏感性(RS)患者之间的生物学功能和新稻垣编码基因的差异。加权基因共表达网络分析(WGCNA)用于探索两个模块中的RT相关性状和枢纽基因之间的关系,即RR和RS;发现RR(MZB1和DERL3)和RS(IFI35和PSMD3)的两个代表性枢纽基因与不同的RT相关性状有关。进一步分析肺癌探险家(LCE),PanglaodB和GSVA资源的枢纽基因揭示了基因表达水平,细胞类型和潜在功能的差异。在此基础上,使用肿瘤和免疫系统相互作用数据库(TISIDB)来鉴定RR基因和B细胞浸润​​之间的潜在关联。最后,我们使用对抗性(护理)数据库的计算分析来鉴定RR患者的特定基因相关药物,发现GSK525762A和NILOTINIB可能是RR治疗的承诺候选者。总之,这些结果表明,TME中的B细胞可能对RT产生显着影响,这两种药物候选者GSK525762A和NILOTINIB可能有助于治疗RR患者。

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