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低级别胶质瘤中有前途的新型生物标志物和候选小分子药物:高通量数据的生物信息学分析证据。

The promising novel biomarkers and candidate small molecule drugs in lower-grade glioma: Evidence from bioinformatics analysis of high-throughput data.

机构信息

Medical School, Nantong University, Nantong, P.R. China.

The Hand Surgery Research Center, Department of Hand Surgery, Affiliated Hospital of Nantong University, Nantong, P.R. China.

出版信息

J Cell Biochem. 2019 Sep;120(9):15106-15118. doi: 10.1002/jcb.28773. Epub 2019 Apr 24.

DOI:10.1002/jcb.28773
PMID:31020692
Abstract

Overall survival of patients with low-grade glioma (LGG) has shown no significant improvement over the past 30 years, with survival averaging approximately 7 years. This study aimed to identify novel promising biomarkers of LGG and reveal its potential molecular mechanisms by integrated bioinformatics analysis. The microarray datasets of GSE68848 and GSE4290 were selected from GEO database for integrated analysis. In total, 293 overlapping differentially expressed genes (DEGs) were detected using the limma package. One hundred and eighty-eight nodes with 603 interactions were obtained from the establishment of protein-protein interaction (PPI) network. Functional and signaling pathway enriched were significantly correlated with the synapse and calcium signaling pathway, respectively. Module analysis revealed eight hub genes with high connectivity, which included CHRM1, DLG2, GABRD, GRIN1, HTR2A, KCNJ3, KCNJ9, and NUSAP1, and they were markedly correlated with patients' prognosis. The mining of the Gene Expression Profiling Interactive Analysis database and qPCR further confirmed the abnormal expression of these key genes with their prognostic value in LGG. We eventually predicted the 20 most vital small molecule drugs, which potentially reverse the carcinogenic state of LGG, as per the CMap (connectivity map) database and these DEGs, and MS-275 (enrichment score = -0.939) was considered as the most promising small molecule to treat LGG. In conclusion, our study provided eight reliable novel molecular biomarkers for diagnosis, prognosis prediction, and treatment targets for LGG. These conclusions will contribute to a better comprehension of molecular mechanisms fundamental to LGG occurrence and progression, and providing new insights for future development of genomic individualized treatment in LGG.

摘要

低级别胶质瘤(LGG)患者的总体生存率在过去 30 年中没有显著提高,平均生存时间约为 7 年。本研究旨在通过综合生物信息学分析,确定 LGG 的新型有前途的生物标志物,并揭示其潜在的分子机制。从 GEO 数据库中选择了 GSE68848 和 GSE4290 的微阵列数据集进行综合分析。使用 limma 软件包共检测到 293 个重叠的差异表达基因(DEGs)。从建立蛋白质-蛋白质相互作用(PPI)网络中获得了 188 个节点和 603 个相互作用。功能和信号通路富集分别与突触和钙信号通路显著相关。模块分析显示了 8 个具有高连通性的枢纽基因,包括 CHRM1、DLG2、GABRD、GRIN1、HTR2A、KCNJ3、KCNJ9 和 NUSAP1,它们与患者的预后显著相关。通过 Gene Expression Profiling Interactive Analysis 数据库和 qPCR 的挖掘进一步证实了这些关键基因的异常表达及其在 LGG 中的预后价值。根据 CMap(连接图谱)数据库和这些 DEGs,我们最终预测了 20 种最有潜力的小分子药物,这些药物可能逆转 LGG 的致癌状态,其中 MS-275(富集得分=-0.939)被认为是治疗 LGG 的最有前途的小分子。总之,我们的研究为 LGG 的诊断、预后预测和治疗靶点提供了 8 个可靠的新型分子生物标志物。这些结论将有助于更好地理解 LGG 发生和进展的分子机制,并为 LGG 基因组个体化治疗的未来发展提供新的思路。

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