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鉴定脑胶质瘤患者的潜在生物标志物:加权基因共表达网络分析。

Identification of the potential biomarkers in patients with glioma: a weighted gene co-expression network analysis.

机构信息

Center for Evidence-Based Medicine and Clinical Research, Shiyan, China.

Department of Neurosurgery, Shiyan, China.

出版信息

Carcinogenesis. 2020 Jul 10;41(6):743-750. doi: 10.1093/carcin/bgz194.

Abstract

Glioma is the most common brain tumor with high mortality. However, there are still challenges for the timely and accurate diagnosis and effective treatment of the tumor. One hundred and twenty-one samples with grades II, III and IV from the Gene Expression Omnibus database were used to construct gene co-expression networks to identify hub modules closely related to glioma grade, and performed pathway enrichment analysis on genes from significant modules. In gene co-expression network constructed by 2345 differentially expressed genes from 121 gene expression profiles for glioma, we identified the black and blue modules that associated with grading. The module preservation analysis based on 118 samples indicates that the two modules were replicable. Enrichment analysis showed that the extracellular matrix genes were enriched for blue module, while cell division genes were enriched for black module. According to survival analysis, 21 hub genes were significantly up-regulated and one gene was significantly down-regulated. What's more, IKBIP, SEC24D, and FAM46A are the genes with little attention among the 22 hub genes. In this study, IKBIP, SEC24D, and FAM46A related to glioma were mentioned for the first time to the current knowledge, which might provide a new idea for us to study the disease in the future. IKBIP, SEC24D and FAM46A among the 22 hub genes identified that are related to the malignancy degree of glioma might be used as new biomarkers to improve the diagnosis, treatment and prognosis of glioma.

摘要

神经胶质瘤是最常见的脑肿瘤,死亡率高。然而,对于肿瘤的及时准确诊断和有效治疗仍然存在挑战。从基因表达综合数据库中使用 121 个 II、III 和 IV 级样本构建基因共表达网络,以识别与神经胶质瘤分级密切相关的枢纽模块,并对显著模块中的基因进行途径富集分析。在从 121 个神经胶质瘤基因表达谱中 2345 个差异表达基因构建的基因共表达网络中,我们确定了与分级相关的黑色和蓝色模块。基于 118 个样本的模块保存分析表明,这两个模块是可复制的。富集分析表明,细胞外基质基因在蓝色模块中富集,而细胞分裂基因在黑色模块中富集。根据生存分析,有 21 个枢纽基因显著上调,一个基因显著下调。此外,在 22 个枢纽基因中,IKBIP、SEC24D 和 FAM46A 是关注较少的基因。在这项研究中,首次提到 IKBIP、SEC24D 和 FAM46A 与神经胶质瘤有关,这可能为我们未来研究该疾病提供新的思路。在鉴定的 22 个枢纽基因中,IKBIP、SEC24D 和 FAM46A 与神经胶质瘤的恶性程度有关,可能作为新的生物标志物用于改善神经胶质瘤的诊断、治疗和预后。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ed24/7351128/2641bc19ced5/bgz194f0001.jpg

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