MicroRNA-575 acts as a novel oncogene via targeting multiple signaling pathways in glioblastoma

IF 2.8 4区医学 Q2 PATHOLOGY Experimental and molecular pathology Pub Date : 2022-10-01 DOI:10.1016/j.yexmp.2022.104813

Ashley Gray , Tiantian Cui , Erica Hlavin Bell , Joseph McElroy , Ebin Sebastian , Fuhai Li , Marjolein Geurts , Kevin Liu , Pierre Robe , S. Jaharul Haque , Arnab Chakravarti

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引用次数: 1

Abstract

Purpose

Glioblastoma (GBM) patients currently face poor survival outcomes with an average survival period of <15 months, while only 3–5% of patients survive longer than 36 months. Although the mechanisms of tumorigenesis are still being elucidated, miRNAs are promising candidates to explore as novel and prognostic biomarkers in GBM. In this study, we identified the association between miR-575 expression and overall survival (OS) of primary GBM patients and undertook functional studies to discern the contribution of miR-575 to GBM tumorigenesis.

Methods

Total RNAs were isolated from 254 FFPE GBM tumor samples and miR expression was assayed (simultaneously) using NanoString Technologies. To determine the association between miR-575 and patients' prognosis, Kaplan-Meier, univariable and multivariable Cox regression analyses were performed. Cell proliferation, colony formation, migration assays were conducted to investigate the function of miR-575 in vitro and in vivo. In silico target gene network analysis was performed to identify the putative targets of miR-575 in GBM, which were further verified by luciferase reporter assay, as well as qPCR and immunoblotting.

Results

Our clinical data (n = 254) show that miR-575 is associated with worse GBM OS by univariable analysis (UVA, HR = 1.27, p-value<0.001) and multivariable (MVA, HR = 1.23, p = 0.007) analysis incorporating critical clinical variables. Functional studies indicated that overexpression of miR-575 significantly increased cell proliferation and migration of GBM cells in vitro, as well as tumor growth in vivo. Subsequent in silico target gene network and mechanistic studies identified CDKN1B/p27 and PTEN, as potential targets of miR-575 in GBM. MicroRNA-575 can also regulate the activity of AKT and ERK pathways in GBM.

Conclusion

miR-575 has prognostic value in GBM, with higher expression associating with worse OS of patients, and contributes to GBM tumorigenesis by regulating multiple signaling pathways in GBM.

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MicroRNA-575在胶质母细胞瘤中作为一种新的致癌基因，通过靶向多种信号通路发挥作用

目的胶质母细胞瘤(GBM)患者目前面临较差的生存结果，平均生存期为15个月，而只有3-5%的患者存活时间超过36个月。尽管肿瘤发生的机制仍未被阐明，但mirna有望作为GBM的新型和预后生物标志物进行探索。在这项研究中，我们确定了miR-575表达与原发性GBM患者总生存期(OS)之间的关联，并进行了功能研究，以确定miR-575对GBM肿瘤发生的贡献。方法从254例FFPE GBM肿瘤中分离总rna，同时利用NanoString技术检测miR的表达。为了确定miR-575与患者预后的关系，我们进行Kaplan-Meier、单变量和多变量Cox回归分析。通过细胞增殖、集落形成、迁移实验研究miR-575在体外和体内的功能。通过计算机靶基因网络分析来确定miR-575在GBM中的推测靶点，并通过荧光素酶报告基因实验、qPCR和免疫印迹法进一步验证。结果我们的临床数据(n = 254)显示，单变量分析(UVA, HR = 1.27, p值<0.001)和包含关键临床变量的多变量分析(MVA, HR = 1.23, p = 0.007)表明，miR-575与较差的GBM OS相关。功能研究表明，过表达miR-575可显著增加体外GBM细胞的增殖和迁移，以及体内肿瘤的生长。随后的硅靶基因网络和机制研究发现CDKN1B/p27和PTEN是miR-575在GBM中的潜在靶点。MicroRNA-575还可以调节GBM中AKT和ERK通路的活性。结论mir -575在GBM中具有预后价值，表达水平越高，患者OS越差，mir -575通过调节GBM中多种信号通路参与GBM的发生。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Experimental and molecular pathology 医学-病理学

CiteScore

8.90

自引率

0.00%

发文量

审稿时长

11.5 weeks

期刊介绍： Under new editorial leadership, Experimental and Molecular Pathology presents original articles on disease processes in relation to structural and biochemical alterations in mammalian tissues and fluids and on the application of newer techniques of molecular biology to problems of pathology in humans and other animals. The journal also publishes selected interpretive synthesis reviews by bench level investigators working at the "cutting edge" of contemporary research in pathology. In addition, special thematic issues present original research reports that unravel some of Nature''s most jealously guarded secrets on the pathologic basis of disease. Research Areas include: Stem cells; Neoangiogenesis; Molecular diagnostics; Polymerase chain reaction; In situ hybridization; DNA sequencing; Cell receptors; Carcinogenesis; Pathobiology of neoplasia; Complex infectious diseases; Transplantation; Cytokines; Flow cytomeric analysis; Inflammation; Cellular injury; Immunology and hypersensitivity; Athersclerosis.