Enhancer-driven transcription of MCM8 by E2F4 promotes ATR pathway activation and glioma stem cell characteristics.

IF 2.7 3区 生物学 Hereditas Pub Date : 2023-06-22 DOI:10.1186/s41065-023-00292-x
Yu-Meng Sun, Yi-Meng Zhang, Hai-Liang Shi, Song Yang, Yin-Long Zhao, Hong-Jiang Liu, Chen Li, Hong-Lei Liu, Ji-Peng Yang, Jian Song, Guo-Zhu Sun, Jian-Kai Yang
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引用次数: 0

Abstract

Background: Glioma stem cells (GSCs) are responsible for glioma recurrence and drug resistance, yet the mechanisms underlying their maintenance remains unclear. This study aimed to identify enhancer-controlled genes involved in GSCs maintenance and elucidate the mechanisms underlying their regulation.

Methods: We analyzed RNA-seq data and H3K27ac ChIP-seq data from GSE119776 to identify differentially expressed genes and enhancers, respectively. Gene Ontology analysis was performed for functional enrichment. Transcription factors were predicted using the Toolkit for Cistrome Data Browser. Prognostic analysis and gene expression correlation was conducted using the Chinese Glioma Genome Atlas (CGGA) data. Two GSC cell lines, GSC-A172 and GSC-U138MG, were isolated from A172 and U138MG cell lines. qRT-PCR was used to detect gene transcription levels. ChIP-qPCR was used to detect H3K27ac of enhancers, and binding of E2F4 to target gene enhancers. Western blot was used to analyze protein levels of p-ATR and γH2AX. Sphere formation, limiting dilution and cell growth assays were used to analyze GSCs growth and self-renewal.

Results: We found that upregulated genes in GSCs were associated with ataxia-telangiectasia-mutated-and-Rad3-related kinase (ATR) pathway activation, and that seven enhancer-controlled genes related to ATR pathway activation (LIN9, MCM8, CEP72, POLA1, DBF4, NDE1, and CDKN2C) were identified. Expression of these genes corresponded to poor prognosis in glioma patients. E2F4 was identified as a transcription factor that regulates enhancer-controlled genes related to the ATR pathway activation, with MCM8 having the highest hazard ratio among genes positively correlated with E2F4 expression. E2F4 bound to MCM8 enhancers to promote its transcription. Overexpression of MCM8 partially restored the inhibition of GSCs self-renewal, cell growth, and the ATR pathway activation caused by E2F4 knockdown.

Conclusion: Our study demonstrated that E2F4-mediated enhancer activation of MCM8 promotes the ATR pathway activation and GSCs characteristics. These findings offer promising targets for the development of new therapies for gliomas.

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E2F4增强子驱动的MCM8转录促进ATR通路激活和胶质瘤干细胞特性。
背景:胶质瘤干细胞(GSCs)与胶质瘤复发和耐药有关,但其维持机制尚不清楚。本研究旨在鉴定参与GSCs维持的增强控制基因,并阐明其调控机制。方法:分析GSE119776的RNA-seq数据和H3K27ac ChIP-seq数据,分别鉴定差异表达基因和增强子。基因本体分析进行功能富集。使用Cistrome数据浏览器工具包预测转录因子。使用中国胶质瘤基因组图谱(CGGA)数据进行预后分析和基因表达相关性分析。从A172和U138MG细胞株中分离得到GSC-A172和GSC-U138MG两株GSC细胞株。采用qRT-PCR检测基因转录水平。ChIP-qPCR检测增强子的H3K27ac,以及E2F4与靶基因增强子的结合情况。Western blot检测p-ATR和γ - h2ax蛋白水平。球体形成、极限稀释和细胞生长试验用于分析GSCs的生长和自我更新。结果:我们发现GSCs中上调的基因与ATR通路激活相关,并鉴定出7个与ATR通路激活相关的增强子控制基因(LIN9、MCM8、CEP72、POLA1、DBF4、NDE1和CDKN2C)。这些基因的表达与胶质瘤患者预后不良有关。E2F4是调控ATR通路激活相关增强子控制基因的转录因子,在与E2F4表达呈正相关的基因中,MCM8的风险比最高。E2F4结合到MCM8增强子上促进其转录。MCM8过表达部分恢复了E2F4敲低引起的GSCs自我更新、细胞生长和ATR通路激活的抑制。结论:我们的研究表明,e2f4介导的MCM8增强子激活促进了ATR通路的激活和GSCs的特性。这些发现为胶质瘤新疗法的开发提供了有希望的靶点。
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来源期刊
Hereditas
Hereditas Biochemistry, Genetics and Molecular Biology-Genetics
CiteScore
3.80
自引率
3.70%
发文量
0
期刊介绍: For almost a century, Hereditas has published original cutting-edge research and reviews. As the Official journal of the Mendelian Society of Lund, the journal welcomes research from across all areas of genetics and genomics. Topics of interest include human and medical genetics, animal and plant genetics, microbial genetics, agriculture and bioinformatics.
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