GNAO1 overexpression promotes neural differentiation of glioma stem-like cells and reduces tumorigenicity through TRIM21/CREB/HES1 axis.

IF 6.9 1区 医学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY
Bowen Sun, Ge Wang, Guoyu Chen, Yingwen Zhang, Ru Yang, He Hua, Yanxin Li, Haizhong Feng
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引用次数: 0

Abstract

Inducing tumor cell differentiation is a promising strategy for treating malignant cancers, including glioma, yet the critical regulator(s) underlying glioma cell differentiation is poorly understood. Here, we identify G Protein Subunit Alpha O1 (GNAO1) as a critical regulator of neural differentiation of glioma stem-like cells (GSCs). GNAO1 expression was lower in gliomas than in normal neuronal tissues and high expression of GNAO1 correlated with a better prognosis. GNAO1 overexpression markedly promoted neural differentiation of GSCs, leading to decreased cell proliferation and colony formation. Mechanistically, GNAO1 recruited TRIM21 and facilitated TRIM21-mediated ubiquitination. This ubiquitination resulted in the degradation of CREB and further reduced p300-mediated H3K27ac levels of the HES1 promoter. As a result, GNAO1 overexpression downregulated HES1 expression, which reinforced neuronal differentiation. In addition, knockdown of METTL3, a key writer of the N6-methyladenosine (m6A), enhanced GNAO1 mRNA stability. Treatment with GNAO1 adenovirus increased neuronal differentiation of tumor cells and reduced tumor cell proliferation in orthotopic GSC xenografts and temozolomide further enhanced GNAO1 adenovirus effects, resulting in extended animal survival. Our study presents that engineering GNAO1 overexpression-inducing neural differentiation of GSCs is a potential therapy strategy via synergistic inhibition of malignant proliferation and chemotherapy resistance.

GNAO1过表达可促进胶质瘤干样细胞的神经分化,并通过TRIM21/CREB/HES1轴降低致瘤性。
诱导肿瘤细胞分化是治疗包括胶质瘤在内的恶性癌症的一种很有前景的策略,然而胶质瘤细胞分化的关键调节因子却鲜为人知。在这里,我们发现G蛋白亚基α O1(GNAO1)是胶质瘤干样细胞(GSCs)神经分化的关键调控因子。GNAO1在胶质瘤中的表达低于正常神经元组织,而GNAO1的高表达与较好的预后相关。GNAO1的过表达明显促进了GSCs的神经分化,导致细胞增殖和集落形成减少。从机理上讲,GNAO1 会招募 TRIM21 并促进 TRIM21 介导的泛素化。这种泛素化导致了 CREB 的降解,并进一步降低了 p300 介导的 HES1 启动子的 H3K27ac 水平。因此,GNAO1 的过量表达下调了 HES1 的表达,从而加强了神经元的分化。此外,敲除 METTL3(N6-甲基腺苷(m6A)的关键写入者)可增强 GNAO1 mRNA 的稳定性。用GNAO1腺病毒治疗可增加肿瘤细胞的神经元分化,减少正位GSC异种移植物中肿瘤细胞的增殖,替莫唑胺可进一步增强GNAO1腺病毒的作用,从而延长动物的存活期。我们的研究表明,GNAO1过表达诱导GSC神经分化工程是一种潜在的治疗策略,可协同抑制恶性肿瘤增殖和化疗耐药性。
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
Oncogene
Oncogene 医学-生化与分子生物学
CiteScore
15.30
自引率
1.20%
发文量
404
审稿时长
1 months
期刊介绍: Oncogene is dedicated to advancing our understanding of cancer processes through the publication of exceptional research. The journal seeks to disseminate work that challenges conventional theories and contributes to establishing new paradigms in the etio-pathogenesis, diagnosis, treatment, or prevention of cancers. Emphasis is placed on research shedding light on processes driving metastatic spread and providing crucial insights into cancer biology beyond existing knowledge. Areas covered include the cellular and molecular biology of cancer, resistance to cancer therapies, and the development of improved approaches to enhance survival. Oncogene spans the spectrum of cancer biology, from fundamental and theoretical work to translational, applied, and clinical research, including early and late Phase clinical trials, particularly those with biologic and translational endpoints.
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