Androgen receptor variant 7 exacerbates hepatocarcinogenesis in a c-MYC-driven mouse HCC model.

IF 5.9 2区 医学 Q1 ONCOLOGY
Tatsuo Kido, Yun-Fai Chris Lau
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引用次数: 0

Abstract

Androgen receptor variant 7 (AR-V7), an AR isoform with a truncated ligand-binding domain, functions as a transcription factor in an androgen-independent manner. AR-V7 is expressed in a subpopulation of hepatocellular carcinoma (HCC), however, its role(s) in this cancer is undefined. In this study, we investigated the potential roles of AR-V7 in hepatocarcinogenesis in vivo in a c-MYC-driven mouse HCC model generated by the hydrodynamic tail-vein injection system. The impacts of AR-V7 on gene expression in mouse HCC were elucidated by RNA-seq transcriptome and ontology analyses. The results showed that AR-V7 significantly exacerbated the c-MYC-mediated oncogenesis in the livers of both sexes. The transcriptome and bioinformatics analyses revealed that AR-V7 and c-MYC synergistically altered the gene sets involved in various cancer-related biological processes, particularly in lipid and steroid/sterol metabolisms. Importantly, AR-V7 suppressed a tumor suppressor Claudin 7 expression, upregulated by c-MYC overexpression via the p53 signaling pathway. Claudin 7 overexpression significantly suppressed the c-MYC-driven HCC development under p53-deficient conditions. Our results suggest that the AR-V7 exacerbates the c-MYC-driven hepatocarcinogenesis by potentiating the oncogenic roles and minimizing the anti-oncogenic functions of c-MYC. Since AR-V7 is expressed in a subpopulation of HCC cases, it could contribute to the inter- and intra-heterogeneity of HCC.

Abstract Image

Abstract Image

Abstract Image

在c- myc驱动的小鼠HCC模型中,雄激素受体变异7加剧了肝癌的发生。
雄激素受体变异7 (AR- v7)是一种具有截断配体结合域的AR异构体,以雄激素不依赖的方式作为转录因子。AR-V7在肝细胞癌(HCC)的一个亚群中表达,然而,它在这种癌症中的作用尚不明确。在这项研究中,我们研究了AR-V7在体内由水动力尾静脉注射系统产生的c- myc驱动的小鼠HCC模型中的潜在作用。通过RNA-seq转录组和本体论分析,阐明AR-V7对小鼠肝癌基因表达的影响。结果显示,AR-V7显著加重了两性肝脏中c- myc介导的肿瘤发生。转录组和生物信息学分析显示,AR-V7和c-MYC协同改变了参与各种癌症相关生物过程的基因集,特别是脂质和类固醇/固醇代谢。重要的是,AR-V7通过p53信号通路抑制c-MYC过表达的肿瘤抑制因子Claudin 7的表达。在p53缺乏的情况下,Claudin 7过表达显著抑制c- myc驱动的HCC发展。我们的研究结果表明,AR-V7通过增强c-MYC的致癌作用和最小化c-MYC的抗癌功能,加剧了c-MYC驱动的肝癌发生。由于AR-V7在HCC病例的一个亚群中表达,因此它可能导致HCC的内部异质性和内部异质性。
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来源期刊
Oncogenesis
Oncogenesis ONCOLOGY-
CiteScore
11.90
自引率
0.00%
发文量
70
审稿时长
26 weeks
期刊介绍: Oncogenesis is a peer-reviewed open access online journal that publishes full-length papers, reviews, and short communications exploring the molecular basis of cancer and related phenomena. It seeks to promote diverse and integrated areas of molecular biology, cell biology, oncology, and genetics.
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