ZFP64 drives glycolysis-mediated stem cell-like properties and tumorigenesis in breast cancer

IF 5.7 2区 生物学 Q1 BIOLOGY
Jiayi Sun, Jinquan Liu, Yudong Hou, Jianheng Bao, Teng Wang, Longbi Liu, Yidan Zhang, Rui Zhong, Zhenxuan Sun, Yan Ye, Jintao Liu
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Abstract

Breast cancer (BC) is a great clinical challenge because of its aggressiveness and poor prognosis. Zinc Finger Protein 64 (ZFP64), as a transcriptional factor, is responsible for the development and progression of cancers. This study aims to investigate whether ZFP64 regulates stem cell-like properties and tumorigenesis in BC by the glycolytic pathway. It was demonstrated that ZFP64 was overexpressed in BC specimens compared to adjacent normal tissues, and patients with high ZFP64 expression had shorter overall survival and disease-free survival. The analysis of the association of ZFP64 expression with clinicopathological characteristics showed that high ZFP64 expression is closely associated with N stage, TNM stage, and progesterone receptor status. Knockdown of ZFP64 suppressed the viability and colony formation capacity of BC cells by CCK8 and colony formation assays. The subcutaneous xenograft models revealed that ZFP64 knockdown reduced the volume of formatted tumors, and decreased Ki67 expression in tumors. The opposite effects on cell proliferation and tumorigenesis were demonstrated by ZFP64 overexpression. Furthermore, we suggested that the stem cell-like properties of BC cells were inhibited by ZFP64 depletion, as evidenced by the decreased size and number of formatted mammospheres, the downregulated expressions of OCT4, Nanog, and SOX2 proteins, as well as the reduced proportion of CD44+/CD24− subpopulations. Mechanistically, glycolysis was revealed to mediate the effect of ZFP64 using mRNA-seq analysis. Results showed that ZFP64 knockdown blocked the glycolytic process, as indicated by decreasing glycolytic metabolites, inhibiting glucose consumption, and reducing lactate and ATP production. As a transcription factor, we identified that ZFP64 was directly bound to the promoters of glycolysis-related genes (ALDOC, ENO2, HK2, and SPAG4), and induced the transcription of these genes by ChIP and dual-luciferase reporter assays. Blocking the glycolytic pathway by the inhibition of glycolytic enzymes ENO2/HK2 suppressed the high proliferation and stem cell-like properties of BC cells induced by ZFP64 overexpression. These data support that ZFP64 promotes stem cell-like properties and tumorigenesis of BC by activating glycolysis in a transcriptional mechanism.
ZFP64 驱动糖酵解介导的乳腺癌干细胞样特性和肿瘤发生
乳腺癌(BC)因其侵袭性强、预后差而成为临床上的一大难题。锌指蛋白64(ZFP64)作为一种转录因子,对癌症的发生和发展负有责任。本研究旨在探讨ZFP64是否通过糖酵解途径调控BC的干细胞样特性和肿瘤发生。研究表明,与邻近的正常组织相比,ZFP64在BC标本中过表达,ZFP64高表达的患者总生存期和无病生存期较短。ZFP64表达与临床病理特征的关联分析表明,ZFP64的高表达与N分期、TNM分期和孕激素受体状态密切相关。通过CCK8和集落形成试验,敲除ZFP64抑制了BC细胞的活力和集落形成能力。皮下异种移植模型显示,ZFP64的敲除减少了成形肿瘤的体积,并降低了肿瘤中Ki67的表达。ZFP64过表达则对细胞增殖和肿瘤发生产生了相反的影响。此外,我们还发现,BC细胞的干细胞样特性受到了ZFP64耗竭的抑制,这表现在成形乳球的大小和数量减少,OCT4、Nanog和SOX2蛋白的表达下调,以及CD44+/CD24-亚群比例降低。mRNA-seq分析揭示了糖酵解介导ZFP64效应的机制。结果显示,ZFP64基因敲除阻断了糖酵解过程,表现为糖酵解代谢产物减少、葡萄糖消耗受到抑制、乳酸和ATP生成减少。作为一种转录因子,我们发现 ZFP64 直接与糖酵解相关基因(ALDOC、ENO2、HK2 和 SPAG4)的启动子结合,并通过 ChIP 和双荧光素酶报告实验诱导了这些基因的转录。通过抑制糖酵解酶ENO2/HK2阻断糖酵解途径,抑制了ZFP64过表达诱导的BC细胞的高增殖和干细胞样特性。这些数据支持ZFP64在转录机制中通过激活糖酵解促进BC的干细胞样特性和肿瘤发生。
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
Biology Direct
Biology Direct 生物-生物学
CiteScore
6.40
自引率
10.90%
发文量
32
审稿时长
7 months
期刊介绍: Biology Direct serves the life science research community as an open access, peer-reviewed online journal, providing authors and readers with an alternative to the traditional model of peer review. Biology Direct considers original research articles, hypotheses, comments, discovery notes and reviews in subject areas currently identified as those most conducive to the open review approach, primarily those with a significant non-experimental component.
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