CCT3/ACTN4/TFRC axis protects hepatocellular carcinoma cells from ferroptosis by inhibiting iron endocytosis.

IF 11.4 1区 医学 Q1 ONCOLOGY Journal of Experimental & Clinical Cancer Research Pub Date : 2024-08-29 DOI:10.1186/s13046-024-03169-7
Huihui Zhu, Qiuhong Liu, Qinna Meng, Lingjian Zhang, Siwei Ju, Jiaheng Lang, Danhua Zhu, Yongxia Chen, Nadire Aishan, Xiaoxi Ouyang, Sainan Zhang, Lidan Jin, Lanlan Xiao, Linbo Wang, Lanjuan Li, Feiyang Ji
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Abstract

Sorafenib is widely used in treating advanced hepatocellular carcinoma (HCC). However, its effectiveness in prolonging patient survival is limited by the development of drug resistance. To systematically investigate the resistance mechanisms of Sorafenib, an integrative analysis combining posttranslational modification (PTM) omics and CRISPR/Cas9 knockout library screening was conducted. This analysis identified ubiquitination at lysine 21 (K21) on chaperonin-containing TCP1 subunit 3 (CCT3) as being associated with Sorafenib resistance. Transcriptomic data from HCC patients treated with Sorafenib revealed that CCT3 expression was lower in responders compared to non-responders. Experimentally, inhibiting the expression of CCT3 sensitized HCC cells to Sorafenib and enhanced Sorafenib-induced ferroptosis. Additionally, CCT3 was found to interact with ACTN4, hindering the recycling of transferrin receptor protein 1 (TFRC) to the cell membrane, thus obstructing iron endocytosis. Mechanistically, the inhibition of ferroptosis by CCT3 depends on the deubiquitination of K6-linked non-degradative ubiquitination at its K21, which occurs upon Sorafenib treatment. Moreover, CCT3 knockdown enhanced the anti-tumor effects of Sorafenib in nude mice. In summary, we have identified a novel function of the chaperone protein. Targeting the CCT3/ACTN4/TFRC axis offers a promising strategy to enhance ferroptosis and overcome Sorafenib resistance in HCC.

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CCT3/ACTN4/TFRC轴通过抑制铁的内吞保护肝癌细胞免于铁中毒。
索拉非尼被广泛用于治疗晚期肝细胞癌(HCC)。然而,由于耐药性的产生,它在延长患者生存期方面的有效性受到了限制。为了系统地研究索拉非尼的耐药机制,研究人员结合翻译后修饰(PTM)omics和CRISPR/Cas9基因敲除文库筛选进行了综合分析。该分析确定了含伴侣素的TCP1亚基3(CCT3)上赖氨酸21(K21)处的泛素化与索拉非尼耐药相关。接受索拉非尼治疗的HCC患者的转录组数据显示,与无应答者相比,应答者的CCT3表达量较低。实验表明,抑制 CCT3 的表达可使 HCC 细胞对索拉非尼敏感,并增强索拉非尼诱导的铁变态反应。此外,研究还发现CCT3与ACTN4相互作用,阻碍转铁蛋白受体蛋白1(TFRC)向细胞膜的再循环,从而阻碍铁的内吞。从机理上讲,CCT3对铁的吞吐抑制取决于其K21处与K6相连的非降解泛素化,而这种泛素化在索拉非尼处理后发生。此外,CCT3的敲除增强了索拉非尼对裸鼠的抗肿瘤作用。总之,我们发现了伴侣蛋白的一种新功能。以CCT3/ACTN4/TFRC轴为靶点,为增强铁蛋白沉降和克服HCC对索拉非尼的耐药性提供了一种前景广阔的策略。
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
CiteScore
18.20
自引率
1.80%
发文量
333
审稿时长
1 months
期刊介绍: The Journal of Experimental & Clinical Cancer Research is an esteemed peer-reviewed publication that focuses on cancer research, encompassing everything from fundamental discoveries to practical applications. We welcome submissions that showcase groundbreaking advancements in the field of cancer research, especially those that bridge the gap between laboratory findings and clinical implementation. Our goal is to foster a deeper understanding of cancer, improve prevention and detection strategies, facilitate accurate diagnosis, and enhance treatment options. We are particularly interested in manuscripts that shed light on the mechanisms behind the development and progression of cancer, including metastasis. Additionally, we encourage submissions that explore molecular alterations or biomarkers that can help predict the efficacy of different treatments or identify drug resistance. Translational research related to targeted therapies, personalized medicine, tumor immunotherapy, and innovative approaches applicable to clinical investigations are also of great interest to us. We provide a platform for the dissemination of large-scale molecular characterizations of human tumors and encourage researchers to share their insights, discoveries, and methodologies with the wider scientific community. By publishing high-quality research articles, reviews, and commentaries, the Journal of Experimental & Clinical Cancer Research strives to contribute to the continuous improvement of cancer care and make a meaningful impact on patients' lives.
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