A CRISPR-Cas9 library screening identifies CARM1 as a critical inhibitor of ferroptosis in hepatocellular carcinoma cells

被引:7
|
作者
Cheng, Yiming [1 ]
Wang, Xiaochen [1 ]
Huang, Shuyu [1 ]
Zhang, Liang [2 ]
Lan, Bei [1 ]
Li, Xuanyuan [1 ]
Chen, Hao [1 ]
Liu, Zhenfeng [1 ]
Su, Yijie [1 ]
Xi, Lishan [1 ]
Feng, Shengyun [1 ]
Guo, Yanxuan [1 ]
Zhou, Jun [3 ]
Wang, Yingmei [4 ,5 ]
Xuan, Chenghao [1 ,6 ]
机构
[1] Tianjin Med Univ, Gen Hosp, Prov & Minist Cosponsored Collaborat Innovat Ctr M, Dept Biochem & Mol Biol,Tianjin Key Lab Female Rep, Tianjin 300070, Peoples R China
[2] Shandong First Med Univ, Jinan Cent Hosp, Res Ctr Translat Med, Jinan 250013, Shandong, Peoples R China
[3] Shandong Normal Univ, Coll Life Sci, Inst Biomed Sci, Jinan 250014, Shandong, Peoples R China
[4] Tianjin Med Univ, Gen Hosp, Dept Gynecol & Obstet, Tianjin 300052, Peoples R China
[5] Tianjin Med Univ, Gen Hosp, Prov & Minist Cosponsored Collaborat Innovat Ctr M, Dept Biochem & Mol Biol,Tianjin Key Lab Female Rep, Tianjin 300070, Peoples R China
[6] Tianjin Med Univ, Gen Hosp, Dept Gynecol & Obstet, Tianjin 300052, Peoples R China
来源
MOLECULAR THERAPY NUCLEIC ACIDS | 2023年 / 34卷
基金
中国国家自然科学基金;
关键词
MECHANISMS; DEATH; SORAFENIB; PROTECTS; RESISTANCE; PATHWAY;
D O I
10.1016/j.omtn.2023.102063
中图分类号
R-3 [医学研究方法]; R3 [基础医学];
学科分类号
1001 ;
摘要
Ferroptosis is an iron-catalyzed form of regulated cell death that results from the accumulation of lipid peroxidation products and reactive oxygen species to a lethal content. However, the transcriptional regulation of ferroptosis is not well under-stood. Sorafenib, a standard drug for hepatocellular carcinoma (HCC), induces ferroptosis in HCC cells. In this study, we con-ducted a CRISPR-Cas9 library screening targeting epigenetic factors and identified coactivator-associated arginine methyl-transferase 1 (CARM1) as a critical inhibitor of ferroptosis. CARM1 depletion intensified Sorafenib-induced ferroptosis, resulting in decreased cell viability, reduced cellular glutathione level, increased lipid peroxidation, and altered mitochondrial crista structure. Additionally, we investigated a CARM1 inhibitor (CARM1i) as a potential ferroptosis inducer. Combining the CARM1i with Sorafenib enhanced the induction of ferroptosis. Notably, both CARM1 knockdown and CARM1i showed cooperative effects with Sorafenib in inhibiting HCC growth in mice. The underlying mechanism involves CARM1-catalyzed H3R26me2a on the promoter of glutathione peroxidase 4, leading to its transcriptional activation and sub-sequent ferroptosis inhibition. Furthermore, Sorafenib treatment induced the transcription of CARM1 through the MDM2-p53 axis. In summary, our findings establish CARM1 as a critical ferroptosis inhibitor and highlight the potential of CARM1is as novel ferroptosis inducers, providing promising therapeutic strategies for HCC treatment.
引用
收藏
页数:13
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