Residential College | false |
Status | 已發表Published |
YTHDC1 as a tumor progression suppressor through modulating FSP1-dependent ferroptosis suppression in lung cancer | |
Yuan, Shuai1; Xi, Shu1; Weng, Hong1; Guo, Meng Meng1; Zhang, Jin Hui1; Yu, Zhi Ping1; Zhang, Haozhe2; Yu, Zhaojun3; Xing, Zengzhen2; Liu, Meng Yang1; Ming, Dao Jing1; Sah, Rajiv Kumar2; Zhou, Yi2; Li, Gang4![]() ![]() ![]() ![]() | |
2023-10-30 | |
Source Publication | Cell Death and Differentiation
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ISSN | 1350-9047 |
Volume | 30Pages:2477-2490 |
Abstract | Ferroptosis is a regulated cell death process initiated by iron-dependent phospholipid peroxidation and is mainly suppressed by GPX4-dependent and FSP1-dependent surveillance mechanisms. However, how the ferroptosis surveillance system is regulated during cancer development remains largely unknown. Here, we report that the YTHDC1-mediated mA epigenetic regulation of FSP1 alleviates the FSP1-dependent ferroptosis suppression that partially contributes to the tumor suppressive role of YTHDC1 in lung cancer progression. YTHDC1 knockdown promoted the lung tumor progression and upregulated FSP1 protein level that resulted in ferroptosis resistance of lung cancer cells. Silencing FSP1 abrogated YTHDC1 knockdown-induced proliferation increase and ferroptosis resistance. Mechanistically, YTHDC1 binding to the mA sites in the FSP1 3’-UTR recruited the alternative polyadenylation regulator CSTF3 to generate a less stable shorter 3’-UTR contained FSP1 mRNA, whereas YTHDC1 downregulation generated the longer 3’-UTR contained FSP1 mRNA that is stabilized by RNA binding protein HuR and thus led to the enhanced FSP1 protein level. Therefore, our findings identify YTHDC1 as a tumor progression suppressor in lung cancer and a ferroptosis regulator through modulating the FSP1 mRNA stability and thus suggest a ferroptosis-related therapeutic option for YTHDC1 lung cancer. |
Keyword | Alternative Polyadenylation Cell-death Methylation Roles |
DOI | 10.1038/s41418-023-01234-w |
URL | View the original |
Indexed By | SCIE |
Language | 英語English |
WOS Research Area | Biochemistry & Molecular Biology ; Cell Biology |
WOS Subject | Biochemistry & Molecular Biology ; Cell Biology |
WOS ID | WOS:001096035200001 |
Publisher | SPRINGERNATURE, CAMPUS, 4 CRINAN ST, LONDON N1 9XW, ENGLAND |
Scopus ID | 2-s2.0-85175146434 |
Fulltext Access | |
Citation statistics | |
Document Type | Journal article |
Collection | Ministry of Education Frontiers Science Center for Precision Oncology, University of Macau Faculty of Health Sciences Cancer Centre |
Corresponding Author | Li, Yafei; Zeng, Xian Tao; Hu, Hailiang |
Affiliation | 1.Center for Evidence-Based and Translational Medicine, Zhongnan Hospital of Wuhan University, Wuhan, China 2.Department of Biochemistry, School of Medicine, Southern University of Science and Technology, Shenzhen, China 3.Department of Urology, The Second Affiliated Hospital of Nanchang University, Nanchang, China 4.Cancer Center, Faculty of Health Sciences, MoE Frontier Science Center for Precision Oncology, University of Macau, Taipa, SAR, Macao 5.Key University Laboratory of Metabolism and Health of Guangdong, Southern University of Science and Technology, Shenzhen, China 6.Department of Epidemiology, College of Preventive Medicine, Army Medical University, Chongqing, China |
Recommended Citation GB/T 7714 | Yuan, Shuai,Xi, Shu,Weng, Hong,et al. YTHDC1 as a tumor progression suppressor through modulating FSP1-dependent ferroptosis suppression in lung cancer[J]. Cell Death and Differentiation, 2023, 30, 2477-2490. |
APA | Yuan, Shuai., Xi, Shu., Weng, Hong., Guo, Meng Meng., Zhang, Jin Hui., Yu, Zhi Ping., Zhang, Haozhe., Yu, Zhaojun., Xing, Zengzhen., Liu, Meng Yang., Ming, Dao Jing., Sah, Rajiv Kumar., Zhou, Yi., Li, Gang., Zeng, Tao., Hong, Xin., Li, Yafei., Zeng, Xian Tao., & Hu, Hailiang (2023). YTHDC1 as a tumor progression suppressor through modulating FSP1-dependent ferroptosis suppression in lung cancer. Cell Death and Differentiation, 30, 2477-2490. |
MLA | Yuan, Shuai,et al."YTHDC1 as a tumor progression suppressor through modulating FSP1-dependent ferroptosis suppression in lung cancer".Cell Death and Differentiation 30(2023):2477-2490. |
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