| Literature DB >> 33910046 |
Yi Liu1, Guanghao Liang2, Hongjiao Xu3, Wenxin Dong1, Ze Dong3, Zhiwei Qiu1, Zihao Zhang1, Fangle Li2, Yue Huang4, Yilin Li1, Jun Wu5, Shenyi Yin6, Yawei Zhang2, Peijin Guo1, Jun Liu7, Jianzhong Jeff Xi6, Peng Jiang5, Dali Han8, Cai-Guang Yang9, Meng Michelle Xu10.
Abstract
The ever-increasing understanding of the complexity of factors and regulatory layers that contribute to immune evasion facilitates the development of immunotherapies. However, the diversity of malignant tumors limits many known mechanisms in specific genetic and epigenetic contexts, manifesting the need to discover general driver genes. Here, we have identified the m6A demethylase FTO as an essential epitranscriptomic regulator utilized by tumors to escape immune surveillance through regulation of glycolytic metabolism. We show that FTO-mediated m6A demethylation in tumor cells elevates the transcription factors c-Jun, JunB, and C/EBPβ, which allows the rewiring of glycolytic metabolism. Fto knockdown impairs the glycolytic activity of tumor cells, which restores the function of CD8+ T cells, thereby inhibiting tumor growth. Furthermore, we developed a small-molecule compound, Dac51, that can inhibit the activity of FTO, block FTO-mediated immune evasion, and synergize with checkpoint blockade for better tumor control, suggesting reprogramming RNA epitranscriptome as a potential strategy for immunotherapy.Entities:
Keywords: RNA m6A modification; demethylase FTO; epitranscriptome; glycolytic metabolism; immune surveillance and immunotherapy
Mesh:
Substances:
Year: 2021 PMID: 33910046 DOI: 10.1016/j.cmet.2021.04.001
Source DB: PubMed Journal: Cell Metab ISSN: 1550-4131 Impact factor: 27.287