癌变
RNA甲基化
核糖核酸
Wnt信号通路
生物
N6-甲基腺苷
细胞生物学
机制(生物学)
甲基化
翻译(生物学)
小核RNA
信使核糖核酸
信号转导
化学
癌症研究
生物化学
甲基转移酶
基因
非编码RNA
认识论
哲学
作者
Xin Xu,Lifang Ma,Xiao Zhang,Susu Guo,Wanxin Guo,Yikun Wang,Shiyu Qiu,Xiaoting Tian,Yayou Miao,Yongchun Yu,Jiayi Wang
标识
DOI:10.1016/j.ymthe.2022.12.013
摘要
N6-Methyladenosine (m6A) RNA modification, methylation at the N6 position of adenosine, plays critical roles in tumorigenesis. m6A readers recognize m6A modifications and thus act as key executors for the biological consequences of RNA methylation. However, knowledge about the regulatory mechanism(s) of m6A readers is extremely limited. In this study, RN7SK was identified as a small nuclear RNA that interacts with m6A readers. m6A readers recognized and facilitated secondary structure formation of m6A-modified RN7SK, which in turn prevented m6A reader mRNA degradation from exonucleases. Thus, a positive feedback circuit between RN7SK and m6A readers is established in tumor cells. From findings on the interaction with RN7SK, new m6A readers, such as EWS RNA binding protein 1 (EWSR1) and KH RNA binding domain containing, signal transduction-associated 1 (KHDRBS1), were identified and shown to boost Wnt/β-catenin signaling and tumorigenesis by suppressing translation of Cullin1 (CUL1). Moreover, several Food and Drug Administration-approved small molecules were demonstrated to reduce RN7SK expression and inhibit tumorigenesis. Together, these findings reveal a common regulatory mechanism of m6A readers and indicate that targeting RN7SK has strong potential for tumor treatment.
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