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Epitranscriptic regulation of <i>HRAS</i> by <i>N</i> <sup>6</sup> -methyladenosine drives tumor progression

Yongbo Pan, Yinmin Gu, Tihui Liu, Qingqing Zhang, Facai Yang, Liqiang Duan, Shuwen Cheng, Xiao‐Feng Zhu, Yibo Xi, Xiaoli Chang, Qinong Ye, Shan Gao

2023Proceedings of the National Academy of Sciences30 citationsDOIOpen Access PDF

Abstract

Overexpression of Ras, in addition to the oncogenic mutations, occurs in various human cancers. However, the mechanisms for epitranscriptic regulation of RAS in tumorigenesis remain unclear. Here, we report that the widespread N 6 -methyladenosine (m 6 A) modification of HRAS , but not KRAS and NRAS , is higher in cancer tissues compared with the adjacent tissues, which results in the increased expression of H-Ras protein, thus promoting cancer cell proliferation and metastasis. Mechanistically, three m 6 A modification sites of HRAS 3′ UTR, which is regulated by FTO and bound by YTHDF1, but not YTHDF2 nor YTHDF3, promote its protein expression by the enhanced translational elongation. In addition, targeting HRAS m 6 A modification decreases cancer proliferation and metastasis. Clinically, up-regulated H-Ras expression correlates with down-regulated FTO and up-regulated YTHDF1 expression in various cancers. Collectively, our study reveals a linking between specific m 6 A modification sites of HRAS and tumor progression, which provides a new strategy to target oncogenic Ras signaling.

Topics & Concepts

HRASNeuroblastoma RAS viral oncogene homologCarcinogenesisCancer researchKRASBiologyCancerMetastasisChemistryGeneticsColorectal cancerRNA modifications and cancerCancer-related gene regulationRNA Research and Splicing
Epitranscriptic regulation of <i>HRAS</i> by <i>N</i> <sup>6</sup> -methyladenosine drives tumor progression | Litcius