Cancer mutations rewire the RNA methylation specificity of METTL3-METTL14

Author:

Zhang ChiORCID,Tunes LuizaORCID,Hsieh Meng-Hsiung,Wang Ping,Kumar Ashwani,Khadgi Brijesh B.,Yang YenYu,Doxtader Katelyn A.,Herrell Emily,Koczy Oliwia,Setlem Rohit,Zhang Xunzhi,Evers Bret,Wang Yinsheng,Xing ChaoORCID,Zhu Hao,Nam YunsunORCID

Abstract

AbstractChemical modification of RNAs is important for post-transcriptional gene regulation. The METTL3-METTL14 complex generates mostN6-methyladenosine (m6A) modifications in mRNAs, and dysregulated methyltransferase expression has been linked to numerous cancers. Here we show that changes in m6A modification location can impact oncogenesis. A gain-of-function missense mutation found in cancer patients, METTL14R298P, promotes malignant cell growth in culture and in transgenic mice. The mutant methyltransferase preferentially modifies noncanonical sites containing a GGAU motif and transforms gene expression without increasing global m6A levels in mRNAs. The altered substrate specificity is intrinsic to METTL3-METTL14, helping us to propose a structural model for how the METTL3-METTL14 complex selects the cognate RNA sequences for modification. Together, our work highlights that sequence-specific m6A deposition is important for proper function of the modification and that noncanonical methylation events can impact aberrant gene expression and oncogenesis.

Publisher

Cold Spring Harbor Laboratory

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