N(6)‐methyladenosine‐binding protein YTHDF1 suppresses EBV replication and promotes EBV RNA decay |
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| Authors: | Tian&#x Liang Xia,Xingyang Li,Xueping Wang,Yun&#x Jia Zhu,Hua Zhang,Weisheng Cheng,Mei&#x Ling Chen,Ying Ye,Yan Li,Ao Zhang,Dan&#x Ling Dai,Qian&#x Ying Zhu,Li Yuan,Jian Zheng,Huilin Huang,Si&#x Qi Chen,Zhi&#x Wen Xiao,Hong&#x Bo Wang,Gaurab Roy,Qian Zhong,Dongxin Lin,Yi&#x Xin Zeng,Jinkai Wang,Bo Zhao,Benjamin E Gewurz,Jianjun Chen,Zhixiang Zuo,Mu&#x Sheng Zeng |
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| Abstract: | N 6‐methyladenosine (m6A) modification of mRNA mediates diverse cellular and viral functions. Infection with Epstein–Barr virus (EBV) is causally associated with nasopharyngeal carcinoma (NPC), 10% of gastric carcinoma, and various B‐cell lymphomas, in which the viral latent and lytic phases both play vital roles. Here, we show that EBV transcripts exhibit differential m6A modification in human NPC biopsies, patient‐derived xenograft tissues, and cells at different EBV infection stages. m6A‐modified EBV transcripts are recognized and destabilized by the YTHDF1 protein, which leads to the m6A‐dependent suppression of EBV infection and replication. Mechanistically, YTHDF1 hastens viral RNA decapping and mediates RNA decay by recruiting RNA degradation complexes, including ZAP, DDX17, and DCP2, thereby post‐transcriptionally downregulating the expression of EBV genes. Taken together, our results reveal the critical roles of m6A modifications and their reader YTHDF1 in EBV replication. These findings contribute novel targets for the treatment of EBV‐associated cancers. |
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| Keywords: | Epstein– Barr virus, m6A modification, RNA decay, viral replication, YTHDF1 |
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