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N6-methyladenosine modification enables viral RNA to escape recognition by RNA sensor RIG-I.

Nat Microbiol. 2020; 
Lu M, Zhang Z, Xue M, Zhao BS, Harder O, Li A, Liang X, Gao TZ, Xu Y, Zhou J, Feng Z,, Niewiesk S, Peeples ME,, He C,,,, Li J0.
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Molecular Biology Tools These mutations were introduced in pCAGGS-G or an infectious HMPV cDNA clone, lineage A strain NL/1/00. We avoided changes that would alter the RNA secondary structures or codon usage, as predicted by the M-fold and Genscript software. Get A Quote

摘要

Internal N6-methyladenosine (m6A) modification is one of the most common and abundant modifications of RNA. However, the biological roles of viral RNA m6A remain elusive. Here, using human metapneumovirus (HMPV) as a model, we demonstrate that m6A serves as a molecular marker for innate immune discrimination of self from non-self RNAs. We show that HMPV RNAs are m6A methylated and that viral m6A methylation promotes HMPV replication and gene expression. Inactivating m6A addition sites with synonymous mutations or demethylase resulted in m6A-deficient recombinant HMPVs and virion RNAs that induced increased expression of type I interferon, which was dependent on the cytoplasmic RNA sensor RIG-I, and not on melan... More

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