Publication
2'-O methylation of the viral mRNA cap evades host restriction by IFIT family members
Journal Paper/Review - Nov 18, 2010
Daffis Stephane, Shi Pei-Yong, Gale Jr Michael, Buller R Mark, Pierson Theodore C, Klimstra William B, Fensterl Volker, Sen Ganes C, Thiel Volker, Dong Hongping, Züst Roland, Schneller Stewart, Lin Tsai-Yu, Errett John, Youn Soonjeon, Li Jianqing, Schriewer Jill, Szretter Kristy J, Diamond Michael S
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PubMed
Doi
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Journal
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Issn Electronic
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Brief description/objective
Cellular messenger RNA (mRNA) of higher eukaryotes and many viral RNAs are methylated at the N-7 and 2'-O positions of the 5' guanosine cap by specific nuclear and cytoplasmic methyltransferases (MTases), respectively. Whereas N-7 methylation is essential for RNA translation and stability, the function of 2'-O methylation has remained uncertain since its discovery 35 years ago. Here we show that a West Nile virus (WNV) mutant (E218A) that lacks 2'-O MTase activity was attenuated in wild-type primary cells and mice but was pathogenic in the absence of type I interferon (IFN) signalling. 2'-O methylation of viral RNA did not affect IFN induction in WNV-infected fibroblasts but instead modulated the antiviral effects of IFN-induced proteins with tetratricopeptide repeats (IFIT), which are interferon-stimulated genes (ISGs) implicated in regulation of protein translation. Poxvirus and coronavirus mutants that lacked 2'-O MTase activity similarly showed enhanced sensitivity to the antiviral actions of IFN and, specifically, IFIT proteins. Our results demonstrate that the 2'-O methylation of the 5' cap of viral RNA functions to subvert innate host antiviral responses through escape of IFIT-mediated suppression, and suggest an evolutionary explanation for 2'-O methylation of cellular mRNA: to distinguish self from non-self RNA. Differential methylation of cytoplasmic RNA probably serves as an example for pattern recognition and restriction of propagation of foreign viral RNA in host cells.