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    Date Issued2020 (1)2017 (1)AuthorGu, Weifeng (2)
    Li, Lichao (2)
    Mello, Craig C. (2)Chaves, Daniel A. (1)Conte, Darryl Jr. (1)View MoreUMass Chan AffiliationRNA Therapeutics Institute (2)Department of Medicine, Division of Infectious Diseases and Immunology (1)Program in Molecular Medicine (1)Document TypeJournal Article (1)Preprint (1)KeywordNucleic Acids, Nucleotides, and Nucleosides (2)Animal Experimentation and Research (1)antiviral immunity (1)arbovirus (1)Caenorhabditis elegans (1)View MoreJournalbioRxiv (1)Current biology : CB (1)

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    The RNA phosphatase PIR-1 regulates endogenous small RNA pathways in C. elegans [preprint]

    Chaves, Daniel A.; Dai, Hui; Li, Lichao; Moresco, James J.; Eun Oh, Myung; Conte, Darryl Jr.; Yates, John R. III; Mello, Craig C.; Gu, Weifeng (2020-08-05)
    Eukaryotic cells regulate 5' triphosphorylated (ppp-) RNAs to promote cellular functions and prevent recognition by antiviral RNA sensors. For example, RNA capping enzymes possess triphosphatase domains that remove the γ phosphates of ppp-RNAs during RNA capping. Members of the closely related PIR1 family of RNA polyphosphatases remove both the β and γ phosphates from ppp-RNAs. Here we show that C. elegans PIR-1 dephosphorylates ppp-RNAs made by cellular RdRPs and is required for the maturation of 26G-RNAs, Dicer-dependent small RNAs that regulate thousands of genes during spermatogenesis and embryogenesis. PIR-1 also regulates the CSR-1 22G-RNA pathway and has critical functions in both somatic and germline development. Our findings suggest that PIR-1 modulates both Dicer-dependent and -independent Argonaute pathways, and provide insight into how cells and viruses use a conserved RNA phosphatase to regulate and respond to ppp-RNA species.
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    The Antiviral RNA Interference Response Provides Resistance to Lethal Arbovirus Infection and Vertical Transmission in Caenorhabditis elegans

    Gammon, Don B.; Ishidate, Takao; Li, Lichao; Gu, Weifeng; Silverman, Neal S.; Mello, Craig C. (2017-03-20)
    The recent discovery of the positive-sense single-stranded RNA (ssRNA) Orsay virus (OV) as a natural pathogen of the nematode Caenorhabditis elegans has stimulated interest in exploring virus-nematode interactions. However, OV infection is restricted to a small number of intestinal cells, even in nematodes defective in their antiviral RNA interference (RNAi) response, and is neither lethal nor vertically transmitted. Using a fluorescent reporter strain of the negative-sense ssRNA vesicular stomatitis virus (VSV), we show that microinjection of VSV particles leads to a dose-dependent, muscle tissue-tropic, lethal infection in C. elegans. Furthermore, we find nematodes deficient for components of the antiviral RNAi pathway, such as Dicer-related helicase 1 (DRH-1), to display hypersusceptibility to VSV infection as evidenced by elevated infection rates, virus replication in multiple tissue types, and earlier mortality. Strikingly, infection of oocytes and embryos could also be observed in drh-1 mutants. Our results suggest that the antiviral RNAi response not only inhibits vertical VSV transmission but also promotes transgenerational inheritance of antiviral immunity. Our study introduces a new, in vivo virus-host model system for exploring arbovirus pathogenesis and provides the first evidence for vertical pathogen transmission in C. elegans.
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