๐ Activation of RNase L by murine coronavirus in myeloid cells is dependent on basal Oas gene expression and independent of virus-induced interferon
ยฉ 2016, American Society for Microbiology. The oligoadenylate synthetase (OAS)-RNase L pathway is a potent interferon (IFN)-induced antiviral activity. Upon sensing double-stranded RNA, OAS produces 2',5'-oligoadenylates (2-5A), which activate RNase L. Murine coronavirus (mouse hepatitis virus [MHV]) nonstructural protein 2 (ns2) is a 2',5'-phosphodiesterase (PDE) that cleaves 2-5A, thereby antagonizing RNase L activation. PDE activity is required for robust replication in myeloid cells, as a mutant of MHV (ns2H126R) encoding an inactive PDE fails to antagonize RNase L activation and replicates poorly in bone marrow-derived macrophages (BMM), while ns2H126R replicates to high titer in several types of nonmyeloid cells, as well as in IFN receptor-deficient (Ifnar1-/-) BMM. We reported previously that myeloid cells express significantly higher basal levels of OAS transcripts than nonmyeloid cells. Here, we investigated the contributions of Oas gene expression, basal IFN signaling, and virus-induced IFN to RNase L activation. Infection with ns2H126R activated RNase L in Ifih1-/- BMM to a similar extent as in wild-type (WT) BMM, despite the lack of IFN induction in the absence of MDA5 expression. However, ns2H126R failed to induce RNase L activation in BMM treated with IFNAR1-blocking antibody, as well as in Ifnar1-/- BMM, both expressing low basal levels of Oas genes. Thus, activation of RNase L does not require virus-induced IFN but rather correlates with adequate levels of basal Oas gene expression, maintained by basal IFN signaling. Finally, overexpression of RNase L is not sufficient to compensate for inadequate basal OAS levels.
keywords
๐ significantly higher (104)
๐ hepatitis virus (437)
๐ bone marrow (31)
๐ mouse hepatitis (371)
author
๐ค Birdwell, L. Dillon
๐ค Zalinger, Zachary B.
๐ค Li, Yize
๐ค Wright, Patrick W.
๐ค Elliott, Ruth
๐ค Rose, Kristine M.
๐ค Silverman, Robert H.
๐ค Weiss, Susan R.
year
โฐ 2016
journal
๐ Journal of Virology
issn
๐ 10985514 0022538X
volume
90
number
6
page
3160-3172
citedbycount
14
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