RNA Exosome Complex Regulates Stability of the Hepatitis B Virus X-mRNA Transcript in a Non-stop-mediated (NSD) RNA Quality Control Mechanism

Hepatitis B virus (HBV) is a stealth virus, minimally inducing the interferon system required for efficient induction of both innate and adaptive immune responses. However, 90% of acutely infected adults can clear the virus, suggesting the presence of other, interferon-independent pathways leading t...

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Bibliographic Details
Published in:The Journal of biological chemistry 2016-07, Vol.291 (31), p.15958-15974
Main Authors: Aly, Hussein H., Suzuki, Junya, Watashi, Koichi, Chayama, Kazuaki, Hoshino, Shin-ichi, Hijikata, Makoto, Kato, Takanobu, Wakita, Takaji
Format: Article
Language:English
Subjects:
Codon, Initiator - genetics
Codon, Initiator - metabolism
DNA Helicases - genetics
DNA Helicases - metabolism
exosome complex
Exosome Multienzyme Ribonuclease Complex - genetics
Exosome Multienzyme Ribonuclease Complex - metabolism
HBS1L
Hep G2 Cells
hepatitis B virus (HBV, Hep B)
Hepatitis B virus - genetics
Hepatitis B virus - metabolism
Humans
Microbiology
Non-Stop mediated RNA Decay (NSD)
RNA degradation
RNA Exosome
RNA helicase
RNA Stability
RNA, Messenger - genetics
RNA, Messenger - metabolism
RNA, Viral - genetics
RNA, Viral - metabolism
RNA-binding protein
SKIV2L
Trans-Activators - biosynthesis
Trans-Activators - genetics
Viral Regulatory and Accessory Proteins
virus restriction factor
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Summary:Hepatitis B virus (HBV) is a stealth virus, minimally inducing the interferon system required for efficient induction of both innate and adaptive immune responses. However, 90% of acutely infected adults can clear the virus, suggesting the presence of other, interferon-independent pathways leading to viral clearance. Given the known ability of helicases to bind viral nucleic acids, we performed a functional screening assay to identify helicases that regulate HBV replication. We identified the superkiller viralicidic activity 2-like (SKIV2L) RNA helicase (a homolog of the Saccharomyces cerevisiae Ski2 protein) on the basis of its direct and preferential interaction with HBV X-mRNA. This interaction was essential for HBV X-mRNA degradation at the RNA exosome. The degradation of HBV X-mRNA at the RNA exosome was also mediated by HBS1L (HBS1-like translational GTPase) protein, a known component of the host RNA quality control system. We found that the redundant HBV-precore translation initiation site present at the 3′-end of HBV X-mRNA (3′ precore) is translationally active. The initiation of translation from this site without a proper stop codon was identified by the non-stop-mediated RNA decay mechanism leading to its degradation. Although 3′ precore is present in the five main HBV-RNA transcripts, only X-mRNA lacks the presence of an upstream start codons for large, middle, and small (L, M, and S) HBV surface proteins. These upstream codons are in-frame with 3′ precore translation initiation site, blocking its translation from the other HBV-mRNA transcripts. To our knowledge, this is the first demonstration of the anti-viral function of the non-stop-mediated RNA decay mechanism.
ISSN:0021-9258
1083-351X
DOI:10.1074/jbc.M116.724641