PLoS Pathogens (Oct 2017)

miRNA independent hepacivirus variants suggest a strong evolutionary pressure to maintain miR-122 dependence.

  • Yingpu Yu,
  • Troels K H Scheel,
  • Joseph M Luna,
  • Hachung Chung,
  • Eiko Nishiuchi,
  • Margaret A Scull,
  • Natalia Echeverría,
  • Inna Ricardo-Lax,
  • Amit Kapoor,
  • W Ian Lipkin,
  • Thomas J Divers,
  • Douglas F Antczak,
  • Bud C Tennant,
  • Charles M Rice

DOI
https://doi.org/10.1371/journal.ppat.1006694
Journal volume & issue
Vol. 13, no. 10
p. e1006694

Abstract

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Hepatitis C virus (HCV) requires the liver specific micro-RNA (miRNA), miR-122, to replicate. This was considered unique among RNA viruses until recent discoveries of HCV-related hepaciviruses prompting the question of a more general miR-122 dependence. Among hepaciviruses, the closest known HCV relative is the equine non-primate hepacivirus (NPHV). Here, we used Argonaute cross-linking immunoprecipitation (AGO-CLIP) to confirm AGO binding to the single predicted miR-122 site in the NPHV 5'UTR in vivo. To study miR-122 requirements in the absence of NPHV-permissive cell culture systems, we generated infectious NPHV/HCV chimeric viruses with the 5' end of NPHV replacing orthologous HCV sequences. These chimeras were viable even in cells lacking miR-122, although miR-122 presence enhanced virus production. No other miRNAs bound this region. By random mutagenesis, we isolated HCV variants partially dependent on miR-122 as well as robustly replicating NPHV/HCV variants completely independent of any miRNAs. These miRNA independent variants even replicate and produce infectious particles in non-hepatic cells after exogenous delivery of apolipoprotein E (ApoE). Our findings suggest that miR-122 independent HCV and NPHV variants have arisen and been sampled during evolution, yet miR-122 dependence has prevailed. We propose that hepaciviruses may use this mechanism to guarantee liver tropism and exploit the tolerogenic liver environment to avoid clearance and promote chronicity.