| Literature DB >> 27841874 |
Abigail Jarret1, Adelle P McFarland1, Stacy M Horner1, Alison Kell1, Johannes Schwerk1, MeeAe Hong1, Samantha Badil1, Rochelle C Joslyn1, Darren P Baker2, Mary Carrington3,4, Curt H Hagedorn5, Michael Gale1, Ram Savan1.
Abstract
Hepatitis C virus (HCV) infects 200 million people globally, and 60-80% of cases persist as a chronic infection that will progress to cirrhosis and liver cancer in 2-10% of patients. We recently demonstrated that HCV induces aberrant expression of two host microRNAs (miRNAs), miR-208b and miR-499a-5p, encoded by myosin genes in infected hepatocytes. These miRNAs, along with AU-rich-element-mediated decay, suppress IFNL2 and IFNL3, members of the type III interferon (IFN) gene family, to support viral persistence. In this study, we show that miR-208b and miR-499a-5p also dampen type I IFN signaling in HCV-infected hepatocytes by directly down-regulating expression of the type I IFN receptor chain, IFNAR1. Inhibition of these miRNAs by using miRNA inhibitors during HCV infection increased expression of IFNAR1. Additionally, inhibition rescued the antiviral response to exogenous type I IFN, as measured by a marked increase in IFN-stimulated genes and a decrease in HCV load. Treatment of HCV-infected hepatocytes with type I IFN increased expression of myosins over HCV infection alone. Since these miRNAs can suppress type III IFN family members, these data collectively define a novel cross-regulation between type I and III IFNs during HCV infection.Entities:
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Year: 2016 PMID: 27841874 PMCID: PMC5551900 DOI: 10.1038/nm.4211
Source DB: PubMed Journal: Nat Med ISSN: 1078-8956 Impact factor: 53.440