MiR-942 mediates hepatitis C virus-induced apoptosis via regulation of ISG12a.

MiR-942 mediates hepatitis C virus-induced apoptosis via regulation of ISG12a.

The interaction between hepatitis C virus (HCV) and human hepatic innate antiviral responses is unclear. The aim of this study was to examine how human hepatocytes respond to HCV infection. An infectious HCV isolate, JFH1, was used to infect a newly established human hepatoma cell line HLCZ01. Viral...

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Main Authors: Darong Yang, Xianghe Meng, Binbin Xue, Nianli Liu, Xiaohong Wang, Haizhen Zhu
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2014-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3984147?pdf=render
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spelling doaj-68424a15b8ee4baa9f9080d248f0373c2020-11-25T00:40:04ZengPublic Library of Science (PLoS)PLoS ONE1932-62032014-01-0194e9450110.1371/journal.pone.0094501MiR-942 mediates hepatitis C virus-induced apoptosis via regulation of ISG12a.Darong YangXianghe MengBinbin XueNianli LiuXiaohong WangHaizhen ZhuThe interaction between hepatitis C virus (HCV) and human hepatic innate antiviral responses is unclear. The aim of this study was to examine how human hepatocytes respond to HCV infection. An infectious HCV isolate, JFH1, was used to infect a newly established human hepatoma cell line HLCZ01. Viral RNA or NS5A protein was examined by real-time PCR or immunofluorescence respectively. The mechanisms of HCV-induced IFN-β and apoptosis were explored. Our data showed that HLCZ01 cells supported the entire HCV lifecycle and IFN-β and interferon-stimulated genes (ISGs) were induced in HCV-infected cells. Viral infection caused apoptosis of HLCZ01 cells. Silencing of RIG-I, IRF3 or TRAIL inhibited ISG12a expression and blocked apoptosis of viral-infected HLCZ01 cells. Knockdown ISG12a blocked apoptosis of viral-infected cells. MiR-942 is a candidate negative regulator of ISG12a predicted by bioinformatics search. Moreover, HCV infection decreased miR-942 expression in HLCZ01 cells and miR-942 was inversely correlated with ISG12a expression in both HCV-infected cells and liver biopsies. MiR-942 forced expression in HLCZ01 cells decreased ISG12a expression and subsequently suppressed apoptosis triggered by HCV infection. Conversely, silencing of miR-942 expression by anti-miR-942 increased ISG12a expression and enhanced apoptosis in HCV-infected cells. Induction of Noxa by HCV infection contributed to ISG12a-mediated apoptosis. All the data indicated that innate host response is intact in HCV-infected hepatocytes. MiR-942 regulates HCV-induced apoptosis of human hepatocytes by targeting ISG12a. Our study provides a novel mechanism by which human hepatocytes respond to HCV infection.http://europepmc.org/articles/PMC3984147?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Darong Yang
Xianghe Meng
Binbin Xue
Nianli Liu
Xiaohong Wang
Haizhen Zhu
spellingShingle Darong Yang
Xianghe Meng
Binbin Xue
Nianli Liu
Xiaohong Wang
Haizhen Zhu
MiR-942 mediates hepatitis C virus-induced apoptosis via regulation of ISG12a.
PLoS ONE
author_facet Darong Yang
Xianghe Meng
Binbin Xue
Nianli Liu
Xiaohong Wang
Haizhen Zhu
author_sort Darong Yang
title MiR-942 mediates hepatitis C virus-induced apoptosis via regulation of ISG12a.
title_short MiR-942 mediates hepatitis C virus-induced apoptosis via regulation of ISG12a.
title_full MiR-942 mediates hepatitis C virus-induced apoptosis via regulation of ISG12a.
title_fullStr MiR-942 mediates hepatitis C virus-induced apoptosis via regulation of ISG12a.
title_full_unstemmed MiR-942 mediates hepatitis C virus-induced apoptosis via regulation of ISG12a.
title_sort mir-942 mediates hepatitis c virus-induced apoptosis via regulation of isg12a.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2014-01-01
description The interaction between hepatitis C virus (HCV) and human hepatic innate antiviral responses is unclear. The aim of this study was to examine how human hepatocytes respond to HCV infection. An infectious HCV isolate, JFH1, was used to infect a newly established human hepatoma cell line HLCZ01. Viral RNA or NS5A protein was examined by real-time PCR or immunofluorescence respectively. The mechanisms of HCV-induced IFN-β and apoptosis were explored. Our data showed that HLCZ01 cells supported the entire HCV lifecycle and IFN-β and interferon-stimulated genes (ISGs) were induced in HCV-infected cells. Viral infection caused apoptosis of HLCZ01 cells. Silencing of RIG-I, IRF3 or TRAIL inhibited ISG12a expression and blocked apoptosis of viral-infected HLCZ01 cells. Knockdown ISG12a blocked apoptosis of viral-infected cells. MiR-942 is a candidate negative regulator of ISG12a predicted by bioinformatics search. Moreover, HCV infection decreased miR-942 expression in HLCZ01 cells and miR-942 was inversely correlated with ISG12a expression in both HCV-infected cells and liver biopsies. MiR-942 forced expression in HLCZ01 cells decreased ISG12a expression and subsequently suppressed apoptosis triggered by HCV infection. Conversely, silencing of miR-942 expression by anti-miR-942 increased ISG12a expression and enhanced apoptosis in HCV-infected cells. Induction of Noxa by HCV infection contributed to ISG12a-mediated apoptosis. All the data indicated that innate host response is intact in HCV-infected hepatocytes. MiR-942 regulates HCV-induced apoptosis of human hepatocytes by targeting ISG12a. Our study provides a novel mechanism by which human hepatocytes respond to HCV infection.
url http://europepmc.org/articles/PMC3984147?pdf=render
work_keys_str_mv AT darongyang mir942mediateshepatitiscvirusinducedapoptosisviaregulationofisg12a
AT xianghemeng mir942mediateshepatitiscvirusinducedapoptosisviaregulationofisg12a
AT binbinxue mir942mediateshepatitiscvirusinducedapoptosisviaregulationofisg12a
AT nianliliu mir942mediateshepatitiscvirusinducedapoptosisviaregulationofisg12a
AT xiaohongwang mir942mediateshepatitiscvirusinducedapoptosisviaregulationofisg12a
AT haizhenzhu mir942mediateshepatitiscvirusinducedapoptosisviaregulationofisg12a
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