Rapid reversal of innate immune dysregulation in blood of patients and livers of humanized mice with HCV following DAA therapy

Chronic hepatitis C virus (HCV) infection results in sustained immune activation in both the periphery and hepatic tissue. HCV infection induces innate immune signaling that is responsible for recognition of dsRNA, leading to activation of transcription factors and production of Type I and III IFNs,...

Descripción completa

Detalles Bibliográficos
Autores principales: Burchill, Matthew A., Roby, Justin A., Crochet, Nanette, Wind-Rotolo, Megan, Stone, Amy E., Edwards, Michael G., Dran, Rachael J., Kriss, Michael S., Gale, Michael, Rosen, Hugo R.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2017
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5645093/
https://www.ncbi.nlm.nih.gov/pubmed/29040318
http://dx.doi.org/10.1371/journal.pone.0186213
_version_ 1783271831697883136
author Burchill, Matthew A.
Roby, Justin A.
Crochet, Nanette
Wind-Rotolo, Megan
Stone, Amy E.
Edwards, Michael G.
Dran, Rachael J.
Kriss, Michael S.
Gale, Michael
Rosen, Hugo R.
author_facet Burchill, Matthew A.
Roby, Justin A.
Crochet, Nanette
Wind-Rotolo, Megan
Stone, Amy E.
Edwards, Michael G.
Dran, Rachael J.
Kriss, Michael S.
Gale, Michael
Rosen, Hugo R.
author_sort Burchill, Matthew A.
collection PubMed
description Chronic hepatitis C virus (HCV) infection results in sustained immune activation in both the periphery and hepatic tissue. HCV infection induces innate immune signaling that is responsible for recognition of dsRNA, leading to activation of transcription factors and production of Type I and III IFNs, as well as pro-inflammatory cytokines and chemokines. Continued activation of host-immune mediated inflammation is thought to contribute to pathologic changes that result in progressive hepatic fibrosis. The current standard treatment for chronic HCV infection is directly-acting antivirals (DAAs), which have provided the unique opportunity to determine whether successful, rapid treatment-induced eradication of viral RNA normalizes the dysregulated antiviral innate immune response in patients chronically infected with HCV. RESULTS: First, in patients receiving two different combinations of DAAs, we found that DAAs induced not only rapid viral clearance, but also a re-setting of antiviral immune responses in the peripheral blood. Specifically, we see a rapid decline in the expression of genes associated with chronic IFN stimulation (IFIT3, USP18, IFIT1) as well as a rapid decline in genes associated with inflammation (IL1β, CXCL10, CXCL11) in the peripheral blood that precedes the complete removal of virus from the blood. Interestingly, this rapid reversal of innate immune activation was not seen in patients who successfully clear chronic HCV infection using IFN-based therapy. Next, using a novel humanized mouse model (Fah(-/-)RAG2(-/-)IL2rg(null)—FRG), we assessed the changes that occur in the hepatic tissue following DAA treatment. DAA-mediated rapid HCV clearance resulted in blunting of the expression of proinflammatory responses while functionally restoring the RIG-I/MAVS axis in the liver of humanized mice. CONCLUSIONS: Collectively, our data demonstrate that the rapid viral clearance following treatment with DAAs results in the rebalancing of innate antiviral response in both the peripheral blood and the liver as well as enhanced antiviral signaling within previously infected hepatocytes.
format Online
Article
Text
id pubmed-5645093
institution National Center for Biotechnology Information
language English
publishDate 2017
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-56450932017-10-30 Rapid reversal of innate immune dysregulation in blood of patients and livers of humanized mice with HCV following DAA therapy Burchill, Matthew A. Roby, Justin A. Crochet, Nanette Wind-Rotolo, Megan Stone, Amy E. Edwards, Michael G. Dran, Rachael J. Kriss, Michael S. Gale, Michael Rosen, Hugo R. PLoS One Research Article Chronic hepatitis C virus (HCV) infection results in sustained immune activation in both the periphery and hepatic tissue. HCV infection induces innate immune signaling that is responsible for recognition of dsRNA, leading to activation of transcription factors and production of Type I and III IFNs, as well as pro-inflammatory cytokines and chemokines. Continued activation of host-immune mediated inflammation is thought to contribute to pathologic changes that result in progressive hepatic fibrosis. The current standard treatment for chronic HCV infection is directly-acting antivirals (DAAs), which have provided the unique opportunity to determine whether successful, rapid treatment-induced eradication of viral RNA normalizes the dysregulated antiviral innate immune response in patients chronically infected with HCV. RESULTS: First, in patients receiving two different combinations of DAAs, we found that DAAs induced not only rapid viral clearance, but also a re-setting of antiviral immune responses in the peripheral blood. Specifically, we see a rapid decline in the expression of genes associated with chronic IFN stimulation (IFIT3, USP18, IFIT1) as well as a rapid decline in genes associated with inflammation (IL1β, CXCL10, CXCL11) in the peripheral blood that precedes the complete removal of virus from the blood. Interestingly, this rapid reversal of innate immune activation was not seen in patients who successfully clear chronic HCV infection using IFN-based therapy. Next, using a novel humanized mouse model (Fah(-/-)RAG2(-/-)IL2rg(null)—FRG), we assessed the changes that occur in the hepatic tissue following DAA treatment. DAA-mediated rapid HCV clearance resulted in blunting of the expression of proinflammatory responses while functionally restoring the RIG-I/MAVS axis in the liver of humanized mice. CONCLUSIONS: Collectively, our data demonstrate that the rapid viral clearance following treatment with DAAs results in the rebalancing of innate antiviral response in both the peripheral blood and the liver as well as enhanced antiviral signaling within previously infected hepatocytes. Public Library of Science 2017-10-17 /pmc/articles/PMC5645093/ /pubmed/29040318 http://dx.doi.org/10.1371/journal.pone.0186213 Text en © 2017 Burchill et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Burchill, Matthew A.
Roby, Justin A.
Crochet, Nanette
Wind-Rotolo, Megan
Stone, Amy E.
Edwards, Michael G.
Dran, Rachael J.
Kriss, Michael S.
Gale, Michael
Rosen, Hugo R.
Rapid reversal of innate immune dysregulation in blood of patients and livers of humanized mice with HCV following DAA therapy
title Rapid reversal of innate immune dysregulation in blood of patients and livers of humanized mice with HCV following DAA therapy
title_full Rapid reversal of innate immune dysregulation in blood of patients and livers of humanized mice with HCV following DAA therapy
title_fullStr Rapid reversal of innate immune dysregulation in blood of patients and livers of humanized mice with HCV following DAA therapy
title_full_unstemmed Rapid reversal of innate immune dysregulation in blood of patients and livers of humanized mice with HCV following DAA therapy
title_short Rapid reversal of innate immune dysregulation in blood of patients and livers of humanized mice with HCV following DAA therapy
title_sort rapid reversal of innate immune dysregulation in blood of patients and livers of humanized mice with hcv following daa therapy
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5645093/
https://www.ncbi.nlm.nih.gov/pubmed/29040318
http://dx.doi.org/10.1371/journal.pone.0186213
work_keys_str_mv AT burchillmatthewa rapidreversalofinnateimmunedysregulationinbloodofpatientsandliversofhumanizedmicewithhcvfollowingdaatherapy
AT robyjustina rapidreversalofinnateimmunedysregulationinbloodofpatientsandliversofhumanizedmicewithhcvfollowingdaatherapy
AT crochetnanette rapidreversalofinnateimmunedysregulationinbloodofpatientsandliversofhumanizedmicewithhcvfollowingdaatherapy
AT windrotolomegan rapidreversalofinnateimmunedysregulationinbloodofpatientsandliversofhumanizedmicewithhcvfollowingdaatherapy
AT stoneamye rapidreversalofinnateimmunedysregulationinbloodofpatientsandliversofhumanizedmicewithhcvfollowingdaatherapy
AT edwardsmichaelg rapidreversalofinnateimmunedysregulationinbloodofpatientsandliversofhumanizedmicewithhcvfollowingdaatherapy
AT dranrachaelj rapidreversalofinnateimmunedysregulationinbloodofpatientsandliversofhumanizedmicewithhcvfollowingdaatherapy
AT krissmichaels rapidreversalofinnateimmunedysregulationinbloodofpatientsandliversofhumanizedmicewithhcvfollowingdaatherapy
AT galemichael rapidreversalofinnateimmunedysregulationinbloodofpatientsandliversofhumanizedmicewithhcvfollowingdaatherapy
AT rosenhugor rapidreversalofinnateimmunedysregulationinbloodofpatientsandliversofhumanizedmicewithhcvfollowingdaatherapy

Ejemplares similares