Lower respiratory tract infection induced by a genetically modified picornavirus in its natural murine host.

Lower respiratory tract infection induced by a genetically modified picornavirus in its natural murine host.

Infections with the picornavirus, human rhinovirus (HRV), are a major cause of wheezing illnesses and asthma exacerbations. In developing a murine model of picornaviral airway infection, we noted the absence of murine rhinoviruses and that mice are not natural hosts for HRV. The picornavirus, mengov...

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Main Authors: Louis A Rosenthal, Renee J Szakaly, Svetlana P Amineva, Yina Xing, Marchel R Hill, Ann C Palmenberg, James E Gern, Ronald L Sorkness
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2012-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3280220?pdf=render
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spelling doaj-687b7b64e1774621af3d917d701de9392020-11-25T01:48:33ZengPublic Library of Science (PLoS)PLoS ONE1932-62032012-01-0172e3206110.1371/journal.pone.0032061Lower respiratory tract infection induced by a genetically modified picornavirus in its natural murine host.Louis A RosenthalRenee J SzakalySvetlana P AminevaYina XingMarchel R HillAnn C PalmenbergJames E GernRonald L SorknessInfections with the picornavirus, human rhinovirus (HRV), are a major cause of wheezing illnesses and asthma exacerbations. In developing a murine model of picornaviral airway infection, we noted the absence of murine rhinoviruses and that mice are not natural hosts for HRV. The picornavirus, mengovirus, induces lethal systemic infections in its natural murine hosts, but small genetic differences can profoundly affect picornaviral tropism and virulence. We demonstrate that inhalation of a genetically attenuated mengovirus, vMC(0), induces lower respiratory tract infections in mice. After intranasal vMC(0) inoculation, lung viral titers increased, peaking at 24 h postinoculation with viral shedding persisting for 5 days, whereas HRV-A01a lung viral titers decreased and were undetectable 24 h after intranasal inoculation. Inhalation of vMC(0), but not vehicle or UV-inactivated vMC(0), induced an acute respiratory illness, with body weight loss and lower airway inflammation, characterized by increased numbers of airway neutrophils and lymphocytes and elevated pulmonary expression of neutrophil chemoattractant CXCR2 ligands (CXCL1, CXCL2, CXCL5) and interleukin-17A. Mice inoculated with vMC(0), compared with those inoculated with vehicle or UV-inactivated vMC(0), exhibited increased pulmonary expression of interferon (IFN-α, IFN-β, IFN-λ), viral RNA sensors [toll-like receptor (TLR)3, TLR7, nucleotide-binding oligomerization domain containing 2 (NOD2)], and chemokines associated with HRV infection in humans (CXCL10, CCL2). Inhalation of vMC(0), but not vehicle or UV-inactivated vMC(0), was accompanied by increased airway fluid myeloperoxidase levels, an indicator of neutrophil activation, increased MUC5B gene expression, and lung edema, a sign of infection-related lung injury. Consistent with experimental HRV inoculations of nonallergic, nonasthmatic human subjects, there were no effects on airway hyperresponsiveness after inhalation of vMC(0) by healthy mice. This novel murine model of picornaviral airway infection and inflammation should be useful for defining mechanisms of HRV pathogenesis in humans.http://europepmc.org/articles/PMC3280220?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Louis A Rosenthal
Renee J Szakaly
Svetlana P Amineva
Yina Xing
Marchel R Hill
Ann C Palmenberg
James E Gern
Ronald L Sorkness
spellingShingle Louis A Rosenthal
Renee J Szakaly
Svetlana P Amineva
Yina Xing
Marchel R Hill
Ann C Palmenberg
James E Gern
Ronald L Sorkness
Lower respiratory tract infection induced by a genetically modified picornavirus in its natural murine host.
PLoS ONE
author_facet Louis A Rosenthal
Renee J Szakaly
Svetlana P Amineva
Yina Xing
Marchel R Hill
Ann C Palmenberg
James E Gern
Ronald L Sorkness
author_sort Louis A Rosenthal
title Lower respiratory tract infection induced by a genetically modified picornavirus in its natural murine host.
title_short Lower respiratory tract infection induced by a genetically modified picornavirus in its natural murine host.
title_full Lower respiratory tract infection induced by a genetically modified picornavirus in its natural murine host.
title_fullStr Lower respiratory tract infection induced by a genetically modified picornavirus in its natural murine host.
title_full_unstemmed Lower respiratory tract infection induced by a genetically modified picornavirus in its natural murine host.
title_sort lower respiratory tract infection induced by a genetically modified picornavirus in its natural murine host.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2012-01-01
description Infections with the picornavirus, human rhinovirus (HRV), are a major cause of wheezing illnesses and asthma exacerbations. In developing a murine model of picornaviral airway infection, we noted the absence of murine rhinoviruses and that mice are not natural hosts for HRV. The picornavirus, mengovirus, induces lethal systemic infections in its natural murine hosts, but small genetic differences can profoundly affect picornaviral tropism and virulence. We demonstrate that inhalation of a genetically attenuated mengovirus, vMC(0), induces lower respiratory tract infections in mice. After intranasal vMC(0) inoculation, lung viral titers increased, peaking at 24 h postinoculation with viral shedding persisting for 5 days, whereas HRV-A01a lung viral titers decreased and were undetectable 24 h after intranasal inoculation. Inhalation of vMC(0), but not vehicle or UV-inactivated vMC(0), induced an acute respiratory illness, with body weight loss and lower airway inflammation, characterized by increased numbers of airway neutrophils and lymphocytes and elevated pulmonary expression of neutrophil chemoattractant CXCR2 ligands (CXCL1, CXCL2, CXCL5) and interleukin-17A. Mice inoculated with vMC(0), compared with those inoculated with vehicle or UV-inactivated vMC(0), exhibited increased pulmonary expression of interferon (IFN-α, IFN-β, IFN-λ), viral RNA sensors [toll-like receptor (TLR)3, TLR7, nucleotide-binding oligomerization domain containing 2 (NOD2)], and chemokines associated with HRV infection in humans (CXCL10, CCL2). Inhalation of vMC(0), but not vehicle or UV-inactivated vMC(0), was accompanied by increased airway fluid myeloperoxidase levels, an indicator of neutrophil activation, increased MUC5B gene expression, and lung edema, a sign of infection-related lung injury. Consistent with experimental HRV inoculations of nonallergic, nonasthmatic human subjects, there were no effects on airway hyperresponsiveness after inhalation of vMC(0) by healthy mice. This novel murine model of picornaviral airway infection and inflammation should be useful for defining mechanisms of HRV pathogenesis in humans.
url http://europepmc.org/articles/PMC3280220?pdf=render
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