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dc.contributor.authorde Jong, E.
dc.contributor.authorLauzon-Joset, J.F.
dc.contributor.authorLeffler, J.
dc.contributor.authorSerralha, M.
dc.contributor.authorLarcombe, Alexander
dc.contributor.authorChristophersen, Claus
dc.contributor.authorHolt, P.G.
dc.contributor.authorStrickland, D.H.
dc.contributor.authorBosco, A.
dc.date.accessioned2021-11-18T07:50:23Z
dc.date.available2021-11-18T07:50:23Z
dc.date.issued2021
dc.identifier.citationde Jong, E. and Lauzon-Joset, J.F. and Leffler, J. and Serralha, M. and Larcombe, A.N. and Christophersen, C.T. and Holt, P.G. et al. 2021. IRF7-Associated Immunophenotypes Have Dichotomous Responses to Virus/Allergen Coexposure and OM-85-Induced Reprogramming. Frontiers in Immunology. 12: Article No. 699633.
dc.identifier.urihttp://hdl.handle.net/20.500.11937/86510
dc.identifier.doi10.3389/fimmu.2021.699633
dc.description.abstract

High risk for virus-induced asthma exacerbations in children is associated with an IRF7lo immunophenotype, but the underlying mechanisms are unclear. Here, we applied a Systems Biology approach to an animal model comprising rat strains manifesting high (BN) versus low susceptibility (PVG) to experimental asthma, induced by virus/allergen coexposure, to elucidate the mechanism(s)-of-action of the high-risk asthma immunophenotype. We also investigated potential risk mitigation via pretreatment with the immune training agent OM-85. Virus/allergen coexposure in low-risk PVG rats resulted in rapid and transient airways inflammation alongside IRF7 gene network formation. In contrast, responses in high-risk BN rats were characterized by severe airways eosinophilia and exaggerated proinflammatory responses that failed to resolve, and complete absence of IRF7 gene networks. OM-85 had more profound effects in high-risk BN rats, inducing immune-related gene expression changes in lung at baseline and reducing exaggerated airway inflammatory responses to virus/allergen coexposure. In low-risk PVG rats, OM-85 boosted IRF7 gene networks in the lung but did not alter baseline gene expression or cellular influx. Distinct IRF7-associated asthma risk immunophenotypes have dichotomous responses to virus/allergen coexposure and respond differentially to OM-85 pretreatment. Extrapolating to humans, our findings suggest that the beneficial effects OM-85 pretreatment may preferentially target those in high-risk subgroups.

dc.languageEnglish
dc.publisherFRONTIERS MEDIA SA
dc.relation.sponsoredbyhttp://purl.org/au-research/grants/nhmrc/1129996
dc.rights.urihttp://creativecommons.org/licenses/by/4.0/
dc.subjectScience & Technology
dc.subjectLife Sciences & Biomedicine
dc.subjectImmunology
dc.subjectasthma exacerbation
dc.subjectrhinovirus
dc.subjectallergen
dc.subjectimmunomodulation
dc.subjectIRF7
dc.subjectsystems biology
dc.subjectGROWTH-FACTOR-BETA
dc.subjectASTHMA EXACERBATIONS
dc.subjectADHESION MOLECULES
dc.subjectIMMUNE-RESPONSES
dc.subjectDENDRITIC CELLS
dc.subjectRISK
dc.subjectSUSCEPTIBILITY
dc.subjectINFECTION
dc.subjectSEVERITY
dc.subjectATOPY
dc.titleIRF7-Associated Immunophenotypes Have Dichotomous Responses to Virus/Allergen Coexposure and OM-85-Induced Reprogramming
dc.typeJournal Article
dcterms.source.volume12
dcterms.source.issn1664-3224
dcterms.source.titleFrontiers in Immunology
dc.date.updated2021-11-18T07:50:17Z
curtin.note

© 2021 The Authors. Published in Frontiers in Immunology

curtin.departmentCurtin School of Population Health
curtin.departmentSchool of Molecular and Life Sciences (MLS)
curtin.accessStatusOpen access
curtin.facultyFaculty of Health Sciences
curtin.facultyFaculty of Science and Engineering
curtin.contributor.orcidChristophersen, Claus [0000-0003-1591-5871]
curtin.contributor.orcidLarcombe, Alexander [0000-0003-4196-4482]
curtin.contributor.researcheridLarcombe, Alexander [A-7704-2011]
curtin.identifier.article-numberARTN 699633
dcterms.source.eissn1664-3224
curtin.contributor.scopusauthoridChristophersen, Claus [7006206487]
curtin.contributor.scopusauthoridLarcombe, Alexander [6508025368]


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