2016
DOI: 10.1002/alr.21805
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Rhinovirus infection in murine chronic allergic rhinosinusitis model

Abstract: We successfully established a mouse model of upper airway RV infection by nasal inoculation with RV1B. Although there was histologically-proven increased RV infection in the CARS model, the infection did not intensify sinonasal inflammation.

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Cited by 12 publications
(13 citation statements)
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References 28 publications
(39 reference statements)
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“…Alternatively, the reduced response to MHV by epithelial cells may reflect the different cellular tropism of MHV. In contrast to PR8 and RV, which are known to infect epithelial cells in the murine respiratory tract, MHV-1 has only been reported in alveolar macrophages [2,6,12].…”
Section: Identification Of Signature Genes That Were Uniquely Alteredmentioning
confidence: 97%
See 3 more Smart Citations
“…Alternatively, the reduced response to MHV by epithelial cells may reflect the different cellular tropism of MHV. In contrast to PR8 and RV, which are known to infect epithelial cells in the murine respiratory tract, MHV-1 has only been reported in alveolar macrophages [2,6,12].…”
Section: Identification Of Signature Genes That Were Uniquely Alteredmentioning
confidence: 97%
“…The signature genes up-regulated by RV included kallikrein-1 and ten kallikrein-1-related peptidases and additional proteins involved in tissue remodeling (S4 Table). Although tissue remodeling is not likely to be relevant in murine models of rhinovirus infection alone, due to the limited damage, it may be an important factor in murine models of rhinovirus-induced allergic asthma [1,2,41]. Rhinovirus infections are a significant cause of asthma exacerbations, which correspond with inflammatory responses in the airways.…”
Section: Identification Of Signature Genes That Were Uniquely Alteredmentioning
confidence: 99%
See 2 more Smart Citations
“…A mouse model of chronic allergic rhinosinusitis was induced by 5 weeks of repetitive nasal OVA challenges. 194 Increased RV-A1 yields were reported in the nasal tissue of mice with rhinosinusitis, although inflammatory cytokine production and histopathology were unaffected. 194 This study served to illustrate the range of additional diseases where RV infection has been shown to be relevant in human populations where animal models are available for future research (e.g., cystic fibrosis).…”
Section: Mouse Chronic Sinusitis Exacerbation Modelsmentioning
confidence: 99%