Prostaglandin E2 production during neonatal respiratory infection with mouse adenovirus type 1

Procario, Megan C.; McCarthy, Mary K.; Levine, Rachael E.; Molloy, Caitlyn T.; Weinberg, Jason B.

doi:10.1016/j.virusres.2016.01.007

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“…The strict species specificity of the adenoviruses precludes detailed studies of HAdV pathogenesis in mouse models. We have used mouse adenovirus type 1 (MAV-1) to study the pathogenesis of adenovirus respiratory infection in its natural host (McCarthy et al, 2013; McCarthy et al, 2015b; McCarthy et al, 2014; Procario et al, 2012; Procario et al, 2016; Weinberg et al, 2005). Recently, we used MAV-1 to establish a mouse model of adenovirus myocarditis (McCarthy et al, 2015a) in which intranasal (i.n.)…”

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confidence: 99%

Interferon-dependent immunoproteasome activity during mouse adenovirus type 1 infection

et al. 2016

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The immunoproteasome is an inducible host mechanism that aids in the clearance of damaged proteins. The immunoproteasome also influences immune function by enhancing peptide presentation by MHC class I and promotes inflammation via IκB degradation and activation of NF-κB. We used mouse adenovirus type 1 (MAV-1) to characterize the role of the immunoproteasome in adenovirus pathogenesis. Following intranasal infection of mice, immunoproteasome activity in the heart and lung was significantly increased in an IFN-γ-dependent manner. Absence of the β5i immunoproteasome subunit and pharmacological inhibition of β5i activity had minimal effects on viral replication, virus-induced cellular inflammation, or induction of cytokine expression. Likewise, the establishment of protective immunity following primary infection was not significantly altered by β5i deficiency. Thus, although immunoproteasome activity is robustly induced during acute infection with MAV-1, our data suggest that other mechanisms are capable of compensating for immunoproteasome activity to maintain antiviral immunity and appropriate inflammatory responses.

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