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Peer-reviewed veterinary case report

IL-17E (IL-25) and IL-17RB promote respiratory syncytial virus-induced pulmonary disease.

Journal:
Journal of leukocyte biology
Year:
2014
Authors:
Petersen, Bryan C et al.
Affiliation:
Department of Pathology · United States

Abstract

One of the most severe pathologic responses of RSV infection is associated with overproduction of cytokines and inflammation, leading to mucus hypersecretion. This study investigated the role of IL-25 in the development of RSV-associated immunopathology. IL-25 and its receptor IL-17RB were increased following RSV infection, and IL-25 blockade using neutralizing antibodies reduced RSV-associated pathology, AHR, and type 2 cytokine production. Likewise, IL-17RBmice demonstrated a modified inflammatory response during RSV infection characterized by decreased Th2 and increased Th17 cytokine production. Additionally, the IL-17RBmice demonstrated significantly reduced inflammation and cytokine production in a model of RSV-driven asthma exacerbation. These results indicate that IL-25 regulates the inflammatory response to RSV infection and that its inhibition may enable a reduction in the severity of RSV-associated pulmonary inflammation, including during viral-induced asthma exacerbation.

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Original publication: https://pubmed.ncbi.nlm.nih.gov/24407884/