RAGE deficiency predisposes mice to virus-induced paucigranulocytic asthma Arikkatt, J, Ullah, MA, Short, KR, Zhang, V, Gan, WJ, Loh, Z, Werder, RB, Simpson, J, Sly, Peter, Mazzone, SB, Spann, KM, Ferreira, MAR, Upham, JW, Sukkar, MB and Phipps, S 2017, RAGE deficiency predisposes mice to virus-induced paucigranulocytic asthma, eLife, vol. 6, doi: 10.7554/eLife.21199. Title RAGE deficiency predisposes mice to virus-induced paucigranulocytic asthma Author(s) Arikkatt, J Ullah, MA Short, KR Zhang, V Gan, WJ Loh, Z Werder, RB Simpson, J Sly, Peter Mazzone, SB Spann, KM Ferreira, MAR Upham, JW Sukkar, MB Phipps, S Journal name eLife Volume number 6 Article ID e21199 Publisher eLife Sciences Publications Place of publication Cambridge, Eng. Publication date 2017-01-18 ISSN 2050-084X 2050-084X Keyword(s) Biology DENDRITIC CELLS HMGB1 PROTEIN INFLAMMATORY SUBTYPES INNATE LYMPHOID-CELLS Life Sciences & Biomedicine PATHOGENESIS PATHWAY PNEUMONIA VIRUS PNEUMOVIRUS INFECTION RECEPTOR Science & Technology Life Sciences & Biomedicine - Other Topics SMOOTH-MUSCLE HMGB1 RAGE asthma immunology infectious disease microbiology mouse paucigranulocytic virus infection Summary Asthma is a chronic inflammatory disease. Although many patients with asthma develop type-2 dominated eosinophilic inflammation, a number of individuals develop paucigranulocytic asthma, which occurs in the absence of eosinophilia or neutrophilia. The aetiology of paucigranulocytic asthma is unknown. However, both respiratory syncytial virus (RSV) infection and mutations in the receptor for advanced glycation endproducts (RAGE) are risk factors for asthma development. Here, we show that RAGE deficiency impairs anti-viral immunity during an early-life infection with pneumonia virus of mice (PVM; a murine analogue of RSV). The elevated viral load was associated with the release of high mobility group box-1 (HMGB1) which triggered airway smooth muscle remodelling in early-life. Re-infection with PVM in later-life induced many of the cardinal features of asthma in the absence of eosinophilic or neutrophilic inflammation. Anti-HMGB1 mitigated both early-life viral disease and asthma-like features, highlighting HMGB1 as a possible novel therapeutic target. Language eng DOI 10.7554/eLife.21199 Field of Research 0601 Biochemistry and Cell Biology HERDC Research category C1 Refereed article in a scholarly journal Free to Read? Yes Persistent URL http://hdl.handle.net/10536/DRO/DU:30164949 Document type: Journal Article Collections: Faculty of Health School of Medicine Open Access Collection Related Links Link Description Link to full-text (open access)   Connect to published version Go to link with your DU access privileges   Author URL Go to link with your DU access privileges   Connect to Elements publication management system Go to link with your DU access privileges     Unless expressly stated otherwise, the copyright for items in DRO is owned by the author, with all rights reserved. Every reasonable effort has been made to ensure that permission has been obtained for items included in DRO. If you believe that your rights have been infringed by this repository, please contact drosupport@deakin.edu.au. Versions Version Filter Type Mon, 21 Mar 2022, 08:51:51 EST Mon, 21 Mar 2022, 17:35:44 EST Wed, 06 Apr 2022, 09:04:17 EST Thu, 21 Apr 2022, 13:31:55 EST Thu, 21 Apr 2022, 14:25:54 EST Thu, 21 Apr 2022, 16:57:06 EST Thu, 05 May 2022, 22:39:05 EST Filtered Full Citation counts:   Cited 20 times in TR Web of Science Cited 19 times in Scopus Search Google Scholar Access Statistics: 9 Abstract Views  -  Detailed Statistics Created: Mon, 21 Mar 2022, 08:51:51 EST