Abstract
This is the first comprehensive analysis of secretome in a hRSV-infected paediatric airway epithelium, which identified skewing of apical/basolateral abundance ratios for individual proteins, and validated three novel biomarkers (CXCL6, CXCL16 and CSF3) and a novel antiviral protein (CEACAM1).
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Highlights
•Proteome of airway secretions derived from mock- and hRSV-infected WD-PBEC cultures.•A polarised secretome in uninfected WD-PBECs, skewed in hRSV-infected cultures.•CXCL6, CXCL16, CECACAM1 and CSF3 induced only upon hRSV-infection.•Detection of CXCL6, CXCL16 and CSF3 in NPAs from hRSV-positive children.
The respiratory epithelium comprises polarized cells at the interface between the environment and airway tissues. Polarized apical and basolateral protein secretions are a feature of airway epithelium homeostasis. Human respiratory syncytial virus (hRSV) is a major human pathogen that primarily targets the respiratory epithelium. However, the consequences of hRSV infection on epithelium secretome polarity and content remain poorly understood. To investigate the hRSV-associated apical and basolateral secretomes, a proteomics approach was combined with an ex vivo pediatric human airway epithelial (HAE) model of hRSV infection (data are available via ProteomeXchange and can be accessed at https://www.ebi.ac.uk/pride/ with identifier PXD013661). Following infection, a skewing of apical/basolateral abundance ratios was identified for several individual proteins. Novel modulators of neutrophil and lymphocyte activation (CXCL6, CSF3, SECTM1 or CXCL16), and antiviral proteins (BST2 or CEACAM1) were detected in infected, but not in uninfected cultures. Importantly, CXCL6, CXCL16, CSF3 were also detected in nasopharyngeal aspirates (NPA) from hRSV-infected infants but not healthy controls. Furthermore, the antiviral activity of CEACAM1 against RSV was confirmed in vitro using BEAS-2B cells. hRSV infection disrupted the polarity of the pediatric respiratory epithelial secretome and was associated with immune modulating proteins (CXCL6, CXCL16, CSF3) never linked with this virus before. In addition, the antiviral activity of CEACAM1 against hRSV had also never been previously characterized. This study, therefore, provides novel insights into RSV pathogenesis and endogenous antiviral responses in pediatric airway epithelium.