TY - JOUR
T1 - Influenza A induces the major secreted airway mucin MUC5AC in a protease-EGFR-extracellular regulated kinase-Sp1-dependent pathway
AU - Barbier, Diane
AU - Garcia-Verdugo, Ignacio
AU - Pothlichet, Julien
AU - Khazen, Roxana
AU - Descamps, Delphyne
AU - Rousseau, Karine
AU - Thornton, David
AU - Si-Tahar, Mustapha
AU - Touqui, Lhousseine
AU - Chignard, Michel
AU - Sallenave, Jean Michel
PY - 2012/8
Y1 - 2012/8
N2 - Mucins, the main glycoproteins present within mucus, modulate the rheologic properties of airways and participate in lung defense. They are thought to be able to trap and eliminate microorganisms from the lung. Among the mucins secreted in the lung, MUC5AC is the most prominent factor secreted bysurface epithelial cells. Although much is known about the signaling pathways involved in the regulation of MUC5AC by host factors suchas cytokines or proteases, less is known about the pathways triggered by microorganisms and, specifically, by influenza Avirus (IAV). We therefore set up experiments to dissect the molecular mechanisms responsible for the potential modulation of MUC5AC by IAV. Using epithelial cells, C57/Bl6 mice, and IAV strains, we measured MUC5AC expression at the RNA and protein levels, specificity protein 1 (Sp1) activation, and protease activity. Intermediate molecular partners were confirmed using pharmacological inhibitors, blocking antibodies, and small interfering (si)RNAs. We showed in vitro and in vivo that IAV upregulates epithelial cell-derived MUC5AC and Muc5ac expression in mice, both at transcriptional (through the induction of Sp1) and translational levels. In addition, we determined that this induction was dependent on a protease-epithelial growth factor receptor-extracellular regulated kinase-Sp1 signaling cascade, involving in particular the human airway trypsin. Our data point to MUC5AC as a potential modulatory mechanism by which the lung epithelia respond to IAV infection, and we dissect, for the first time to the best of our knowledge, the molecular partners involved. Future experiments using MUC5AC-targeted strategies should help further unravel the pathophysiological consequences of IAV-induced MUC5AC expression for lung homeostasis. Copyright © 2012 by the American Thoracic Society.
AB - Mucins, the main glycoproteins present within mucus, modulate the rheologic properties of airways and participate in lung defense. They are thought to be able to trap and eliminate microorganisms from the lung. Among the mucins secreted in the lung, MUC5AC is the most prominent factor secreted bysurface epithelial cells. Although much is known about the signaling pathways involved in the regulation of MUC5AC by host factors suchas cytokines or proteases, less is known about the pathways triggered by microorganisms and, specifically, by influenza Avirus (IAV). We therefore set up experiments to dissect the molecular mechanisms responsible for the potential modulation of MUC5AC by IAV. Using epithelial cells, C57/Bl6 mice, and IAV strains, we measured MUC5AC expression at the RNA and protein levels, specificity protein 1 (Sp1) activation, and protease activity. Intermediate molecular partners were confirmed using pharmacological inhibitors, blocking antibodies, and small interfering (si)RNAs. We showed in vitro and in vivo that IAV upregulates epithelial cell-derived MUC5AC and Muc5ac expression in mice, both at transcriptional (through the induction of Sp1) and translational levels. In addition, we determined that this induction was dependent on a protease-epithelial growth factor receptor-extracellular regulated kinase-Sp1 signaling cascade, involving in particular the human airway trypsin. Our data point to MUC5AC as a potential modulatory mechanism by which the lung epithelia respond to IAV infection, and we dissect, for the first time to the best of our knowledge, the molecular partners involved. Future experiments using MUC5AC-targeted strategies should help further unravel the pathophysiological consequences of IAV-induced MUC5AC expression for lung homeostasis. Copyright © 2012 by the American Thoracic Society.
KW - EGFR
KW - Influenza
KW - MUC5AC
KW - Proteases
KW - TACE
U2 - 10.1165/rcmb.2011-0405OC
DO - 10.1165/rcmb.2011-0405OC
M3 - Article
C2 - 22383584
SN - 1044-1549
VL - 47
SP - 149
EP - 157
JO - American Journal of Respiratory Cell and Molecular Biology
JF - American Journal of Respiratory Cell and Molecular Biology
IS - 2
ER -