IL‐17A deficiency mitigates bleomycin‐induced complement activation during lung fibrosis

Aug 20, 2017FASEB journal : official publication of the Federation of American Societies for Experimental Biology

Lack of IL-17A reduces immune system activation in lung scarring caused by bleomycin

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Abstract

IL-17A was shown to induce complement components in normal human alveolar epithelial cells at a concentration of 100 ng/ml.

IL-17A is associated with the regulation of complement activation in lung fibrosis.
Microarray analyses revealed that IL-17A induces the expression of various complement components and cytokines in human lung cells.
Neutralization of IL-17A in mice protected against bleomycin-induced lung fibrosis and collagen accumulation.
Mice lacking IL-17A exhibited reduced levels of markers associated with alveolar epithelial injury and stress.
RNA interference targeting specific genes in fibrotic mice halted fibrosis progression and reduced apoptosis and collagen deposition.

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Interleukin 17A (IL-17A) and complement (C') activation have each been implicated in the pathogenesis of idiopathic pulmonary fibrosis (IPF). We have reported that IL-17A induces epithelial injuryTGF-β in murine bronchiolitis obliterans; that TGF-β and the C' cascade present signaling interactions in mediating epithelial injury; and that the blockade of C' receptors mitigates lung fibrosis. In the present study, we investigated the role of IL-17A in regulating C' in lung fibrosis. Microarray analyses of mRNA isolated from primary normal human small airway epithelial cells indicated that IL-17A (100 ng/ml; 24 h;= 5 donor lungs) induces C' components (C' factor B,, and GPCR kinase isoform 5), cytokines (,, and), and cytokine ligands (,,,,, and). IL-17A induces protein and mRNA regulation of C' components and the synthesis of active C' 3a (C3a) in normal primary human alveolar type II epithelial cells (AECs). Wild-type mice subjected to IL-17A neutralization and IL-17A knockout () mice were protected against bleomycin (BLEO)-induced fibrosis and collagen deposition. Further, BLEO-injuredmice had diminished levels of circulating Krebs Von Den Lungen 6 (alveolar epithelial injury marker), local caspase-3/7, and local endoplasmic reticular stress-related genes. BLEO-induced local C' activation [C3a, C5a, and terminal C' complex (C5b-9)] was attenuated inmice, and IL-17A neutralization prevented the loss of epithelial C' inhibitors (C' receptor-1 related isoform Y and decay accelerating factor), and an increase in local TUNEL levels. RNAi-mediated gene silencing ofin fibrotic mice arrested the progression of lung fibrosis, attenuated cellular apoptosis (caspase-3/7) and lung deposition of collagen and C' (C5b-9). Compared to normals, plasma from IPF patients showed significantly higher hemolytic activity. Our findings demonstrate that limiting complement activation by neutralizing IL-17A is a potential mechanism in ameliorating lung fibrosis.-Cipolla, E., Fisher, A. J., Gu, H., Mickler, E. A., Agarwal, M., Wilke, C. A., Kim, K. K., Moore, B. B., Vittal, R. IL-17A deficiency mitigates bleomycin-induced complement activation during lung fibrosis. via n C3IL8 -6 -1B CXCL1 -2 -3 -5 -6 -16il17a -/-il17a -/-il17a -/-il17a

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