NF-[kappa]B dependent and independent mechanisms of quartz-induced proinflammatory activation of lung epithelial cells
In the initiation and progression of pulmonary inflammation, macrophages have classically been considered as a crucial cell type. However, evidence for the role of epithelial type II cells in pulmonary inflammation has been accumulating. In the current study, a combined in vivo and in vitro approach...
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| Veröffentlicht in: | Particle and fibre toxicology 2010-05, Vol.7, p.13-13 |
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| creator | van Berlo, Damien Knaapen, Ad M van Schooten, Frederik-Jan Schins, Roel PF Albrecht, Catrin |
| description | In the initiation and progression of pulmonary inflammation, macrophages have classically been considered as a crucial cell type. However, evidence for the role of epithelial type II cells in pulmonary inflammation has been accumulating. In the current study, a combined in vivo and in vitro approach has been employed to investigate the mechanisms of quartz-induced proinflammatory activation of lung epithelial cells. In vivo, enhanced expression of the inflammation- and oxidative stress-related genes HO-1 and iNOS was found on the mRNA level in rat lungs after instillation with DQ12 respirable quartz. Activation of the classical NF-[kappa]B pathway in macrophages and type II pneumocytes was indicated by enhanced immunostaining of phospho-I[kappa]B[alpha] in these specific lung cell types. In vitro, the direct, particle-mediated effect on proinflammatory signalling in a rat lung epithelial (RLE) cell line was compared to the indirect, macrophage product-mediated effect. Treatment with quartz particles induced HO-1 and COX-2 mRNA expression in RLE cells in an NF-[kappa]B independent manner. Supernatant from quartz-treated macrophages rapidly activated the NF-[kappa]B signalling pathway in RLE cells and markedly induced iNOS mRNA expression up to 2000-fold compared to non-treated control cells. Neutralisation of TNF[alpha] and IL-1[beta] in macrophage supernatant did not reduce its ability to elicit NF-[kappa]B activation of RLE cells. In addition the effect was not modified by depletion or supplementation of intracellular glutathione. |
| doi_str_mv | 10.1186/1743-8977-7-13 |
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However, evidence for the role of epithelial type II cells in pulmonary inflammation has been accumulating. In the current study, a combined in vivo and in vitro approach has been employed to investigate the mechanisms of quartz-induced proinflammatory activation of lung epithelial cells. In vivo, enhanced expression of the inflammation- and oxidative stress-related genes HO-1 and iNOS was found on the mRNA level in rat lungs after instillation with DQ12 respirable quartz. Activation of the classical NF-[kappa]B pathway in macrophages and type II pneumocytes was indicated by enhanced immunostaining of phospho-I[kappa]B[alpha] in these specific lung cell types. In vitro, the direct, particle-mediated effect on proinflammatory signalling in a rat lung epithelial (RLE) cell line was compared to the indirect, macrophage product-mediated effect. Treatment with quartz particles induced HO-1 and COX-2 mRNA expression in RLE cells in an NF-[kappa]B independent manner. Supernatant from quartz-treated macrophages rapidly activated the NF-[kappa]B signalling pathway in RLE cells and markedly induced iNOS mRNA expression up to 2000-fold compared to non-treated control cells. Neutralisation of TNF[alpha] and IL-1[beta] in macrophage supernatant did not reduce its ability to elicit NF-[kappa]B activation of RLE cells. In addition the effect was not modified by depletion or supplementation of intracellular glutathione.</description><identifier>ISSN: 1743-8977</identifier><identifier>EISSN: 1743-8977</identifier><identifier>DOI: 10.1186/1743-8977-7-13</identifier><language>eng</language><publisher>London: BioMed Central Ltd</publisher><subject>Atoms & subatomic particles ; Autoimmune diseases ; Disease ; Epithelial cells ; Genetic aspects ; Highway construction ; Inflammation ; Lung cancer ; Macrophages ; Messenger RNA ; Nitric oxide ; Oxidative stress ; Properties ; Quartz ; Respiratory physiology ; Rodents ; Studies ; TNF inhibitors ; Toxicology</subject><ispartof>Particle and fibre toxicology, 2010-05, Vol.7, p.13-13</ispartof><rights>COPYRIGHT 2010 BioMed Central Ltd.</rights><rights>2010 van Berlo et al; licensee BioMed Central Ltd. 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However, evidence for the role of epithelial type II cells in pulmonary inflammation has been accumulating. In the current study, a combined in vivo and in vitro approach has been employed to investigate the mechanisms of quartz-induced proinflammatory activation of lung epithelial cells. In vivo, enhanced expression of the inflammation- and oxidative stress-related genes HO-1 and iNOS was found on the mRNA level in rat lungs after instillation with DQ12 respirable quartz. Activation of the classical NF-[kappa]B pathway in macrophages and type II pneumocytes was indicated by enhanced immunostaining of phospho-I[kappa]B[alpha] in these specific lung cell types. In vitro, the direct, particle-mediated effect on proinflammatory signalling in a rat lung epithelial (RLE) cell line was compared to the indirect, macrophage product-mediated effect. Treatment with quartz particles induced HO-1 and COX-2 mRNA expression in RLE cells in an NF-[kappa]B independent manner. 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| source | BioMed Central; SpringerOpen; DOAJ Directory of Open Access Journals; Springer Journals; PubMed Central; Free Full-Text Journals in Chemistry; EZB Electronic Journals Library; PubMed Central Open Access |
| subjects | Atoms & subatomic particles Autoimmune diseases Disease Epithelial cells Genetic aspects Highway construction Inflammation Lung cancer Macrophages Messenger RNA Nitric oxide Oxidative stress Properties Quartz Respiratory physiology Rodents Studies TNF inhibitors Toxicology |
| title | NF-[kappa]B dependent and independent mechanisms of quartz-induced proinflammatory activation of lung epithelial cells |
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