Impaired resolution of inflammatory response in the lungs of JF1/Msf mice following carbon nanoparticle instillation

BACKGROUND: Declined lung function is a risk factor for particulate matter associated respiratory diseases like asthma and chronic obstructive pulmonary disease (COPD). Carbon nanoparticles (CNP) are a prominent component of outdoor air pollution that causes pulmonary toxicity mainly through inflamm...

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Autores principales: Ganguly, Koustav, Upadhyay, Swapna, Irmler, Martin, Takenaka, Shinji, Pukelsheim, Katrin, Beckers, Johannes, De Angelis, Martin Hrabé, Hamelmann, Eckard, Stoeger, Tobias, Schulz, Holger
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2011
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3145576/
https://www.ncbi.nlm.nih.gov/pubmed/21756372
http://dx.doi.org/10.1186/1465-9921-12-94
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author Ganguly, Koustav
Upadhyay, Swapna
Irmler, Martin
Takenaka, Shinji
Pukelsheim, Katrin
Beckers, Johannes
De Angelis, Martin Hrabé
Hamelmann, Eckard
Stoeger, Tobias
Schulz, Holger
author_facet Ganguly, Koustav
Upadhyay, Swapna
Irmler, Martin
Takenaka, Shinji
Pukelsheim, Katrin
Beckers, Johannes
De Angelis, Martin Hrabé
Hamelmann, Eckard
Stoeger, Tobias
Schulz, Holger
author_sort Ganguly, Koustav
collection PubMed
description BACKGROUND: Declined lung function is a risk factor for particulate matter associated respiratory diseases like asthma and chronic obstructive pulmonary disease (COPD). Carbon nanoparticles (CNP) are a prominent component of outdoor air pollution that causes pulmonary toxicity mainly through inflammation. Recently we demonstrated that mice (C3H/HeJ) with higher than normal pulmonary function resolved the elicited pulmonary inflammation following CNP exposure through activation of defense and homeostasis maintenance pathways. To test whether CNP-induced inflammation is affected by declined lung function, we exposed JF1/Msf (JF1) mice with lower than normal pulmonary function to CNP and studied the pulmonary inflammation and its resolution. METHODS: 5 μg, 20 μg and 50 μg CNP (Printex 90) were intratracheally instilled in JF1 mice to determine the dose response and the time course of inflammation over 7 days (20 μg dosage). Inflammation was assessed using histology, bronchoalveolar lavage (BAL) analysis and by a panel of 62 protein markers. RESULTS: 24 h after instillation, 20 μg and 50 μg CNP caused a 25 fold and 19 fold increased polymorphonuclear leucocytes (PMN) respectively while the 5 μg represented the 'no observable adverse effect level' as reflected by PMN influx (9.7 × 10E3 vs 8.9 × 10E3), and BAL/lung concentrations of pro-inflammatory cytokines. Time course assessment of the inflammatory response revealed that compared to day1 the elevated BAL PMN counts (246.4 × 10E3) were significantly decreased at day 3 (72.9 × 10E3) and day 7 (48.5 × 10E3) but did not reach baseline levels indicating slow PMN resolution kinetics. Strikingly on day 7 the number of macrophages doubled (455.0 × 10E3 vs 204.7 × 10E3) and lymphocytes were 7-fold induced (80.6 × 10E3 vs 11.2 × 10E3) compared to day1. At day 7 elevated levels of IL1B, TNF, IL4, MDC/CCL22, FVII, and vWF were detected in JF1 lungs which can be associated to macrophage and lymphocyte activation. CONCLUSION: This explorative study indicates that JF1 mice with impaired pulmonary function also exhibits delayed resolution of particle mediated lung inflammation as evident from elevated PMN and accumulation of macrophages and lymphocytes on day7. It is plausible that elevated levels of IL1B, IL4, TNF, CCL22/MDC, FVII and vWF counteract defense and homeostatic pathways thereby driving this phenomenon.
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spelling pubmed-31455762011-07-29 Impaired resolution of inflammatory response in the lungs of JF1/Msf mice following carbon nanoparticle instillation Ganguly, Koustav Upadhyay, Swapna Irmler, Martin Takenaka, Shinji Pukelsheim, Katrin Beckers, Johannes De Angelis, Martin Hrabé Hamelmann, Eckard Stoeger, Tobias Schulz, Holger Respir Res Research BACKGROUND: Declined lung function is a risk factor for particulate matter associated respiratory diseases like asthma and chronic obstructive pulmonary disease (COPD). Carbon nanoparticles (CNP) are a prominent component of outdoor air pollution that causes pulmonary toxicity mainly through inflammation. Recently we demonstrated that mice (C3H/HeJ) with higher than normal pulmonary function resolved the elicited pulmonary inflammation following CNP exposure through activation of defense and homeostasis maintenance pathways. To test whether CNP-induced inflammation is affected by declined lung function, we exposed JF1/Msf (JF1) mice with lower than normal pulmonary function to CNP and studied the pulmonary inflammation and its resolution. METHODS: 5 μg, 20 μg and 50 μg CNP (Printex 90) were intratracheally instilled in JF1 mice to determine the dose response and the time course of inflammation over 7 days (20 μg dosage). Inflammation was assessed using histology, bronchoalveolar lavage (BAL) analysis and by a panel of 62 protein markers. RESULTS: 24 h after instillation, 20 μg and 50 μg CNP caused a 25 fold and 19 fold increased polymorphonuclear leucocytes (PMN) respectively while the 5 μg represented the 'no observable adverse effect level' as reflected by PMN influx (9.7 × 10E3 vs 8.9 × 10E3), and BAL/lung concentrations of pro-inflammatory cytokines. Time course assessment of the inflammatory response revealed that compared to day1 the elevated BAL PMN counts (246.4 × 10E3) were significantly decreased at day 3 (72.9 × 10E3) and day 7 (48.5 × 10E3) but did not reach baseline levels indicating slow PMN resolution kinetics. Strikingly on day 7 the number of macrophages doubled (455.0 × 10E3 vs 204.7 × 10E3) and lymphocytes were 7-fold induced (80.6 × 10E3 vs 11.2 × 10E3) compared to day1. At day 7 elevated levels of IL1B, TNF, IL4, MDC/CCL22, FVII, and vWF were detected in JF1 lungs which can be associated to macrophage and lymphocyte activation. CONCLUSION: This explorative study indicates that JF1 mice with impaired pulmonary function also exhibits delayed resolution of particle mediated lung inflammation as evident from elevated PMN and accumulation of macrophages and lymphocytes on day7. It is plausible that elevated levels of IL1B, IL4, TNF, CCL22/MDC, FVII and vWF counteract defense and homeostatic pathways thereby driving this phenomenon. BioMed Central 2011 2011-07-15 /pmc/articles/PMC3145576/ /pubmed/21756372 http://dx.doi.org/10.1186/1465-9921-12-94 Text en Copyright © 2011 Ganguly et al; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research
Ganguly, Koustav
Upadhyay, Swapna
Irmler, Martin
Takenaka, Shinji
Pukelsheim, Katrin
Beckers, Johannes
De Angelis, Martin Hrabé
Hamelmann, Eckard
Stoeger, Tobias
Schulz, Holger
Impaired resolution of inflammatory response in the lungs of JF1/Msf mice following carbon nanoparticle instillation
title Impaired resolution of inflammatory response in the lungs of JF1/Msf mice following carbon nanoparticle instillation
title_full Impaired resolution of inflammatory response in the lungs of JF1/Msf mice following carbon nanoparticle instillation
title_fullStr Impaired resolution of inflammatory response in the lungs of JF1/Msf mice following carbon nanoparticle instillation
title_full_unstemmed Impaired resolution of inflammatory response in the lungs of JF1/Msf mice following carbon nanoparticle instillation
title_short Impaired resolution of inflammatory response in the lungs of JF1/Msf mice following carbon nanoparticle instillation
title_sort impaired resolution of inflammatory response in the lungs of jf1/msf mice following carbon nanoparticle instillation
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3145576/
https://www.ncbi.nlm.nih.gov/pubmed/21756372
http://dx.doi.org/10.1186/1465-9921-12-94
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