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Nanoparticles modulate surfactant protein A and D mediated protection against influenza A infection in vitro

Numerous epidemiological and toxicological studies have indicated that respiratory infections are exacerbated following enhanced exposure to airborne particulates. Surfactant protein A (SP-A) and SP-D form an important part of the innate immune response in the lung and can interact with nanoparticle...

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Autores principales: McKenzie, Zofi, Kendall, Michaela, Mackay, Rose-Marie, Tetley, Teresa D., Morgan, Cliff, Griffiths, Mark, Clark, Howard W., Madsen, Jens
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The Royal Society 2015
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4275912/
https://www.ncbi.nlm.nih.gov/pubmed/25533100
http://dx.doi.org/10.1098/rstb.2014.0049
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author McKenzie, Zofi
Kendall, Michaela
Mackay, Rose-Marie
Tetley, Teresa D.
Morgan, Cliff
Griffiths, Mark
Clark, Howard W.
Madsen, Jens
author_facet McKenzie, Zofi
Kendall, Michaela
Mackay, Rose-Marie
Tetley, Teresa D.
Morgan, Cliff
Griffiths, Mark
Clark, Howard W.
Madsen, Jens
author_sort McKenzie, Zofi
collection PubMed
description Numerous epidemiological and toxicological studies have indicated that respiratory infections are exacerbated following enhanced exposure to airborne particulates. Surfactant protein A (SP-A) and SP-D form an important part of the innate immune response in the lung and can interact with nanoparticles to modulate the cellular uptake of these particles. We hypothesize that this interaction will also affect the ability of these proteins to combat infections. TT1, A549 and differentiated THP-1 cells, representing the predominant cell types found in the alveolus namely alveolar type I (ATI) epithelial cells, ATII cells and macrophages, were used to examine the effect of two model nanoparticles, 100 nm amine modified (A-PS) and unmodified polystyrene (U-PS), on the ability of SP-A and SP-D to neutralize influenza A infections in vitro. Pre-incubation of low concentrations of U-PS with SP-A resulted in a reduction of SP-A anti-influenza activity in A549 cells, whereas at higher concentrations there was an increase in SP-A antiviral activity. This differential pattern of U-PS concentration on surfactant protein mediated protection against IAV was also shown with SP-D in TT1 cells. On the other hand, low concentrations of A-PS particles resulted in a reduction of SP-A activity in TT1 cells and a reduction in SP-D activity in A549 cells. These results indicate that nanoparticles can modulate the ability of SP-A and SP-D to combat viral challenges. Furthermore, the nanoparticle concentration, surface chemistry and cell type under investigation are important factors in determining the extent of these modulations.
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spelling pubmed-42759122015-02-05 Nanoparticles modulate surfactant protein A and D mediated protection against influenza A infection in vitro McKenzie, Zofi Kendall, Michaela Mackay, Rose-Marie Tetley, Teresa D. Morgan, Cliff Griffiths, Mark Clark, Howard W. Madsen, Jens Philos Trans R Soc Lond B Biol Sci Articles Numerous epidemiological and toxicological studies have indicated that respiratory infections are exacerbated following enhanced exposure to airborne particulates. Surfactant protein A (SP-A) and SP-D form an important part of the innate immune response in the lung and can interact with nanoparticles to modulate the cellular uptake of these particles. We hypothesize that this interaction will also affect the ability of these proteins to combat infections. TT1, A549 and differentiated THP-1 cells, representing the predominant cell types found in the alveolus namely alveolar type I (ATI) epithelial cells, ATII cells and macrophages, were used to examine the effect of two model nanoparticles, 100 nm amine modified (A-PS) and unmodified polystyrene (U-PS), on the ability of SP-A and SP-D to neutralize influenza A infections in vitro. Pre-incubation of low concentrations of U-PS with SP-A resulted in a reduction of SP-A anti-influenza activity in A549 cells, whereas at higher concentrations there was an increase in SP-A antiviral activity. This differential pattern of U-PS concentration on surfactant protein mediated protection against IAV was also shown with SP-D in TT1 cells. On the other hand, low concentrations of A-PS particles resulted in a reduction of SP-A activity in TT1 cells and a reduction in SP-D activity in A549 cells. These results indicate that nanoparticles can modulate the ability of SP-A and SP-D to combat viral challenges. Furthermore, the nanoparticle concentration, surface chemistry and cell type under investigation are important factors in determining the extent of these modulations. The Royal Society 2015-02-05 /pmc/articles/PMC4275912/ /pubmed/25533100 http://dx.doi.org/10.1098/rstb.2014.0049 Text en http://creativecommons.org/licenses/by/4.0/ © 2014 The Authors. Published by the Royal Society under the terms of the Creative Commons Attribution License http://creativecommons.org/licenses/by/4.0/, which permits unrestricted use, provided the original author and source are credited.
spellingShingle Articles
McKenzie, Zofi
Kendall, Michaela
Mackay, Rose-Marie
Tetley, Teresa D.
Morgan, Cliff
Griffiths, Mark
Clark, Howard W.
Madsen, Jens
Nanoparticles modulate surfactant protein A and D mediated protection against influenza A infection in vitro
title Nanoparticles modulate surfactant protein A and D mediated protection against influenza A infection in vitro
title_full Nanoparticles modulate surfactant protein A and D mediated protection against influenza A infection in vitro
title_fullStr Nanoparticles modulate surfactant protein A and D mediated protection against influenza A infection in vitro
title_full_unstemmed Nanoparticles modulate surfactant protein A and D mediated protection against influenza A infection in vitro
title_short Nanoparticles modulate surfactant protein A and D mediated protection against influenza A infection in vitro
title_sort nanoparticles modulate surfactant protein a and d mediated protection against influenza a infection in vitro
topic Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4275912/
https://www.ncbi.nlm.nih.gov/pubmed/25533100
http://dx.doi.org/10.1098/rstb.2014.0049
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