Direct deposition of gas phase generated aerosol gold nanoparticles into biological fluids--corona formation and particle size shifts.

Direct deposition of gas phase generated aerosol gold nanoparticles into biological fluids--corona formation and particle size shifts.

An ongoing discussion whether traditional toxicological methods are sufficient to evaluate the risks associated with nanoparticle inhalation has led to the emergence of Air-Liquid interface toxicology. As a step in this process, this study explores the evolution of particle characteristics as they m...

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Main Authors: Christian R Svensson, Maria E Messing, Martin Lundqvist, Alexander Schollin, Knut Deppert, Joakim H Pagels, Jenny Rissler, Tommy Cedervall
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2013-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3785473?pdf=render
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spelling doaj-73d546def0b64073b6717931d90705612020-11-25T01:20:49ZengPublic Library of Science (PLoS)PLoS ONE1932-62032013-01-0189e7470210.1371/journal.pone.0074702Direct deposition of gas phase generated aerosol gold nanoparticles into biological fluids--corona formation and particle size shifts.Christian R SvenssonMaria E MessingMartin LundqvistAlexander SchollinKnut DeppertJoakim H PagelsJenny RisslerTommy CedervallAn ongoing discussion whether traditional toxicological methods are sufficient to evaluate the risks associated with nanoparticle inhalation has led to the emergence of Air-Liquid interface toxicology. As a step in this process, this study explores the evolution of particle characteristics as they move from the airborne state into physiological solution. Airborne gold nanoparticles (AuNP) are generated using an evaporation-condensation technique. Spherical and agglomerate AuNPs are deposited into physiological solutions of increasing biological complexity. The AuNP size is characterized in air as mobility diameter and in liquid as hydrodynamic diameter. AuNP:Protein aggregation in physiological solutions is determined using dynamic light scattering, particle tracking analysis, and UV absorption spectroscopy. AuNPs deposited into homocysteine buffer form large gold-aggregates. Spherical AuNPs deposited in solutions of albumin were trapped at the Air-Liquid interface but was readily suspended in the solutions with a size close to that of the airborne particles, indicating that AuNP:Protein complex formation is promoted. Deposition into serum and lung fluid resulted in larger complexes, reflecting the formation of a more complex protein corona. UV absorption spectroscopy indicated no further aggregation of the AuNPs after deposition in solution. The corona of the deposited AuNPs shows differences compared to AuNPs generated in suspension. Deposition of AuNPs from the aerosol phase into biological fluids offers a method to study the protein corona formed, upon inhalation and deposition in the lungs in a more realistic way compared to particle liquid suspensions. This is important since the protein corona together with key particle properties (e.g. size, shape and surface reactivity) to a large extent may determine the nanoparticle effects and possible translocation to other organs.http://europepmc.org/articles/PMC3785473?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Christian R Svensson
Maria E Messing
Martin Lundqvist
Alexander Schollin
Knut Deppert
Joakim H Pagels
Jenny Rissler
Tommy Cedervall
spellingShingle Christian R Svensson
Maria E Messing
Martin Lundqvist
Alexander Schollin
Knut Deppert
Joakim H Pagels
Jenny Rissler
Tommy Cedervall
Direct deposition of gas phase generated aerosol gold nanoparticles into biological fluids--corona formation and particle size shifts.
PLoS ONE
author_facet Christian R Svensson
Maria E Messing
Martin Lundqvist
Alexander Schollin
Knut Deppert
Joakim H Pagels
Jenny Rissler
Tommy Cedervall
author_sort Christian R Svensson
title Direct deposition of gas phase generated aerosol gold nanoparticles into biological fluids--corona formation and particle size shifts.
title_short Direct deposition of gas phase generated aerosol gold nanoparticles into biological fluids--corona formation and particle size shifts.
title_full Direct deposition of gas phase generated aerosol gold nanoparticles into biological fluids--corona formation and particle size shifts.
title_fullStr Direct deposition of gas phase generated aerosol gold nanoparticles into biological fluids--corona formation and particle size shifts.
title_full_unstemmed Direct deposition of gas phase generated aerosol gold nanoparticles into biological fluids--corona formation and particle size shifts.
title_sort direct deposition of gas phase generated aerosol gold nanoparticles into biological fluids--corona formation and particle size shifts.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2013-01-01
description An ongoing discussion whether traditional toxicological methods are sufficient to evaluate the risks associated with nanoparticle inhalation has led to the emergence of Air-Liquid interface toxicology. As a step in this process, this study explores the evolution of particle characteristics as they move from the airborne state into physiological solution. Airborne gold nanoparticles (AuNP) are generated using an evaporation-condensation technique. Spherical and agglomerate AuNPs are deposited into physiological solutions of increasing biological complexity. The AuNP size is characterized in air as mobility diameter and in liquid as hydrodynamic diameter. AuNP:Protein aggregation in physiological solutions is determined using dynamic light scattering, particle tracking analysis, and UV absorption spectroscopy. AuNPs deposited into homocysteine buffer form large gold-aggregates. Spherical AuNPs deposited in solutions of albumin were trapped at the Air-Liquid interface but was readily suspended in the solutions with a size close to that of the airborne particles, indicating that AuNP:Protein complex formation is promoted. Deposition into serum and lung fluid resulted in larger complexes, reflecting the formation of a more complex protein corona. UV absorption spectroscopy indicated no further aggregation of the AuNPs after deposition in solution. The corona of the deposited AuNPs shows differences compared to AuNPs generated in suspension. Deposition of AuNPs from the aerosol phase into biological fluids offers a method to study the protein corona formed, upon inhalation and deposition in the lungs in a more realistic way compared to particle liquid suspensions. This is important since the protein corona together with key particle properties (e.g. size, shape and surface reactivity) to a large extent may determine the nanoparticle effects and possible translocation to other organs.
url http://europepmc.org/articles/PMC3785473?pdf=render
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