Literature DB >> 18236223

Concordance between in vitro and in vivo dosimetry in the proinflammatory effects of low-toxicity, low-solubility particles: the key role of the proximal alveolar region.

K Donaldson1, P J A Borm, G Oberdorster, K E Pinkerton, V Stone, C L Tran.   

Abstract

We previously demonstrated the importance of the surface area burden as the key dose metric in the elicitation of inflammation in rat lungs by low-solubility, low-toxicity particles (LSLTP). We have now explored the dosimetry of LSLTP in vitro using epithelial cell interleukin (IL)-8 gene expression as a surrogate for potential of particles to cause inflammation. The proximal alveolar region (PAR) of the lung has been identified as a key site for the retention of respirable particles, as it receives high deposition but has slow clearance compared to the larger airways. For these reasons, a few days after exposure to particles the residual dose is concentrated in the PAR region. Re-expressing our rat lung data as particle surface area burden per unit of PAR surface area we obtained a threshold value for onset of inflammation of 1 cm(2)/cm(2). We carried out dose responses in vitro for onset of IL-8 gene expression with the same particles as we had used in vivo. When we expressed the in vitro dose as surface area dose per unit A549cell culture surface area, we obtained a threshold of 1 cm(2)/cm(2). This concordance between proinflammatory effects in vivo (PMN in BAL) and in vitro (epithelial IL-8 gene expression) confirms and supports the utility of the particle surface area metric and the importance of the PAR. These studies also open the way for future in vitro approaches to studying proinflammatory effects of a range of toxic particles based on sound dosimetry that complements animal use in particle toxicology.

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Year:  2008        PMID: 18236223     DOI: 10.1080/08958370701758742

Source DB:  PubMed          Journal:  Inhal Toxicol        ISSN: 0895-8378            Impact factor:   2.724


  32 in total

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4.  Three human cell types respond to multi-walled carbon nanotubes and titanium dioxide nanobelts with cell-specific transcriptomic and proteomic expression patterns.

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5.  A quantitative framework to group nanoscale and microscale particles by hazard potency to derive occupational exposure limits: Proof of concept evaluation.

Authors:  Nathan M Drew; Eileen D Kuempel; Ying Pei; Feng Yang
Journal:  Regul Toxicol Pharmacol       Date:  2017-08-05       Impact factor: 3.271

6.  Aerosolized ZnO nanoparticles induce toxicity in alveolar type II epithelial cells at the air-liquid interface.

Authors:  Yumei Xie; Nolann G Williams; Ana Tolic; William B Chrisler; Justin G Teeguarden; Bettye L S Maddux; Joel G Pounds; Alexander Laskin; Galya Orr
Journal:  Toxicol Sci       Date:  2011-09-28       Impact factor: 4.849

7.  Shifts in oxidation states of cerium oxide nanoparticles detected inside intact hydrated cells and organelles.

Authors:  Craig J Szymanski; Prabhakaran Munusamy; Cosmin Mihai; Yumei Xie; Dehong Hu; Mary K Gilles; Tolek Tyliszczak; Suntharampillai Thevuthasan; Donald R Baer; Galya Orr
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9.  Health effects of residential wood smoke particles: the importance of combustion conditions and physicochemical particle properties.

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Journal:  Part Fibre Toxicol       Date:  2009-11-06       Impact factor: 9.400

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