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Study of TiO2 P25 nanoparticles genotoxicity on lung, blood and liver cells in lung overload and non-overload conditions after repeated respiratory exposure in rats.

TitleStudy of TiO2 P25 nanoparticles genotoxicity on lung, blood and liver cells in lung overload and non-overload conditions after repeated respiratory exposure in rats.
Publication TypeArticolo su Rivista peer-reviewed
Year of Publication2017
AuthorsRelier, Charlène, Dubreuil Marielle, Garcia Omar Lozano, Cordelli Eugenia, Mejia Jorge, Eleuteri Patrizia, Robidel Franck, Loret Thomas, Pacchierotti Francesca, Lucas Stéphane, Lacroix Ghislaine, and Trouiller Bénédicte
JournalToxicol Sci
Volume156
Pagination527-537
Date Published2017 Jan 13
ISSN10960929
Abstract

Inhaled titanium dioxide (TiO2) nanoparticles (NPs) can have negative health effects, and have been shown to cause respiratory tract cancer in rats. Inflammation has been linked to oxidative stress, and both have been described as possible mechanisms for genotoxicity of NPs, but rarely examined side-by-side in animal studies. In the present study, a wide range of complementary endpoints have been performed to study TiO2 P25 NP-induced genotoxicity in lung overload and non-overload conditions. Additionally, lung burden, inflammation, cytotoxicity and oxidative stress have also been evaluated in order to link genotoxicity with these responses. To assess quick and delayed responses after recovery, endpoints were evaluated at two time points: 2 hours and 35 days after 3 repeated instillations. This study confirmed the previously described lung overload threshold at approximately 200-300 cm(2) of lung burden for total particle surface area lung deposition or 4.2 µL/kg for volume-based cumulative lung exposure dose, above which lung clearance is impaired and inflammation is induced. Our results went on to show that these overload doses induced delayed genotoxicity in lung, associated with persistent inflammation only at the highest dose. The lowest tested doses had no toxicity or genotoxicity effects in the lung. In blood, no lymphocyte DNA damage, erythrocytes chromosomal damage or gene mutation could be detected. Our data also demonstrated that only overload doses induced liver DNA lesions irrespective of the recovery time. Tested doses of TiO2 P25 NPs did not induce glutathione changes in lung, blood or liver at both recovery times.

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URLhttps://www.scopus.com/inward/record.uri?eid=2-s2.0-85017096305&doi=10.1093%2ftoxsci%2fkfx006&partnerID=40&md5=9ca078280aa0d170316087a8d4b30b85
DOI10.1093/toxsci/kfx006
Alternate JournalToxicol. Sci.
Citation Key4901
PubMed ID28087835