4.5 Article

Differential Mouse Pulmonary Dose and Time Course Responses to Titanium Dioxide Nanospheres and Nanobelts

Journal

TOXICOLOGICAL SCIENCES
Volume 131, Issue 1, Pages 179-193

Publisher

OXFORD UNIV PRESS
DOI: 10.1093/toxsci/kfs261

Keywords

titanium dioxide nanospheres; titanium dioxide nanobelts; pulmonary inflammation; pulmonary fibrosis; pulmonary clearance

Categories

Funding

  1. National Science Foundation [CBET-0834233, CBET-1065931, EPS 1003907]
  2. National Institute of Environmental Health Sciences [1RC2ES018742-01, P20 RR017670]
  3. Div Of Chem, Bioeng, Env, & Transp Sys
  4. Directorate For Engineering [1065931] Funding Source: National Science Foundation

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Three anatase titanium dioxide (TiO2) nanoparticles (NPs) were prepared; nanospheres (NSs), short nanobelts (NB1), and long nanobelts (NB2). These NPs were used to investigate the effect of NP shape and length on lung toxicity. Mice were exposed (030 g per mouse) by pharyngeal aspiration and pulmonary toxicity was assessed over a 112-day time course. Whole lung lavage data indicated that NB1- and NB2-exposed mice, but not NS-exposed mice, had significant dose- and time-dependent pulmonary inflammation and damage. Histopathological analyses at 112 days postexposure determined no interstitial fibrosis in any NS-exposed mice, an increased incidence in 30 g NB1-exposed mice, and significant interstitial fibrosis in 30 g NB2-exposed mice. At 112 days postexposure, lung burden of NS was decreased by 96.4% and NB2 by 80.5% from initial deposition levels. At 112 days postexposure, enhanced dark field microscopy determined that alveolar macro- phages were the dominant deposition site, but a fraction of NB1 and NB2 was observed in the alveolar interstitial spaces. For the 30 g exposure groups at 112 days postexposure, confocal micro- scopy and immunofluorescent staining demonstrated that retained NB2 but not NS were present in the interstitium subjacent to the terminal bronchiole near the normal location of the smallest lymphatic capillaries in the lung. These lymphatic capillaries play a critical role in particle clearance, and the accumulation of NB2, but not NS, suggests possible impaired lymphatic clearance by the high aspect ratio particles. In summary, our data indicate that TiO2 NP shape alters pulmonary responses, with severity of responses being ranked as NS < NB1 < NB2.

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