Genotoxicity of inhaled nanosized TiO(2) in mice

Hanna K Lindberg; Ghita C-M Falck; Julia Catalán; Antti J Koivisto; Satu Suhonen; Hilkka Järventaus; Elina M Rossi; Heli Nykäsenoja; Yrjö Peltonen; Carlos Moreno; Harri Alenius; Timo Tuomi; Kai M Savolainen; Hannu Norppa

doi:10.1016/j.mrgentox.2011.10.011

Genotoxicity of inhaled nanosized TiO(2) in mice

Mutat Res. 2012 Jun 14;745(1-2):58-64. doi: 10.1016/j.mrgentox.2011.10.011. Epub 2011 Nov 7.

Authors

Hanna K Lindberg¹, Ghita C-M Falck, Julia Catalán, Antti J Koivisto, Satu Suhonen, Hilkka Järventaus, Elina M Rossi, Heli Nykäsenoja, Yrjö Peltonen, Carlos Moreno, Harri Alenius, Timo Tuomi, Kai M Savolainen, Hannu Norppa

Affiliation

¹ Nanosafety Research Center, Finnish Institute of Occupational Health, FI-00250 Helsinki, Finland.

PMID: 22094288
DOI: 10.1016/j.mrgentox.2011.10.011

Abstract

In vitro studies have suggested that nanosized titanium dioxide (TiO(2)) is genotoxic. The significance of these findings with respect to in vivo effects is unclear, as few in vivo studies on TiO(2) genotoxicity exist. Recently, nanosized TiO(2) administered in drinking water was reported to increase, e.g., micronuclei (MN) in peripheral blood polychromatic erythrocytes (PCEs) and DNA damage in leukocytes. Induction of micronuclei in mouse PCEs was earlier also described for pigment-grade TiO(2) administered intraperitoneally. The apparent systemic genotoxic effects have been suggested to reflect secondary genotoxicity of TiO(2) due to inflammation. However, a recent study suggested that induction of DNA damage in mouse bronchoalveolar lavage (BAL) cells after intratracheal instillation of nanosized or fine TiO(2) is independent of inflammation. We examined here, if inhalation of freshly generated nanosized TiO(2) (74% anatase, 26% brookite; 5 days, 4 h/day) at 0.8, 7.2, and (the highest concentration allowing stable aerosol production) 28.5 mg/m(3) could induce genotoxic effects in C57BL/6J mice locally in the lungs or systematically in peripheral PCEs. DNA damage was assessed by the comet assay in lung epithelial alveolar type II and Clara cells sampled immediately following the exposure. MN were analyzed by acridine orange staining in blood PCEs collected 48 h after the last exposure. A dose-dependent deposition of Ti in lung tissue was seen. Although the highest exposure level produced a clear increase in neutrophils in BAL fluid, indicating an inflammatory effect, no significant effect on the level of DNA damage in lung epithelial cells or micronuclei in PCEs was observed, suggesting no genotoxic effects by the 5-day inhalation exposure to nanosized TiO(2) anatase. Our inhalation exposure resulted in much lower systemic TiO(2) doses than the previous oral and intraperitoneal treatments, and lung epithelial cells probably received considerably less TiO(2) than BAL cells in the earlier intratracheal study.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Administration, Inhalation
Animals
Comet Assay
DNA Damage
Inflammation / chemically induced
Lung / drug effects
Male
Mice
Mice, Inbred C57BL
Micronucleus Tests
Mutagens / toxicity*
Nanoparticles / administration & dosage
Nanoparticles / toxicity*
Titanium / administration & dosage
Titanium / toxicity*

Substances

Mutagens
titanium dioxide
Titanium