4.6 Article

Intratracheally instilled titanium dioxide nanoparticles translocate to heart and liver and activate complement cascade in the heart of C57BL/6 mice

Journal

NANOTOXICOLOGY
Volume 9, Issue 8, Pages 1013-1022

Publisher

TAYLOR & FRANCIS LTD
DOI: 10.3109/17435390.2014.996192

Keywords

Complement cascade; gene expression; hyperspectral microscopy; inflammation; nanoparticles; translocation

Funding

  1. Health Canada's Genomics Research and Development Initiative and Chemicals Management Plan
  2. Danish Centre for Nanosafety grant from the Danish Working Environment Research Foundation [20110092173-3]
  3. NanoKem grant from the Danish Working Environment Research Foundation [20060068816]

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An estimated 1% or less of nanoparticles (NPs) deposited in the lungs translocate to systemic circulation and enter other organs; however, this estimation may not be accurate given the low sensitivity of existing in vivo NP detection methods. Moreover, the biological effects of such low levels of translocation are unclear. We employed a nano-scale hyperspectral microscope to spatially observe and spectrally profile NPs in tissues and blood following pulmonary deposition in mice. In addition, we characterized effects occurring in blood, liver and heart at the mRNA and protein level following translocation from the lungs. Adult female C57BL/6 mice were exposed via intratracheal instillation to 18 or 162 mu g of industrially relevant titanium dioxide nanoparticles (nano-TiO2) alongside vehicle controls. Using the nano-scale hyperspectral microscope, translocation to heart and liver was confirmed at both doses, and to blood at the highest dose, in mice analyzed 24 h post-exposure. Global gene expression profiling and ELISA analysis revealed activation of complement cascade and inflammatory processes in heart and specific activation of complement factor 3 in blood, suggesting activation of an early innate immune response essential for particle opsonisation and clearance. The liver showed a subtle response with changes in the expression of genes associated with acute phase response. This study characterizes the subtle systemic effects that occur in liver and heart tissues following pulmonary exposure and low levels of translocation of nano-TiO2 from lungs.

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