4.7 Article

Exposure to TiO2 Nanostructured Aerosol Induces Specific Gene Expression Profile Modifications in the Lungs of Young and Elderly Rats

Journal

NANOMATERIALS
Volume 11, Issue 6, Pages -

Publisher

MDPI
DOI: 10.3390/nano11061466

Keywords

inhalation; titanium dioxide; lung; age; transcriptomics; rat

Funding

  1. European Commission through the EU Horizon 2020 Framework Programme [Project SmartNanoTox] [686098]
  2. French Agency for Food, Environmental and Occupational Health Safety (ANSES)
  3. European Commission

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This study aimed to compare the pulmonary toxicity of inhaled nanostructured aerosol of titanium dioxide (TiO2) between young and elderly rats. While there were differences in neutrophilic granulocytes influx and inflammation-related gene expression between the two age groups, slight variation was observed in physiological responses following TiO2 exposure. Age-related differences were mainly reflected in gene expression profiles, highlighting disrupted signaling pathways in rats based on their age.
Although aging is associated with a higher risk of developing respiratory pathologies, very few studies have assessed the impact of age on the adverse effects of inhaled nanoparticles. Using conventional and transcriptomic approaches, this study aimed to compare in young (12-13-week-old) and elderly (19-month-old) fisher F344 rats the pulmonary toxicity of an inhaled nanostructured aerosol of titanium dioxide (TiO2). Animals were nose-only exposed to this aerosol at a concentration of 10 mg/m(3) for 6 h per day, 5 days per week for 4 weeks. Tissues were collected immediately (D0), and 28 days after exposure (D28). A pulmonary influx of neutrophilic granulocytes was observed in exposed rats at D0, but diminished with time while remaining significant until D28. Similarly, an increased expression of several genes involved in inflammation at the two post-exposure time-points was seen. Apart from an age-specific pulmonary influx of lymphocyte, only slight differences in physio-pathological responses following TiO2 exposure between young and elderly animals were noticed. Conversely, marked age-related differences in gene expression profiles were observed making possible to establish lists of genes specific to each age group and post-exposure times. These results highlight different signaling pathways that were disrupted in rats according to their age.

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