4.5 Article

Pulmonary toxicity and gene expression changes after short-term inhalation exposure to surface-modified copper oxide nanoparticles

NANOIMPACT (2021)

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Journal

NANOIMPACT
Volume 22, Issue -, Pages -

Publisher

ELSEVIER
DOI: 10.1016/j.impact.2021.100313

Keywords

Nanoparticles; Copper oxide; Safe-by-design; Pulmonary toxicity; Transcriptomics

Categories

Environmental Sciences Nanoscience & Nanotechnology

Funding

  1. SUN ('sustainable nanotechnology') project - Seventh Framework Program of the European Commission [604305]
  2. RIVM Strategic Research Program, the Netherlands (SPR) [E/121504]
  3. Fundacao para a Ciencia e Tecnologia (FCT, Portugal) [UIDB/04378/2020]
  4. Health Canada Genomics Research and Development Initiative

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This study found that both ASC and PEI coated CuO NPs can cause dose-dependent pulmonary inflammation and cell damage, leading to activation of inflammation and cell proliferation pathways post-exposure. Although there were no differences in toxic effects and potency between the two surface coatings, evidence of dysregulation of drug metabolism-related genes was found in rats exposed to ASC-coated CuO NPs.
Copper oxide nanoparticles (CuO NPs) have previously been shown to cause dose-dependent pulmonary toxicity following inhalation. Here, CuO NPs (10 nm), coated with polyethylenimine (PEI) or ascorbate (ASC) resulting in positively or negatively charged NPs, respectively, were evaluated. Rats were exposed nose-only to similar exposure dose levels of ASC or PEI coated CuO NPs for 5 consecutive days. On day 6 and day 27 post-exposure, pulmonary toxicity markers in bronchoalveolar lavage fluid (BALF), lung histopathology and genome-wide transcriptomic changes in lungs, were assessed. BALF analyses showed a dose-dependent pulmonary inflammation and cell damage, which was supported by the lung histopathological findings of hypertrophy/hyperplasia of bronchiolar and alveolar epithelium, interstitial and alveolar inflammation, and paracortical histiocytosis in mediastinal lymph nodes for both types of CuO NPs. Transcriptomics analysis showed that pathways related to inflammation and cell proliferation were significantly activated. Additionally, we found evidence for the dysregulation of drug metabolism-related genes, especially in rats exposed to ASC-coated CuO NPs. Overall, no differences in the type of toxic effects and potency between the two surface coatings could be established, except with respect to the (regional) dose that initiates bronchiolar and alveolar hypertrophy. This disproves our hypothesis that differences in surface coatings affect the pulmonary toxicity of CuO NPs.

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