3.8 Article

Pre-validation of a reporter gene assay for oxidative stress for the rapid screening of nanobiomaterials

Journal

FRONTIERS IN TOXICOLOGY
Volume 4, Issue -, Pages -

Publisher

FRONTIERS MEDIA SA
DOI: 10.3389/ftox.2022.974429

Keywords

Nrf2; nanomaterial; interlaboratory validation; oxidative stress; nanotoxicology

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Funding

  1. European Union [760928]

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This study evaluated the oxidative stress responses induced by different nanobiomaterials using the NRF2 reporter gene assay. The results showed that Fe3O4-PEG-PLGA nanomaterials induced limited NRF2 mediated gene expression, while Ag nanomaterials induced NRF2 mediated gene expression and TiO2 nanomaterials did not. The NRF2 reporter gene assay is considered suitable for screening nanobiomaterial-induced oxidative stress responses.
Engineered nanomaterials have been found to induce oxidative stress. Cellular oxidative stress, in turn, can result in the induction of antioxidant and detoxification enzymes which are controlled by the nuclear erythroid 2-related factor 2 (NRF2) transcription factor. Here, we present the results of a pre-validation study which was conducted within the frame of BIORIMA (biomaterial risk management) an EU-funded research and innovation project. For this we used an NRF2 specific chemically activated luciferase expression reporter gene assay derived from the human U2OS osteosarcoma cell line to screen for the induction of the NRF2 mediated gene expression following exposure to biomedically relevant nanobiomaterials. Specifically, we investigated Fe3O4-PEG-PLGA nanomaterials while Ag and TiO2 benchmark nanomaterials from the Joint Research Center were used as reference materials. The viability of the cells was determined by using the Alamar blue assay. We performed an interlaboratory study involving seven different laboratories to assess the applicability of the NRF2 reporter gene assay for the screening of nanobiomaterials. The latter work was preceded by online tutorials to ensure that the procedures were harmonized across the different participating laboratories. Fe3O4-PEG-PLGA nanomaterials were found to induce very limited NRF2 mediated gene expression, whereas exposure to Ag nanomaterials induced NRF2 mediated gene expression. TiO2 nanomaterials did not induce NRF2 mediated gene expression. The variability in the results obtained by the participating laboratories was small with mean intra-laboratory standard deviation of 0.16 and mean inter laboratory standard deviation of 0.28 across all NRF2 reporter gene assay results. We conclude that the NRF2 reporter gene assay is a suitable assay for the screening of nanobiomaterial-induced oxidative stress responses.

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