AI Article Synopsis
- Public health agencies are concerned about consumer exposure to aluminum-containing nanomaterials (Al NMs) due to limited data on their genotoxicity.
- The study tested the genotoxic effects of Al NMs and AlO in intestinal (Caco-2) and liver (HepaRG) cells, along with ionic aluminum (AlCl), using various assays to measure cytotoxicity, oxidative stress, and DNA damage.
- While Al NMs did not cause chromosomal damage, they resulted in significant oxidative DNA damage in Caco-2 cells and considerable DNA damage in both cell lines, whereas no genotoxic effects were found with AlCl or any of the aluminum compounds tested.
Article Abstract
Exposure of consumers to aluminum-containing nanomaterials (Al NMs) is an area of concern for public health agencies. As the available data on the genotoxicity of AlO and Al NMs are inconclusive or rare, the present study investigated their in vitro genotoxic potential in intestinal and liver cell models, and compared with the ionic form AlCl. Intestinal Caco-2 and hepatic HepaRG cells were exposed to Al and AlO NMs (0.03 to 80 μg/cm). Cytotoxicity, oxidative stress and apoptosis were measured using High Content Analysis. Genotoxicity was investigated through γH2AX labelling, the alkaline comet and micronucleus assays. Moreover, oxidative DNA damage and carcinogenic properties were assessed using the Fpg-modified comet assay and the cell transforming assay in Bhas 42 cells respectively. The three forms of Al did not induce chromosomal damage. However, although no production of oxidative stress was detected, AlO NMs induced oxidative DNA damage in Caco-2 cells but not likely related to ion release in the cell media. Considerable DNA damage was observed with Al NMs in both cell lines in the comet assay, likely due to interference with these NMs. No genotoxic effects were observed with AlCl. None of the Al compounds induced cytotoxicity, apoptosis, γH2AX or cell transformation.
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| http://dx.doi.org/10.1016/j.tiv.2021.105257 | DOI Listing |
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