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Effects of Zinc Oxide Nanoparticle Exposure on Human Glial Cells and Zebrafish Embryos

International Journal of Molecular Sciences 2023 29 citations ? Citation count from OpenAlex, updated daily. May differ slightly from the publisher's own count. Score: 55 ? 0–100 AI score estimating relevance to the microplastics field. Papers below 30 are filtered from public browse.

Vanessa Valdiglesias, Anabel Alba‐González, Natalia Fernández‐Bertólez, Jorge Moreda–Piñeiro, Jorge Moreda–Piñeiro, A. Touzani, Lucía Ramos-Pan, Ana Teresa Reis, Jorge Moreda–Piñeiro, Julián Yáñez, Blanca Laffón, Mónica Folgueira

Summary

Researchers investigated the toxicity of zinc oxide nanoparticles on human brain glial cells and zebrafish embryos, finding that both were harmed at relatively low concentrations. The nanoparticles reduced cell viability in the glial cells and caused developmental abnormalities in the zebrafish embryos. The study suggests that the dissolved zinc ions released from these widely used nanoparticles play a significant role in their toxic effects on the nervous system.

Body Systems

Nervous

Models

Zebrafish

Study Type In vivo

Zinc oxide nanoparticles (ZnO NPs) are among the most widely used nanomaterials. They have multiple applications in cosmetics, textiles, paints, electronics and, recently, also in biomedicine. This extensive use of ZnO NPs notably increases the probability that both humans and wildlife are subjected to undesirable effects. Despite being among the most studied NPs from a toxicological point of view, much remains unknown about their ecotoxicological effects or how they may affect specific cell types, such as cells of the central nervous system. The main objective of this work was to investigate the effects of ZnO NPs on human glial cells and zebrafish embryo development and to explore the role of the released Zn2+ ions in these effects. The effects on cell viability on human A172 glial cells were assessed with an MTT assay and morphological analysis. The potential acute and developmental toxicity was assessed employing zebrafish (Danio rerio) embryos. To determine the role of Zn2+ ions in the in vitro and in vivo observed effects, we measured their release from ZnO NPs with flame atomic absorption spectrometry. Then, cells and zebrafish embryos were treated with a water-soluble salt (zinc sulfate) at concentrations that equal the number of Zn2+ ions released by the tested concentrations of ZnO NPs. Exposure to ZnO NPs induced morphological alterations and a significant decrease in cell viability depending on the concentration and duration of treatment, even after removing the overestimation due to NP interference. Although there were no signs of acute toxicity in zebrafish embryos, a decrease in hatching was detected after exposure to the highest ZnO NP concentrations tested. The ability of ZnO NPs to release Zn2+ ions into the medium in a concentration-dependent manner was confirmed. Zn2+ ions did not seem entirely responsible for the effects observed in the glial cells, but they were likely responsible for the decrease in zebrafish hatching rate. The results obtained in this work contribute to the knowledge of the toxicological potential of ZnO NPs.

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