4.6 Article

Impact of in vitro digested zinc oxide nanoparticles on intestinal model systems

Journal

PARTICLE AND FIBRE TOXICOLOGY
Volume 19, Issue 1, Pages -

Publisher

BMC
DOI: 10.1186/s12989-022-00479-6

Keywords

Caco-2; Coculture; HT29-MTX; In vitro digestion; Nanoparticles; Toxicity; Transwell; Zinc oxide

Categories

Funding

  1. Projekt DEAL

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This study investigates the fate and impact of two different sized ZnO NP during in vitro digestion on model systems of the intestinal barrier. The results show that digested ZnO NP interact with the cells of an intact intestinal barrier without causing serious cell damage.
Background Zinc oxide nanoparticles (ZnO NP) offer beneficial properties for many applications, especially in the food sector. Consequently, as part of the human food chain, they are taken up orally. The toxicological evaluation of orally ingested ZnO NP is still controversial. In addition, their physicochemical properties can change during digestion, which leads to an altered biological behaviour. Therefore, the aim of our study was to investigate the fate of two different sized ZnO NP (< 50 nm and < 100 nm) during in vitro digestion and their effects on model systems of the intestinal barrier. Differentiated Caco-2 cells were used in mono- and coculture with mucus-producing HT29-MTX cells. The cellular uptake, the impact on the monolayer barrier integrity and cytotoxic effects were investigated after 24 h exposure to 123-614 mu M ZnO NP. Results In vitro digested ZnO NP went through a morphological and chemical transformation with about 70% free zinc ions after the intestinal phase. The cellular zinc content increased dose-dependently up to threefold in the monoculture and fourfold in the coculture after treatment with digested ZnO NP. This led to reactive oxygen species but showed no impact on cellular organelles, the metabolic activity, and the mitochondrial membrane potential. Only very small amounts of zinc (< 0.7%) reached the basolateral area, which is due to the unmodified transepithelial electrical resistance, permeability, and cytoskeletal morphology. Conclusions Our results reveal that digested and, therefore, modified ZnO NP interact with cells of an intact intestinal barrier. But this is not associated with serious cell damage.

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