Bioavailability and biodistribution of differently charged polystyrene nanoparticles upon oral exposure in rats

生物利用度 体内 体内分布 体外 材料科学 生物物理学 药理学 化学 生物化学 生物 生物技术
作者
Agata P. Walczak,Peter J.M. Hendriksen,R.A. Woutersen,Meike van der Zande,Anna K. Undas,Richard Helsdingen,Hans H. J. van den Berg,Ivonne M.C.M. Rietjens,Hans Bouwmeester
出处
期刊:Journal of Nanoparticle Research [Springer Science+Business Media]
卷期号:17 (5) 被引量:149
标识
DOI:10.1007/s11051-015-3029-y
摘要

The likelihood of oral exposure to nanoparticles (NPs) is increasing, and it is necessary to evaluate the oral bioavailability of NPs. In vitro approaches could help reducing animal studies, but validation against in vivo studies is essential. Previously, we assessed the translocation of 50 nm polystyrene NPs of different charges (neutral, positive and negative) using a Caco-2/HT29-MTX in vitro intestinal translocation model. The NPs translocated in a surface charge-dependent manner. The present study aimed to validate this in vitro intestinal model by an in vivo study. For this, rats were orally exposed to a single dose of these polystyrene NPs and the uptake in organs was determined. A negatively charged NP was taken up more than other NPs, with the highest amounts in kidney (37.4 µg/g tissue), heart (52.8 µg/g tissue), stomach wall (98.3 µg/g tissue) and small intestinal wall (94.4 µg/g tissue). This partly confirms our in vitro findings, where the same NPs translocated to the highest extent. The estimated bioavailability of different types of NPs ranged from 0.2 to 1.7 % in vivo, which was much lower than in vitro (1.6-12.3 %). Therefore, the integrated in vitro model cannot be used for a direct prediction of the bioavailability of orally administered NPs. However, the model can be used for prioritizing NPs before further in vivo testing for risk assessment.
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