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微塑料和纳米塑料:尺寸、表面与分散剂——影响因素究竟是什么?

Microplastics and nanoplastics: Size, surface and dispersant - What causes the effect?

作者信息

Stock Valerie, Böhmert Linda, Coban Gülcin, Tyra Gina, Vollbrecht Marie-Luise, Voss Linn, Paul Maxi B, Braeuning Albert, Sieg Holger

机构信息

German Federal Institute for Risk Assessment, Max-Dohrn-Str. 8-10, 10589 Berlin, Germany.

German Federal Institute for Risk Assessment, Max-Dohrn-Str. 8-10, 10589 Berlin, Germany.

出版信息

Toxicol In Vitro. 2022 Apr;80:105314. doi: 10.1016/j.tiv.2022.105314. Epub 2022 Jan 14.

Abstract

There is increasing evidence that humans are exposed to microplastic particles through contaminated food. Although suitable analytical methods are still lacking, it is likely that these contaminations also contain a nanoplastics fraction. It is known from nanotoxicology that particles may acquire altered toxicological properties with decreasing particle sizes. Particles can also have different surface modalities and functionalizations. Moreover, nano- and microplastics as materials with probably a relatively low toxicity are often applied at high concentrations in in vitro tests, and therefore the solvating agent, namely the dispersant in which the particles are supplied may have a major impact on the outcome. This might be misinterpreted as particle effect. Therefore, it is crucial to determine what causes the effect - size, surface or dispersant? In this study this question was investigated by applying established in vitro models for the intestinal barrier (differentiated Caco-2 monoculture and mucus- and M-cell co-culture) and hepatocytes (differentiated HepaRG cells), mimicking the oral route of particle uptake. A complex set of nine different polystyrene micro- and nanoparticles was used to elucidate the effect of particle size, surface modification and dispersant. Uptake and transport as well as biochemical endpoints were measured, complemented by particle characterization. The results show that indeed some dispersants can cause a more pronounced cytotoxic effect than the particles themselves. Surface modification and particle size show a clear influence on the uptake and cytotoxicity of nano- and microplastic particles.

摘要

越来越多的证据表明,人类通过受污染的食物接触到微塑料颗粒。尽管仍缺乏合适的分析方法,但这些污染物很可能也含有一部分纳米塑料。从纳米毒理学可知,随着颗粒尺寸减小,颗粒可能会获得改变的毒理学特性。颗粒还可以具有不同的表面形态和功能化。此外,纳米塑料和微塑料作为毒性可能相对较低的材料,在体外试验中经常以高浓度使用,因此溶剂化剂,即提供颗粒的分散剂,可能会对结果产生重大影响。这可能会被误解为颗粒效应。因此,确定造成这种效应的原因是颗粒大小、表面还是分散剂至关重要。在本研究中,通过应用已建立的用于肠道屏障(分化的Caco-2单培养物以及黏液和M细胞共培养物)和肝细胞(分化的HepaRG细胞)的体外模型来研究这个问题,模拟颗粒摄取的口服途径。使用一组复杂的九种不同的聚苯乙烯微塑料和纳米颗粒来阐明颗粒大小、表面改性和分散剂的影响。测量了摄取、转运以及生化终点,并辅以颗粒表征。结果表明,确实有些分散剂会比颗粒本身引起更明显的细胞毒性作用。表面改性和颗粒大小对纳米塑料和微塑料颗粒的摄取和细胞毒性有明显影响。

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