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聚苯乙烯微塑料对细胞类型、分化状态和暴露后时间的细胞和生物能量影响。

Cellular and bioenergetic effects of polystyrene microplastic in function of cell type, differentiation status and post-exposure time.

机构信息

Laboratory of Environmental Toxicology and Aquatic Ecology, Faculty of Bioscience Engineering, Ghent University, Coupure Links 653, 9000, Ghent, Belgium; Blue Growth Research Lab, Ghent University, Wetenschapspark 1, 8400, Oostende, Belgium.

Laboratory of Environmental Toxicology and Aquatic Ecology, Faculty of Bioscience Engineering, Ghent University, Coupure Links 653, 9000, Ghent, Belgium; Blue Growth Research Lab, Ghent University, Wetenschapspark 1, 8400, Oostende, Belgium.

出版信息

Environ Pollut. 2023 Nov 15;337:122550. doi: 10.1016/j.envpol.2023.122550. Epub 2023 Sep 15.

Abstract

The ubiquity of microplastics (MPs) in food sources and personal care products increasingly raises concerns on human health. However, little is known about the duration of the effects of MPs and whether effects depend on cellular differentiation status. Herein, cellular and bioenergetic effects of MPs in different exposure scenarios on four types of human cell lines derived from lung (A549 and BEAS-2B), colon (Caco-2) and liver (HepG2) were investigated. These cell lines are models for the major exposure routes in the body (inhalation, ingestion and physiological transport through the liver by the portal vein). To this aim, different scenarios were implemented by exposing undifferentiated and differentiated cells to single dosing of 2-μm polystyrene (PS) (10-10 particles/mL) for 48 h and 12 days. The undifferentiated Caco-2 cells with short exposure (48 h) showed the highest uptake rate of PS yet without significant cellular and mitochondrial responses. The biological effects, with the exception of ROS production, were not influenced by differentiation states of A549 and Caco-2 cells although differentiated cells showed much weaker ability to internalize PS. However, PS had significantly long-term impacts on cellular and mitochondrial functions even after the initial exposure period. In particular, Caco-2 cells that were post-exposed for 12 days after single PS dosing suffered higher oxidative stress and exhibited mitochondrial dysfunction than that for short exposure. Correspondingly, we observed that PS particles still remained in cell membrane and even in nuclei with high retention rate by 14-d post exposure during which metabolism and exchange of internalization and release occurred in cells. This indicates PS could induce chronic stress and even harmful effects on human cells after single intake that persists for a long time. This study paves the way for assessing the influence of PS on human health at low particle concentrations and with multiple exposure scenarios.

摘要

微塑料(MPs)在食物来源和个人护理产品中的普遍存在,日益引起人们对人类健康的关注。然而,人们对 MPs 的影响持续时间知之甚少,也不清楚这些影响是否取决于细胞分化状态。在此,我们研究了不同暴露场景下 MPs 对四种源自肺(A549 和 BEAS-2B)、结肠(Caco-2)和肝脏(HepG2)的人类细胞系的细胞和生物能效应。这些细胞系是体内主要暴露途径(吸入、摄入和通过门静脉生理运输到肝脏)的模型。为此,我们通过对未分化和分化细胞进行单次 2μm 聚苯乙烯(PS)(10-10 个颗粒/mL)暴露 48 小时和 12 天,实施了不同的暴露场景。短暂暴露(48 小时)的未分化 Caco-2 细胞表现出最高的 PS 摄取率,但没有明显的细胞和线粒体反应。除了 ROS 产生之外,生物学效应不受 A549 和 Caco-2 细胞分化状态的影响,尽管分化细胞内化 PS 的能力较弱。然而,PS 对细胞和线粒体功能的长期影响仍然显著,即使在初始暴露期之后。特别是,在单次 PS 给药后再暴露 12 天的 Caco-2 细胞比短期暴露时遭受更高的氧化应激并表现出线粒体功能障碍。相应地,我们观察到,在 14 天的暴露后,PS 颗粒仍然存在于细胞膜中,甚至存在于细胞核中,保留率很高,在此期间,细胞内的代谢和内化与释放的交换发生。这表明 PS 单次摄入后,可能会对人类细胞造成慢性应激甚至有害影响,且这种影响会持续很长时间。本研究为评估低浓度 PS 和多种暴露场景对人类健康的影响铺平了道路。

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