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提出尿路上皮和肌肉体外细胞模型作为评估纳米颗粒长期毒性的新方法。

Proposing Urothelial and Muscle In Vitro Cell Models as a Novel Approach for Assessment of Long-Term Toxicity of Nanoparticles.

机构信息

Group for nano and biotechnological applications, Faculty of Electrical Engineering, University of Ljubljana, SI -1000 Ljubljana, Slovenia.

Institute of Pathophysiology, Faculty of Medicine, University of Ljubljana, SI -1000 Ljubljana, Slovenia.

出版信息

Int J Mol Sci. 2020 Oct 13;21(20):7545. doi: 10.3390/ijms21207545.

Abstract

Many studies evaluated the short-term in vitro toxicity of nanoparticles (NPs); however, long-term effects are still not adequately understood. Here, we investigated the potential toxic effects of biomedical (polyacrylic acid and polyethylenimine coated magnetic NPs) and two industrial (SiO and TiO) NPs following different short-term and long-term exposure protocols on two physiologically different in vitro models that are able to differentiate: L6 rat skeletal muscle cell line and biomimetic normal porcine urothelial (NPU) cells. We show that L6 cells are more sensitive to NP exposure then NPU cells. Transmission electron microscopy revealed an uptake of NPs into L6 cells but not NPU cells. In L6 cells, we obtained a dose-dependent reduction in cell viability and increased reactive oxygen species (ROS) formation after 24 h. Following continuous exposure, more stable TiO and polyacrylic acid (PAA) NPs increased levels of nuclear factor Nrf2 mRNA, suggesting an oxidative damage-associated response. Furthermore, internalized magnetic PAA and TiO NPs hindered the differentiation of L6 cells. We propose the use of L6 skeletal muscle cells and NPU cells as a novel approach for assessment of the potential long-term toxicity of relevant NPs that are found in the blood and/or can be secreted into the urine.

摘要

许多研究评估了纳米颗粒(NPs)的短期体外毒性;然而,长期影响仍未得到充分理解。在这里,我们研究了生物医学(聚丙烯酸和聚乙烯亚胺涂层磁性 NPs)和两种工业(SiO 和 TiO)NPs 在不同的短期和长期暴露方案下对两种具有生理差异的体外模型的潜在毒性影响,这两种模型能够分化:L6 大鼠骨骼肌细胞系和仿生正常猪尿路上皮(NPU)细胞。我们表明,L6 细胞对 NP 暴露比 NPU 细胞更敏感。透射电子显微镜显示 NPs 被摄取到 L6 细胞中,但没有摄取到 NPU 细胞中。在 L6 细胞中,我们在 24 小时后获得了细胞活力下降和活性氧(ROS)形成增加的剂量依赖性。在连续暴露后,更多稳定的 TiO 和聚丙烯酸(PAA)NPs 增加了核因子 Nrf2 mRNA 的水平,表明存在与氧化损伤相关的反应。此外,内化的磁性 PAA 和 TiO NPs 阻碍了 L6 细胞的分化。我们建议使用 L6 骨骼肌细胞和 NPU 细胞作为评估血液中存在的相关 NPs 或可能分泌到尿液中的 NPs 的潜在长期毒性的新方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3551/7589566/2f4b1db3e7c4/ijms-21-07545-g001.jpg

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