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低剂量暴露的WS纳米片诱导肺上皮细胞发生差异性凋亡。

Low-Dose Exposure of WS Nanosheets Induces Differential Apoptosis in Lung Epithelial Cells.

作者信息

Coreas Roxana, Li Zongbo, Chen Junyi, Zhong Wenwan

机构信息

Environmental Toxicology Graduate Program, University of California-Riverside, Riverside, California 92521, United States.

Department of Chemistry, University of California-Riverside, Riverside, California 92521, United States.

出版信息

Environ Sci Technol. 2023 Oct 3;57(39):14493-14501. doi: 10.1021/acs.est.3c01843. Epub 2023 Sep 19.

Abstract

Escalating the production and application of tungsten disulfide (WS) nanosheets inevitably increases environmental human exposure and warrants the necessity of studies to elucidate their biological impacts. Herein, we assessed the toxicity of WS nanosheets and focused on the impacts of low doses (≤10 μg/mL) on normal (BEAS-2B) and tumorigenic (A549) lung epithelial cells. The low doses, which approximate real-world exposures, were found to induce cell apoptosis, while doses ≥ 50 μg/mL cause necrosis. Focused studies on low-dose exposure to WS nanosheets revealed more details of the impacts on both cell lines, including reduction of cell metabolic activity, induction of lipid peroxidation in cell membranes, and uncoupling of mitochondrial oxidative phosphorylation that led to the loss of ATP production. These phenomena, along with the expression situations of a few key proteins involved in apoptosis, point toward the occurrence of mitochondria-dependent apoptotic signaling in exposed cells. Substantial differences in responses to WS exposure between normal and tumorigenic lung epithelial cells were noticed as well. Specifically, BEAS-2B cells experienced more adverse effects and took up more nanosheets than A549 cells. Our results highlight the importance of dose and cell model selection in the assessment of nanotoxicity. By using doses consistent with real-world exposures and comparing normal and diseased cells, we can gain knowledge to guide the development of safety precautions for mitigating the adverse impacts of nanomaterial exposure on human health.

摘要

二硫化钨(WS)纳米片产量和应用的不断增加不可避免地增加了人类对环境的接触,因此有必要开展研究以阐明其生物学影响。在此,我们评估了WS纳米片的毒性,并重点关注低剂量(≤10μg/mL)对正常(BEAS-2B)和致瘤性(A549)肺上皮细胞的影响。发现接近实际环境暴露水平的低剂量会诱导细胞凋亡,而≥50μg/mL的剂量会导致细胞坏死。对低剂量WS纳米片暴露的重点研究揭示了对两种细胞系影响的更多细节,包括细胞代谢活性降低、细胞膜脂质过氧化诱导以及线粒体氧化磷酸化解偶联导致ATP生成减少。这些现象,连同参与凋亡的一些关键蛋白的表达情况,表明暴露细胞中发生了线粒体依赖性凋亡信号传导。正常和致瘤性肺上皮细胞对WS暴露的反应也存在显著差异。具体而言,BEAS-2B细胞比A549细胞受到的不利影响更大,摄取的纳米片更多。我们的结果强调了剂量和细胞模型选择在纳米毒性评估中的重要性。通过使用与实际环境暴露一致的剂量并比较正常细胞和病变细胞,我们可以获得相关知识,以指导制定安全预防措施,减轻纳米材料暴露对人类健康的不利影响。

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