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少即是多:长期体外暴露于低浓度银纳米颗粒为纳米材料评估提供新的见解。

Less is more: long-term in vitro exposure to low levels of silver nanoparticles provides new insights for nanomaterial evaluation.

机构信息

Molecular Bioeffects Branch, Air Force Research Laboratory, Wright-Patterson AFB , 2729 R Street, Bldg 837, Dayton, Ohio 45433, United States.

出版信息

ACS Nano. 2014 Apr 22;8(4):3260-71. doi: 10.1021/nn5009116. Epub 2014 Mar 19.

Abstract

In view of the vast number of new nanomaterials (NMs) that require testing and the constraints associated with animal models, the majority of studies to elucidate nanotoxicological effects have occurred in vitro, with limited correlation and applicability to in vivo systems and realistic, occupational exposure scenarios. In this study, we developed and implemented a chronic in vitro model coupled with lower, regulatory dosages in order to provide a more realistic assessment of NM-dependent consequences and illuminate the implications of long-term NM exposure. When keratinocytes were exposed to 50 nm silver nanoparticles (Ag-NPs), we determined that chronically dosed cells operated under augmented stress and modified functionality in comparison to their acute counterparts. Specifically, Ag-NP exposure through a chronic mechanism increased p38 activation, actin disorganization, heightened ki67 expression, and extensive gene modification. Additionally, chronic Ag-NP exposure altered the way in which cells perceived and responded to epidermal growth factor stimulation, indicating a transformation of cell functionality. Most importantly, this study demonstrated that chronic exposure in the pg/mL range to Ag-NPs did not induce a cytotoxic response, but instead activated sustained stress and signaling responses, suggesting that cells are able to cope with prolonged, low levels of Ag-NP exposure. In summary, we demonstrated that through implementation of a chronic dosimetry paradigm, which more closely resembles realistic NM exposure scenarios, it is possible to illuminate long-term cellular consequences, which greatly differ from previously obtained acute assessments.

摘要

鉴于需要测试的新型纳米材料(NMs)数量众多,并且受到动物模型的限制,大多数阐明纳米毒理学效应的研究都是在体外进行的,与体内系统和现实、职业暴露情况的相关性和适用性有限。在这项研究中,我们开发并实施了慢性体外模型,并采用较低的监管剂量,以便更真实地评估 NM 依赖性后果,并阐明长期 NM 暴露的影响。当角质形成细胞暴露于 50nm 银纳米颗粒(Ag-NPs)时,我们发现与急性细胞相比,慢性给药细胞在增强的应激和功能改变下运作。具体来说,通过慢性机制暴露于 Ag-NP 会增加 p38 激活、肌动蛋白解聚、ki67 表达增加和广泛的基因修饰。此外,慢性 Ag-NP 暴露改变了细胞感知和对表皮生长因子刺激的反应方式,表明细胞功能发生了转化。最重要的是,这项研究表明,在 pg/mL 范围内的慢性 Ag-NP 暴露不会引起细胞毒性反应,而是激活持续的应激和信号反应,表明细胞能够应对长期低水平的 Ag-NP 暴露。总之,我们证明通过实施更接近现实 NM 暴露情况的慢性剂量测定范式,可以阐明与以前获得的急性评估大不相同的长期细胞后果。

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