Silver nanoparticles induce formation of multi-protein aggregates that contain cadherin but do not colocalize with nanoparticles

IF 2.6 3区 医学 Q3 TOXICOLOGY Toxicology in Vitro Pub Date : 2024-04-30 DOI:10.1016/j.tiv.2024.105837
Kaden M. Thomas, Nadja Spitzer
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Abstract

Silver nanoparticles (AgNPs) are increasingly incorporated in diverse products to confer antimicrobial properties. They are released into the environment during manufacture, after disposal, and from the products during use. Because AgNPs bioaccumulate in brain, it is important to understand how they interact with neural cell physiology. We found that the focal adhesion (FA)-associated protein cadherin aggregated in a dose-dependent response to AgNP exposure in differentiating cultured B35 neuroblastoma cells. These aggregates tended to colocalize with F-actin inclusions that form in response to AgNP and also contain β-catenin. However, using hyperspectral microscopy, we demonstrate that these multi-protein aggregates did not colocalize with the AgNPs themselves. Furthermore, expression and organization of the FA protein vinculin did not change in cells exposed to AgNP. Our findings suggest that AgNPs activate an intermediate mechanism which leads to formation of aggregates via specific protein-protein interactions. Finally, we detail the changes in hyperspectral profiles of AgNPs during different stages of cell culture and immunocytochemistry processing. AgNPs in citrate-stabilized solution present mostly blue with some rainbow spectra and these are maintained upon mounting in Prolong Gold. Exposure to tissue culture medium results in a uniform green spectral shift that is not further altered by fixation and protein block steps of immunocytochemistry.

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银纳米粒子可诱导多蛋白聚集体的形成,这些聚集体含有固着蛋白,但不与纳米粒子共定位。
银纳米粒子(AgNPs)被越来越多地应用到各种产品中,以赋予其抗菌特性。它们在生产过程中、废弃后以及使用过程中从产品中释放到环境中。由于 AgNPs 会在大脑中生物累积,因此了解它们如何与神经细胞的生理机能相互作用非常重要。我们发现,在分化培养的 B35 神经母细胞瘤细胞中,局灶粘附(FA)相关蛋白粘连蛋白的聚集与暴露于 AgNP 的剂量有关。这些聚集体倾向于与F-肌动蛋白包涵体共聚焦,F-肌动蛋白包涵体是在AgNP作用下形成的,其中也含有β-catenin。然而,我们利用高光谱显微镜证明,这些多蛋白聚集体与 AgNPs 本身并不共聚焦。此外,FA 蛋白 vinculin 的表达和组织在暴露于 AgNP 的细胞中没有变化。我们的研究结果表明,AgNPs 激活了一种中间机制,通过特定的蛋白质-蛋白质相互作用形成聚集体。最后,我们详细介绍了 AgNPs 在细胞培养和免疫细胞化学处理不同阶段的高光谱特征变化。柠檬酸盐稳定溶液中的 AgNPs 主要呈现蓝色,也有一些彩虹光谱,这些光谱在装入 Prolong Gold 后保持不变。暴露在组织培养基中会产生均匀的绿色光谱偏移,这种偏移不会因免疫细胞化学的固定和蛋白阻断步骤而进一步改变。
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来源期刊
Toxicology in Vitro
Toxicology in Vitro 医学-毒理学
CiteScore
6.50
自引率
3.10%
发文量
181
审稿时长
65 days
期刊介绍: Toxicology in Vitro publishes original research papers and reviews on the application and use of in vitro systems for assessing or predicting the toxic effects of chemicals and elucidating their mechanisms of action. These in vitro techniques include utilizing cell or tissue cultures, isolated cells, tissue slices, subcellular fractions, transgenic cell cultures, and cells from transgenic organisms, as well as in silico modelling. The Journal will focus on investigations that involve the development and validation of new in vitro methods, e.g. for prediction of toxic effects based on traditional and in silico modelling; on the use of methods in high-throughput toxicology and pharmacology; elucidation of mechanisms of toxic action; the application of genomics, transcriptomics and proteomics in toxicology, as well as on comparative studies that characterise the relationship between in vitro and in vivo findings. The Journal strongly encourages the submission of manuscripts that focus on the development of in vitro methods, their practical applications and regulatory use (e.g. in the areas of food components cosmetics, pharmaceuticals, pesticides, and industrial chemicals). Toxicology in Vitro discourages papers that record reporting on toxicological effects from materials, such as plant extracts or herbal medicines, that have not been chemically characterized.
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