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Implementation of physiological fluids to provide insight into the characterization, fate, and biological interactions of silver nanoparticles

机译:生理流体的实施,以了解银纳米粒子的表征,命运和生物相互作用的洞察

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Silver nanoparticles (AgNPs) are being increasingly utilized in consumer and medical applications. However, there remains conflicting reports on their safety, which are evaluated through a combination of in vitro and in vivo exposure models. These discrepancies may arise, in part, due to the inherent differences between cell-based and animal systems. It is well established that nanotoxicological effects are highly dependent on the unique physicochemical properties and behavior of the particle set, including size, surface chemistry, agglomeration, and ionic dissolution. However, recent studies have identified that these properties vary as a function of exposure environment; providing a rationale for the contradictory results between in vitro and in vivo assessments. Artificial physiological fluids are emerging as a powerful tool as they allow for the characterization of NPs in an environment which they would likely encounter in vivo, in addition to having the experimental advantages of flexibility and consistency. Here, we demonstrated that the utilization of artificial fluids provided a mechanism to assess AgNP behavior and induced bioresponses in environments that they would likely encounter in vivo. AgNPs were introduced within an alveolar-based exposure model, which included alveolar epithelial (A549) cells incubated within artificial alveolar fluid (AF). Additionally, the particles underwent extensive characterization within both AF and lysosomal fluid, which the AgNPs would encounter following cellular internalization. Following incubation in physiological environments AgNP properties were significantly modified versus a traditional media environment, including alterations to both extent of agglomeration and rate of ionic dissolution. Moreover, when A549s were exposed to AgNPs in AF, the cells displayed lower cytotoxicity and stress rates, corresponding to a fluid-dependent drop in silver ion production. This work highlights the need for enhanced in vitro model
机译:银纳米粒子(AGNPS)越来越多地用于消费和医疗应用。但是,仍然存在对其安全性相互矛盾的报道,其通过体外和体内曝光模型的组合进行评估。由于基于细胞和动物系统之间的固有差异,这些差异可能会出现。很好地确定,纳米毒理学效应高度依赖于颗粒集的独特物理化学性质和行为,包括尺寸,表面化学,附聚和离子溶解。然而,最近的研究已经确定了这些性质随着曝光环境的函数而变化;在体外和体内评估之间提供矛盾结果的理由。人造生理流体正在作为一种强大的工具,因为它们允许在它们在体内遇到的环境中表征NPS,除了具有灵活性和一致性的实验优势。在这里,我们证明了人造流体的利用提供了一种机制来评估AGNP行为,并在环境中遇到的环境中的诱导的生物绝望。在肺泡的曝光模型中引入AgNP,其包括在人造肺泡液(AF)内孵育的肺泡上皮(A549)细胞。另外,颗粒在AF和溶酶体液中进行了广泛的表征,agnps在细胞内化之后会遇到。在生理环境中孵育后,AGNP性质与传统媒体环境有显着修饰,包括改变聚集的程度和离子溶解速率。此外,当A549S暴露于AF中的AgNP时,细胞显示细胞毒性和应力速率,对应于银离子产生中的流体依赖性下降。这项工作突出了对体外模型增强的需求

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