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在 Balb/3T3 小鼠成纤维细胞中,钴纳米颗粒、微颗粒和离子与培养基成分的相互作用、细胞摄取和细胞内分布。

Interaction with culture medium components, cellular uptake and intracellular distribution of cobalt nanoparticles, microparticles and ions in Balb/3T3 mouse fibroblasts.

机构信息

ECSIN - European Center for the Sustainable Impact of Nanotechnologies, Veneto Nanotech ScpA , Rovigo , Italy.

出版信息

Nanotoxicology. 2014 Feb;8(1):88-99. doi: 10.3109/17435390.2012.752051. Epub 2012 Dec 21.

Abstract

The mechanistic understanding of nanotoxicity requires the physico-chemical characterisation of nanoparticles (NP), and their comparative investigation relative to the corresponding ions and microparticles (MP). Following this approach, the authors studied the dissolution, interaction with medium components, bioavailability in culture medium, uptake and intracellular distribution of radiolabelled Co forms (CoNP, CoMP and Co(2+)) in Balb/3T3 mouse fibroblasts. Co(2+) first saturates the binding sites of molecules in the extracellular milieu (e.g., albumin and histidine) and on the cell surface. Only after saturation, Co(2+) is actively uptaken. CoNP, instead, are predicted to be internalised by endocytosis. Dissolution of Co particles allows the formation of Co compounds (CoNP-rel), whose mechanism of cellular internalisation is unknown. Co uptake (ranking CoMP > CoNP > Co(2+)) reached maximum at 4 h. Once inside the cell, CoNP spread into the cytosol and organelles. Consequently, massive amounts of Co ions and CoNP-rel can reach subcellular compartments normally unexposed to Co(2+). This could explain the fact that the nuclear and mitochondrial Co concentrations resulted significantly higher than those obtained with Co(2+).

摘要

纳米毒性的机制理解需要对纳米粒子(NP)进行物理化学特性分析,并将其与相应的离子和微米粒子(MP)进行比较研究。按照这种方法,作者研究了放射性标记 Co 形态(CoNP、CoMP 和 Co(2+))在 Balb/3T3 小鼠成纤维细胞中的溶解、与介质成分的相互作用、在培养基中的生物利用度、摄取和细胞内分布。Co(2+)首先饱和细胞外环境(例如白蛋白和组氨酸)和细胞表面分子的结合位点。只有在饱和后,Co(2+)才被主动摄取。相反,CoNP 被预测通过内吞作用被内化。Co 颗粒的溶解允许形成 Co 化合物(CoNP-rel),其细胞内化机制尚不清楚。Co 的摄取(CoMP > CoNP > Co(2+))在 4 小时达到最大值。一旦进入细胞,CoNP 就会扩散到细胞质和细胞器中。因此,大量的 Co 离子和 CoNP-rel 可以到达通常不会暴露于 Co(2+)的亚细胞区室。这可以解释为什么核和线粒体中的 Co 浓度明显高于用 Co(2+)获得的浓度。

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