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Interactions of silica nanoparticles with lung epithelial cells and the association to flotillins

机译:二氧化硅纳米颗粒与肺上皮细胞的相互作用以及与氟钙素的关系

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摘要

Amorphous silica nanoparticles (aSNPs) gain increasing popularity for industrial and therapeutic claims. The lung with its surface area of 100–140 m2 displays an ideal target for therapeutic approaches, but it represents also a serious area of attack for harmful nanomaterials. The exact nature of the cytotoxic effects of NPs is still unknown. Furthermore, cellular pathways and the destiny of internalized NPs are still poorly understood. Therefore, we examined the cytotoxicity (MTS, LDH) and inflammatory responses (IL-8) for different-sized aSNPs (30, 70, 300 nm) on our lung epithelial cells line NCI H441 and endothelial cell line ISO-HAS-1. Additionally, colocalization studies have been conducted via immunofluorescence staining for flotillin-1- and flotillin-2-bearing endocytic vesicles. Subsequently, the relevance of flotillins concerning the viability of aSNP-exposed epithelial cells has been evaluated using flotillin-1/2 depleted cells (siRNA). This study reveals the relevance of the nanoparticle size regarding cytotoxicity (MTS, LDH) and inflammatory responses (IL-8), whereat the smaller the size of the nanoparticle is, the more harmful are the effects. All different aSNP sizes have been incorporated in flotillin-1- and flotillin-2-labelled vesicles in lung epithelial and endothelial cells, which display a marker for late endosomal or lysosomal structures and appear to exhibit a clathrin- or caveolae-independent mode of endocytosis. Flotillin-depleted H441 showed a clearly decreased uptake of aSNPs. Additionally, the viability of aSNP-exposed cells was reduced in these cells. These findings indicate a contribution of flotillins in as yet unknown (clathrin or caveolae-independent) endocytosis mechanisms and (or) endosomal storage.
机译:非晶态二氧化硅纳米粒子(aSNPs)在工业和治疗方面越来越受欢迎。表面积为100–140 m 2 的肺部是治疗方法的理想靶标,但它也代表了有害纳米材料的严重攻击领域。 NPs的细胞毒性作用的确切性质仍然未知。此外,细胞途径和内在的NPs的命运仍然知之甚少。因此,我们检查了肺上皮细胞系NCI H441和内皮细胞系ISO-HAS-1对不同大小的aSNPs(30、70、300 nm)的细胞毒性(MTS,LDH)和炎症反应(IL-8)。另外,通过免疫荧光染色对含弗洛林-1和含弗洛林-2的内吞囊泡进行了共定位研究。随后,已经使用弗洛林素1/2耗竭的细胞(siRNA)评估了弗洛替林与aSNP暴露的上皮细胞的生存能力的相关性。这项研究揭示了纳米颗粒尺寸与细胞毒性(MTS,LDH)和炎性反应(IL-8)的相关性,纳米颗粒尺寸越小,作用越有害。所有不同的aSNP大小已被并入肺上皮和内皮细胞的flotillin-1和flotillin-2标记的囊泡中,这些囊泡显示晚期内体或溶酶体结构的标志物,并表现出与网格蛋白或小窝无关的内吞作用模式。去除了花青素的H441显示aSNP的摄取明显减少。另外,在这些细胞中暴露于aSNP的细胞的活力降低。这些发现表明,花青素在尚不知道的(clathrin或caveolae依赖性)内吞机制和(或)内体贮藏中有贡献。

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