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大小分离的亲脂性硅纳米粒子的增强细胞摄取。

Enhanced cellular uptake of size-separated lipophilic silicon nanoparticles.

机构信息

Department of Biological Science, Florida State University, Tallahassee, Florida, USA.

Department of Chemistry, University of Toronto, Toronto, Canada.

出版信息

Sci Rep. 2017 Mar 8;7:43731. doi: 10.1038/srep43731.

Abstract

Specific size, shape and surface chemistry influence the biological activity of nanoparticles. In the case of lipophilic nanoparticles, which are widely used in consumer products, there is evidence that particle size and formulation influences skin permeability and that lipophilic particles smaller than 6 nm can embed in lipid bilayers. Since most nanoparticle synthetic procedures result in mixtures of different particles, post-synthetic purification promises to provide insights into nanostructure-function relationships. Here we used size-selective precipitation to separate lipophilic allyl-benzyl-capped silicon nanoparticles into monodisperse fractions within the range of 1 nm to 5 nm. We measured liposomal encapsulation and cellular uptake of the monodisperse particles and found them to have generally low cytotoxicities in Hela cells. However, specific fractions showed reproducibly higher cytotoxicity than other fractions as well as the unseparated ensemble. Measurements indicate that the cytotoxicity mechanism involves oxidative stress and the differential cytotoxicity is due to enhanced cellular uptake by specific fractions. The results indicate that specific particles, with enhanced suitability for incorporation into lipophilic regions of liposomes and subsequent in vitro delivery to cells, are enriched in certain fractions.

摘要

特定的尺寸、形状和表面化学性质会影响纳米粒子的生物活性。在亲脂性纳米粒子的情况下,广泛应用于消费产品,有证据表明,粒径和配方会影响皮肤通透性,并且小于 6nm 的亲脂性粒子可以嵌入脂质双层。由于大多数纳米粒子的合成过程会产生不同粒子的混合物,因此合成后的纯化有望提供关于纳米结构-功能关系的深入了解。在这里,我们使用尺寸选择性沉淀将亲脂性烯丙基-苄基封端的硅纳米粒子分离成 1nm 至 5nm 范围内的单分散颗粒。我们测量了单分散颗粒的脂质体包封和细胞摄取,发现它们在 Hela 细胞中通常具有较低的细胞毒性。然而,特定的颗粒比其他颗粒以及未分离的混合物表现出可重复的更高的细胞毒性。测量结果表明,细胞毒性机制涉及氧化应激,并且不同的细胞毒性是由于特定颗粒的增强的细胞摄取所致。结果表明,具有更好的适用于脂质体亲脂区域的整合和随后的体外细胞递药的特定颗粒在某些颗粒中富集。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2453/5341124/f401ac3a30e3/srep43731-f1.jpg

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