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双层 DNA 脂质体将双层锚定在水凝胶核心上。

Liposomes with double-stranded DNA anchoring the bilayer to a hydrogel core.

机构信息

Mork Family Department of Chemical Engineering and Materials Science, University of Southern California , Los Angeles, California 90089, United States.

出版信息

Biomacromolecules. 2013 Oct 14;14(10):3380-5. doi: 10.1021/bm401155a. Epub 2013 Oct 3.

DOI:10.1021/bm401155a
PMID:24083513
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3874235/
Abstract

Liposomes are important biomolecular nanostructures for handling membrane-associated molecules in the lab and delivering drugs in the clinic. In addition to their biomedical applications, they have been widely used as model cell membranes in biophysical studies. Here we present a liposome-based model membrane that mimics the attachment of membrane-resident molecules to the cytoskeleton. To facilitate this attachment, we have developed a lipid-based hybrid nanostructure in which the liposome bilayer membrane is covalently anchored to a biocompatible poly(ethylene) glycol (PEG) hydrogel core using short double-stranded DNA (dsDNA) linkers. The dsDNA linkers connect cholesterol groups that reside in the bilayer to vinyl groups that are incorporated in the cross-linked hydrogel backbone. Size exclusion chromatography (SEC) of intact and surfactant-treated nanoparticles confirms the formation of anchored hydrogel structures. Transmission electron microscopy (TEM) shows ~100 nm nanoparticles even after removal of unanchored phospholipids. The location of dsDNA groups at the hydrogel-bilayer interface is confirmed with a fluorescence assay. Using DNA as a linker between the bilayer and a hydrogel core allows for temperature-dependent release of the anchoring interaction, produces polymer nanogels with addressible hybridization sites on their surface, and provides a prototype structure for potential future oligonucleotide drug delivery applications.

摘要

脂质体是处理实验室中与膜相关的分子和在临床中输送药物的重要生物分子纳米结构。除了它们在生物医学上的应用,它们还被广泛用作生物物理研究中模型细胞膜。在这里,我们提出了一种基于脂质体的模型膜,模拟了膜驻留分子与细胞骨架的附着。为了促进这种附着,我们开发了一种基于脂质的混合纳米结构,其中脂质体双层膜通过短的双链 DNA (dsDNA) 接头共价锚定在生物相容性的聚乙二醇 (PEG) 水凝胶核心上。dsDNA 接头将双层膜中的胆固醇基团与交联水凝胶骨架中的乙烯基基团连接起来。完整和表面活性剂处理的纳米粒子的尺寸排阻色谱 (SEC) 证实了锚定水凝胶结构的形成。透射电子显微镜 (TEM) 显示,即使去除未锚定的磷脂,也存在约 100nm 的纳米颗粒。荧光测定证实了 dsDNA 基团在水凝胶-双层界面处的位置。使用 DNA 作为双层和水凝胶核心之间的连接物,可以实现锚定相互作用的温度依赖性释放,在其表面产生具有可寻址杂交位点的聚合物纳米凝胶,并为潜在的未来寡核苷酸药物输送应用提供原型结构。

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