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30nm 大小的稳定单分子核酸脂质颗粒的自组装。

Self-assembly of stable monomolecular nucleic acid lipid particles with a size of 30 nm.

机构信息

Ludwig-Maximilians-University, Geschwister-Scholl-Platz 1, D-80539 Munich, Germany.

出版信息

J Am Chem Soc. 2012 Jul 18;134(28):11652-8. doi: 10.1021/ja302930b. Epub 2012 Jul 3.

DOI:10.1021/ja302930b
PMID:22694262
Abstract

The design of efficient nucleic acid complexes is key to progress in genetic research and therapies based on RNA interference. For optimal transport within tissue and across extracellular barriers, nucleic acid carriers need to be small and stable. In this Article, we prepare and characterize mono-nucleic acid lipid particles (mono-NALPs). The particles consist of single short double-stranded oligonucleotides or single siRNA molecules each encapsulated within a closed shell of a cationic-zwitterionic lipid bilayer, furnished with an outer polyethylene glycol (PEG) shield. The particles self-assemble by solvent exchange from a solution containing nucleic acid mixed with the four lipid components DOTAP, DOPE, DOPC, and DSPE-PEG(2000). Using fluorescence correlation spectroscopy, we monitor the formation of mono-NALPs from short double-stranded oligonucleotides or siRNA and lipids into monodisperse particles of approximately 30 nm in diameter. Small angle neutron and X-ray scattering and transmission electron microscopy experiments substantiate a micelle-like core-shell structure of the particles. The PEGylated lipid shell protects the nucleic acid core against degradation by nucleases, sterically stabilizes the mono-NALPs against disassembly in collagen networks, and prevents nonspecific binding to cells. Hence, PEG-lipid shielded mono-NALPs are the smallest stable siRNA lipid system possible and may provide a structural design to be built upon for the development of novel nucleic acid delivery systems with enhanced biodistribution in vivo.

摘要

高效核酸复合物的设计是基于 RNA 干扰的遗传研究和治疗进展的关键。为了在组织内和细胞外屏障中进行最佳运输,核酸载体需要小而稳定。在本文中,我们制备并表征了单核酸脂质颗粒(mono-NALPs)。这些颗粒由单个短双链寡核苷酸或单个 siRNA 分子组成,每个分子都被封闭在阳离子-两性离子脂质双层的壳内,并带有外层聚乙二醇(PEG)屏蔽。颗粒通过溶剂交换自含有核酸与四种脂质成分 DOTAP、DOPE、DOPC 和 DSPE-PEG(2000)混合的溶液中自组装而成。使用荧光相关光谱法,我们监测了短双链寡核苷酸或 siRNA 和脂质形成单分散约 30nm 直径的 mono-NALPs 的过程。小角中子和 X 射线散射以及透射电子显微镜实验证实了颗粒具有类似胶束的核壳结构。PEG 化脂质壳可保护核酸核心免受核酸酶的降解,在胶原网络中稳定 mono-NALPs 以防解体,并防止与细胞的非特异性结合。因此,PEG 脂质屏蔽的 mono-NALPs 是可能的最小稳定的 siRNA 脂质系统,可为新型核酸递系统的开发提供结构设计,以增强体内的生物分布。

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