Functional siRNA Delivery by Extracellular Vesicle–Liposome Hybrid Nanoparticles

脂质体 细胞生物学 RNA干扰 微泡 基因传递 细胞 药物输送 生物物理学 小干扰RNA 转染 基因沉默 纳米技术 化学 生物 材料科学 细胞培养 核糖核酸 生物化学 基因 小RNA 遗传学
作者
Martijn J.W. Evers,Simonides Immanuel van de Wakker,Ellis M. de Groot,Olivier G. de Jong,Jerney J. Gitz-Francois,Cor S. Seinen,Joost P. G. Sluijter,Raymond M. Schiffelers,Pieter Vader
出处
期刊:Advanced Healthcare Materials [Wiley]
卷期号:11 (5): e2101202-e2101202 被引量:181
标识
DOI:10.1002/adhm.202101202
摘要

Abstract The therapeutic use of RNA interference is limited by the inability of siRNA molecules to reach their site of action, the cytosol of target cells. Lipid nanoparticles, including liposomes, are commonly employed as siRNA carrier systems to overcome this hurdle, although their widespread use remains limited due to a lack of delivery efficiency. More recently, nature's own carriers of RNA, extracellular vesicles (EVs), are increasingly being considered as alternative siRNA delivery vehicles due to their intrinsic properties. However, they are difficult to load with exogenous cargo. Here, EV–liposome hybrid nanoparticles (hybrids) are prepared and evaluated as an alternative delivery system combining properties of both liposomes and EVs. It is shown that hybrids are spherical particles encapsulating siRNA, contain EV‐surface makers, and functionally deliver siRNA to different cell types. The functional behavior of hybrids, in terms of cellular uptake, toxicity, and gene‐silencing efficacy, is altered as compared to liposomes and varies among recipient cell types. Moreover, hybrids produced with cardiac progenitor cell (CPC) derived‐EVs retain functional properties attributed to CPC‐EVs such as activation of endothelial signaling and migration. To conclude, hybrids combine benefits of both synthetic and biological drug delivery systems and might serve as future therapeutic carriers of siRNA.
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