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温度非依赖性脂质体-细胞膜相互作用在多组分脂质体增效中的作用。

Role of temperature-independent lipoplex-cell membrane interactions in the efficiency boost of multicomponent lipoplexes.

机构信息

Department of Bioscience and Biotechnology, University of Camerino, Italy.

出版信息

Cancer Gene Ther. 2011 Aug;18(8):543-52. doi: 10.1038/cgt.2011.12. Epub 2011 Mar 11.

Abstract

Multicomponent lipoplexes have recently emerged as especially promising transfection candidates, as they are from 10 to 100 times more efficient than binary complexes usually employed for gene delivery purposes. Previously, we investigated a number of chemical-physical properties of DNA-lipid complexes that were proposed to affect transfection efficiency (TE) of lipoplexes, such as nanoscale structure, size, surface potential, DNA-protection ability and DNA release from complexes upon interaction with cellular lipids. Although some minor differences between multicomponent and binary lipoplexes were found, they did not correlate clearly with efficiency. Instead, here we show that a marked difference between the cell internalization mechanism of binary and multicomponent lipoplexes does exist. Multicomponent lipoplexes significantly transfect cells at 4 °C, when endocytosis does not take place suggesting that they can enter cells via a temperature-independent mechanism. Confocal fluorescence microscopy experiments showed the existence of a correlation between endosomal escape and TE. Multicomponent lipoplexes exhibited a distinctive ability of endosomal escape and release DNA into the nucleus, whereas, poorly efficient binary lipoplexes exhibited minor, if any, endosomal rupture ability and remained confined in perinuclear late endosomes. Stopped-flow mixing measurements showed that the fusion rates of multicomponent cationic liposomes with anionic vesicles, used as model systems of cell membranes, were definitely shorter than those of binary liposomes. As either lipoplex uptake and endosomal escape involve fusion between lipoplex and cellular membranes, we suggest that a mechanism of lipoplex-cellular membrane interaction, driven by lipid mixing between cationic and anionic cellular lipids, does explain the TE boost of multicomponent lipoplexes.

摘要

多组分脂质体作为特别有前途的转染候选物,最近已经出现,因为它们的基因传递效率比通常用于基因传递目的的二元复合物高 10 到 100 倍。 以前,我们研究了一些被认为影响脂质体转染效率(TE)的 DNA-脂质复合物的理化性质,例如纳米结构、大小、表面电位、DNA 保护能力以及复合物与细胞脂质相互作用时 DNA 的释放。 尽管在多组分和双组分脂质体之间发现了一些较小的差异,但它们与效率之间没有明显的相关性。 相反,我们在这里表明,双组分和多组分脂质体的细胞内化机制之间确实存在明显的差异。 多组分脂质体在 4°C 时显著转染细胞,此时内吞作用不会发生,这表明它们可以通过与温度无关的机制进入细胞。 共焦荧光显微镜实验表明内体逃逸与 TE 之间存在相关性。 多组分脂质体表现出独特的内体逃逸能力,并将 DNA 释放到细胞核中,而效率较低的双组分脂质体表现出较小的(如果有的话)内体破裂能力,并保留在核周晚期内体中。 停流混合测量表明,作为细胞膜模型体系的阴离子囊泡与阳离子脂质体的融合速率明显短于二元脂质体。 由于无论是脂质体摄取还是内体逃逸都涉及脂质体与细胞膜之间的融合,我们认为脂质体与细胞膜相互作用的机制,由阳离子和阴离子细胞脂质之间的脂质混合驱动,确实可以解释多组分脂质体 TE 提升的原因。

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Transfection efficiency boost by designer multicomponent lipoplexes.设计型多组分脂质体复合物提高转染效率
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