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Peptide-Mediated Lipofection Is Governed by Lipoplex Physical Properties and the Density of Surface-Displayed Amines

机译:肽介导的脂质转染受脂质复合物的物理性质和表面展示的胺的密度控制

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摘要

Peptides can potentiate lipid-mediated gene delivery by modifying lipoplex physiochemical properties to overcome rate-limiting steps to gene transfer. The objectives of this study were to determine the regimes over which cationic peptides enhance lipofection and to investigate the mechanism of action, such as increased cellular association resulting from changes in lipoplex physical properties. Short, cationic peptides were incorporated into lipoplexes by mixing peptide, lipid and DNA. Lipoplexes were characterized using gel retardation, dynamic light scattering, and fluorescent microscopy, and the amount of surface-displayed amines was quantified by fluorescamine. Size, zeta potential, and surface amines for lipoplexes were dependent on peptide/DNA ratio. Inclusion of peptides in lipoplexes resulted in up to a 13-fold increase in percentage of cells transfected, and up to a 76-fold increase in protein expression. This transfection enhancement corresponded to a small particle diameter and positive zeta potential of lipoplexes, as well as increased amount of surface-displayed amines. Relative to lipid alone, these properties of the peptide-modified lipoplexes enhanced cellular association, which has been reported as a rate-limiting step for transfection with lipoplexes. The addition of peptides is a simple method of lipofection enhancement, as direct chemical modification of lipids is not necessary for increased transfection.
机译:肽可以通过修饰lipoplex的理化特性来增强脂质介导的基因传递,从而克服基因转移的限速步骤。这项研究的目的是确定阳离子肽增强脂转染的机制,并研究其作用机制,例如因脂质复合物物理性质的改变而导致细胞缔合增加。通过混合肽,脂质和DNA将短的阳离子肽掺入脂质复合物中。使用凝胶阻滞,动态光散射和荧光显微镜对脂质体进行表征,并通过荧光胺对表面展示的胺进行定量。脂质复合物的大小,ζ电位和表面胺取决于肽/ DNA比率。脂质复合物中包含肽导致转染细胞百分比最多增加13倍,蛋白质表达最多增加76倍。这种转染增强对应于脂质复合物的小粒径和正ζ电势,以及表面展示的胺的增加量。相对于单独的脂质,肽修饰的脂质复合物的这些特性增强了细胞结合,据报道这是用脂质复合物转染的限速步骤。肽的添加是增强脂质转染的简单方法,因为脂质的直接化学修饰对于增加转染不是必需的。

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