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Skeleton-Controlled pDNA Delivery of Renewable Steroid-Based Cationic Lipids the Endocytosis Pathway Analysis and Intracellular Localization

机译:骨架控制的可再生类固醇基阳离子脂质的pDNA传递内吞途径分析和细胞内定位。

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摘要

Using renewable and biocompatible natural-based resources to construct functional biomaterials has attracted great attention in recent years. In this work, we successfully prepared a series of steroid-based cationic lipids by integrating various steroid skeletons/hydrophobes with (l-)-arginine headgroups via facile and efficient synthetic approach. The plasmid DNA (pDNA) binding affinity of the steroid-based cationic lipids, average particle sizes, surface potentials, morphologies and stability of the steroid-based cationic lipids/pDNA lipoplexes were disclosed to depend largely on the steroid skeletons. Cellular evaluation results revealed that cytotoxicity and gene transfection efficiency of the steroid-based cationic lipids in H1299 and HeLa cells strongly relied on the steroid hydrophobes. Interestingly, the steroid lipids/pDNA lipoplexes inclined to enter H1299 cells mainly through caveolae and lipid-raft mediated endocytosis pathways, and an intracellular trafficking route of “lipid-raft-mediated endocytosis→lysosome→cell nucleic localization” was accordingly proposed. The study provided possible approach for developing high-performance steroid-based lipid gene carriers, in which the cytotoxicity, gene transfection capability, endocytosis pathways, and intracellular trafficking/localization manners could be tuned/controlled by introducing proper steroid skeletons/hydrophobes. Noteworthy, among the lipids, Cho-Arg showed remarkably high gene transfection efficacy, even under high serum concentration (50% fetal bovine serum), making it an efficient gene transfection agent for practical application.
机译:近年来,使用可再生和生物相容性的天然资源来构建功能性生物材料引起了极大的关注。在这项工作中,我们通过简便有效的合成方法,将各种类固醇骨架/疏水物与(1-)-精氨酸头基相结合,成功制备了一系列基于类固醇的阳离子脂质。公开了基于类固醇的阳离子脂质的质粒DNA(pDNA)结合亲和力,基于类固醇的阳离子脂质/ pDNA脂质复合物的平均粒径,表面电势,形态和稳定性在很大程度上取决于类固醇骨架。细胞评估结果显示,H1299和HeLa细胞中基于类固醇的阳离子脂质的细胞毒性和基因转染效率强烈依赖于类固醇疏水物。有趣的是,类固醇脂质/ pDNA脂质复合体倾向于主要通过小窝和脂筏介导的内吞途径进入H1299细胞,因此提出了“脂筏介导的内吞→溶酶体→细胞核酸定位”的细胞内运输途径。该研究为开发高性能基于类固醇的脂质基因载体提供了可能的方法,其中可以通过引入适当的类固醇骨架/疏水物来调节/控制细胞毒性,基因转染能力,内吞途径和细胞内运输/定位方式。值得注意的是,在脂质中,即使在高血清浓度(50%胎牛血清)下,Cho-Arg仍具有很高的基因转染效率,使其成为实用的有效基因转染剂。

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