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首页> 外文期刊>Journal of Medicinal Chemistry >Design of Ionizable Lipids To Overcome the Limiting Step of Endosomal Escape: Application in the Intracellular Delivery of mRNA, DNA, and siRNA
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Design of Ionizable Lipids To Overcome the Limiting Step of Endosomal Escape: Application in the Intracellular Delivery of mRNA, DNA, and siRNA

机译:克服脂质体内逃逸限制步骤的可离子化脂质的设计:在mRNA,DNA和siRNA的细胞内递送中的应用

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摘要

The intracellular delivery of nucleic acid molecules is a complex process involving several distinct steps; among these the endosomal escape appeared to be of particular importance for an efficient protein production (or inhibition) into host cells. In the present study, a new series of ionizable vectors, derived from naturally occurring aminoglycoside tobramycin, was prepared using improved synthetic procedures that allow structural variations on the linker and hydrophobic domain levels. Complexes formed between the new ionizable lipids and mRNA, DNA, or siRNA were characterized by cryo-TEM experiments and their transfection potency was evaluated using different cell types. We demonstrated that lead molecule 30, bearing a biodegradable diester linker, formed small complexes with nucleic acids and provided very high transfection efficiency with all nucleic acids and cell types tested. The obtained results suggested that the improved and "universal" delivery properties of 30 resulted from an optimized endosomal escape, through the lipid-mixing mechanism.
机译:核酸分子的细胞内递送是一个复杂的过程,涉及几个不同的步骤。其中,对于有效地向宿主细胞中产生蛋白质(或抑制),内体逃逸似乎特别重要。在本研究中,使用改良的合成程序制备了一系列新的可离子化的载体,这些载体均来自天然存在的氨基糖苷妥布霉素,可在接头和疏水域上进行结构变化。新的可电离脂质与mRNA,DNA或siRNA之间形成的复合物通过冷冻TEM实验进行表征,并使用不同的细胞类型评估其转染能力。我们证明了带有可生物降解的二酯接头的铅分子30与核酸形成了小的复合物,并且对所有测试的核酸和细胞类型均具有非常高的转染效率。获得的结果表明,通过脂质混合机制,优化的内体逃逸导致了30的改善和“通用”递送特性。

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