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Structure-Activity Relationship of Mono-Ion Complexes for Plasmid DNA Delivery by Muscular Injection

机译:肌肉注射液对质粒DNA递送单离子复合物的结构 - 活性关系

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摘要

The structure-activity relationship of mono-ion complexes (MICs) for plasmid DNA (pDNA) delivery by muscular injection is demonstrated. MICs were formed between pDNA and monocationic poly(ethylene glycol) (PEG) macromolecules. As monocationic PEGs, the ω-amide-pentylimidazolium (APe-Im) end-modified PEGs with a stable amide (Am) and hydrolytic ester (Es) bond, that is, APe-Im-Am-PEG and APe-Im-Es-PEG, respectively, are synthesized. The difference between the APe-Im-Am-PEG and APe-Im-Es-PEG was only a spacer structure between a terminal cation and a PEG chain. The resulting pDNA MICs with APe-Im-Am-PEG at a charge ratio (+/−) of 32 or 64 were more stable than those with APe-Im-Es-PEG in the presence of serum proteins. The highest gene expression by muscular injection was achieved using the APe-Im-Am-PEG/pDNA MIC at a charge ratio (+/−) of 32 with a smaller particle diameter of approximately 50 nm, as compared to that charge ratio of 64. Consequently, the pDNA MIC with the monocationic PEG with a stable amide spacer, as compared to a hydrolytic ester spacer, is considered to be suitable for the highest gene expression by muscular injection.
机译:证明了通过肌肉注射肌肉注射质粒DNA(PDNA)递送的单离子复合物(MIC)的结构 - 活性关系。在PDNA和单子系聚(乙二醇)(PEG)大分子之间形成MIC。作为单分子栓,具有稳定酰胺(AM)和水解酯(ES)键的ω-酰胺 - 戊基咪唑鎓(APE-IM)的末端改性栓,即APE-IM-AM-PEG和APE-IM-ES -peg分别合成。 APE-IM-AM-PEG和APE-IM-ES-PEG之间的差异仅是终端阳离子和PEG链之间的间隔结构。在血清蛋白质存在下,在32或64的电荷比(+/-)的电荷比(+/-)的PDNA MIC与32或64的电荷比(+/-)的稳定性更稳定。与较小粒径为约50nm的电荷比(+/-)的电荷比(+/-),相比,使用较小的粒径为约50nm,实现了肌肉注射的最高基因表达。 。因此,与水解酯间隔物相比,与具有稳定酰胺间隔物的单子系Peg的PDNA MIC被认为是适用于通过肌肉注射的最高基因表达。

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