首页> 外文期刊>Journal of Materials Chemistry, B. materials for biology and medicine >PEGylated poly(amine-co-ester) micelles as biodegradable non-viral gene vectors with enhanced stability, reduced toxicity and higher in vivo transfection efficacy
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PEGylated poly(amine-co-ester) micelles as biodegradable non-viral gene vectors with enhanced stability, reduced toxicity and higher in vivo transfection efficacy

机译:聚乙二醇化聚(胺-共-酯)胶束作为可生物降解的非病毒基因载体,具有增强的稳定性,降低的毒性和更高的体内转染功效

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摘要

Nanosized micelles based on cationic, amphiphilic poly(ethytene glycol)-poly(ω-pentadecalactone-co-N-methyldiethyleneamine-co-sebacate) (PEG-PPMS) block copolymers have been successfully developed to serve as a new type of biodegradable non-viral vectors for DNA delivery. PEG-PPMS copolymers with various compositions were synthesized in one step via lipase-catalyzed copolymerization of ω-pentadecalactone (PDL), N-methyldiethanolamine (MDEA) and diethyl sebacate (DES) with poly(ethylene glycol) methyl ether (MeO-PEG-OH). The effects of PEG molecular weight, PEG and PDL contents on the biological properties (including the gene transfection efficiency) of the copolymer micelles were investigated. The LucDNA-loaded micelles formed from the copolymers with 30-50 wt% PEG showed high stability in serum-containing aqueous medium, which is in sharp contrast to rapid aggregation of LucDNA/PPMS polyplex particles. The conjugation of PEG to PPMS chains significantly reduces the cytotoxicity and hemolysis activity of the PEG-PPMS micelles. Compared to PEG-free PPMS, the micelles of PEG-PPMS copolymers with optimal compositions (e.g., 42%PEG5K-PPMS-10%PDL and 42%PEG5K-PPMS-20%PDL) exhibited enhanced capability to condense and protect DNA. Although the optimized micelles showed comparable or slightly lower gene transfection efficacy than the reference PPMS in vitro, the efficiency of LucDNA/42%PEG5K-PPMS-20%PDL micelles in transfecting tumor cells in mice was twice as high as that of LucDNA/PPMS polyplex particles due to their strong DNA condensation ability and excellent stability under physiological conditions. The PEG-PPMS micelle system with improved properties is a family of potentially promising non-viral vectors for in vivo delivery of therapeutic genes to treat tumors.
机译:已成功开发了基于阳离子,两亲性聚(乙撑二醇)-聚(ω-十五烯内酯-共-N-甲基二亚乙基胺-癸二酸酯)(PEG-PPMS)嵌段共聚物的纳米胶束,可作为一种新型的可生物降解的非DNA传递的病毒载体。通过脂肪酶催化ω-十五烯内酯(PDL),N-甲基二乙醇胺(MDEA)和癸二酸二乙酯(DES)与聚(乙二醇)甲醚(MeO-PEG-哦)。研究了PEG分子量,PEG和PDL含量对共聚物胶束生物学特性(包括基因转染效率)的影响。由具有30-50 wt%PEG的共聚物形成的装载LucDNA的胶束在含血清的水性介质中显示出高稳定性,这与LucDNA / PPMS复合颗粒的快速聚集形成鲜明对比。 PEG与PPMS链的缀合显着降低了PEG-PPMS胶束的细胞毒性和溶血活性。与不含PEG的PPMS相比,具有最佳组成(例如42%PEG5K-PPMS-10%PDL和42%PEG5K-PPMS-20%PDL)的PEG-PPMS共聚物的胶束具有增强的缩合和保护DNA的能力。尽管优化的胶束在体外显示出与参考PPMS相当或略低的基因转染效率,但LucDNA / 42%PEG5K-PPMS-20%PDL胶束在转染小鼠肿瘤细胞中的效率是LucDNA / PPMS的两倍Polyplex颗粒具有强大的DNA凝聚能力和在生理条件下极好的稳定性。具有改进特性的PEG-PPMS胶束系统是一类潜在的有前途的非病毒载体,用于体内递送治疗性基因来治疗肿瘤。

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