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Evaluation of Tris2-(Acryloyloxy)EthylIsocyanurate Cross-Linked Polyethylenimine as Antisense Morpholino Oligomer Delivery Vehicle in Cell Culture and Dystrophic mdx Mice

机译:三2-(丙烯酰氧基)乙基异氰脲酸酯交联的聚乙烯亚胺作为反义吗啉代寡聚物递送载体在细胞培养和营养不良mdx小鼠中的评价

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摘要

Hyperbranched poly(ester amine)s (PEAs) based on tris[2-(acryloyloxy)ethyl]isocyanurate (TAEI) cross-linked low-molecular-weight polyethylenimine (Mw: 0.8k/1.2k/2.0k) have been evaluated for delivering antisense phosphorodiamidate morpholino oligomer (PMO) in vitro and in vivo in the dystrophic mdx mouse. The results show that the PEAs constructed with polyethylenimine (PEI) 2.0k (C series) improved PMO delivery more efficiently than those constructed with PEI 0.8k (A series) or 1.2k (B series) in a GFP reporter-based C2C12 mouse myoblast culture system. The highest efficiency of exon-skipping in vitro with the PMO oligonucleotide targeting human dystrophin exon 50 was obtained when the PEA C12 [TAEI-PEI 2.0k (1:2)] was used. Nearly all of the PEAs improved dystrophin expression in mdx mice by local injection with a 2–4-fold increase when compared with PMO alone. Improved transfection efficiency and lower toxicity indicate the potential of the biodegradable PEA polymers as safe and efficient PMO delivery vectors for in vivo applications.
机译:已经评估了基于三[2-(丙烯酰氧基)乙基]异氰脲酸酯(TAEI)交联的低分子量聚乙烯亚胺(Mw:0.8k / 1.2k / 2.0k)的超支化聚(酯胺)(PEA)的在营养不良的mdx小鼠体内和体外递送反义二氨基磷酸二氨基吗啉代寡聚物(PMO)。结果表明,在基于GFP报告基因的C2C12小鼠成肌细胞中,用聚乙烯亚胺(PEI)2.0k(C系列)构建的PEA比用PEI 0.8k(A系列)或1.2k(B系列)构建的PEA更有效地改善了PMO传递。文化体系。当使用PEA C12 [TAEI-PEI 2.0k(1:2)]时,获得了针对人肌营养不良蛋白外显子50的PMO寡核苷酸体外跳跃的最高效率。与单独的PMO相比,几乎所有的PEA都可以通过局部注射改善mdx小鼠中抗肌萎缩蛋白的表达,并增加2至4倍。转染效率的提高和毒性的降低表明可生物降解的PEA聚合物作为安全有效的PMO载体在体内应用的潜力。

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