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聚山梨醇酯85接枝的聚乙烯亚胺在体外和肌营养不良mdx小鼠体内增强了反义2'-O-甲基硫代磷酸酯寡核苷酸的递送。

Tween 85 grafted PEIs enhanced delivery of antisense 2'-O-methyl phosphorothioate oligonucleotides in vitro and in dystrophic mdx mice.

作者信息

Wang Mingxing, Wu Bo, Tucker Jason D, Lu Peijuan, Bollinger Lauren E, Lu Qilong

机构信息

Department of Neurology, McColl-Lockwood Laboratory for Muscular Dystrophy Research, Cannon Research Center, Carolinas Medical Center, 1000 Blythe Blvd, Charlotte, NC 28231, USA.

出版信息

J Mater Chem B. 2015 Jul 14;3(26):5330-5340. doi: 10.1039/c5tb00139k. Epub 2015 Jun 10.

DOI:10.1039/c5tb00139k
PMID:32262609
Abstract

A series of cationic amphiphlic copolymers (Z series) constructed from Tween 85 and low molecular weight (M) polyethyleneimine (LPEI) have been evaluated for the delivery of antisense 2'-O-methyl phosphorothioate RNA (2'-OMePS) in both cell culture and dystrophic mdx mice. All Z copolymers improved the 2'-OMePS-induced dystrophin expression both in vitro and in vivo compared with PEI 25k formulated or 2'-OMePS alone. The most effective polymers are in the order of Z9 > Z3 > Z7, Z1, Z2, Z6 > others by formulation at the dose of 20 μg mL in myoblast cell culture. Significantly enhanced exon-skipping of 2'-OMePS with Z polymers in mdx mice was obtained in the order of Z7 > Z9, Z3 > Z8, Z6 > others. The highest efficiency of targeted exon-skipping with Z7 [T85-PEI 2k (1 : 1)] reached over 8 fold compared with 2'-OMePS alone in mdx mice. Further analyses of the structure and function indicate that the more hydrophobicity and lower PEI content of the polymer microstructure are, the greater are the delivery efficiency and exon-skipping. The unique hydrophobic interactions between the Z polymers and 2'-OMePS likely create more stable complexes in primarily hydrophilic environments both in vitro and in vivo. The overall results suggested that Tween 85 modified LPEIs provide a promising delivery approach for applications of 2'-OMePS oligonucleotides as therapeutic reagents.

摘要

一系列由吐温85和低分子量(M)聚乙烯亚胺(LPEI)构建的阳离子两亲性共聚物(Z系列)已在细胞培养和营养不良性mdx小鼠中评估了其用于递送反义2'-O-甲基硫代磷酸酯RNA(2'-OMePS)的能力。与单独配制的25k聚醚酰亚胺或单独使用2'-OMePS相比,所有Z共聚物在体外和体内均提高了2'-OMePS诱导的抗肌萎缩蛋白表达。在成肌细胞培养中,以20μg/mL的剂量配制时,最有效的聚合物顺序为Z9>Z3>Z7、Z1、Z2、Z6>其他。在mdx小鼠中,Z聚合物显著增强了2'-OMePS的外显子跳跃,顺序为Z7>Z9、Z3>Z8、Z6>其他。与mdx小鼠中单独使用2'-OMePS相比,Z7 [吐温85-PEI 2k(1:1)]的靶向外显子跳跃最高效率达到了8倍以上。对结构和功能的进一步分析表明,聚合物微观结构的疏水性越强且PEI含量越低,递送效率和外显子跳跃就越大。Z聚合物与2'-OMePS之间独特的疏水相互作用可能在体外和体内的主要亲水环境中形成更稳定的复合物。总体结果表明,吐温85修饰的LPEIs为将2'-OMePS寡核苷酸用作治疗试剂提供了一种有前景的递送方法。

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引用本文的文献

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