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Therapeutic efficiency of folated poly(ethylene glycol)-chitosan-graft-polyethylenimine-Pdcd4 complexes in H-ras12V mice with liver cancer.叶酸化聚乙二醇-壳聚糖接枝-聚乙烯亚胺-Pdcd4 复合物在肝癌 H-ras12V 小鼠中的治疗效果。
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聚合物-肽递送平台:寡肽取向对基于聚合物的DNA递送的影响。

Polymer-peptide delivery platforms: effect of oligopeptide orientation on polymer-based DNA delivery.

作者信息

Parelkar Sangram S, Letteri Rachel, Chan-Seng Delphine, Zolochevska Olga, Ellis Jayne, Figueiredo Marxa, Emrick Todd

机构信息

Polymer Science and Engineering Department, University of Massachusetts , 120 Governors Drive, Amherst, Massachusetts 01003, United States.

出版信息

Biomacromolecules. 2014 Apr 14;15(4):1328-36. doi: 10.1021/bm401878p. Epub 2014 Mar 7.

DOI:10.1021/bm401878p
PMID:24606402
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4084789/
Abstract

The success of nonviral transfection using polymers hinges on efficient nuclear uptake of nucleic acid cargo and overcoming intra- and extracellular barriers. By incorporating PKKKRKV heptapeptide pendent groups as nuclear localization signals (NLS) on a polymer backbone, we demonstrate protein expression levels higher than those obtained from JetPEI and Lipofectamine 2000, the latter being notorious for coupling high transfection efficiency with cytotoxicity. The orientation of the NLS peptide grafts markedly affected transfection performance. Polymers with the sequence attached to the backbone from the valine residue achieved a level of nuclear translocation higher than the levels of those having the NLS groups attached in the opposite orientation. The differences in nuclear localization and DNA complexation strength between the two orientations correlated with a striking difference in protein expression, both in cell culture and in vivo. Polyplexes formed from these comb polymer structures exhibited transfection efficiencies superior to those of Lipofectamine 2000 but with greatly reduced toxicity. Moreover, these novel polymers, when administered by intramuscular ultrasound-mediated delivery, allowed a high level of reporter gene expression in mice, demonstrating their therapeutic promise in vivo.

摘要

使用聚合物进行非病毒转染的成功取决于核酸货物的有效核摄取以及克服细胞内和细胞外障碍。通过在聚合物主链上引入PKKKRKV七肽侧链基团作为核定位信号(NLS),我们证明了其蛋白质表达水平高于从JetPEI和Lipofectamine 2000获得的水平,后者因高转染效率与细胞毒性相关而声名狼藉。NLS肽接枝的方向显著影响转染性能。从缬氨酸残基连接到主链上的序列的聚合物实现了比以相反方向连接NLS基团的聚合物更高水平的核转位。两种方向之间核定位和DNA络合强度的差异与细胞培养和体内蛋白质表达的显著差异相关。由这些梳状聚合物结构形成的多聚体表现出优于Lipofectamine 2000的转染效率,但毒性大大降低。此外,这些新型聚合物通过肌肉内超声介导递送时,在小鼠中允许高水平的报告基因表达,证明了它们在体内的治疗前景。