Induced Self‐Assembly of Vitamin E‐Spermine/siRNA Nanocomplexes via Spermine/Helix Groove‐Specific Interaction for Efficient siRNA Delivery and Antitumor Therapy

Author:

Zhao Xiaoran1,Xu Qi1,Wang Qian1,Liang Xingxing1,Wang Jing1,Jin Hongwei1,Man Yizhi2,Guo Dongyang1,Gao Feng2,Tang Xinjing1ORCID

Affiliation:

1. State Key Laboratory of Natural and Biomimetic Drugs and Chemical Biology Center School of Pharmaceutical Sciences Peking University NO. 38, Xueyuan Rd. Beijing 100191 China

2. School of Chemistry and Materials Science Anhui Normal University NO. 189 Jiuhua South Rd. Anhui, Wuhu 241002 China

Abstract

AbstractGene therapy has been one of potential strategies for the treatment of different diseases, where efficient and safe gene delivery systems are also extremely in need. Current lipid nanoparticles (LNP) technology highly depends on the packing and condensation of nucleic acids with amine moieties. Here, an attempt to covalently link two natural compounds, spermine and vitamin E, is made to develop self‐assembled nucleic acid delivery systems. Among them, the spermine moieties specifically interact with the major groove of siRNA helix through salt bridge interaction, while vitamin E moieties are located around siRNA duplex. Such amphiphilic vitamin E‐spermine/siRNA complexes can further self‐assemble into nanocomplexes like multiblade wheels. Further studies indicate that these siRNA nanocomplexes with the neutrally charged surface of vitamin E can enter cells via caveolin/lipid raft mediated endocytosis pathway and bypass lysosome trapping. With these self‐assembled delivery systems, efficient siRNA delivery is successfully achieved for Eg5 and Survivin gene silencing as well as DNA plasmid delivery. Further in vivo study indicates that VE‐Su‐Sper/DSPE‐PEG2000/siSurvivin self‐assembled nanocomplexes can accumulate in cancer cells and gradually release siRNA in tumor tissues and show significant antitumor effect in vivo. The self‐assembled delivery system provides a novel strategy for highly efficient siRNA delivery.

Funder

National Natural Science Foundation of China

National Key Research and Development Program of China

Publisher

Wiley

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