The transition from linear to highly branched poly(β-amino ester)s: Branching matters for gene delivery

支化(高分子化学) 转染 脂质体 基因传递 体内 体外 单体 氨基酸 基因 化学 载体(分子生物学) 计算生物学 聚合物 生物 生物化学 遗传学 有机化学 重组DNA 遗传增强
作者
Dezhong Zhou,Lara Cutlar,Yongsheng Gao,Wei Wang,Jonathan O’Keeffe Ahern,Seán McMahon,Blanca Duarte,Fernando Larcher,Brian J. Rodriguez,Udo Greiser,Wenxin Wang,Wenxin Wang,Wenxin Wang
出处
期刊:Science Advances [American Association for the Advancement of Science]
卷期号:2 (6): e1600102-e1600102 被引量:216
标识
DOI:10.1126/sciadv.1600102
摘要

Nonviral gene therapy holds great promise but has not delivered treatments for clinical application to date. Lack of safe and efficient gene delivery vectors is the major hurdle. Among nonviral gene delivery vectors, poly(β-amino ester)s are one of the most versatile candidates because of their wide monomer availability, high polymer flexibility, and superior gene transfection performance both in vitro and in vivo. However, to date, all research has been focused on vectors with a linear structure. A well-accepted view is that dendritic or branched polymers have greater potential as gene delivery vectors because of their three-dimensional structure and multiple terminal groups. Nevertheless, to date, the synthesis of dendritic or branched polymers has been proven to be a well-known challenge. We report the design and synthesis of highly branched poly(β-amino ester)s (HPAEs) via a one-pot "A2 + B3 + C2"-type Michael addition approach and evaluate their potential as gene delivery vectors. We find that the branched structure can significantly enhance the transfection efficiency of poly(β-amino ester)s: Up to an 8521-fold enhancement in transfection efficiency was observed across 12 cell types ranging from cell lines, primary cells, to stem cells, over their corresponding linear poly(β-amino ester)s (LPAEs) and the commercial transfection reagents polyethyleneimine, SuperFect, and Lipofectamine 2000. Moreover, we further demonstrate that HPAEs can correct genetic defects in vivo using a recessive dystrophic epidermolysis bullosa graft mouse model. Our findings prove that the A2 + B3 + C2 approach is highly generalizable and flexible for the design and synthesis of HPAEs, which cannot be achieved by the conventional polymerization approach; HPAEs are more efficient vectors in gene transfection than the corresponding LPAEs. This provides valuable insight into the development and applications of nonviral gene delivery and demonstrates great prospect for their translation to a clinical environment.
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