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用于细胞内蛋白质递送的基于多酚的纳米颗粒 竞争性超分子相互作用

Polyphenol-Based Nanoparticles for Intracellular Protein Delivery Competing Supramolecular Interactions.

作者信息

Han Yiyuan, Zhou Jiajing, Hu Yingjie, Lin Zhixing, Ma Yutian, Richardson Joseph J, Caruso Frank

机构信息

ARC Centre of Excellence in Convergent Bio-Nano Science and Technology, and the Department of Chemical Engineering, The University of Melbourne, Parkville, Victoria 3010, Australia.

出版信息

ACS Nano. 2020 Oct 27;14(10):12972-12981. doi: 10.1021/acsnano.0c04197. Epub 2020 Sep 30.

Abstract

Intracellular delivery of proteins is a promising strategy for regulating cellular behavior and therefore has attracted interest for biomedical applications. Despite the emergence of various nanoparticle-based intracellular delivery approaches, it remains challenging to engineer a versatile delivery system capable of responding to various physiological triggers without the need for complex chemical synthesis of the delivery system. Herein, we develop a template-mediated supramolecular assembly strategy to synthesize protein-polyphenol nanoparticles (NPs) capable of endosomal escape and subsequent protein release in the cytosol. These NPs are stable in serum and undergo surface charge reversal from negative to positive in acidic environments, leading to spontaneous endosomal escape. In the cytosol, endogenous small peptides and amino acids with relatively high charge densities, such as glutathione, trigger NP disassembly through competitive supramolecular interactions, thereby releasing functional bioactive proteins, as validated using cytochrome C and β-galactosidase. The versatility of the present strategy in terms of nanoparticle size, protein type, and functional protein delivery makes this a promising platform for potential application in the field of protein therapeutics.

摘要

蛋白质的细胞内递送是一种调节细胞行为的有前景的策略,因此在生物医学应用中引起了人们的兴趣。尽管出现了各种基于纳米颗粒的细胞内递送方法,但设计一种能够响应各种生理触发因素而无需对递送系统进行复杂化学合成的通用递送系统仍然具有挑战性。在此,我们开发了一种模板介导的超分子组装策略,以合成能够实现内体逃逸并随后在细胞质中释放蛋白质的蛋白质 - 多酚纳米颗粒(NPs)。这些NPs在血清中稳定,并且在酸性环境中经历表面电荷从负到正的反转,从而导致自发的内体逃逸。在细胞质中,具有相对高电荷密度的内源性小肽和氨基酸,如谷胱甘肽,通过竞争性超分子相互作用触发NP解体,从而释放功能性生物活性蛋白质,这已通过细胞色素C和β - 半乳糖苷酶得到验证。本策略在纳米颗粒大小、蛋白质类型和功能性蛋白质递送方面的通用性使其成为蛋白质治疗领域潜在应用的有前景的平台。

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