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氧化还原响应性 DTSSP 交联对聚(赖氨酸)接枝聚(乙二醇)纳米粒子递送蛋白质的影响。

Effect of redox-responsive DTSSP crosslinking on poly(l-lysine)-grafted-poly(ethylene glycol) nanoparticles for delivery of proteins.

机构信息

School of Chemical Engineering, Oklahoma State University, Stillwater, Oklahoma.

出版信息

Biotechnol Bioeng. 2020 Aug;117(8):2504-2515. doi: 10.1002/bit.27369. Epub 2020 Jun 8.

DOI:10.1002/bit.27369
PMID:32364622
Abstract

Therapeutic proteins are utilized in a variety of clinical applications, but side effects and rapid in vivo clearance still present hurdles. An approach that addresses both drawbacks is protein encapsulation within in a polymeric nanoparticle, which is effective but introduces the additional challenge of destabilizing the nanoparticle shell in clinically relevant locations. This study examined the effects of crosslinking self-assembled poly(l-lysine)-grafted-poly(ethylene glycol) nanoparticles with redox-responsive 3,3'-dithiobis(sulfosuccinimidyl propionate) (DTSSP) to achieve nanoparticle destabilization in a reductive environment. The polymer-protein nanoparticles (DTSSP NPs) were formed through electrostatic self-assembly and crosslinked with DTSSP, which contains a glutathione-reducible disulfide. As glutathione is upregulated in various cancers, DTSSP NPs could display destabilization within cancer cells. A library of DTSSP NPs was formed with varying copolymer to protein (C:P) and crosslinker to protein (X:P) mass ratios and characterized by size and encapsulation efficiency. DTSSP NPs with a 7:1 C:P ratio and 2:1 X:P ratio were further characterized by stability in the presence proteases and reducing agents. DTSSP NPs fully encapsulated the model protein and displayed 81% protein release when incubated with 5 mM dithiothreitol for 12 hr. This study contributes to understanding stimulus-responsive crosslinking of polymeric nanoparticles and could be foundational to clinical administration of therapeutic proteins.

摘要

治疗性蛋白被广泛应用于各种临床应用中,但副作用和体内快速清除仍然存在障碍。一种解决这两个问题的方法是将蛋白封装在聚合物纳米粒子中,这种方法虽然有效,但引入了在临床相关部位使纳米粒子外壳不稳定的额外挑战。本研究考察了通过氧化还原响应性 3,3'-二硫代双(磺基琥珀酰亚胺基丙酸酯)(DTSSP)交联自组装聚(L-赖氨酸)-接枝聚(乙二醇)纳米粒子以实现还原环境下纳米粒子失稳的效果。聚合物-蛋白纳米粒子(DTSSP NPs)通过静电自组装形成,并通过含有谷胱甘肽还原型二硫键的 DTSSP 交联。由于谷胱甘肽在各种癌症中上调,DTSSP NPs 可以在癌细胞内显示失稳。通过改变共聚物与蛋白(C:P)和交联剂与蛋白(X:P)的质量比形成了一系列 DTSSP NPs,并通过粒径和包封效率进行了表征。具有 7:1 C:P 比和 2:1 X:P 比的 DTSSP NPs 进一步通过在存在蛋白酶和还原剂时的稳定性进行了表征。DTSSP NPs 完全封装了模型蛋白,并在孵育 5 mM 二硫苏糖醇 12 小时后释放了 81%的蛋白。本研究有助于理解聚合物纳米粒子的刺激响应性交联,并可能为治疗性蛋白的临床应用奠定基础。

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