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Nanocarriers for Protein Delivery to the Cytosol: Assessing the Endosomal Escape of Poly(Lactide-co-Glycolide)-Poly(Ethylene Imine) Nanoparticles

机译:纳米载体的蛋白质传递到胞质溶胶:评估聚(丙交酯-共-乙醇酸内酯)-聚(亚乙基亚胺)纳米粒子的内体逸出。

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摘要

Therapeutic proteins and enzymes are a group of interesting candidates for the treatment of numerous diseases, but they often require a carrier to avoid degradation and rapid clearance in vivo. To this end, organic nanoparticles (NPs) represent an excellent choice due to their biocompatibility, and cross-linked enzyme aggregates (CLEAs)-loaded poly (lactide-co-glycolide) (PLGA) NPs have recently attracted attention as versatile tools for targeted enzyme delivery. However, PLGA NPs are taken up by cells via endocytosis and are typically trafficked into lysosomes, while many therapeutic proteins and enzymes should reach the cellular cytosol to perform their activity. Here, we designed a CLEAs-based system implemented with a cationic endosomal escape agent (poly(ethylene imine), PEI) to extend the use of CLEA NPs also to cytosolic enzymes. We demonstrated that our system can deliver protein payloads at cytoplasm level by two different mechanisms: Endosomal escape and direct translocation. Finally, we applied this system to the cytoplasmic delivery of a therapeutically relevant enzyme (superoxide dismutase, SOD) in vitro.
机译:治疗性蛋白质和酶是用于治疗多种疾病的一组有趣的候选物,但它们通常需要载体以避免体内降解和快速清除。为此,有机纳米颗粒(NPs)由于其生物相容性而成为极佳的选择,而负载交联酶聚集体(CLEAs)的聚(丙交酯-乙交酯)(PLGA)NPs作为用于靶向的多功能工具已引起关注。酶传递。然而,PLGA NP被细胞通过内吞作用吸收,通常被运输到溶酶体中,而许多治疗性蛋白质和酶应到达细胞质以发挥其活性。在这里,我们设计了一种基于CLEAs的系统,该系统使用阳离子内体逃逸剂(聚(乙烯亚胺),PEI)实施,以将CLEA NP的用途也扩展至胞质酶。我们证明了我们的系统可以通过两种不同的机制在细胞质水平上递送蛋白质负载:内体逃逸和直接易位。最后,我们将此系统应用于体外治疗相关酶(超氧化物歧化酶,SOD)的细胞质传递。

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