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Reprogramming Extracellular Vesicles for Protein Therapeutics Delivery

机译:用于蛋白质治疗递送的重新编程细胞外囊

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摘要

Delivering protein therapeutics specifically into target cells and tissues is a promising avenue in medicine. Advancing this process will significantly enhance the efficiency of the designed drugs. In this regard, natural membrane-based systems are of particular interest. Extracellular vesicles (EVs), being the bilayer lipid particles secreted by almost all types of cells, have several principal advantages: biocompatibility, carrier stability, and blood–brain barrier penetrability, which make them a perspective tool for protein therapeutic delivery. Here, we evaluate the engineered genetically encoded EVs produced by a human cell line, which allow efficient cargo loading. In the devised system, the protein of interest is captured by self-assembling structures, i.e., “enveloped protein nanocages” (EPN). In their turn, EPNs are encapsulated in fusogenic EVs by the overexpression of vesicular stomatitis virus G protein (VSV-G). The proteomic profiles of different engineered EVs were determined for a comprehensive evaluation of their therapeutic potential. EVs loading mediated by bio-safe Fos–Jun heterodimerization demonstrates an increased efficacy of active cargo loading and delivery into target cells. Our results emphasize the outstanding technological and biomedical potential of the engineered EV systems, including their application in adoptive cell transfer and targeted cell reprogramming.
机译:特异性分为靶细胞和组织的蛋白质治疗剂是医学中有希望的大道。推进此过程将大大提高设计的药物的效率。在这方面,基于天然膜的系统特别感兴趣。细胞外囊(EVS)是几乎所有类型细胞分泌的双层脂质颗粒,具有几个主要优点:生物相容性,载体稳定性和血脑屏障渗透性,这使得它们成为蛋白质治疗递送的透视工具。在这里,我们评估由人细胞系产生的工程化遗传编码的EV,允许有效的货物负载。在设计的系统中,通过自组装结构,即“包络蛋白纳米病”(EPN)来捕获感兴趣的蛋白质。轮到他们,EPNS通过过表达囊泡口炎病毒G蛋白(VSV-G)封装在致沉菌EV中。确定不同工程EVS的蛋白质组学轮廓,用于综合评估其治疗潜力。 EVS加载由生物安全FOS-Jun杂交化介导的,表明活性货物加载和输送到靶细胞的疗效增加。我们的结果强调了工程勘探系统的突出技术和生物医学潜力,包括它们在采用细胞转移和靶向细胞重新编程中的应用。

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