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Endosomal escape enhancing compounds facilitate functional delivery of extracellular vesicle cargo

机译:内体逸出增强化合物促进细胞外囊泡货物的功能性分娩

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Aim: Extracellular vesicles (EVs) are desirable delivery vehicles for therapeutic cargoes. We aimed to load EVs with Cre recombinase protein and determine whether functional delivery to cells could be improved by using endosomal escape enhancing compounds. Materials & methods: Overexpressed CreFRB protein was actively loaded into EVs by rapalog-induced dimerization to CD81FKBP, or passively loaded by overexpression in the absence of rapalog. Functional delivery of CreFRB was analysed using a HEK293 Cre reporter cell line in the absence and presence of endosomal escape enhancing compounds. Results: The EVs loaded with CreFRB by both active and passive mechanisms were able to deliver functional CreFRB to recipient cells only in the presence of endosomal escape enhancing compounds chloroquine and UNC10217832A. Conclusion: The use of endosomal escape enhancing compounds in conjunction with EVs loaded with therapeutic cargoes may improve efficacy of future EV based therapeutics.
机译:目的:细胞外囊泡(EVS)是治疗货物的理想递送载体。 我们旨在用Cre重组酶蛋白加载EV,并通过使用内体逸出增强化合物来确定是否可以改善功能递送给细胞。 材料和方法:通过Rapalog诱导的rapalog诱导的CD81FKBP积极装入EV的过表达CrefrB蛋白,或者在没有Rapalog的情况下被过表达被动地装载。 使用HEK293 CRE报告细胞系分析CREFRB的功能递送,在没有和存在内体逸出增强化合物的情况下。 结果:通过主动和无源机制加载CrefRB的EVS能够仅在内体逸出增强化合物的存在下仅在内体逸出的氯喹和UNC10217832A中向受体细胞递送功能性CrefRB。 结论:使用内体逸出增强化合物与载有治疗货物的EVS,可以提高基于EV的治疗的疗效。

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