小泡
小RNA
微泡
细胞生物学
细胞外小泡
生物物理学
化学
细胞外
生物
生物化学
膜
基因
作者
Anjana Jeyaram,Tek N. Lamichhane,Sheng Wang,Lin Zou,Eshan Dahal,Stephanie M. Kronstadt,Daniel Levy,Babita Parajuli,Daphne R Knudsen-Palmer,Wei Chao,Steven M. Jay
标识
DOI:10.1016/j.ymthe.2019.12.007
摘要
Based on their identification as physiological nucleic acid carriers in humans and other organisms, extracellular vesicles (EVs) have been explored as therapeutic delivery vehicles for DNA, RNA, and other cargo. However, efficient loading and functional delivery of nucleic acids remain a challenge, largely because of potential sources of degradation and aggregation. Here, we report that protonation of EVs to generate a pH gradient across EV membranes can be utilized to enhance vesicle loading of nucleic acid cargo, specifically microRNA (miRNA), small interfering RNA (siRNA), and single-stranded DNA (ssDNA). The loading process did not impair cellular uptake of EVs, nor did it promote any significant EV-induced toxicity response in mice. Cargo functionality was verified by loading HEK293T EVs with either pro- or anti-inflammatory miRNAs and observing the effective regulation of corresponding cellular cytokine levels. Critically, this loading increase is comparable with what can be accomplished by methods such as sonication and electroporation, and is achievable without the introduction of energy associated with these methods that can potentially damage labile nucleic acid cargo.
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