1.
Exosome-based delivery of super-repressor IκBα relieves sepsis-associated organ damage and mortality.
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Choi, H
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Kim, Y
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Mirzaaghasi, A
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Heo, J
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Kim, YN
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Shin, JH
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Kim, S
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Kim, NH
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Cho, ES
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In Yook, J
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Yoo, TH
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Song, E
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Kim, P
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Shin, EC
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Chung, K
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Choi, K
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Choi, C
Abstract:
As extracellular vesicles that play an active role in intercellular communication by transferring cellular materials to recipient cells, exosomes offer great potential as a natural therapeutic drug delivery vehicle. The inflammatory responses in various disease models can be attenuated through introduction of super-repressor IκB (srIκB), which is the dominant active form of IκBα and can inhibit translocation of nuclear factor κB into the nucleus. An optogenetically engineered exosome system (EXPLOR) that we previously developed was implemented for loading a large amount of srIκB into exosomes. We showed that intraperitoneal injection of purified srIκB-loaded exosomes (Exo-srIκBs) attenuates mortality and systemic inflammation in septic mouse models. In a biodistribution study, Exo-srIκBs were observed mainly in the neutrophils, and in monocytes to a lesser extent, in the spleens and livers of mice. Moreover, we found that Exo-srIκB alleviates inflammatory responses in monocytic THP-1 cells and human umbilical vein endothelial cells.
2.
Exosome engineering for efficient intracellular delivery of soluble proteins using optically reversible protein-protein interaction module.
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Yim, N
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Ryu, SW
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Choi, K
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Lee, KR
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Lee, S
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Choi, H
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Kim, J
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Shaker, MR
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Sun, W
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Park, JH
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Kim, D
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Heo, WD
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Choi, C
Abstract:
Nanoparticle-mediated delivery of functional macromolecules is a promising method for treating a variety of human diseases. Among nanoparticles, cell-derived exosomes have recently been highlighted as a new therapeutic strategy for the in vivo delivery of nucleotides and chemical drugs. Here we describe a new tool for intracellular delivery of target proteins, named 'exosomes for protein loading via optically reversible protein-protein interactions' (EXPLORs). By integrating a reversible protein-protein interaction module controlled by blue light with the endogenous process of exosome biogenesis, we are able to successfully load cargo proteins into newly generated exosomes. Treatment with protein-loaded EXPLORs is shown to significantly increase intracellular levels of cargo proteins and their function in recipient cells in vitro and in vivo. These results clearly indicate the potential of EXPLORs as a mechanism for the efficient intracellular transfer of protein-based therapeutics into recipient cells and tissues.
