Dual-mode action of scalable, high-quality engineered stem cell-derived SIRPα-extracellular vesicles for treating acute liver failure

Authors
Kim, SeohyunKim, Yoon KyoungKim, SeonghyunChoi, Yong-SoonLee, InkyuJoo, HyeminKim, JaehyunKwon, MinjeongPark, SeryoungJo, Min KyoungChoi, YoonjeongD'Souza, TheresaJung, Jae WoongZakhem, ElieLenzini, StephenWoo, JiwanChoi, HongyoonPark, JeongbinPark, Seung-YoonKim, Gi BeomNam, Gi-HoonKim, In-San
Issue Date
2025-02
Publisher
Nature Publishing Group
Citation
Nature Communications, v.16, no.1
Abstract
Acute liver failure (ALF) is a life-threatening condition caused by rapid hepatocyte death and impaired liver regeneration. Here we show that extracellular vesicles engineered to express Signal Regulatory Protein Alpha (SIRP-EVs), produced via a scalable 3D bioreactor process with high yield and purity, exhibit significant therapeutic potential by targeting damaged cells and promoting tissue repair. SIRP-EVs block CD47, a crucial inhibitory signal on necroptotic cells, to enhance macrophage-mediated clearance of dying hepatocytes. They also deliver regenerative cargo from mesenchymal stem cells, reprogramming macrophages to support liver regeneration. In male animal models, SIRP-EVs significantly reduce liver injury markers and improve survival, demonstrating their dual-function therapeutic efficacy. By integrating the resolution of necroptosis with regenerative macrophage reprogramming, SIRP-EVs represent a promising platform for restoring liver function. These findings support the development of EV-based in vivo macrophage reprogramming therapies for ALF and other inflammation-driven diseases, paving the way for the clinical application of engineered EV therapeutics.
Keywords
SCALE
URI
https://pubs.kist.re.kr/handle/201004/152089
DOI
10.1038/s41467-025-57133-w
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KIST Article > Others
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