Novel enzymatic cross-linking-based hydrogel nanofilm caging system on pancreatic β cell spheroid for long-term blood glucose regulation

Pancreatic β cell therapy for type 1 diabetes is limited by low cell survival rate owing to physical stress and aggressive host immune response. In this study, we demonstrate a multilayer hydrogel nanofilm caging strategy capable of protecting cells from high shear stress and reducing immune respons...

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Veröffentlicht in:Science advances 2021-06, Vol.7 (26)
Hauptverfasser: Kim, Minji, Kim, Hyunbum, Lee, Young-Sun, Lee, Sangjun, Kim, Seong-Eun, Lee, Uk-Jae, Jung, Sungwon, Park, Chung-Gyu, Hong, Jinkee, Doh, Junsang, Lee, Dong Yun, Kim, Byung-Gee, Hwang, Nathaniel S
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Sprache:eng
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Zusammenfassung:Pancreatic β cell therapy for type 1 diabetes is limited by low cell survival rate owing to physical stress and aggressive host immune response. In this study, we demonstrate a multilayer hydrogel nanofilm caging strategy capable of protecting cells from high shear stress and reducing immune response by interfering cell-cell interaction. Hydrogel nanofilm is fabricated by monophenol-modified glycol chitosan and hyaluronic acid that cross-link each other to form a nanothin hydrogel film on the cell surface via tyrosinase-mediated reactions. Furthermore, hydrogel nanofilm formation was conducted on mouse β cell spheroids for the islet transplantation application. The cytoprotective effect against physical stress and the immune protective effect were evaluated. Last, caged mouse β cell spheroids were transplanted into the type 1 diabetes mouse model and successfully regulated its blood glucose level. Overall, our enzymatic cross-linking-based hydrogel nanofilm caging method will provide a new platform for clinical applications of cell-based therapies.
ISSN:2375-2548
2375-2548
DOI:10.1126/sciadv.abf7832