info:eu-repo/semantics/article
Assembly and Function of a Bioengineered Human Liver for Transplantation Generated Solely from Induced Pluripotent Stem Cells
Date
2020-06Registration in:
Takeishi, Kazuki; Collin de I'Hortet, Alexandra; Wang, Yang; Handa, Kan; Guzman Lepe, Jorge; et al.; Assembly and Function of a Bioengineered Human Liver for Transplantation Generated Solely from Induced Pluripotent Stem Cells; Cell Press; Cell Reports; 31; 9; 6-2020; 1-30
2211-1247
CONICET Digital
CONICET
Author
Takeishi, Kazuki
Collin de I'Hortet, Alexandra
Wang, Yang
Handa, Kan
Guzman Lepe, Jorge
Matsubara, Kentaro
Morita, Kazutoyo
Jang, Sae
Haep, Nils
Florentino, Rodrigo M.
Yuan, Fangchao
Fukumitsu, Ken
Tobita, Kimimasa
Sun, Wendell
Franks, Jonathan
Delgado, Evan R.
Shapiro, Erik M.
Fraunhoffer Navarro, Nicolas Alejandro
Duncan, Andrew W.
Yagi, Hiroshi
Mashimo, Tomoji
Fox, Ira J.
Soto Gutierrez, Alejandro
Abstract
The availability of an autologous transplantable auxiliary liver would dramatically affect the treatment of liver disease. Assembly and function in vivo of a bioengineered human liver derived from induced pluripotent stem cells (iPSCs) has not been previously described. By improving methods for liver decellularization, recellularization, and differentiation of different liver cellular lineages of human iPSCs in an organ-like environment, we generated functional engineered human mini livers and performed transplantation in a rat model. Whereas previous studies recellularized liver scaffolds largely with rodent hepatocytes, we repopulated not only the parenchyma with human iPSC-hepatocytes but also the vascular system with human iPS-endothelial cells, and the bile duct network with human iPSC-biliary epithelial cells. The regenerated human iPSC-derived mini liver containing multiple cell types was tested in vivo and remained functional for 4 days after auxiliary liver transplantation in immunocompromised, engineered (IL2rg−/−) rats.
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