3D hepatic organoid production from human pluripotent stem cells

Zhe Long Jin, Kang He Xu, Jonghun Kim, Hao Guo, Xuerui Yao, Yong Nan Xu, Ying Hua Li, Dong Hee Ryu, Kee Pyo Kim, Kwonho Hong, Yong June Kim, Lin Wang, Qilong Cao, Kyun Hwan Kim, Nam Hyung Kim, Dong Wook Han

Research output: Contribution to journalArticlepeer-review

Abstract

Hepatic organoids might provide a golden opportunity for realizing precision medicine in various hepatic diseases. Previously described hepatic organoid protocols from pluripotent stem cells rely on complicated multiple differentiation steps consisting of both 2D and 3D differentiation procedures. Therefore, the spontaneous formation of hepatic organoids from 2D monolayer culture is associated with a low-throughput production, which might hinder the standardization of hepatic organoid production and hamper the translation of this technology to the clinical or industrial setting. Here we describe the stepwise and fully 3D production of hepatic organoids from human pluripotent stem cells. We optimized every differentiation step by screening for optimal concentrations and timing of differentiation signals in each differentiation step. Hepatic organoids are stably expandable without losing their hepatic functionality. Moreover, upon treatment of drugs with known hepatotoxicity, we found hepatic organoids are more sensitive to drug-induced hepatotoxicity compared with 2D hepatocytes differentiated from PSCs, making them highly suitable for in vitro toxicity screening of drug candidates. The standardized fully 3D protocol described in the current study for producing functional hepatic organoids might serve as a novel platform for the industrial and clinical translation of hepatic organoid technology.

Original languageEnglish
Article number100742
JournalDifferentiation
Volume135
DOIs
StatePublished - 1 Jan 2024

Keywords

  • 3D high-throughput production
  • Hepatic organoids
  • Human pluripotent stem cells
  • In vitro toxicity screening

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