1. The nuclear receptor THRB facilitates differentiation of human PSCs into more mature hepatocytes
- Author
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Ma, Haiting, de Zwaan, Esmée, Guo, Yang Eric, Cejas, Paloma, Thiru, Prathapan, van de Bunt, Martijn, Jeppesen, Jacob F., Syamala, Sudeepa, Dall’Agnese, Alessandra, Abraham, Brian J., Fu, Dongdong, Garrett-Engele, Carrie, Lee, Tony, Long, Henry W, Griffith, Linda G., Young, Richard A., and Jaenisch, Rudolf
- Subjects
Mice ,Hepatocytes ,Genetics ,Animals ,Humans ,Receptors, Cytoplasmic and Nuclear ,Molecular Medicine ,Cell Differentiation ,Cell Biology ,Regulatory Sequences, Nucleic Acid ,Polymorphism, Single Nucleotide ,Article ,Chromatin - Abstract
To understand the mechanisms regulating the in vitro maturation of hPSC-derived hepatocytes, we developed a 3D differentiation system and compared gene regulatory elements in human primary hepatocytes with those in hPSC-hepatocytes that were differentiated in 2D or 3D conditions by RNA-seq, ATAC-seq, and H3K27Ac ChIP-seq. Regulome comparisons showed a reduced enrichment of thyroid receptor THRB motifs in accessible chromatin and active enhancers without a reduced transcription of THRB. The addition of thyroid hormone T3 increased the binding of THRB to the CYP3A4 proximal enhancer, restored the super-enhancer status and gene expression of NFIC, and reduced the expression of AFP. The resultant hPSC-hepatocytes showed gene expression, epigenetic status, and super-enhancer landscape closer to primary hepatocytes and activated regulatory regions including non-coding SNPs associated with liver-related diseases. Transplanting the hPSC-hepatocytes resulted in the engraftment of human hepatocytes into the mouse liver without disrupting normal liver histology. This work implicates the environmental factor-nuclear receptor axis in regulating the maturation of hPSC-hepatocytes.
- Published
- 2022
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