The embryonic development of the liver is initiated by the emergence of hepatoblasts, originating from the ventral foregut endoderm adjacent to the heart. Here, we identify and characterize a previously unrecognized population of early hepatoblasts at the ventroposterior part of the emerging liver bud, traced from Cdx2-positive endoderm progenitors, which we term primitive hepatoblasts. Mouse and human single-cell transcriptomics reveals the expression of both canonical hepatoblast markers TBX3, FGB, and KRT8/18 and primitive-specific mesenchymal markers ID3, VIM, and GATA4. Lineage tracing revealed the notable contribution up to 12.6% of LIV2+ hepatoblasts at E11.5 but diminishes in late fetal and postnatal development. Epigenetic and functional perturbation studies further uncover that primitive hepatoblast emergence is primed by WNT-suppression on RA-permissive CDX2+FOXA2+ progenitors. Furthermore, human pluripotent stem cell-derived primitive hepatoblast-like cells secrete pleiotrophin and midkine to amplify hepatoblast populations and develop epithelial-mesenchymal hybrid tissues in vivo. Our results provide a new framework for understanding lineage heterogeneity during early hepatogenesis and offer revised insights into strategies to model normal and abnormal liver development.
Primitive Hepatoblasts Driving Early Liver Development.
原始肝母细胞驱动早期肝脏发育
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作者:Iwasawa Kentaro, Koike Hiroyuki, Al Reza Hasan, Milton Yuka, Kishimoto Keishi, Thorner Konrad, Granitto Marissa, Saiki Norikazu, Santangelo Connie, Glaser Kathryn, Kimura Masaki, Bondoc Alexander, Lim Hee-Wong, Morimoto Mitsuru, Iwafuchi Makiko, Wells James M, Zorn Aaron M, Takebe Takanori
| 期刊: | bioRxiv | 影响因子: | 0.000 |
| 时间: | 2025 | 起止号: | 2025 Jun 8 |
| doi: | 10.1101/2025.06.08.658502 | 研究方向: | 发育与干细胞、细胞生物学 |
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