| Literature DB >> 28614297 |
J Gray Camp1, Keisuke Sekine2, Tobias Gerber1, Henry Loeffler-Wirth3, Hans Binder3, Malgorzata Gac1, Sabina Kanton1, Jorge Kageyama1, Georg Damm4,5, Daniel Seehofer4,5, Lenka Belicova6, Marc Bickle6, Rico Barsacchi6, Ryo Okuda2, Emi Yoshizawa2, Masaki Kimura2, Hiroaki Ayabe2, Hideki Taniguchi2, Takanori Takebe2,7, Barbara Treutlein1,6.
Abstract
Conventional two-dimensional differentiation from pluripotency fails to recapitulate cell interactions occurring during organogenesis. Three-dimensional organoids generate complex organ-like tissues; however, it is unclear how heterotypic interactions affect lineage identity. Here we use single-cell RNA sequencing to reconstruct hepatocyte-like lineage progression from pluripotency in two-dimensional culture. We then derive three-dimensional liver bud organoids by reconstituting hepatic, stromal, and endothelial interactions, and deconstruct heterogeneity during liver bud development. We find that liver bud hepatoblasts diverge from the two-dimensional lineage, and express epithelial migration signatures characteristic of organ budding. We benchmark three-dimensional liver buds against fetal and adult human liver single-cell RNA sequencing data, and find a striking correspondence between the three-dimensional liver bud and fetal liver cells. We use a receptor-ligand pairing analysis and a high-throughput inhibitor assay to interrogate signalling in liver buds, and show that vascular endothelial growth factor (VEGF) crosstalk potentiates endothelial network formation and hepatoblast differentiation. Our molecular dissection reveals interlineage communication regulating organoid development, and illuminates previously inaccessible aspects of human liver development.Entities:
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Year: 2017 PMID: 28614297 DOI: 10.1038/nature22796
Source DB: PubMed Journal: Nature ISSN: 0028-0836 Impact factor: 49.962