Literature DB >> 31142540

Lgr5+ stem and progenitor cells reside at the apex of a heterogeneous embryonic hepatoblast pool.

Nicole Prior1, Christopher J Hindley1,2, Fabian Rost3, Elena Meléndez1, Winnie W Y Lau4, Berthold Göttgens4, Steffen Rulands1,2,3,5, Benjamin D Simons1,2,6, Meritxell Huch7,6,8.   

Abstract

During mouse embryogenesis, progenitors within the liver known as hepatoblasts give rise to adult hepatocytes and cholangiocytes. Hepatoblasts, which are specified at E8.5-E9.0, have been regarded as a homogeneous progenitor population that initiate differentiation from E13.5. Recently, scRNA-seq analysis has identified sub-populations of transcriptionally distinct hepatoblasts at E11.5. Here, we show that hepatoblasts are not only transcriptionally but also functionally heterogeneous, and that a subpopulation of E9.5-E10.0 hepatoblasts exhibit a previously unidentified early commitment to cholangiocyte fate. Importantly, we also identify a subpopulation constituting 2% of E9.5-E10.0 hepatoblasts that express the adult stem cell marker Lgr5, and generate both hepatocyte and cholangiocyte progeny that persist for the lifespan of the mouse. Combining lineage tracing and scRNA-seq, we show that Lgr5 marks E9.5-E10.0 bipotent liver progenitors residing at the apex of a hepatoblast hierarchy. Furthermore, isolated Lgr5+ hepatoblasts can be clonally expanded in vitro into embryonic liver organoids, which can commit to either hepatocyte or cholangiocyte fates. Our study demonstrates functional heterogeneity within E9.5 hepatoblasts and identifies Lgr5 as a marker for a subpopulation of bipotent liver progenitors.
© 2019. Published by The Company of Biologists Ltd.

Entities:  

Keywords:  Bipotent; Hepatoblast; Lgr5; Liver development; Liver stem/progenitor cells; Organoid

Mesh:

Substances:

Year:  2019        PMID: 31142540      PMCID: PMC6602348          DOI: 10.1242/dev.174557

Source DB:  PubMed          Journal:  Development        ISSN: 0950-1991            Impact factor:   6.868


  57 in total

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