Single-cell atlas of human liver development reveals pathways directing hepatic cell fates

Author:

Wesley Brandon T.,Ross Alexander D. B.,Muraro Daniele,Miao Zhichao,Saxton Sarah,Tomaz Rute A.,Morell Carola M.,Ridley Katherine,Zacharis Ekaterini D.,Petrus-Reurer Sandra,Kraiczy Judith,Mahbubani Krishnaa T.,Brown Stephanie,Garcia-Bernardo Jose,Alsinet Clara,Gaffney DanielORCID,Tysoe Olivia C.,Botting Rachel A.,Stephenson Emily,Popescu Dorin-Mirel,MacParland Sonya,Bader GaryORCID,McGilvray Ian D.,Ortmann Daniel,Sampaziotis Fotios,Saeb-Parsy Kourosh,Haniffa Muzlifah,Stevens Kelly R.,Zilbauer Matthias,Teichmann Sarah A.,Vallier LudovicORCID

Abstract

The liver has been studied extensively due to the broad number of diseases affecting its vital functions. However, therapeutic advances, especially in regenerative medicine, are currently hampered by the lack of knowledge concerning human hepatic cell development. Here, we addressed this limitation by describing the developmental trajectories of different cell types comprising the human fetal liver at single-cell resolution. These transcriptomic analyses revealed that sequential cell-to-cell interactions direct functional maturation of hepatocytes, with non-parenchymal cells playing critical, supportive roles during organogenesis. We utilised this information to derive bipotential hepatoblast organoids and then exploited this novel model system to validate the importance of key signalling pathways and developmental cues. Furthermore, these insights into hepatic maturation enabled the identification of stage-specific transcription factors to improve the functionality of hepatocyte-like cells generated from human pluripotent stem cells. Thus, our study establishes a new platform to investigate the basic mechanisms of human liver development and to produce cell types for clinical applications.

Publisher

Cold Spring Harbor Laboratory

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