Litcius/Paper detail

Leveraging interacting signaling pathways to robustly improve the quality and yield of human pluripotent stem cell-derived hepatoblasts and hepatocytes

Claudia Raggi, Marie-Agnès M’Callum, Quang Toan Pham, Perrine Gaub, Silvia Selleri, Nissan Baratang, C. Mangahas, Gaël Cagnone, Bruno Reversade, Jean‐Sébastien Joyal, Massimiliano Paganelli

2022Stem Cell Reports25 citationsDOIOpen Access PDF

Abstract

Pluripotent stem cell (PSC)-derived hepatocyte-like cells (HLCs) have shown great potential as an alternative to primary human hepatocytes (PHHs) for in vitro modeling. Several differentiation protocols have been described to direct PSCs toward the hepatic fate. Here, by leveraging recent knowledge of the signaling pathways involved in liver development, we describe a robust, scalable protocol that allowed us to consistently generate high-quality bipotent human hepatoblasts and HLCs from both embryonic stem cells and induced PSC (iPSCs). Although not yet fully mature, such HLCs were more similar to adult PHHs than were cells obtained with previously described protocols, showing good potential as a physiologically representative alternative to PHHs for in vitro modeling. PSC-derived hepatoblasts effectively generated with this protocol could differentiate into mature hepatocytes and cholangiocytes within syngeneic liver organoids, thus opening the way for representative human 3D in vitro modeling of liver development and pathophysiology.

Topics & Concepts

BiologyInduced pluripotent stem cellEmbryonic stem cellCell biologyStem cellComputational biologyHuman Induced Pluripotent Stem CellsHepatocyteNeuroscienceIn vitroGeneGeneticsLiver physiology and pathologyPluripotent Stem Cells ResearchPancreatic function and diabetes
Leveraging interacting signaling pathways to robustly improve the quality and yield of human pluripotent stem cell-derived hepatoblasts and hepatocytes | Litcius