| Literature DB >> 31080134 |
Brian J Pepe-Mooney1, Michael T Dill2, Anna Alemany3, Jose Ordovas-Montanes4, Yuki Matsushita5, Anuradha Rao6, Anushna Sen7, Makoto Miyazaki8, Sayeepriyadarshini Anakk7, Paul A Dawson6, Noriaki Ono5, Alex K Shalek9, Alexander van Oudenaarden3, Fernando D Camargo10.
Abstract
The liver can substantially regenerate after injury, with both main epithelial cell types, hepatocytes and biliary epithelial cells (BECs), playing important roles in parenchymal regeneration. Beyond metabolic functions, BECs exhibit substantial plasticity and in some contexts can drive hepatic repopulation. Here, we performed single-cell RNA sequencing to examine BEC and hepatocyte heterogeneity during homeostasis and after injury. Instead of evidence for a transcriptionally defined progenitor-like BEC cell, we found significant homeostatic BEC heterogeneity that reflects fluctuating activation of a YAP-dependent program. This transcriptional signature defines a dynamic cellular state during homeostasis and is highly responsive to injury. YAP signaling is induced by physiological bile acids (BAs), required for BEC survival in response to BA exposure, and is necessary for hepatocyte reprogramming into biliary progenitors upon injury. Together, these findings uncover molecular heterogeneity within the ductal epithelium and reveal YAP as a protective rheostat and regenerative regulator in the mammalian liver.Entities:
Keywords: YAP signaling; bile acids; biliary epithelial cells; cellular plasticity; cholangiocytes; hepatocytes; liver biology; liver progenitor cells; regeneration; single-cell RNA sequencing
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Year: 2019 PMID: 31080134 PMCID: PMC6814390 DOI: 10.1016/j.stem.2019.04.004
Source DB: PubMed Journal: Cell Stem Cell ISSN: 1875-9777 Impact factor: 24.633