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Hepatic Notch2 deficiency leads to bile duct agenesis perinatally and secondary bile duct formation after weaning

pmid: 25446530
Hepatic Notch2 deficiency leads to bile duct agenesis perinatally and secondary bile duct formation after weaning
Notch signaling plays an acknowledged role in bile-duct development, but its involvement in cholangiocyte-fate determination remains incompletely understood. We investigated the effects of early Notch2 deletion in Notch2(fl/fl)/Alfp-Cre(tg/-) ("Notch2-cKO") and Notch2(fl/fl)/Alfp-Cre(-/-) ("control") mice. Fetal and neonatal Notch2-cKO livers were devoid of cytokeratin19 (CK19)-, Dolichos-biflorus agglutinin (DBA)-, and SOX9-positive ductal structures, demonstrating absence of prenatal cholangiocyte differentiation. Despite extensive cholestatic hepatocyte necrosis and growth retardation, mortality was only ~15%. Unexpectedly, a slow process of secondary cholangiocyte differentiation and bile-duct formation was initiated around weaning that histologically resembled the ductular reaction. Newly formed ducts varied from rare and non-connected, to multiple, disorganized tubular structures that connected to the extrahepatic bile ducts. Jaundice had disappeared in ~30% of Notch2-cKO mice by 6 months. The absence of NOTCH2 protein in postnatally differentiating cholangiocyte nuclei of Notch2-cKO mice showed that these cells had not originated from non-recombined precursor cells. Notch2 and Hnf6 mRNA levels were permanently decreased in Notch2-cKO livers. Perinatally, Foxa1, Foxa2, Hhex, Hnf1β, Cebpα and Sox9 mRNA levels were all significantly lower in Notch2-cKO than control mice, but all except Foxa2 returned to normal or increased levels after weaning, coincident with the observed secondary bile-duct formation. Interestingly, Hhex and Sox9 mRNA levels remained elevated in icteric 6 months old Notch2-cKOs, but decreased to control levels in non-icteric Notch2-cKOs, implying a key role in secondary bile-duct formation.Cholangiocyte differentiation becomes progressively less dependent on NOTCH2 signaling with age, suggesting that ductal-plate formation is dependent on NOTCH2, but subsequent cholangiocyte differentiation is not.
- University of Amsterdam Netherlands
- Université Catholique de Louvain Belgium
- de Duve Institute Belgium
- Academic Medical Center Netherlands
- Boston Children's Hospital United States
Notch2, Mice, Knockout, Analysis of Variance, Cholangiocytes, Organogenesis, Histological Techniques, Cell Biology, Weaning, Ductular reaction, Immunohistochemistry, Polymerase Chain Reaction, Ductal plate, Hepatocyte Nuclear Factor 6, Mice, Liver, Animals, Regression Analysis, Bile Ducts, Receptor, Notch2, Molecular Biology, Developmental Biology, DNA Primers
Notch2, Mice, Knockout, Analysis of Variance, Cholangiocytes, Organogenesis, Histological Techniques, Cell Biology, Weaning, Ductular reaction, Immunohistochemistry, Polymerase Chain Reaction, Ductal plate, Hepatocyte Nuclear Factor 6, Mice, Liver, Animals, Regression Analysis, Bile Ducts, Receptor, Notch2, Molecular Biology, Developmental Biology, DNA Primers
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