Human Fetal Ductal Plate Revisited. I. Ductal Plate Expresses NCAM, KIT, MET, PDGFRA, and Neuroendocrine Antigens (NSE, Chromogranin, Synaptophysin, and CD56)

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TitreHuman Fetal Ductal Plate Revisited. I. Ductal Plate Expresses NCAM, KIT, MET, PDGFRA, and Neuroendocrine Antigens (NSE, Chromogranin, Synaptophysin, and CD56)
Type de publicationJournal Article
Year of Publication2014
AuteursTerada T
JournalMICROSCOPY RESEARCH AND TECHNIQUE
Volume77
Pagination814-824
Date PublishedOCT
Type of ArticleArticle
ISSN1059-910X
Mots-clésDevelopment, Differentiation, ductal plate, embryo, fetus, Human
Résumé

Background: The molecular mechanisms of ductal plate (DP) development and differentiation (DD) in human fetal livers (HFLs) are unclear. Materials and Methods: The author immunohistochemically investigated expressions of NCAM, KIT, KIT, PDGFRA, and neuroendocrine antigens in 32 HFLs. Results: The processes of human intrahepatic bile duct (IBD) DD could be categorized into four stages: DP, remodeling DP, remodeled DP, and mature IBD. NCAM was always expressed in DP and remodeling DP, but not in remodeled DP and mature IBD. The biliary elements were positive for cytokeratin (CK)7, 8, 18, and 19. The hepatoblasts were positive for CK8 and CD18, but negative for CK7 and CK19; however, periportal hepatoblasts showed biliary-type CKs (CK7 and CK19). NCAM was always expressed in DP and remodeling DP, but not in remodeled DP and mature IBD. KIT was occasionally (12/32 cases) expressed in DP and remodeling DP, but not in remodeled DP and mature IBD. NCAM expression was also seen in some hepatoblasts and hematopoietic cells and neurons. KIT was also expressed in some hepatoblasts, hematopoietic cells, and mast cells. MET and PDGFRA were strongly expressed in DP, remodeling DP, remodeled DP, and mature IBD. MET and PDGFRA were also strongly expressed in hepatoblasts and hematopoietic cells. MET and PDGFRA were not expressed in portal mesenchyme, portal veins, sinusoids, and hepatic veins. DP showed immunoreactive chromogranin, synaptophysin, neuron-specific enolase (NSE), and CD56. Expressions of chromogranin and CD56 were infrequently seen in remodeling DP. No expressions of these four neuroendocrine antigens were seen in remodeled DP and mature IBD. The nerve fibers were consistently positive for chromogranin, synaptophysin, NSE, and CD56 in the portal mesenchyme in the stages of remodeling DP, remodeled DP, and mature IBDs. Conclusions: The data suggest that NCAM, KIT/stem cell factor-signaling, NSE, hepatocyte growth factor/MET signaling, PDGF/PDGFRA signaling, chromogranin, synaptophysin, and CD56 play important roles in DD of biliary cells of HFL. They also suggest that the DP cells having neuroendocrine molecules give rise to hepatic stem/progenitor cells. Microsc. Res. Tech. 77:814-824, 2014. (c) 2014 Wiley Periodicals, Inc.

DOI10.1002/jemt.22404