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Human hepatic stem cells from fetal and postnatal donors

Human hepatic stem cells (hHpSCs), which are pluripotent precursors of hepatoblasts and thence of hepatocytic and biliary epithelia, are located in ductal plates in fetal livers and in Canals of Hering in adult livers. They can be isolated by immunoselection for epithelial cell adhesion molecule–pos...

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Autores principales: Schmelzer, Eva, Zhang, Lili, Bruce, Andrew, Wauthier, Eliane, Ludlow, John, Yao, Hsin-lei, Moss, Nicholas, Melhem, Alaa, McClelland, Randall, Turner, William, Kulik, Michael, Sherwood, Sonya, Tallheden, Tommi, Cheng, Nancy, Furth, Mark E., Reid, Lola M.
Formato: Texto
Lenguaje:English
Publicado: The Rockefeller University Press 2007
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2118675/
https://www.ncbi.nlm.nih.gov/pubmed/17664288
http://dx.doi.org/10.1084/jem.20061603
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author Schmelzer, Eva
Zhang, Lili
Bruce, Andrew
Wauthier, Eliane
Ludlow, John
Yao, Hsin-lei
Moss, Nicholas
Melhem, Alaa
McClelland, Randall
Turner, William
Kulik, Michael
Sherwood, Sonya
Tallheden, Tommi
Cheng, Nancy
Furth, Mark E.
Reid, Lola M.
author_facet Schmelzer, Eva
Zhang, Lili
Bruce, Andrew
Wauthier, Eliane
Ludlow, John
Yao, Hsin-lei
Moss, Nicholas
Melhem, Alaa
McClelland, Randall
Turner, William
Kulik, Michael
Sherwood, Sonya
Tallheden, Tommi
Cheng, Nancy
Furth, Mark E.
Reid, Lola M.
author_sort Schmelzer, Eva
collection PubMed
description Human hepatic stem cells (hHpSCs), which are pluripotent precursors of hepatoblasts and thence of hepatocytic and biliary epithelia, are located in ductal plates in fetal livers and in Canals of Hering in adult livers. They can be isolated by immunoselection for epithelial cell adhesion molecule–positive (EpCAM+) cells, and they constitute ∼0.5–2.5% of liver parenchyma of all donor ages. The self-renewal capacity of hHpSCs is indicated by phenotypic stability after expansion for >150 population doublings in a serum-free, defined medium and with a doubling time of ∼36 h. Survival and proliferation of hHpSCs require paracrine signaling by hepatic stellate cells and/or angioblasts that coisolate with them. The hHpSCs are ∼9 μm in diameter, express cytokeratins 8, 18, and 19, CD133/1, telomerase, CD44H, claudin 3, and albumin (weakly). They are negative for α-fetoprotein (AFP), intercellular adhesion molecule (ICAM) 1, and for markers of adult liver cells (cytochrome P450s), hemopoietic cells (CD45), and mesenchymal cells (vascular endothelial growth factor receptor and desmin). If transferred to STO feeders, hHpSCs give rise to hepatoblasts, which are recognizable by cordlike colony morphology and up-regulation of AFP, P4503A7, and ICAM1. Transplantation of freshly isolated EpCAM+ cells or of hHpSCs expanded in culture into NOD/SCID mice results in mature liver tissue expressing human-specific proteins. The hHpSCs are candidates for liver cell therapies.
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spelling pubmed-21186752008-02-06 Human hepatic stem cells from fetal and postnatal donors Schmelzer, Eva Zhang, Lili Bruce, Andrew Wauthier, Eliane Ludlow, John Yao, Hsin-lei Moss, Nicholas Melhem, Alaa McClelland, Randall Turner, William Kulik, Michael Sherwood, Sonya Tallheden, Tommi Cheng, Nancy Furth, Mark E. Reid, Lola M. J Exp Med Articles Human hepatic stem cells (hHpSCs), which are pluripotent precursors of hepatoblasts and thence of hepatocytic and biliary epithelia, are located in ductal plates in fetal livers and in Canals of Hering in adult livers. They can be isolated by immunoselection for epithelial cell adhesion molecule–positive (EpCAM+) cells, and they constitute ∼0.5–2.5% of liver parenchyma of all donor ages. The self-renewal capacity of hHpSCs is indicated by phenotypic stability after expansion for >150 population doublings in a serum-free, defined medium and with a doubling time of ∼36 h. Survival and proliferation of hHpSCs require paracrine signaling by hepatic stellate cells and/or angioblasts that coisolate with them. The hHpSCs are ∼9 μm in diameter, express cytokeratins 8, 18, and 19, CD133/1, telomerase, CD44H, claudin 3, and albumin (weakly). They are negative for α-fetoprotein (AFP), intercellular adhesion molecule (ICAM) 1, and for markers of adult liver cells (cytochrome P450s), hemopoietic cells (CD45), and mesenchymal cells (vascular endothelial growth factor receptor and desmin). If transferred to STO feeders, hHpSCs give rise to hepatoblasts, which are recognizable by cordlike colony morphology and up-regulation of AFP, P4503A7, and ICAM1. Transplantation of freshly isolated EpCAM+ cells or of hHpSCs expanded in culture into NOD/SCID mice results in mature liver tissue expressing human-specific proteins. The hHpSCs are candidates for liver cell therapies. The Rockefeller University Press 2007-08-06 /pmc/articles/PMC2118675/ /pubmed/17664288 http://dx.doi.org/10.1084/jem.20061603 Text en Copyright © 2007, The Rockefeller University Press This article is distributed under the terms of an Attribution–Noncommercial–Share Alike–No Mirror Sites license for the first six months after the publication date (see http://www.rupress.org/terms). After six months it is available under a Creative Commons License (Attribution–Noncommercial–Share Alike 4.0 Unported license, as described at http://creativecommons.org/licenses/by-nc-sa/4.0/).
spellingShingle Articles
Schmelzer, Eva
Zhang, Lili
Bruce, Andrew
Wauthier, Eliane
Ludlow, John
Yao, Hsin-lei
Moss, Nicholas
Melhem, Alaa
McClelland, Randall
Turner, William
Kulik, Michael
Sherwood, Sonya
Tallheden, Tommi
Cheng, Nancy
Furth, Mark E.
Reid, Lola M.
Human hepatic stem cells from fetal and postnatal donors
title Human hepatic stem cells from fetal and postnatal donors
title_full Human hepatic stem cells from fetal and postnatal donors
title_fullStr Human hepatic stem cells from fetal and postnatal donors
title_full_unstemmed Human hepatic stem cells from fetal and postnatal donors
title_short Human hepatic stem cells from fetal and postnatal donors
title_sort human hepatic stem cells from fetal and postnatal donors
topic Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2118675/
https://www.ncbi.nlm.nih.gov/pubmed/17664288
http://dx.doi.org/10.1084/jem.20061603
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