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Literature DB >> 15368439

Immunolocalization of extracellular matrix components and integrins during mouse liver development.

Nobuyoshi Shiojiri¹, Yoshinori Sugiyama.

Abstract

Intrahepatic biliary cell differentiation takes place in periportal hepatoblasts under the influence of the subjacent connective tissue, the mechanism of which is still unclear. This study was undertaken to analyze the immunolocalization of extracellular matrix components and their cellular receptors during mouse liver development, with special attention given to biliary differentiation and vascular development. In young fetal mouse liver, primitive structures of sinusoids were developed between hepatic cords associated with hematopoietic cells demonstrated by immunohistochemistry of basal laminar components, the alpha6 integrin subunit, and PECAM-1. Portal veins and hepatic veins showed different staining intensities of alpha2, alpha3, and alpha6 integrin subunits from early stages of development. Anti-beta4 integrin subunit antibodies reacted with portal veins, but not with hepatic veins after perinatal stages. Their different phenotypes may be related to the preferential differentiation of periportal bile ducts. In intrahepatic bile duct development, periportal hepatoblasts adjacent to the connective tissue were immunostained for each basal laminar component on the basal side at almost the same time; alpha3, alpha5, alpha6, and beta4 integrin subunits were immunohistochemically detectable later than the basal laminar components. These staining patterns of intrahepatic bile duct cells clearly differed from those of extrahepatic bile duct cells from the beginning of their development, suggesting that these ducts are of different origins. In conclusion, the vascular structures, including sinusoids, portal veins, and hepatic veins, develop from early stages of liver development, and the extracellular matrix components may play important roles in biliary differentiation and vascular development. Supplementary material for this article can be found on the HEPATOLOGY website (http://interscience.wiley.com/jpages/0270-9139/suppmat/index.html). Copyright 2004 American Association for the Study of Liver Diseases

Entities: Disease Gene Species

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Year: 2004 PMID： 15368439 DOI： 10.1002/hep.20303

Source DB: PubMed Journal: Hepatology ISSN： 0270-9139 Impact factor: 17.425

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Cited

26 in total

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2. Immunohistochemical analyses of cell-cell interactions during hepatic organoid formation from fetal mouse liver cells cultured in vitro.

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4. Prox1 ablation in hepatic progenitors causes defective hepatocyte specification and increases biliary cell commitment.

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5. Immunomagnetic exclusion of E-cadherin-positive hepatoblasts in fetal mouse liver cell cultures impairs morphogenesis and gene expression of sinusoidal endothelial cells.

Authors: Yurie Takabe; Shinomi Yagi; Toru Koike; Nobuyoshi Shiojiri
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Immunolocalization of extracellular matrix components and integrins during mouse liver development.

1. Liver-specific knockout of GRP94 in mice disrupts cell adhesion, activates liver progenitor cells, and accelerates liver tumorigenesis.

2. Immunohistochemical analyses of cell-cell interactions during hepatic organoid formation from fetal mouse liver cells cultured in vitro.

Review 3. Current strategies to generate mature human induced pluripotent stem cells derived cholangiocytes and future applications.

4. Prox1 ablation in hepatic progenitors causes defective hepatocyte specification and increases biliary cell commitment.

5. Immunomagnetic exclusion of E-cadherin-positive hepatoblasts in fetal mouse liver cell cultures impairs morphogenesis and gene expression of sinusoidal endothelial cells.

6. Definitive endoderm derived from human embryonic stem cells highly express the integrin receptors alphaV and beta5.

7. α1- and α5-containing laminins regulate the development of bile ducts via β1 integrin signals.

8. Expression of matrilin-2 in liver cirrhosis and hepatocellular carcinoma.

9. Abnormal liver differentiation and excessive angiogenesis in mice lacking Runx3.

10. Study of Recellularized Human Acellular Arterial Matrix Repairs Porcine Biliary Segmental Defects.