Hepatocyte Transplantation and the Differentiation Fate of Host Oval Cells in Acute Severe Hepatic Injury

Oval cells and hepatocytes rarely proliferate simultaneously. This study aimed to determine the impacts of hepatocyte transplantation on the response and fate of oval cells that are activated to proliferate in acute severe hepatic injury. Retrorsine + D-galactosamine (R+D-gal) treatment was used to...

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Main Authors: Chun-Hsien Yu, Mei-Hwei Chang, Chin-Sung Chien, Ya-Hui Chen, Ming-Fu Chang, Hui-Ling Chen Ph.D.
Format: Article
Language:English
Published: SAGE Publishing 2010-02-01
Series:Cell Transplantation
Online Access:https://doi.org/10.3727/096368909X479848
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spelling doaj-663b4cb44dc044a49c4126062d9ab5c82020-11-25T03:20:34ZengSAGE PublishingCell Transplantation0963-68971555-38922010-02-011910.3727/096368909X479848Hepatocyte Transplantation and the Differentiation Fate of Host Oval Cells in Acute Severe Hepatic InjuryChun-Hsien Yu0Mei-Hwei Chang1Chin-Sung Chien2Ya-Hui Chen3Ming-Fu Chang4Hui-Ling Chen Ph.D.5Department of Pediatrics, Buddhist Tzu-Chi General Hospital, Taipei Branch, and Buddhist Tzu-Chi University College of Medicine, Taipei, TaiwanHepatitis Research Center, National Taiwan University Hospital and National Taiwan University College of Medicine, Taipei, TaiwanHepatitis Research Center, National Taiwan University Hospital and National Taiwan University College of Medicine, Taipei, TaiwanHepatitis Research Center, National Taiwan University Hospital and National Taiwan University College of Medicine, Taipei, TaiwanGraduate Institute of Biochemistry and Molecular Biology, National Taiwan University Hospital and National Taiwan University College of Medicine, Taipei, TaiwanHepatitis Research Center, National Taiwan University Hospital and National Taiwan University College of Medicine, Taipei, TaiwanOval cells and hepatocytes rarely proliferate simultaneously. This study aimed to determine the impacts of hepatocyte transplantation on the response and fate of oval cells that are activated to proliferate in acute severe hepatic injury. Retrorsine + D-galactosamine (R+D-gal) treatment was used to induce acute hepatic injury and to elicit extensive activation of oval cells in male dipeptidyl peptidase IV-deficient F344 rats. These rats were then randomized to receive wild-type hepatocyte transplantation or vehicle intraportally. The kinetics of oval cell response and their differentiation fate were analyzed. Results showed that oval cells were activated early and differentiated into hepatocytes in R+D-gal-treated rats without hepatocyte transplantation. With hepatocyte transplantation, the oval cells were recruited later and continued to proliferate in parallel with the massive proliferation of transplanted hepatocytes. They formed ductules and differentiated into biliary cells. When hepatocytes were transplanted at the day when oval cells were at their peak response, the numerous activated oval cells ceased to differentiate into hepatocytes and remained in ductular form. The ductular oval cells were capable of differentiating into hepatocytes again when the donor hepatocytes were inhibited to proliferate. We conclude that hepatocyte transplantation changes the mechanism of liver reconstitution and affects the differentiation fate of host oval cells in acute severe hepatic injury.https://doi.org/10.3727/096368909X479848
collection DOAJ
language English
format Article
sources DOAJ
author Chun-Hsien Yu
Mei-Hwei Chang
Chin-Sung Chien
Ya-Hui Chen
Ming-Fu Chang
Hui-Ling Chen Ph.D.
spellingShingle Chun-Hsien Yu
Mei-Hwei Chang
Chin-Sung Chien
Ya-Hui Chen
Ming-Fu Chang
Hui-Ling Chen Ph.D.
Hepatocyte Transplantation and the Differentiation Fate of Host Oval Cells in Acute Severe Hepatic Injury
Cell Transplantation
author_facet Chun-Hsien Yu
Mei-Hwei Chang
Chin-Sung Chien
Ya-Hui Chen
Ming-Fu Chang
Hui-Ling Chen Ph.D.
author_sort Chun-Hsien Yu
title Hepatocyte Transplantation and the Differentiation Fate of Host Oval Cells in Acute Severe Hepatic Injury
title_short Hepatocyte Transplantation and the Differentiation Fate of Host Oval Cells in Acute Severe Hepatic Injury
title_full Hepatocyte Transplantation and the Differentiation Fate of Host Oval Cells in Acute Severe Hepatic Injury
title_fullStr Hepatocyte Transplantation and the Differentiation Fate of Host Oval Cells in Acute Severe Hepatic Injury
title_full_unstemmed Hepatocyte Transplantation and the Differentiation Fate of Host Oval Cells in Acute Severe Hepatic Injury
title_sort hepatocyte transplantation and the differentiation fate of host oval cells in acute severe hepatic injury
publisher SAGE Publishing
series Cell Transplantation
issn 0963-6897
1555-3892
publishDate 2010-02-01
description Oval cells and hepatocytes rarely proliferate simultaneously. This study aimed to determine the impacts of hepatocyte transplantation on the response and fate of oval cells that are activated to proliferate in acute severe hepatic injury. Retrorsine + D-galactosamine (R+D-gal) treatment was used to induce acute hepatic injury and to elicit extensive activation of oval cells in male dipeptidyl peptidase IV-deficient F344 rats. These rats were then randomized to receive wild-type hepatocyte transplantation or vehicle intraportally. The kinetics of oval cell response and their differentiation fate were analyzed. Results showed that oval cells were activated early and differentiated into hepatocytes in R+D-gal-treated rats without hepatocyte transplantation. With hepatocyte transplantation, the oval cells were recruited later and continued to proliferate in parallel with the massive proliferation of transplanted hepatocytes. They formed ductules and differentiated into biliary cells. When hepatocytes were transplanted at the day when oval cells were at their peak response, the numerous activated oval cells ceased to differentiate into hepatocytes and remained in ductular form. The ductular oval cells were capable of differentiating into hepatocytes again when the donor hepatocytes were inhibited to proliferate. We conclude that hepatocyte transplantation changes the mechanism of liver reconstitution and affects the differentiation fate of host oval cells in acute severe hepatic injury.
url https://doi.org/10.3727/096368909X479848
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