Self‐Renewal Capability of Hepatocytic Parental Progenitor Cells Derived From Adult Rat Liver Is Maintained Long Term When Cultured on Laminin 111 in Serum‐Free Medium

Self‐Renewal Capability of Hepatocytic Parental Progenitor Cells Derived From Adult Rat Liver Is Maintained Long Term When Cultured on Laminin 111 in Serum‐Free Medium

In this study, we investigated how the ability of hepatocytic parental progenitor cells (HPPCs) to self‐renew can be maintained and how laminin (LN) isoforms play an important role in their self‐renewal and maturation. Hepatocytes isolated from adult rat livers were cultured on hyaluronic acid to fo...

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Main Authors: Junichi Kino, Norihisa Ichinohe, Masayuki Ishii, Hiromu Suzuki, Toru Mizuguchi, Naoki Tanimizu, Toshihiro Mitaka
Format: Article
Language:English
Published: Wiley 2020-01-01
Series:Hepatology Communications
Online Access:https://doi.org/10.1002/hep4.1442
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spelling doaj-9a8dd347541b4e9e8270be2ff65b7efd2020-11-24T21:21:36ZengWileyHepatology Communications2471-254X2020-01-0141213710.1002/hep4.1442Self‐Renewal Capability of Hepatocytic Parental Progenitor Cells Derived From Adult Rat Liver Is Maintained Long Term When Cultured on Laminin 111 in Serum‐Free MediumJunichi Kino0Norihisa Ichinohe1Masayuki Ishii2Hiromu Suzuki3Toru Mizuguchi4Naoki Tanimizu5Toshihiro Mitaka6Department of Tissue Development and Regeneration Research Institute for Frontier Medicine Sapporo Medical University School of Medicine Sapporo JapanDepartment of Tissue Development and Regeneration Research Institute for Frontier Medicine Sapporo Medical University School of Medicine Sapporo JapanDepartment of Tissue Development and Regeneration Research Institute for Frontier Medicine Sapporo Medical University School of Medicine Sapporo JapanDepartment of Molecular Biology Sapporo Medical University School of Medicine Sapporo JapanDepartment of Surgery Surgical Oncology and Science Sapporo Medical University School of Medicine Sapporo JapanDepartment of Tissue Development and Regeneration Research Institute for Frontier Medicine Sapporo Medical University School of Medicine Sapporo JapanDepartment of Tissue Development and Regeneration Research Institute for Frontier Medicine Sapporo Medical University School of Medicine Sapporo JapanIn this study, we investigated how the ability of hepatocytic parental progenitor cells (HPPCs) to self‐renew can be maintained and how laminin (LN) isoforms play an important role in their self‐renewal and maturation. Hepatocytes isolated from adult rat livers were cultured on hyaluronic acid to form colonies consisting of CD44+ small hepatocytes, which could be passaged on dishes coated with Matrigel. When second‐passage cells were plated on Matrigel, LN111, or LN511, HPPCs appeared on Matrigel and LN111 but not on LN511. We identified two types of cells among the second‐passage cells: Small, round cells and large, flat ones were observed on Matrigel, whereas the former and latter ones were specifically attached on LN111 and LN511, respectively. We hypothesized that small and round cells are the origin of HPPC colonies, and the binding to LN111 could be key to maintaining their self‐renewal capability. Among the integrins involved in LN binding, integrins α3 and β1 were expressed in colonies on LN111 more than in those on LN511, whereas β4 was more strongly expressed in colonies on LN511. Integrin α3highα6β1high cells could form HPPC colonies on LN111 but not on LN511, whereas integrin α6β1low cells could not on either LN111 or LN511. In addition, neutralizing anti‐integrin β1 and anti‐LN111 antibodies inhibited the passaged cells’ ability to attach and form colonies on LN111 by HPPCs. Matrigel overlay induced second‐passage cells growing on LN111 to increase their expression of hepatic functional genes and to form 3‐dimensional colonies with bile canalicular networks, whereas such a shift was poorly induced when they were grown onLN511. Conclusion: These results suggest that the self‐renewal capability of HPPCs depends on LN111 through integrin β1 signaling.https://doi.org/10.1002/hep4.1442
collection DOAJ
language English
format Article
sources DOAJ
author Junichi Kino
Norihisa Ichinohe
Masayuki Ishii
Hiromu Suzuki
Toru Mizuguchi
Naoki Tanimizu
Toshihiro Mitaka
spellingShingle Junichi Kino
Norihisa Ichinohe
Masayuki Ishii
Hiromu Suzuki
Toru Mizuguchi
Naoki Tanimizu
Toshihiro Mitaka
Self‐Renewal Capability of Hepatocytic Parental Progenitor Cells Derived From Adult Rat Liver Is Maintained Long Term When Cultured on Laminin 111 in Serum‐Free Medium
Hepatology Communications
author_facet Junichi Kino
Norihisa Ichinohe
Masayuki Ishii
Hiromu Suzuki
Toru Mizuguchi
Naoki Tanimizu
Toshihiro Mitaka
author_sort Junichi Kino
title Self‐Renewal Capability of Hepatocytic Parental Progenitor Cells Derived From Adult Rat Liver Is Maintained Long Term When Cultured on Laminin 111 in Serum‐Free Medium
title_short Self‐Renewal Capability of Hepatocytic Parental Progenitor Cells Derived From Adult Rat Liver Is Maintained Long Term When Cultured on Laminin 111 in Serum‐Free Medium
title_full Self‐Renewal Capability of Hepatocytic Parental Progenitor Cells Derived From Adult Rat Liver Is Maintained Long Term When Cultured on Laminin 111 in Serum‐Free Medium
title_fullStr Self‐Renewal Capability of Hepatocytic Parental Progenitor Cells Derived From Adult Rat Liver Is Maintained Long Term When Cultured on Laminin 111 in Serum‐Free Medium
title_full_unstemmed Self‐Renewal Capability of Hepatocytic Parental Progenitor Cells Derived From Adult Rat Liver Is Maintained Long Term When Cultured on Laminin 111 in Serum‐Free Medium
title_sort self‐renewal capability of hepatocytic parental progenitor cells derived from adult rat liver is maintained long term when cultured on laminin 111 in serum‐free medium
publisher Wiley
series Hepatology Communications
issn 2471-254X
publishDate 2020-01-01
description In this study, we investigated how the ability of hepatocytic parental progenitor cells (HPPCs) to self‐renew can be maintained and how laminin (LN) isoforms play an important role in their self‐renewal and maturation. Hepatocytes isolated from adult rat livers were cultured on hyaluronic acid to form colonies consisting of CD44+ small hepatocytes, which could be passaged on dishes coated with Matrigel. When second‐passage cells were plated on Matrigel, LN111, or LN511, HPPCs appeared on Matrigel and LN111 but not on LN511. We identified two types of cells among the second‐passage cells: Small, round cells and large, flat ones were observed on Matrigel, whereas the former and latter ones were specifically attached on LN111 and LN511, respectively. We hypothesized that small and round cells are the origin of HPPC colonies, and the binding to LN111 could be key to maintaining their self‐renewal capability. Among the integrins involved in LN binding, integrins α3 and β1 were expressed in colonies on LN111 more than in those on LN511, whereas β4 was more strongly expressed in colonies on LN511. Integrin α3highα6β1high cells could form HPPC colonies on LN111 but not on LN511, whereas integrin α6β1low cells could not on either LN111 or LN511. In addition, neutralizing anti‐integrin β1 and anti‐LN111 antibodies inhibited the passaged cells’ ability to attach and form colonies on LN111 by HPPCs. Matrigel overlay induced second‐passage cells growing on LN111 to increase their expression of hepatic functional genes and to form 3‐dimensional colonies with bile canalicular networks, whereas such a shift was poorly induced when they were grown onLN511. Conclusion: These results suggest that the self‐renewal capability of HPPCs depends on LN111 through integrin β1 signaling.
url https://doi.org/10.1002/hep4.1442
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