Literature DB >> 16501859

Characteristics of rat bone marrow cells differentiated into a liver cell lineage and dynamics of the transplanted cells in the injured liver.

Kazuo Okumoto1, Takafumi Saito, Hiroaki Haga, Etsuko Hattori, Rika Ishii, Tetsuru Karasawa, Akihiko Suzuki, Keiko Misawa, Mai Sanjo, Jun-itsu Ito, Kazuhiko Sugahara, Koji Saito, Hitoshi Togashi, Sumio Kawata.   

Abstract

BACKGROUND: Bone marrow cells (BMCs) have been shown to differentiate into a liver cell lineage, but little is known about their dynamics following transplantation. BMCs were cultured to investigate the expression of liver-specific genes in vitro and transplanted into in vivo liver-injury models to elucidate their dynamics in the liver.
METHODS: The mRNA expression of various liver-specific genes in BMCs cocultured with hepatocytes was analyzed using reverse transcription-polymerase chain reaction. BMCs from transgenic rats expressing green fiuorescent protein were transplanted into the spleen of rat liver-injury models induced with 2-acetylaminofiuorene (2-AAF) or carbon tetrachloride (CCl4). BMCs were also transplanted directly into livers treated with CCl4 to determine which route is better for transplantation.
RESULTS: BMCs differentiated into a liver cell lineage in vitro and expressed mRNAs consistent with mature hepatocytes, including albumin. The transplanted BMCs were found in the liver in the CCl4-induced injury model, but not in the 2-AAF-induced model. The hepatocyte growth factor and fibroblast growth factor mRNA levels in the liver were significantly higher in the CCl4-induced model than in the 2-AAF-induced model. Migration of BMCs to the liver was more effective following injection into the liver, rather than into the spleen.
CONCLUSIONS: Cultured BMCs differentiated into a liver cell lineage are a potential source for cell transplantation. Transplantation is successful in the severely injured liver with a high level of expression of mRNAs for growth factors. Injection of BMCs directly into the liver is the preferred route of administration.

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Year:  2006        PMID: 16501859     DOI: 10.1007/s00535-005-1723-8

Source DB:  PubMed          Journal:  J Gastroenterol        ISSN: 0944-1174            Impact factor:   7.527


  36 in total

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3.  Improved conditions to induce hepatocytes from rat bone marrow cells in culture.

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4.  A subpopulation of bone marrow cells depleted by a novel antibody, anti-Liv8, is useful for cell therapy to repair damaged liver.

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9.  Differentiation of bone marrow cells into cells that express liver-specific genes in vitro: implication of the Notch signals in differentiation.

Authors:  Kazuo Okumoto; Takafumi Saito; Etsuko Hattori; Jun-itsu Ito; Tohru Adachi; Tadashi Takeda; Kazuhiko Sugahara; Hisayoshi Watanabe; Koji Saito; Hitoshi Togashi; Sumio Kawata
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10.  Growth and maturation of small hepatocytes isolated from adult rat liver.

Authors:  T Mitaka; T Kojima; T Mizuguchi; Y Mochizuki
Journal:  Biochem Biophys Res Commun       Date:  1995-09-14       Impact factor: 3.575

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  6 in total

1.  Clinical application of bone marrow cell transplantation for liver diseases.

Authors:  Isao Sakaida
Journal:  J Gastroenterol       Date:  2006-01       Impact factor: 7.527

Review 2.  Bone marrow cell-based regenerative therapy for liver cirrhosis.

Authors:  Takafumi Saito; Kyoko Tomita; Hiroaki Haga; Kazuo Okumoto; Yoshiyuki Ueno
Journal:  World J Methodol       Date:  2013-12-26

3.  Surface markers of liver cancer stem cells and innovative targeted-therapy strategies for HCC.

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4.  Proliferation of L02 human hepatocytes in tolerized genetically immunocompetent rats.

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5.  Murine Sca1(+)Lin(-) bone marrow contains an endodermal precursor population that differentiates into hepatocytes.

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6.  Autologous Stem Cells Transplantation in Egyptian Patients with Liver Cirrhosis on Top of Hepatitis C Virus.

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  6 in total

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