Hepatocytic parental progenitor cells of rat small hepatocytes maintain self-renewal capability after long-term culture

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作者
Masayuki Ishii
Junichi Kino
Norihisa Ichinohe
Naoki Tanimizu
Takafumi Ninomiya
Hiromu Suzuki
Toru Mizuguchi
Koichi Hirata
Toshihiro Mitaka
机构
[1] Research Institute for Frontier Medicine,Department of Tissue Development and Regeneration
[2] Sapporo Medical University School of Medicine,Department of Surgery
[3] Surgical Oncology and Science,Department of Anatomy I
[4] Sapporo Medical University School of Medicine,Department of Molecular Biology
[5] Sapporo Medical University School of Medicine,undefined
[6] Tokushima Research Institute,undefined
[7] Otsuka Pharmaceutical Co. Ltd.,undefined
[8] Sapporo Medical University School of Medicine,undefined
[9] Sapporo Medical University School of Medicine,undefined
[10] Present address: JR Hokkaido Hospital,undefined
[11] North-3,undefined
[12] East-1,undefined
[13] Chuo-ku,undefined
[14] Sapporo 060-0033,undefined
[15] Japan.,undefined
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摘要
The liver has a variety of functions for maintaining homeostasis, and hepatocytes play a major role. In contrast with the high regenerative capacity of mature hepatocytes (MHs) in vivo, they have not been successfully expanded ex vivo. Here we demonstrate that CD44-positive cells sorted from small hepatocyte (SH) colonies derived from a healthy adult rat liver can proliferate on a Matrigel-coated dish in serum-free chemically defined medium; in addition, a subpopulation of the cells can divide more than 50 times in a period of 17 weeks every 4-week-passage. The passage cells retained the capability to recover highly differentiated functions, such as glycogen storage, CYP activity and bile secretion. When Matrigel-treated cells from the third passage were transplanted into retrorsine/partial hepatectomy-treated rat livers, the cells engrafted to differentiate into MHs and cholangiocytes. These results suggest that long-term cultured CD44+ SHs retain hepatocytic characteristics in vitro and the capability to differentiate into hepatocytes and cholangiocytes in vivo. Thus, a newly identified subpopulation of MHs possessing the attributes of hepatocytic stem/progenitor cells can be passaged several times without losing hepatocytic characteristics.
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