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从成年健康小鼠肝脏分离出的肝祖细胞在体外能有效分化为功能性肝细胞并重新填充肝组织。

Liver Progenitors Isolated from Adult Healthy Mouse Liver Efficiently Differentiate to Functional Hepatocytes In Vitro and Repopulate Liver Tissue.

作者信息

Tanimizu Naoki, Ichinohe Norihisa, Ishii Masayuki, Kino Junichi, Mizuguchi Toru, Hirata Koichi, Mitaka Toshihiro

机构信息

Department of Tissue Development and Regeneration, Research Institute for Frontier Medicine, Sapporo Medical University School of Medicine, Sapporo, Japan.

Department of Surgery, Surgical Oncology and Science, Sapporo Medical University School of Medicine, Sapporo, Japan.

出版信息

Stem Cells. 2016 Dec;34(12):2889-2901. doi: 10.1002/stem.2457. Epub 2016 Jul 13.

DOI:10.1002/stem.2457
PMID:27375002
Abstract

It has been proposed that tissue stem cells supply multiple epithelial cells in mature tissues and organs. However, it is unclear whether tissue stem cells generally contribute to cellular turnover in normal healthy organs. Here, we show that liver progenitors distinct from bipotent liver stem/progenitor cells (LPCs) persistently exist in mouse livers and potentially contribute to tissue maintenance. We found that, in addition to LPCs isolated as EpCAM cells, liver progenitors were enriched in CD45 TER119 CD31 EpCAM ICAM-1 fraction isolated from late-fetal and postnatal livers. ICAM-1 liver progenitors were abundant by 4 weeks (4W) after birth. Although their number decreased with age, ICAM-1 liver progenitors existed in livers beyond that stage. We established liver progenitor clones derived from ICAM-1 cells between 1 and 20W and found that those clones efficiently differentiated into mature hepatocytes (MHs), which secreted albumin, eliminated ammonium ion, stored glycogen, and showed cytochrome P450 activity. Even after long-term culture, those clones kept potential to differentiate to MHs. When ICAM-1 clones were transplanted into nude mice after retrorsine treatment and 70% partial hepatectomy, donor cells were incorporated into liver plates and expressed hepatocyte nuclear factor 4α, CCAAT/enhancer binding protein α, and carbamoylphosphate synthetase I. Moreover, after short-term treatment with oncostatin M, ICAM-1 clones could efficiently repopulate the recipient liver tissues. Our results indicate that liver progenitors that can efficiently differentiate to MHs exist in normal adult livers. Those liver progenitors could be an important source of new MHs for tissue maintenance and repair in vivo, and for regenerative medicine ex vivo. Stem Cells 2016;34:2889-2901.

摘要

有人提出,组织干细胞为成熟组织和器官提供多种上皮细胞。然而,尚不清楚组织干细胞是否通常参与正常健康器官的细胞更新。在此,我们表明,与双能肝干细胞/祖细胞(LPCs)不同的肝祖细胞持续存在于小鼠肝脏中,并可能有助于组织维持。我们发现,除了作为EpCAM细胞分离的LPCs外,肝祖细胞在从晚期胎儿和出生后肝脏分离的CD45 TER119 CD31 EpCAM ICAM-1组分中富集。出生后4周(4W)时,ICAM-1肝祖细胞数量丰富。尽管其数量随年龄增长而减少,但ICAM-1肝祖细胞在该阶段之后仍存在于肝脏中。我们建立了源自1至20W的ICAM-1细胞的肝祖细胞克隆,发现这些克隆能有效地分化为成熟肝细胞(MHs),这些成熟肝细胞分泌白蛋白、消除铵离子、储存糖原并显示细胞色素P450活性。即使经过长期培养,这些克隆仍保持分化为MHs的潜能。当将ICAM-1克隆在经倒千里光碱处理和70%部分肝切除后移植到裸鼠中时,供体细胞被整合到肝板中,并表达肝细胞核因子4α、CCAAT/增强子结合蛋白α和氨甲酰磷酸合成酶I。此外,在用制瘤素M进行短期处理后,ICAM-1克隆能够有效地重新填充受体肝脏组织。我们的结果表明,正常成年肝脏中存在能够有效分化为MHs的肝祖细胞。这些肝祖细胞可能是体内组织维持和修复以及体外再生医学中新MHs的重要来源。《干细胞》2016年;34:2889 - 2901。

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