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肝细胞生长因子/细胞表面分化抗原 Mesenchymal-epithelial transition factor 信号对于移植肝细胞的选择很重要。

Hepatocyte growth factor/c-Met signalling is important for the selection of transplanted hepatocytes.

机构信息

Department of Medicine III, RWTH Aachen University, Aachen, Germany.

出版信息

Gut. 2012 Aug;61(8):1209-18. doi: 10.1136/gutjnl-2011-301345. Epub 2012 Jan 27.

DOI:10.1136/gutjnl-2011-301345
PMID:22287599
Abstract

BACKGROUND

At present hepatocyte transplantation is a promising option for cellular therapy of end-stage liver diseases. However, the underlying molecular mechanisms need to be better defined in order to translate this technique into clinical use. This study investigated the cursiv relevance of hepatocyte growth factor (HGF)/c-Met signalling for hepatocyte repopulation after transplantion.

METHODS

Wild-type mice (c-Met(loxP/loxP)) and hepatocyte-specific conditional c-Met (HGF receptor) knockout (c-Met(Δhepa)) mice were used as donors and recipients for hepatocyte transplantation.

RESULTS

Transplantation experiments revealed two major findings. First it was demonstrated that c-Met is indispensable in donor cells, as c-Met(Δhepa) cells did not repopulate recipient livers after transplantation. Second, genetic deletion of c-Met in recipient hepatocytes resulted in enhanced expansion of unmodified donor cells in host livers (up to 250-fold after 12 weeks). The relevant mechanisms for this observation in c-Met(Δhepa) host hepatocytes could be defined. c-Met(Δhepa) hepatocytes showed enhanced apoptosis, reduced cellular proliferation and a lack of AKT-kinase and STAT3 activation. In addition, tissue remodelling was changed in c-Met(Δhepa) recipient livers. Therefore, the lack of pro-proliferative transcription factors, increased apoptosis and changes in matrix-remodelling inhibit host cell proliferation in c-Met(Δhepa) recipient livers and thus favour repopulation of transplanted hepatocytes. Therapeutically liver repopulation could be increased through adenoviral expression of NK-4--an inhibitor of HGF signalling--in host hepatocytes.

CONCLUSION

HGF/c-Met plays a crucial role in host and donor cells of the liver for the cursiv selection of transplanted hepatocytes. Modulating HGF-dependent signalling seems a promising therapeutic option to favour expansion of transplanted hepatocytes.

摘要

背景

目前,肝细胞移植是治疗终末期肝病的细胞疗法的一种很有前途的选择。然而,为了将这项技术转化为临床应用,需要更好地定义其潜在的分子机制。本研究调查了肝细胞生长因子(HGF)/c-Met 信号对移植后肝细胞再增殖的影响。

方法

野生型小鼠(c-Met(loxP/loxP))和肝细胞特异性条件性 c-Met(HGF 受体)敲除(c-Met(Δhepa))小鼠分别作为供体和受体进行肝细胞移植。

结果

移植实验揭示了两个主要发现。首先,证明 c-Met 在供体细胞中是不可或缺的,因为 c-Met(Δhepa)细胞在移植后不能再增殖受体肝脏。其次,在受体肝细胞中基因敲除 c-Met 导致未修饰供体细胞在宿主肝脏中大量扩增(12 周后可达 250 倍)。可以定义 c-Met(Δhepa)宿主肝细胞中观察到的这种现象的相关机制。c-Met(Δhepa)肝细胞表现出增强的细胞凋亡、降低的细胞增殖以及 AKT 激酶和 STAT3 激活的缺失。此外,c-Met(Δhepa)受体肝脏的组织重塑也发生了改变。因此,缺乏促增殖转录因子、细胞凋亡增加和基质重塑改变抑制了 c-Met(Δhepa)受体肝脏中宿主细胞的增殖,从而有利于移植肝细胞的再增殖。通过在宿主肝细胞中表达腺病毒 NK-4(HGF 信号的抑制剂)可以增加肝的再增殖。

结论

HGF/c-Met 在供体和受体肝细胞中对移植肝细胞的选择起着至关重要的作用。调节 HGF 依赖性信号似乎是一种很有前途的治疗选择,可以促进移植肝细胞的扩增。

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