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利用制备性部分肝照射和生长刺激物在体内构建肝组织:对微创技术和祖细胞的研究。

Construction of liver tissue in vivo with preparative partial hepatic irradiation and growth stimulus: investigations of less invasive techniques and progenitor cells.

机构信息

Department of Surgery, Nagasaki University Graduate School of Biomedical Sciences, Nagasaki, Japan.

出版信息

J Surg Res. 2013 Dec;185(2):889-95. doi: 10.1016/j.jss.2013.06.016. Epub 2013 Jun 29.

DOI:10.1016/j.jss.2013.06.016
PMID:23845872
Abstract

BACKGROUND

The selective proliferation of transplanted hepatocytes with a growth stimulus, such as partial hepatectomy or hepatocyte growth factor, concomitant with hepatic irradiation (HIR), which can suppress proliferation of host hepatocytes, has been reported. We have conducted experiments that focused on less invasive and clinically applicable techniques and progenitor cells.

MATERIALS AND METHODS

First, dipeptidyl-peptidase IV-F344 or jaundiced Gunn rats underwent partial HIR (only 30% of whole liver) and portal vein branch ligation (PVBL) of one lobe, followed by intrasplenic hepatocyte transplantation at 1 × 10(7). Second, after partial HIR and PVBL, two types of progenitor cells were transplanted (i.e., small hepatocytes (SHs) or adipose-derived mesenchymal stem cells.

RESULTS

Sixteen weeks after transplantation, the donor cells constituted > 70% of the hepatocytes of the irradiated lobe, showing connexin 32, phosphoenolpyruvate carboxykinase-1, and glycogen storage. Moreover, the serum bilirubin level had decreased significantly in the jaundiced Gunn rats and remained at this level throughout the 24 wk experimental period. The SHs grew more quickly than the hepatocytes. After 8 wk, around 40% of the host hepatocytes had been replaced by transplanted SHs. Although the donor adipose-derived mesenchymal cells were engrafted after 8 wk, their proliferation was not observed.

CONCLUSIONS

HIR, combined with PVBL, can be given to a selective liver lobe and is a less-invasive but effective method for proliferation of transplanted hepatocytes. Even a smaller number of SHs can construct liver tissue with their prevailing proliferative ability.

摘要

背景

已报道,在肝照射(HIR)的同时,使用生长刺激物(如部分肝切除术或肝细胞生长因子)选择性增殖移植的肝细胞,HIR 可抑制宿主肝细胞的增殖。我们进行了专注于微创且临床适用的技术和祖细胞的实验。

材料与方法

首先,二肽基肽酶 IV-F344 或黄疸 Gunn 大鼠接受部分 HIR(仅为整个肝脏的 30%)和一叶门静脉分支结扎(PVBL),然后经脾内移植 1×10(7)个肝细胞。其次,在进行部分 HIR 和 PVBL 后,移植两种类型的祖细胞(即小肝细胞(SHs)或脂肪间充质干细胞)。

结果

移植后 16 周,供体细胞构成照射叶肝细胞的>70%,表现出连接蛋白 32、磷酸烯醇丙酮酸羧激酶-1 和糖原储存。此外,黄疸 Gunn 大鼠的血清胆红素水平显著降低,并在整个 24 周实验期间保持在此水平。SHs 的生长速度比肝细胞快。8 周后,约 40%的宿主肝细胞被移植的 SHs 取代。尽管供体脂肪间充质细胞在 8 周后被植入,但未观察到其增殖。

结论

HIR 联合 PVBL 可用于选择性肝叶,是一种微创但有效的促进移植肝细胞增殖的方法。即使是少量的 SHs 也可以利用其增殖能力构建肝组织。

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