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肝血窦内皮细胞祖细胞促进大鼠肝脏再生。

Liver sinusoidal endothelial cell progenitor cells promote liver regeneration in rats.

机构信息

Division of Gastrointestinal and Liver Disease and University of Southern California Research Center for Liver Disease, Los Angeles, California 90033, USA.

出版信息

J Clin Invest. 2012 Apr;122(4):1567-73. doi: 10.1172/JCI58789. Epub 2012 Mar 12.

Abstract

The ability of the liver to regenerate is crucial to protect liver function after injury and during chronic disease. Increases in hepatocyte growth factor (HGF) in liver sinusoidal endothelial cells (LSECs) are thought to drive liver regeneration. However, in contrast to endothelial progenitor cells, mature LSECs express little HGF. Therefore, we sought to establish in rats whether liver injury causes BM LSEC progenitor cells to engraft in the liver and provide increased levels of HGF and to examine the relative contribution of resident and BM LSEC progenitors. LSEC label-retaining cells and progenitors were identified in liver and LSEC progenitors in BM. BM LSEC progenitors did not contribute to normal LSEC turnover in the liver. However, after partial hepatectomy, BM LSEC progenitor proliferation and mobilization to the circulation doubled. In the liver, one-quarter of the LSECs were BM derived, and BM LSEC progenitors differentiated into fenestrated LSECs. When irradiated rats underwent partial hepatectomy, liver regeneration was compromised, but infusion of LSEC progenitors rescued the defect. Further analysis revealed that BM LSEC progenitors expressed substantially more HGF and were more proliferative than resident LSEC progenitors after partial hepatectomy. Resident LSEC progenitors within their niche may play a smaller role in recovery from partial hepatectomy than BM LSEC progenitors, but, when infused after injury, these progenitors engrafted and expanded markedly over a 2-month period. In conclusion, LSEC progenitor cells are present in liver and BM, and recruitment of BM LSEC progenitors is necessary for normal liver regeneration.

摘要

肝脏的再生能力对于保护肝脏在损伤后和慢性疾病期间的功能至关重要。肝窦内皮细胞(LSEC)中肝细胞生长因子(HGF)的增加被认为驱动肝脏再生。然而,与内皮祖细胞不同,成熟的 LSEC 表达很少的 HGF。因此,我们在大鼠中试图确定肝损伤是否导致 BM LSEC 祖细胞在肝脏中定植,并提供增加的 HGF 水平,并检查驻留和 BM LSEC 祖细胞的相对贡献。在肝脏和 BM 中鉴定了 LSEC 标记保留细胞和祖细胞。BM LSEC 祖细胞不会促进肝脏中正常的 LSEC 转化。然而,在部分肝切除术后,BM LSEC 祖细胞增殖并向循环中动员增加了一倍。在肝脏中,四分之一的 LSEC 来源于 BM,BM LSEC 祖细胞分化为有孔 LSEC。当接受辐射的大鼠进行部分肝切除术后,肝脏再生受到损害,但 LSEC 祖细胞的输注挽救了这种缺陷。进一步分析表明,BM LSEC 祖细胞在部分肝切除术后表达的 HGF 显著增加,并且比驻留的 LSEC 祖细胞更具增殖能力。在其龛位内的驻留 LSEC 祖细胞在部分肝切除术后的恢复中可能发挥的作用小于 BM LSEC 祖细胞,但在损伤后输注时,这些祖细胞在 2 个月的时间内明显定植和扩增。总之,LSEC 祖细胞存在于肝脏和 BM 中,BM LSEC 祖细胞的募集对于正常的肝脏再生是必要的。

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