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Human mesenchymal stem cell-engineered hepatic cell sheets accelerate liver regeneration in mice

机译:人间充质干细胞工程化的肝细胞片促进小鼠肝脏再生

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Mesenchymal stem cells (MSCs) are an attractive cell source for cell therapy. Based on our hypothesis that suppression of Wnt/β-catenin signal enhances hepatic differentiation of human MSCs, we developed human mesenchymal stem cell-engineered hepatic cell sheets by a small molecule compound. Screening of 10 small molecule compounds was performed by WST assay, TCF reporter assay, and albumin mRNA expression. Consequently, hexachlorophene suppressed TCF reporter activity in time- and concentration-dependent manner. Hexachlorophene rapidly induced hepatic differentiation of human MSCs judging from expression of liver-specific genes and proteins, PAS staining, and urea production. The effect of orthotopic transplantation of human mesenchymal stem cell-engineered hepatic cell sheets against acute liver injury was examined in one-layered to three-layered cell sheets system. Transplantation of human mesenchymal stem cell-engineered hepatic cell sheets enhanced liver regeneration and suppressed liver injury. The survival rates of the mice were significantly improved. High expression of complement C3 and its downstream signals including C5a, NF-κB, and IL-6/STAT-3 pathway was observed in hepatic cell sheets-grafted tissues. Expression of phosphorylated EGFR and thioredoxin is enhanced, resulting in reduction of oxidative stress. These findings suggest that orthotopic transplantation of hepatic cell sheets manufactured from MSCs accelerates liver regeneration through complement C3, EGFR and thioredoxin.
机译:间充质干细胞(MSC)是用于细胞治疗的有吸引力的细胞来源。基于我们的Wnt /β-catenin信号抑制作用增强人类MSC肝分化的假设,我们通过小分子化合物开发了人类间充质干细胞工程化的肝细胞片。通过WST分析,TCF报告基因分析和白蛋白mRNA表达进行10种小分子化合物的筛选。因此,六氯酚以时间和浓度依赖性方式抑制了TCF报告基因的活性。从肝特异性基因和蛋白质的表达,PAS染色和尿素生产来看,六氯酚可迅速诱导人MSC的肝分化。在一层到三层细胞片系统中检查了人间充质干细胞工程化的肝细胞片原位移植对急性肝损伤的作用。人间充质干细胞工程化的肝细胞片的移植增强肝脏再生并抑制肝损伤。小鼠的存活率显着提高。在肝细胞片移植组织中观察到补体C3及其下游信号(包括C5a,NF-κB和IL-6 / STAT-3途径)的高表达。磷酸化的EGFR和硫氧还蛋白的表达增强,从而降低了氧化应激。这些发现表明,由MSC制造的肝细胞片原位移植通过补体C3,EGFR和硫氧还蛋白促进了肝再生。

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