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首页> 外文期刊>Differentiation: The Journal of the International Society of Differentiation >Metabolomic profiling during the differentiation of human induced pluripotent stem cells into hepatocyte-like cells
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Metabolomic profiling during the differentiation of human induced pluripotent stem cells into hepatocyte-like cells

机译:将人诱导多能干细胞分化到肝细胞样细胞中的代谢物分析

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Human induced pluripotent stem cells (hiPSCs) are potentially an invaluable source of cells for regenerative medicine, disease modeling and drug discovery. However, the differentiation of hiPSCs into fully functional hepatocytes remains a major challenge. Despite the importance of the information carried by metabolomes, the exploitation of metabolomics for characterizing and understanding hiPSC differentiation remains largely unexplored. Here, to increase knowledge of hiPSC maturation into mature hepatocytes, we investigated their metabolomics profiles during sequential step-by-step differentiation: definitive endoderm (DE), specification into hepatocytes (HB-pro (hepatoblast progenitors)), progenitor hepatocytes (Pro-HEP) and mature hepatocytelike cells (HLCs). Metabolomics analysis illustrated a switch from glycolysis-based respiration in DE step to oxidative phosphorylation in HLCs step. DE was characterized by fatty acid beta oxidation, sorbitol metabolism and pentose phosphate pathway, and glutamine and glucose metabolisms as various potential energy sources. The complex lipid metabolism switch was monitored via the reduction of lipid production from DE to HLCs step, whereas high glycerol production occurred mainly in HLCs. The nitrogen cycle, via urea production, was also a typical mechanism revealed in HLCs step. Our analysis may contribute to better understanding of differentiation and suggest new targets for improving iPSC maturation into functional hepatocytes.
机译:人类诱导多能干细胞(HIPSC)可能是用于再生医学,疾病建模和药物发现的无价细胞来源。然而,HIPSC分化为全功能性肝细胞仍然是一个重大挑战。尽管代谢物携带的信息的重要性,但代谢组织的剥削率仍然很大程度上是未开发的。在这里,为了将HIPSC成熟的知识增加到成熟的肝细胞中,我们在顺序逐步分化期间调查了它们的代谢组科谱:将确定的内胚层(DE),规范成肝细胞(HB-Pro(肝细胞祖)),祖肝肝细胞(Pro- HEP)和成熟的肝细胞般细胞(HLC)。代谢组科分析说明了在步骤中从基于糖酵解的呼吸的切换到HLCS步骤中的氧化磷酸化。 DE的特征在于脂肪酸β氧化,山梨糖醇代谢和磷酸磷酸途径,以及谷氨酰胺和葡萄糖代谢作为各种潜在的能源。通过从DE至HLCS步骤的降低脂质生产来监测复合脂质代谢开关,而高甘油生产主要是HLC。通过尿素产生,氮循环也是HLCS步骤中揭示的典型机制。我们的分析可能有助于更好地理解分化,并建议将IPSC成熟改善为功能性肝细胞的新靶标。

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