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Metabolic profile and differentiation potential of extraembryonic endoderm-like cells

机译:胚外内胚层样细胞的代谢特征和分化潜能

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Glucose metabolism has a crucial role for providing substrates required to generate ATP and regulate the epigenetic landscape. We reported that F9 embryonal carcinoma stem-like cells require cytosolic reactive oxygen species to differentiate into extraembryonic endoderm; however, mitochondrial sources were not examined. To extend these studies, we examined the metabolic profile of early and late-passage F9 cells, and show that their ability to differentiate is similar, even though each population has dramatically different metabolic profiles. Differentiated early-passage cells relied on glycolysis, while differentiated late-passage cells transitioned towards oxidative phosphorylation (OXPHOS). Unexpectedly, electron transport chain protein stoichiometry was disrupted in differentiated late-passage cells, whereas genes encoding mitofusion 1 and 2, which promote mitochondrial fusion and favor OXPHOS, were upregulated in differentiated early-passage cells. Despite this, early-passage cells cultured under conditions to promote glycolysis showed enhanced differentiation, whereas promoting OXPHOS in late-passage cells showed a similar trend. Further analysis revealed that the distinct metabolic profiles seen between the two populations is largely associated with changes in genomic integrity, linking metabolism to passage number. Together, these results indicate that passaging has no effect on the potential for F9 cells to differentiate into extraembryonic endoderm; however, it does impact their metabolic profile. Thus, it is imperative to determine the molecular and metabolic status of a stem cell population before considering its utility as a therapeutic tool for regenerative medicine.
机译:葡萄糖代谢对于提供产生ATP和调节表观遗传环境所需的底物具有至关重要的作用。我们报道,F9胚胎癌干细胞样细胞需要胞质活性氧才能分化为胚外内胚层。但是,未检查线粒体来源。为了扩展这些研究,我们检查了早期和晚期传代F9细胞的代谢谱,并表明它们的分化能力相似,即使每个人群的代谢谱都大不相同。分化的早期传代细胞依赖于糖酵解,而分化的晚期传代细胞则向氧化磷酸化(OXPHOS)过渡。出乎意料的是,电子传递链蛋白的化学计量在分化的后代细胞中被破坏,而编码线粒体1和2的基因(促进线粒体融合并促进OXPHOS)在分化的早代细胞中被上调。尽管如此,在促进糖酵解的条件下培养的早期传代细胞显示出增强的分化,而在晚期传代细胞中促进OXPHOS表现出相似的趋势。进一步的分析表明,这两个种群之间观察到的独特的代谢谱与基因组完整性的改变在很大程度上相关,将代谢与传代次数相关联。总之,这些结果表明传代对F9细胞分化为胚外内胚层的可能性没有影响。但是,它确实会影响他们的新陈代谢。因此,在考虑将其用作再生医学的治疗工具之前,必须确定干细胞群体的分子和代谢状态。

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