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Distinct Metabolic States Can Support Self-Renewal and Lipogenesis in Human Pluripotent Stem Cells under Different Culture Conditions

机译:不同的代谢状态可以支持人多能干细胞在不同培养条件下的自我更新和脂肪生成。

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Recent studies have suggested that human pluripotent stem cells (hPSCs) depend primarily on glycolysis and only increase oxidative metabolism during differentiation. Here, we demonstrate that both glycolytic and oxidative metabolism can support hPSC growth and that the metabolic phenotype of hPSCs is largely driven by nutrient availability. We comprehensively characterized hPSC metabolism by using ^1^3C/^2H stable isotope tracing and flux analysis to define the metabolic pathways supporting hPSC bioenergetics and biosynthesis. Although glycolytic flux consistently supported hPSC growth, chemically defined media strongly influenced the state of mitochondrial respiration and fatty acid metabolism. Lipid deficiency dramatically reprogramed pathways associated with fatty acid biosynthesis and NADPH regeneration, altering the mitochondrial function of cells and driving flux through the oxidative pentose phosphate pathway. Lipid supplementation mitigates this metabolic reprogramming and increases oxidative metabolism. These results demonstrate that self-renewing hPSCs can present distinct metabolic states and highlight the importance of medium nutrients on mitochondrial function and development.
机译:最近的研究表明,人类多能干细胞(hPSC)主要依赖于糖酵解,并且仅在分化过程中增加氧化代谢。在这里,我们证明糖酵解和氧化代谢都可以支持hPSC的生长,hPSCs的代谢表型很大程度上受养分利用率的驱动。我们通过使用^ 1 ^ 3C / ^ 2H稳定同位素示踪和通量分析来全面表征hPSC代谢,以定义支持hPSC生物能和生物合成的代谢途径。尽管糖酵解通量始终支持hPSC的生长,但化学定义的培养基强烈影响线粒体呼吸和脂肪酸代谢的状态。血脂不足会严重地重新编程与脂肪酸生物合成和NADPH再生有关的途径,从而改变细胞的线粒体功能并驱动氧化戊糖磷酸途径的通量。脂质补充减轻了这种代谢重编程并增加了氧化代谢。这些结果表明,自我更新的hPSC可以呈现独特的代谢状态,并突出了中等营养素对线粒体功能和发育的重要性。

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