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Transformation of human mesenchymal stem cells increases their dependency on oxidative phosphorylation for energy production

机译:人间充质干细胞的转化增加了其对氧化磷酸化的依赖性,以产生能量

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An increased dependency on glycolysis for ATP production is considered to be a hallmark of tumor cells. Whether this increase in glycolytic activity is due mainly to inherent metabolic alterations or to the hypoxic microenvironment remains controversial. Here we have transformed human adult mesenchymal stem cells (MSC) using genetic alterations as described for differentiated cells. Our data suggest that MSC require disruption of the same pathways as have been shown for differentiated cells to confer a fully transformed phenotype. Furthermore, we found that MSC are more glycolytic than primary human fibroblasts and, in contrast to differentiated cells, do not depend on increased aerobic glycolysis for ATP production during transformation. These data indicate that aerobic glycolysis (the Warburg effect) is not an intrinsic component of the transformation of adult stem cells, and that oncogenic adaptation to bioenergetic requirements, in some circumstances, may also rely on increases in oxidative phosphorylation. We did find, however, a reversible increase in the transcription of glycolytic enzymes in tumors generated by transformed MSC, indicating this is a secondary phenomenon resulting from adaptation of the tumor to its microenvironment.
机译:ATP产生对糖酵解的依赖性增加被认为是肿瘤细胞的标志。糖酵解活性的增加是否主要是由于固有的代谢改变还是由于低氧的微环境而引起争议。在这里,我们已经使用针对分化细胞的基因改变方法,转化了人类成年间充质干细胞(MSC)。我们的数据表明,MSC需要破坏与分化细胞相同的途径,以赋予其完全转化的表型。此外,我们发现MSC比原代人成纤维细胞更具糖酵解作用,与分化的细胞相比,MSC在转化过程中不依赖增加需氧糖酵解来产生ATP。这些数据表明,有氧糖酵解(Warburg效应)不是成体干细胞转化的内在成分,并且在某些情况下,对生物能需求的致癌适应性也可能依赖于氧化磷酸化的增加。然而,我们确实发现,转化的MSC产生的肿瘤中糖酵解酶的转录可逆地增加,表明这是由于肿瘤适应其微环境而引起的继发现象。

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