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人胚胎干细胞神经分化时,ATP 需求和线粒体活性降低。

A reduction in ATP demand and mitochondrial activity with neural differentiation of human embryonic stem cells.

机构信息

Buck Institute for Age Research, 8001 Redwood Blvd, Novato, CA 94945, USA.

出版信息

J Cell Sci. 2011 Feb 1;124(Pt 3):348-58. doi: 10.1242/jcs.072272.

Abstract

Here, we have investigated mitochondrial biology and energy metabolism in human embryonic stem cells (hESCs) and hESC-derived neural stem cells (NSCs). Although stem cells collectively in vivo might be expected to rely primarily on anaerobic glycolysis for ATP supply, to minimise production of reactive oxygen species, we show that in vitro this is not so: hESCs generate an estimated 77% of their ATP through oxidative phosphorylation. Upon differentiation of hESCs into NSCs, oxidative phosphorylation declines both in absolute rate and in importance relative to glycolysis. A bias towards ATP supply from oxidative phosphorylation in hESCs is consistent with the expression levels of the mitochondrial gene regulators peroxisome-proliferator-activated receptor γ coactivator (PGC)-1α, PGC-1β and receptor-interacting protein 140 (RIP140) in hESCs when compared with a panel of differentiated cell types. Analysis of the ATP demand showed that the slower ATP turnover in NSCs was associated with a slower rate of most energy-demanding processes but occurred without a reduction in the cellular growth rate. This mismatch is probably explained by a higher rate of macromolecule secretion in hESCs, on the basis of evidence from electron microscopy and an analysis of conditioned media. Taken together, our developmental model provides an understanding of the metabolic transition from hESCs to more quiescent somatic cell types, and supports important roles for mitochondria and secretion in hESC biology.

摘要

在这里,我们研究了人类胚胎干细胞(hESC)和 hESC 衍生的神经干细胞(NSC)中的线粒体生物学和能量代谢。尽管人们可能期望体内的干细胞主要依赖无氧糖酵解来提供 ATP,以最小化活性氧物质的产生,但我们表明,在体外并非如此:hESC 通过氧化磷酸化产生估计 77%的 ATP。在 hESC 分化为 NSC 后,氧化磷酸化无论是绝对速率还是相对于糖酵解的重要性都下降了。hESC 中偏向于氧化磷酸化提供 ATP 与线粒体基因调节剂过氧化物酶体增殖物激活受体 γ 共激活因子(PGC)-1α、PGC-1β 和受体相互作用蛋白 140(RIP140)在 hESC 中的表达水平相对于一组分化细胞类型相一致。对 ATP 需求的分析表明,NSC 中较慢的 ATP 周转率与大多数能量需求过程的较慢速率有关,但细胞生长速率没有降低。这种不匹配可能是由于 hESC 中大分子分泌的速度较快,这是基于电子显微镜和条件培养基分析的证据。总之,我们的发育模型提供了对 hESC 向更静止的体细胞类型代谢转变的理解,并支持线粒体和分泌在 hESC 生物学中的重要作用。

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