Metabolic regulation of species-specific developmental rates

被引:0
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作者
Margarete Diaz-Cuadros
Teemu P. Miettinen
Owen S. Skinner
Dylan Sheedy
Carlos Manlio Díaz-García
Svetlana Gapon
Alexis Hubaud
Gary Yellen
Scott R. Manalis
William M. Oldham
Olivier Pourquié
机构
[1] Harvard Medical School,Department of Genetics
[2] Brigham and Women’s Hospital,Department of Pathology
[3] Massachusetts Institute of Technology,Koch Institute for Integrative Cancer Research
[4] Massachusetts General Hospital,Department of Molecular Biology
[5] Harvard Medical School,Department of Systems Biology
[6] Broad Institute,Department of Neurobiology
[7] Harvard Medical School,Department of Biological Engineering
[8] Massachusetts Institute of Technology,Department of Mechanical Engineering
[9] Massachusetts Institute of Technology,Department of Medicine
[10] Harvard Medical School,Department of Medicine
[11] Brigham and Women’s Hospital,Harvard Stem Cell Institute
[12] Harvard University,Department of Molecular Biology
[13] Massachusetts General Hospital,Department of Biochemistry and Molecular Biology
[14] University of Oklahoma Health Sciences Center,undefined
来源
Nature | 2023年 / 613卷
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摘要
Animals display substantial inter-species variation in the rate of embryonic development despite a broad conservation of the overall sequence of developmental events. Differences in biochemical reaction rates, including the rates of protein production and degradation, are thought to be responsible for species-specific rates of development1–3. However, the cause of differential biochemical reaction rates between species remains unknown. Here, using pluripotent stem cells, we have established an in vitro system that recapitulates the twofold difference in developmental rate between mouse and human embryos. This system provides a quantitative measure of developmental speed as revealed by the period of the segmentation clock, a molecular oscillator associated with the rhythmic production of vertebral precursors. Using this system, we show that mass-specific metabolic rates scale with the developmental rate and are therefore higher in mouse cells than in human cells. Reducing these metabolic rates by inhibiting the electron transport chain slowed down the segmentation clock by impairing the cellular NAD+/NADH redox balance and, further downstream, lowering the global rate of protein synthesis. Conversely, increasing the NAD+/NADH ratio in human cells by overexpression of the Lactobacillus brevis NADH oxidase LbNOX increased the translation rate and accelerated the segmentation clock. These findings represent a starting point for the manipulation of developmental rate, with multiple translational applications including accelerating the differentiation of human pluripotent stem cells for disease modelling and cell-based therapies.
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页码:550 / 557
页数:7
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    [J]. NATURE, 2023, 613 (7944) : 550 - 557
  • [2] Author Correction: Metabolic regulation of species-specific developmental rates
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