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Mitochondrial TNAP controls thermogenesis by hydrolysis of phosphocreatine

Author

Listed:
  • Yizhi Sun

    (Dana-Farber Cancer Institute
    Harvard Medical School)

  • Janane F. Rahbani

    (McGill University
    McGill University)

  • Mark P. Jedrychowski

    (Dana-Farber Cancer Institute
    Harvard Medical School)

  • Christopher L. Riley

    (Dana-Farber Cancer Institute
    Harvard Medical School)

  • Sara Vidoni

    (Dana-Farber Cancer Institute
    Harvard Medical School)

  • Dina Bogoslavski

    (Dana-Farber Cancer Institute)

  • Bo Hu

    (Dana-Farber Cancer Institute
    Harvard Medical School)

  • Phillip A. Dumesic

    (Dana-Farber Cancer Institute
    Harvard Medical School)

  • Xing Zeng

    (Dana-Farber Cancer Institute
    Harvard Medical School)

  • Alex B. Wang

    (Dana-Farber Cancer Institute
    Harvard Medical School)

  • Nelson H. Knudsen

    (Dana-Farber Cancer Institute
    Harvard Medical School)

  • Caroline R. Kim

    (Dana-Farber Cancer Institute)

  • Anthony Marasciullo

    (Dana-Farber Cancer Institute)

  • José L. Millán

    (Sanford Burnham Prebys Medical Discovery Institute)

  • Edward T. Chouchani

    (Dana-Farber Cancer Institute
    Harvard Medical School)

  • Lawrence Kazak

    (McGill University
    McGill University)

  • Bruce M. Spiegelman

    (Dana-Farber Cancer Institute
    Harvard Medical School)

Abstract

Adaptive thermogenesis has attracted much attention because of its ability to increase systemic energy expenditure and to counter obesity and diabetes1–3. Recent data have indicated that thermogenic fat cells use creatine to stimulate futile substrate cycling, dissipating chemical energy as heat4,5. This model was based on the super-stoichiometric relationship between the amount of creatine added to mitochondria and the quantity of oxygen consumed. Here we provide direct evidence for the molecular basis of this futile creatine cycling activity in mice. Thermogenic fat cells have robust phosphocreatine phosphatase activity, which is attributed to tissue-nonspecific alkaline phosphatase (TNAP). TNAP hydrolyses phosphocreatine to initiate a futile cycle of creatine dephosphorylation and phosphorylation. Unlike in other cells, TNAP in thermogenic fat cells is localized to the mitochondria, where futile creatine cycling occurs. TNAP expression is powerfully induced when mice are exposed to cold conditions, and its inhibition in isolated mitochondria leads to a loss of futile creatine cycling. In addition, genetic ablation of TNAP in adipocytes reduces whole-body energy expenditure and leads to rapid-onset obesity in mice, with no change in movement or feeding behaviour. These data illustrate the critical role of TNAP as a phosphocreatine phosphatase in the futile creatine cycle.

Suggested Citation

  • Yizhi Sun & Janane F. Rahbani & Mark P. Jedrychowski & Christopher L. Riley & Sara Vidoni & Dina Bogoslavski & Bo Hu & Phillip A. Dumesic & Xing Zeng & Alex B. Wang & Nelson H. Knudsen & Caroline R. K, 2021. "Mitochondrial TNAP controls thermogenesis by hydrolysis of phosphocreatine," Nature, Nature, vol. 593(7860), pages 580-585, May.
  • Handle: RePEc:nat:nature:v:593:y:2021:i:7860:d:10.1038_s41586-021-03533-z
    DOI: 10.1038/s41586-021-03533-z
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    Cited by:

    1. Yating Yu & Kewei Rong & Deqiang Yao & Qing Zhang & Xiankun Cao & Bing Rao & Ying Xia & Yi Lu & Yafeng Shen & Ying Yao & Hongtao Xu & Peixiang Ma & Yu Cao & An Qin, 2023. "The structural pathology for hypophosphatasia caused by malfunctional tissue non-specific alkaline phosphatase," Nature Communications, Nature, vol. 14(1), pages 1-14, December.
    2. Lu Jin & Shuang Han & Xue Lv & Xiaofei Li & Ziyin Zhang & Henry Kuang & Zhimin Chen & Cheng-an Lv & Wei Peng & Zhuoying Yang & Miqi Yang & Lin Mi & Tongyu Liu & Shengshan Ma & Xinyuan Qiu & Qintao Wan, 2023. "The muscle-enriched myokine Musclin impairs beige fat thermogenesis and systemic energy homeostasis via Tfr1/PKA signaling in male mice," Nature Communications, Nature, vol. 14(1), pages 1-23, December.

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