UCP1-independent signaling involving SERCA2b-mediated calcium cycling regulates beige fat thermogenesis and systemic glucose homeostasis.
| Citation | Ikeda, Kenji, et al. “UCP1-Independent Signaling Involving SERCA2b-Mediated Calcium Cycling Regulates Beige Fat Thermogenesis and Systemic Glucose Homeostasis”. 2017. Nature Medicine, vol. 23, no. 12, 2017, pp. 1454–1465.  | 
       
| Center | UCSF | 
| Author | Kenji Ikeda, Qianqian Kang, Takeshi Yoneshiro, Joao Paulo Camporez, Hiroko Maki, Mayu Homma, Kosaku Shinoda, Yong Chen, Xiaodan Lu, Pema Maretich, Kazuki Tajima, Kolapo M Ajuwon, Tomoyoshi Soga, Shingo Kajimura | 
| Abstract | 
   Uncoupling protein 1 (UCP1) plays a central role in nonshivering thermogenesis in brown fat; however, its role in beige fat remains unclear. Here we report a robust UCP1-independent thermogenic mechanism in beige fat that involves enhanced ATP-dependent Ca cycling by sarco/endoplasmic reticulum Ca-ATPase 2b (SERCA2b) and ryanodine receptor 2 (RyR2). Inhibition of SERCA2b impairs UCP1-independent beige fat thermogenesis in humans and mice as well as in pigs, a species that lacks a functional UCP1 protein. Conversely, enhanced Ca cycling by activation of α1- and/or β3-adrenergic receptors or the SERCA2b-RyR2 pathway stimulates UCP1-independent thermogenesis in beige adipocytes. In the absence of UCP1, beige fat dynamically expends glucose through enhanced glycolysis, tricarboxylic acid metabolism and pyruvate dehydrogenase activity for ATP-dependent thermogenesis through the SERCA2b pathway; beige fat thereby functions as a 'glucose sink' and improves glucose tolerance independently of body weight loss. Our study uncovers a noncanonical thermogenic mechanism through which beige fat controls whole-body energy homeostasis via Ca cycling.  | 
        
| Year of Publication | 
   2017 
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| Journal | 
   Nature medicine 
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| Volume | 
   23 
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| Issue | 
   12 
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| Number of Pages | 
   1454-1465 
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| Date Published | 
   12/2017 
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| ISSN Number | 
   1546-170X 
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| DOI | 
   10.1038/nm.4429 
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| Alternate Journal | 
   Nat. Med. 
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| PMCID | 
   PMC5727902 
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| PMID | 
   29131158 
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