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Paracrine FGFs target skeletal muscle to exert potent anti-hyperglycemic effects

Author

Listed:
  • Lei Ying

    (Wenzhou Medical University
    Wenzhou Medical University)

  • Luyao Wang

    (Wenzhou Medical University)

  • Kaiwen Guo

    (Wenzhou Medical University)

  • Yushu Hou

    (Wenzhou Medical University)

  • Na Li

    (Wenzhou Medical University
    Wenzhou Medical University)

  • Shuyi Wang

    (Fudan University)

  • Xingfeng Liu

    (Chinese Academy of Medical Sciences and Peking Union Medical College
    Diabetes Research Center, Chinese Academy of Medical Sciences and Peking Union Medical College
    CAMS Key Laboratory of Molecular Mechanism and Target Discovery of Metabolic Disorder and Tumorigenesis, Chinese Academy of Medical Sciences and Peking Union Medical College)

  • Qijin Zhao

    (Chinese Academy of Medical Sciences and Peking Union Medical College
    Diabetes Research Center, Chinese Academy of Medical Sciences and Peking Union Medical College
    CAMS Key Laboratory of Molecular Mechanism and Target Discovery of Metabolic Disorder and Tumorigenesis, Chinese Academy of Medical Sciences and Peking Union Medical College)

  • Jie Zhou

    (Wenzhou Medical University)

  • Longwei Zhao

    (Wenzhou Medical University)

  • Jianlou Niu

    (Wenzhou Medical University)

  • Chuchu Chen

    (Wenzhou Medical University)

  • Lintao Song

    (Wenzhou Medical University)

  • Shaocong Hou

    (Chinese Academy of Medical Sciences and Peking Union Medical College
    Diabetes Research Center, Chinese Academy of Medical Sciences and Peking Union Medical College
    CAMS Key Laboratory of Molecular Mechanism and Target Discovery of Metabolic Disorder and Tumorigenesis, Chinese Academy of Medical Sciences and Peking Union Medical College)

  • Lijuan Kong

    (Chinese Academy of Medical Sciences and Peking Union Medical College
    Diabetes Research Center, Chinese Academy of Medical Sciences and Peking Union Medical College
    CAMS Key Laboratory of Molecular Mechanism and Target Discovery of Metabolic Disorder and Tumorigenesis, Chinese Academy of Medical Sciences and Peking Union Medical College)

  • Xiaokun Li

    (Wenzhou Medical University)

  • Jun Ren

    (Fudan University)

  • Pingping Li

    (Chinese Academy of Medical Sciences and Peking Union Medical College
    Diabetes Research Center, Chinese Academy of Medical Sciences and Peking Union Medical College
    CAMS Key Laboratory of Molecular Mechanism and Target Discovery of Metabolic Disorder and Tumorigenesis, Chinese Academy of Medical Sciences and Peking Union Medical College)

  • Moosa Mohammadi

    (New York University School of Medicine)

  • Zhifeng Huang

    (Wenzhou Medical University)

Abstract

Several members of the FGF family have been identified as potential regulators of glucose homeostasis. We previously reported that a low threshold of FGF-induced FGF receptor 1c (FGFR1c) dimerization and activity is sufficient to evoke a glucose lowering activity. We therefore reasoned that ligand identity may not matter, and that besides paracrine FGF1 and endocrine FGF21, other cognate paracrine FGFs of FGFR1c might possess such activity. Indeed, via a side-by-side testing of multiple cognate FGFs of FGFR1c in diabetic mice we identified the paracrine FGF4 as a potent anti-hyperglycemic FGF. Importantly, we found that like FGF1, the paracrine FGF4 is also more efficacious than endocrine FGF21 in lowering blood glucose. We show that paracrine FGF4 and FGF1 exert their superior glycemic control by targeting skeletal muscle, which expresses copious FGFR1c but lacks β-klotho (KLB), an obligatory FGF21 co-receptor. Mechanistically, both FGF4 and FGF1 upregulate GLUT4 cell surface abundance in skeletal muscle in an AMPKα-dependent but insulin-independent manner. Chronic treatment with rFGF4 improves insulin resistance and suppresses adipose macrophage infiltration and inflammation. Notably, unlike FGF1 (a pan-FGFR ligand), FGF4, which has more restricted FGFR1c binding specificity, has no apparent effect on food intake. The potent anti-hyperglycemic and anti-inflammatory properties of FGF4 testify to its promising potential for use in the treatment of T2D and related metabolic disorders.

Suggested Citation

  • Lei Ying & Luyao Wang & Kaiwen Guo & Yushu Hou & Na Li & Shuyi Wang & Xingfeng Liu & Qijin Zhao & Jie Zhou & Longwei Zhao & Jianlou Niu & Chuchu Chen & Lintao Song & Shaocong Hou & Lijuan Kong & Xiaok, 2021. "Paracrine FGFs target skeletal muscle to exert potent anti-hyperglycemic effects," Nature Communications, Nature, vol. 12(1), pages 1-14, December.
    • Handle: RePEc:nat:natcom:v:12:y:2021:i:1:d:10.1038_s41467-021-27584-y
    DOI: 10.1038/s41467-021-27584-y
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    References listed on IDEAS

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    1. Alan R. Saltiel & C. Ronald Kahn, 2001. "Insulin signalling and the regulation of glucose and lipid metabolism," Nature, Nature, vol. 414(6865), pages 799-806, December.
    2. Jae Myoung Suh & Johan W. Jonker & Maryam Ahmadian & Regina Goetz & Denise Lackey & Olivia Osborn & Zhifeng Huang & Weilin Liu & Eiji Yoshihara & Theo H. van Dijk & Rick Havinga & Weiwei Fan & Yun-Qia, 2014. "Endocrinization of FGF1 produces a neomorphic and potent insulin sensitizer," Nature, Nature, vol. 513(7518), pages 436-439, September.
    3. Jens Schlossmann & Aldo Ammendola & Keith Ashman & Xiangang Zong & Andrea Huber & Gitte Neubauer & Ge-Xin Wang & Hans-Dieter Allescher & Michael Korth & Matthias Wilm & Franz Hofmann & Peter Ruth, 2000. "Regulation of intracellular calcium by a signalling complex of IRAG, IP3 receptor and cGMP kinase Iβ," Nature, Nature, vol. 404(6774), pages 197-201, March.
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    1. Dandan Wu & Hwang Chan Yu & Hye-Na Cha & Soyoung Park & Yoonji Lee & Sun-Jung Yoon & So-Young Park & Byung-Hyun Park & Eun Ju Bae, 2024. "PAK4 phosphorylates and inhibits AMPKα to control glucose uptake," Nature Communications, Nature, vol. 15(1), pages 1-17, December.

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