iScience (Feb 2024)

Whitening of brown adipose tissue inhibits osteogenic differentiation via secretion of S100A8/A9

  • Ting Wang,
  • Chaoran Zhao,
  • Jiahuan Zhang,
  • Shengfa Li,
  • Youming Zhang,
  • Yan Gong,
  • Yingyue Zhou,
  • Lei Yan,
  • Sheng Zhang,
  • Zhongmin Zhang,
  • Hongling Hu,
  • Anling Liu,
  • Xiaochun Bai,
  • Zhipeng Zou

Journal volume & issue
Vol. 27, no. 2
p. 108857

Abstract

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Summary: The mechanism by which brown adipose tissue (BAT) regulates bone metabolism is unclear. Here, we reveal that BAT secretes S100A8/A9, a previously unidentified BAT adipokine (batokine), to impair bone formation. Brown adipocytes-specific knockout of Rheb (RhebBAD KO), the upstream activator of mTOR, causes BAT malfunction to inhibit osteogenesis. Rheb depletion induces NF-κB dependent S100A8/A9 secretion from brown adipocytes, but not from macrophages. In wild-type mice, age-related Rheb downregulation in BAT is associated with enhanced S100A8/A9 secretion. Either batokines from RhebBAD KO mice, or recombinant S100A8/A9, inhibits osteoblast differentiation of mesenchymal stem cells in vitro by targeting toll-like receptor 4 on their surfaces. Conversely, S100A8/A9 neutralization not only rescues the osteogenesis repressed in the RhebBAD KO mice, but also alleviates age-related osteoporosis in wild-type mice. Collectively, our data revealed an unexpected BAT-bone crosstalk driven by Rheb-S100A8/A9, uncovering S100A8/A9 as a promising target for the treatment, and potentially, prevention of osteoporosis.

Keywords