Nature Communications (Jun 2023)

Senescent immune cells accumulation promotes brown adipose tissue dysfunction during aging

  • Xu Feng,
  • Liwen Wang,
  • Ruoyu Zhou,
  • Rui Zhou,
  • Linyun Chen,
  • Hui Peng,
  • Yan Huang,
  • Qi Guo,
  • Xianghang Luo,
  • Haiyan Zhou

DOI
https://doi.org/10.1038/s41467-023-38842-6
Journal volume & issue
Vol. 14, no. 1
pp. 1 – 17

Abstract

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Abstract Brown adipose tissue (BAT)-mediated thermogenesis declines with age. However, the underlying mechanism remains unclear. Here we reveal that bone marrow-derived pro-inflammatory and senescent S100A8+ immune cells, mainly T cells and neutrophils, invade the BAT of male rats and mice during aging. These S100A8+ immune cells, coupled with adipocytes and sympathetic nerves, compromise axonal networks. Mechanistically, these senescent immune cells secrete abundant S100A8 to inhibit adipose RNA-binding motif protein 3 expression. This downregulation results in the dysregulation of axon guidance-related genes, leading to impaired sympathetic innervation and thermogenic function. Xenotransplantation experiments show that human S100A8+ immune cells infiltrate mice BAT and are sufficient to induce aging-like BAT dysfunction. Notably, treatment with S100A8 inhibitor paquinimod rejuvenates BAT axon networks and thermogenic function in aged male mice. Our study suggests that targeting the bone marrow-derived senescent immune cells presents an avenue to improve BAT aging and related metabolic disorders.