Nature Communications (Aug 2024)

Cxcr4 regulates a pool of adipocyte progenitors and contributes to adiposity in a sex-dependent manner

  • Benjamin M. Steiner,
  • Abigail M. Benvie,
  • Derek Lee,
  • Yuwei Jiang,
  • Daniel C. Berry

DOI
https://doi.org/10.1038/s41467-024-50985-8
Journal volume & issue
Vol. 15, no. 1
pp. 1 – 21

Abstract

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Abstract Sex steroids modulate the distribution of mammalian white adipose tissues. Moreover, WAT remodeling requires adipocyte progenitor cells. Nevertheless, the sex-dependent mechanisms regulating adipocyte progenitors remain undetermined. Here, we uncover Cxcr4 acting in a sexually dimorphic manner to affect a pool of proliferating cells leading to restriction of female fat mass. We find that deletion of Cxcr4 in Pparγ-expressing cells results in female, not male, lipodystrophy, which cannot be restored by high-fat diet consumption. Additionally, Cxcr4 deletion is associated with a loss of a pool of proliferating adipocyte progenitors. Cxcr4 loss is accompanied by the upregulation of estrogen receptor alpha in adipose-derived PPARγ-labelled cells related to estradiol hypersensitivity and stalled adipogenesis. Estrogen removal or administration of antiestrogens restores WAT accumulation and dynamics of adipose-derived cells in Cxcr4-deficient mice. These findings implicate Cxcr4 as a female adipogenic rheostat, which may inform strategies to target female adiposity.