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GDF15 links adipose tissue lipolysis with anxiety

  • Logan K. Townsend
  • , Dongdong Wang
  • , Carly M. Knuth
  • , Russta Fayyazi
  • , Ahmad Mohammad
  • , Léa J. Becker
  • , Evangelia E. Tsakiridis
  • , Eric M. Desjardins
  • , Zeel Patel
  • , Celina M. Valvano
  • , Junfeng Lu
  • , Alice E. Payne
  • , Ofure Itua
  • , Kyle D. Medak
  • , Daniel M. Marko
  • , Jonathan D. Schertzer
  • , David C. Wright
  • , Shawn M. Beaudette
  • , Katherine M. Morrison
  • , André C. Carpentier
  • Denis P. Blondin, Rebecca E.K. MacPherson, Jordan G. McCall, Marc G. Jeschke, Gregory R. Steinberg

Research output: Contribution to journalArticlepeer-review

Abstract

Psychological stress changes both behaviour and metabolism to protect organisms. Adrenaline is an important driver of this response. Anxiety correlates with circulating free fatty acid levels and can be alleviated by a peripherally restricted β-blocker, suggesting a peripheral signal linking metabolism with behaviour. Here we show that adrenaline, the β3 agonist CL316,243 and acute restraint stress induce growth differentiation factor 15 (GDF15) secretion in white adipose tissue of mice. Genetic inhibition of adipose triglyceride lipase or genetic deletion of β-adrenergic receptors blocks β-adrenergic-induced increases in GDF15. Increases in circulating GDF15 require lipolysis-induced free fatty acid stimulation of M2-like macrophages within white adipose tissue. Anxiety-like behaviour elicited by adrenaline or restraint stress is eliminated in mice lacking the GDF15 receptor GFRAL. These data provide molecular insights into the mechanisms linking metabolism and behaviour and suggest that inhibition of GDF15–GFRAL signalling might reduce acute anxiety.

Original languageEnglish
Pages (from-to)1004-1017
Number of pages14
JournalNature Metabolism
Volume7
Issue number5
DOIs
StatePublished - May 2025

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