Short transient receptor potential channel 1 (TrpC1) (Transient receptor protein 1) (TRP-1) [TRP1]

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Ca entry via TRPC1 is essential for cellular differentiation and modulates secretion via the SNARE complex.

Properties of adipocytes, including differentiation and adipokine secretion, are crucial factors in obesity-associated metabolic syndrome. Here, we provide evidence that Ca influx in primary adipocytes, especially upon Ca store depletion, plays an important role in adipocyte differentiation, functionality and subsequently metabolic regulation. The endogenous Ca entry channel in both subcutaneous and visceral adipocytes was found to be dependent on TRPC1-STIM1, and blocking Ca entry with SKF96365 or using TRPC1 knockdown adipocytes inhibited adipocyte differentiation. Additionally, TRPC1 mice have decreased organ weight, but increased adipose deposition and reduced serum adiponectin and leptin concentrations, without affecting total adipokine expression. Mechanistically, TRPC1-mediated Ca entry regulated SNARE complex formation, and agonist-mediated secretion of adipokine-loaded vesicles was inhibited in TRPC1 adipose. These results suggest an unequivocal role of TRPC1 in adipocyte differentiation and adiponectin secretion, and that loss of TRPC1 disturbs metabolic homeostasis.This article has an associated First Person interview with the first author of the paper.

MeSH Terms

  • Adipocytes
  • Adipogenesis
  • Adiponectin
  • Adiposity
  • Aging
  • Animals
  • Calcium
  • Cell Differentiation
  • Male
  • Mice
  • Protein Isoforms
  • SNARE Proteins
  • Subcutaneous Fat
  • TRPC Cation Channels

Keywords

  • Adipocyte differentiation
  • Adiponectin secretion
  • Ca2 entry
  • Metabolic homeostasis
  • TRPC1