FTY720-P, a Biased S1PR Ligand, Increases Mitochondrial Function through STAT3 Activation in Cardiac Cells

Francisco Blanco Vaca, Juan Pablo Muñoz, Paula Sánchez Fernández de Landa, Elena María Goretti Diarte-Añazco, Antonio Zorzano, Josep Julve

Research output: Contribution to journalArticleResearchpeer-review

2 Citations (Scopus)
3 Downloads (Pure)

Abstract

FTY720 is an FDA-approved sphingosine derivative drug for the treatment of multiple sclerosis. This compound blocks lymphocyte egress from lymphoid organs and autoimmunity through sphingosine 1-phosphate (S1P) receptor blockage. Drug repurposing of FTY720 has revealed improvements in glucose metabolism and metabolic diseases. Studies also demonstrate that preconditioning with this compound preserves the ATP levels during cardiac ischemia in rats. The molecular mechanisms by which FTY720 promotes metabolism are not well understood. Here, we demonstrate that nanomolar concentrations of the phosphorylated form of FTY720 (FTY720-P), the active ligand of S1P receptor (S1PR), activates mitochondrial respiration and the mitochondrial ATP production rate in AC16 human cardiomyocyte cells. Additionally, FTY720-P increases the number of mitochondrial nucleoids, promotes mitochondrial morphology alterations, and induces activation of STAT3, a transcription factor that promotes mitochondrial function. Notably, the effect of FTY720-P on mitochondrial function was suppressed in the presence of a STAT3 inhibitor. In summary, our results suggest that FTY720 promotes the activation of mitochondrial function, in part, through a STAT3 action.

Original languageEnglish
Article number7374
Pages (from-to)7374
Number of pages17
JournalInternational journal of molecular sciences
Volume24
Issue number8
DOIs
Publication statusPublished - 17 Apr 2023

Keywords

  • ATP
  • DRP1 S616
  • FTY720-P
  • S1PR
  • STAT3
  • TFAM
  • cardiomyocytes
  • metabolism
  • mitochondria
  • nucleoids

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