Journal of Lipid Research (Oct 2024)

Disruption of nucleotide biosynthesis reprograms mitochondrial metabolism to inhibit adipogenesis

  • Julia A. Pinette,
  • Jacob W. Myers,
  • Woo Yong Park,
  • Heather G. Bryant,
  • Alex M. Eddie,
  • Genesis A. Wilson,
  • Claudia Montufar,
  • Zayedali Shaikh,
  • Zer Vue,
  • Elizabeth R. Nunn,
  • Ryoichi Bessho,
  • Matthew A. Cottam,
  • Volker H. Haase,
  • Antentor O. Hinton,
  • Jessica B. Spinelli,
  • Jean-Philippe Cartailler,
  • Elma Zaganjor

Journal volume & issue
Vol. 65, no. 10
p. 100641

Abstract

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A key organismal response to overnutrition involves the development of new adipocytes through the process of adipogenesis. Preadipocytes sense changes in the systemic nutrient status and metabolites can directly modulate adipogenesis. We previously identified a role of de novo nucleotide biosynthesis in adipogenesis induction, whereby inhibition of nucleotide biosynthesis suppresses the expression of the transcriptional regulators PPARγ and C/EBPα. Here, we set out to identify the global transcriptomic changes associated with the inhibition of nucleotide biosynthesis. Through RNA sequencing (RNAseq), we discovered that mitochondrial signatures were the most altered in response to inhibition of nucleotide biosynthesis. Blocking nucleotide biosynthesis induced rounded mitochondrial morphology, and altered mitochondrial function, and metabolism, reducing levels of tricarboxylic acid cycle intermediates, and increasing fatty acid oxidation (FAO). The loss of mitochondrial function induced by suppression of nucleotide biosynthesis was rescued by exogenous expression of PPARγ. Moreover, inhibition of FAO restored PPARγ expression, mitochondrial protein expression, and adipogenesis in the presence of nucleotide biosynthesis inhibition, suggesting a regulatory role of nutrient oxidation in differentiation. Collectively, our studies shed light on the link between substrate oxidation and transcription in cell fate determination.

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