Cell Reports (Aug 2017)

Uncoupling the Mitogenic and Metabolic Functions of FGF1 by Tuning FGF1-FGF Receptor Dimer Stability

  • Zhifeng Huang,
  • Florian Atger,
  • Loïc Dayon,
  • Antonio Núñez Galindo,
  • Jingkui Wang,
  • Eva Martin,
  • Laetitia Da Silva,
  • Ivan Montoliu,
  • Sebastiano Collino,
  • Francois-Pierre Martin,
  • Joanna Ratajczak,
  • Carles Cantó,
  • Martin Kussmann,
  • Felix Naef,
  • Frédéric Gachon

DOI
https://doi.org/10.1016/j.celrep.2017.06.063
Journal volume & issue
Vol. 20, no. 7
pp. 1717 – 1728

Abstract

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Lysine acetylation is involved in various biological processes and is considered a key reversible post-translational modification in the regulation of gene expression, enzyme activity, and subcellular localization. This post-translational modification is therefore highly relevant in the context of circadian biology, but its characterization on the proteome-wide scale and its circadian clock dependence are still poorly described. Here, we provide a comprehensive and rhythmic acetylome map of the mouse liver. Rhythmic acetylated proteins showed subcellular localization-specific phases that correlated with the related metabolites in the regulated pathways. Mitochondrial proteins were over-represented among the rhythmically acetylated proteins and were highly correlated with SIRT3-dependent deacetylation. SIRT3 activity being nicotinamide adenine dinucleotide (NAD)+ level-dependent, we show that NAD+ is orchestrated by both feeding rhythms and the circadian clock through the NAD+ salvage pathway but also via the nicotinamide riboside pathway. Hence, the diurnal acetylome relies on a functional circadian clock and affects important diurnal metabolic pathways in the mouse liver.

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