Nature Communications (Mar 2025)

High resolution profiling of cell cycle-dependent protein and phosphorylation abundance changes in non-transformed cells

  • Camilla Rega,
  • Ifigenia Tsitsa,
  • Theodoros I. Roumeliotis,
  • Izabella Krystkowiak,
  • Maria Portillo,
  • Lu Yu,
  • Julia Vorhauser,
  • Jonathon Pines,
  • Jörg Mansfeld,
  • Jyoti Choudhary,
  • Norman E. Davey

DOI
https://doi.org/10.1038/s41467-025-57537-8
Journal volume & issue
Vol. 16, no. 1
pp. 1 – 18

Abstract

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Abstract The cell cycle governs a precise series of molecular events, regulated by coordinated changes in protein and phosphorylation abundance, that culminates in the generation of two daughter cells. Here, we present a proteomic and phosphoproteomic analysis of the human cell cycle in hTERT-RPE-1 cells using deep quantitative mass spectrometry by isobaric labelling. By analysing non-transformed cells and improving the temporal resolution and coverage of key cell cycle regulators, we present a dataset of cell cycle-dependent protein and phosphorylation site oscillation that offers a foundational reference for investigating cell cycle regulation. These data reveal regulatory intricacies including proteins and phosphorylation sites exhibiting cell cycle-dependent oscillation, and proteins targeted for degradation during mitotic exit. Integrated with complementary resources, our data link cycle-dependent abundance dynamics to functional changes and are accessible through the Cell Cycle database (CCdb), an interactive web-based resource for the cell cycle community.