PLoS Genetics (Nov 2016)

Proteomic Landscape of Tissue-Specific Cyclin E Functions in Vivo.

  • Junko Odajima,
  • Siddharth Saini,
  • Piotr Jung,
  • Yasmine Ndassa-Colday,
  • Scott Ficaro,
  • Yan Geng,
  • Eugenio Marco,
  • Wojciech Michowski,
  • Yaoyu E Wang,
  • James A DeCaprio,
  • Larisa Litovchick,
  • Jarrod Marto,
  • Piotr Sicinski

DOI
https://doi.org/10.1371/journal.pgen.1006429
Journal volume & issue
Vol. 12, no. 11
p. e1006429

Abstract

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E-type cyclins (cyclins E1 and E2) are components of the cell cycle machinery that has been conserved from yeast to humans. The major function of E-type cyclins is to drive cell division. It is unknown whether in addition to their 'core' cell cycle functions, E-type cyclins also perform unique tissue-specific roles. Here, we applied high-throughput mass spectrometric analyses of mouse organs to define the repertoire of cyclin E protein partners in vivo. We found that cyclin E interacts with distinct sets of proteins in different compartments. These cyclin E interactors are highly enriched for phosphorylation targets of cyclin E and its catalytic partner, the cyclin-dependent kinase 2 (Cdk2). Among cyclin E interactors we identified several novel tissue-specific substrates of cyclin E-Cdk2 kinase. In proliferating compartments, cyclin E-Cdk2 phosphorylates Lin proteins within the DREAM complex. In the testes, cyclin E-Cdk2 phosphorylates Mybl1 and Dmrtc2, two meiotic transcription factors that represent key regulators of spermatogenesis. In embryonic and adult brains cyclin E interacts with proteins involved in neurogenesis, while in adult brains also with proteins regulating microtubule-based processes and microtubule cytoskeleton. We also used quantitative proteomics to demonstrate re-wiring of the cyclin E interactome upon ablation of Cdk2. This approach can be used to study how protein interactome changes during development or in any pathological state such as aging or cancer.