Literature DB >> 27834218

Model-driven experimental approach reveals the complex regulatory distribution of p53 by the circadian factor Period 2.

Tetsuya Gotoh1, Jae Kyoung Kim2, Jingjing Liu1, Marian Vila-Caballer1, Philip E Stauffer1, John J Tyson3, Carla V Finkielstein4.   

Abstract

The circadian clock and cell cycle networks are interlocked on the molecular level, with the core clock loop exerting a multilevel regulatory role over cell cycle components. This is particularly relevant to the circadian factor Period 2 (Per2), which modulates the stability of the tumor suppressor p53 in unstressed cells and transcriptional activity in response to genotoxic stress. Per2 binding prevents Mdm2-mediated ubiquitination of p53 and, therefore, its degradation, and oscillations in the peaks of Per2 and p53 were expected to correspond. However, our findings showed that Per2 and p53 rhythms were significantly out-of-phase relative to each other in cell lysates and in purified cytoplasmic fractions. These seemingly conflicting experimental data motivated the use of a combined theoretical and experimental approach focusing on the role played by Per2 in dictating the phase of p53 oscillations. Systematic modeling of all possible regulatory scenarios predicted that the observed phase relationship between Per2 and p53 could be simulated if (i) p53 was more stable in the nucleus than in the cytoplasm, (ii) Per2 associates to various ubiquitinated forms of p53, and (iii) Per2 mediated p53 nuclear import. These predictions were supported by a sevenfold increase in p53's half-life in the nucleus and by in vitro binding of Per2 to the various ubiquitinated forms of p53. Last, p53's nuclear shuttling was significantly favored by ectopic expression of Per2 and reduced because of Per2 down-regulation. Our combined theoretical/mathematical approach reveals how clock regulatory nodes can be inferred from oscillating time course data.

Entities:  

Keywords:  Period 2; circadian rhythms; mathematical modeling; p53; tumor suppressor

Mesh:

Substances:

Year:  2016        PMID: 27834218      PMCID: PMC5127372          DOI: 10.1073/pnas.1607984113

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


  42 in total

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Review 5.  Systems Chronotherapeutics.

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9.  A detailed map of coupled circadian clock and cell cycle with qualitative dynamics validation.

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