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Mathematical modelling of reversible transition between quiescence and proliferation

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  • Nishtha Pandey
  • P K Vinod

Abstract

Cells switch between quiescence and proliferation states for maintaining tissue homeostasis and regeneration. At the restriction point (R-point), cells become irreversibly committed to the completion of the cell cycle independent of mitogen. The mechanism involving hyper-phosphorylation of retinoblastoma (Rb) and activation of transcription factor E2F is linked to the R-point passage. However, stress stimuli trigger exit from the cell cycle back to the mitogen-sensitive quiescent state after Rb hyper-phosphorylation but only until APC/CCdh1 inactivation. In this study, we developed a mathematical model to investigate the reversible transition between quiescence and proliferation in mammalian cells with respect to mitogen and stress signals. The model integrates the current mechanistic knowledge and accounts for the recent experimental observations with cells exiting quiescence and proliferating cells. We show that Cyclin E:Cdk2 couples Rb-E2F and APC/CCdh1 bistable switches and temporally segregates the R-point and the G1/S transition. A redox-dependent mutual antagonism between APC/CCdh1 and its inhibitor Emi1 makes the inactivation of APC/CCdh1 bistable. We show that the levels of Cdk inhibitor (CKI) and mitogen control the reversible transition between quiescence and proliferation. Further, we propose that shifting of the mitogen-induced transcriptional program to G2-phase in proliferating cells might result in an intermediate Cdk2 activity at the mitotic exit and in the immediate inactivation of APC/CCdh1. Our study builds a coherent framework and generates hypotheses that can be further explored by experiments.

Suggested Citation

  • Nishtha Pandey & P K Vinod, 2018. "Mathematical modelling of reversible transition between quiescence and proliferation," PLOS ONE, Public Library of Science, vol. 13(6), pages 1-15, June.
    • Handle: RePEc:plo:pone00:0198420
    DOI: 10.1371/journal.pone.0198420
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    References listed on IDEAS

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    1. Hee Won Yang & Mingyu Chung & Takamasa Kudo & Tobias Meyer, 2017. "Competing memories of mitogen and p53 signalling control cell-cycle entry," Nature, Nature, vol. 549(7672), pages 404-408, September.
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    3. Peng Dong & Manoj V. Maddali & Jaydeep K. Srimani & François Thélot & Joseph R. Nevins & Bernard Mathey-Prevot & Lingchong You, 2014. "Division of labour between Myc and G1 cyclins in cell cycle commitment and pace control," Nature Communications, Nature, vol. 5(1), pages 1-11, December.
    4. Wenyi Wei & Nagi G. Ayad & Yong Wan & Guo-Jun Zhang & Marc W. Kirschner & William G. Kaelin, 2004. "Degradation of the SCF component Skp2 in cell-cycle phase G1 by the anaphase-promoting complex," Nature, Nature, vol. 428(6979), pages 194-198, March.
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