Coupling of cell fate selection model enhances DNA damage response and may underlie BE phenomenon

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Date

2020

Authors

Goekhan Demirkiran
Guleser Kalayc Demir
Cuneyt Guzelis

Journal Title

Journal ISSN

Volume Title

Publisher

INST ENGINEERING TECHNOLOGY-IET

Open Access Color

GOLD

Green Open Access

Yes

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Abstract

Double-strand break-induced (DSB) cells send signal that induces DSBs in neighbour cells resulting in the interaction among cells sharing the same medium. Since p53 network gives oscillatory response to DSBs such interaction among cells could be modelled as an excitatory coupling of p53 network oscillators. This study proposes a plausible coupling model of three-mode two-dimensional oscillators which models the p53-mediated cell fate selection in globally coupled DSB-induced cells. The coupled model consists of ATM and Wip1 proteins as variables. The coupling mechanism is realised through ATM variable via a mean-field modelling the bystander signal in the intercellular medium. Investigation of the model reveals that the coupling generates more sensitive DNA damage response by affecting cell fate selection. Additionally the authors search for the cause-effect relationship between coupled p53 network oscillators and bystander effect (BE) endpoints. For this they search for the possible values of uncertain parameters that may replicate BE experiments' results. At certain parametric regions there is a correlation between the outcomes of cell fate and endpoints of BE suggesting that the intercellular coupling of p53 network may manifest itself as the form of observed BEs.

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Keywords

biological effects of ionising particles, molecular biophysics, biochemistry, DNA, cellular biophysics, physiological models, biomolecular effects of radiation, cellular effects of radiation, biological effects of X-rays, oscillations, proteins, three-mode two-dimensional oscillators, p53-mediated cell fate selection, globally coupled DSB-induced cells, coupled model consists, coupling mechanism, ATM variable, bystander signal, intercellular medium, sensitive DNA damage response, coupled p53 network oscillators, intercellular coupling, cell fate selection model, double-strand break-induced cells, DSBs, neighbour cells, oscillatory response, excitatory coupling, plausible coupling model, DOUBLE-STRAND BREAKS, DOSE HYPER-RADIOSENSITIVITY, BYSTANDER RESPONSE, CIRCADIAN CLOCKS, NITRIC-OXIDE, RADIATION, P53, COMMUNICATION, REPAIR, INITIATION, Oscillatory Response, Cellular Biophysics, ATM Variable, DSBs, Neighbour Cells, Physiological Models, Globally Coupled DSB-Induced Cells, DNA, proteinS, Excitatory Coupling, Biological Effects of Ionising Particles, Coupled P53 Network Oscillators, Biological Effects of X-Rays, Oscillations, Coupled Model Consists, Cell Fate Selection Model, Plausible Coupling Model, Coupling Mechanism, Sensitive DNA Damage Response, Biomolecular Effects of Radiation, Bystander Signal, Three-Mode Two-Dimensional Oscillators, P53-Mediated Cell Fate Selection, Intercellular Medium, Biochemistry, Intercellular Coupling, Double-Strand Break-Induced Cells, Molecular Biophysics, Cellular Effects of Radiation, Intracellular Space, Uncertainty, DNA Breaks, Double-Stranded, Bystander Effect, Tumor Suppressor Protein p53, Models, Biological, DNA Damage

Fields of Science

0301 basic medicine, 0303 health sciences, 03 medical and health sciences

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OpenCitations Citation Count
1

Source

IET Systems Biology

Volume

14

Issue

2

Start Page

96

End Page

106
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CrossRef : 1

Scopus : 1

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Mendeley Readers : 8

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1

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1

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