A Data-Driven, Mathematical Model of Mammalian Cell Cycle Regulation

Weis, Michael; Avva, Jayant; Jacobberger, James W.; Sreenath, Sree N.

doi:10.1371/journal.pone.0097130

Cited by 32 publications

(29 citation statements)

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“…As mentioned, the correlation between DNA replication and expression of the cyclins D1, E and A is consistent with cytometric analysis of these cyclin proteins based on analysis of BrdU incorporation and SBIP methodology presented in the prior reports [ 74 - 76 ]. The presented data conform also to the assessments of the cell cycle kinetics based on multiparameter analysis of cyclins expression with respect to other proteins of the cell cycle machinery as reported by Jacobberger and his colleagues [ 77 - 79 ]. Their studies however were based on static analysis of presentation of these proteins vis-a-vis cellular DNA content (cell cycle phase) and did not include the kinetic information pertaining initiation and completion of DNA replication, or the rate of DNA replication that can be inferred from the degree of EdU incorporation during the pulse labeling.…”

Section: Positive Markers Of Dna Replication: Cyclin E Cyclin a Pcnsupporting

confidence: 85%

Initiation and termination of DNA replication during S phase in relation to cyclins D1, E and A, p21WAF1, Cdt1 and the p12 subunit of DNA polymerase δ revealed in individual cells by cytometry

et al. 2015

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During our recent studies on mechanism of the regulation of human DNA polymerase δ in preparation for DNA replication or repair, multiparameter imaging cytometry as exemplified by laser scanning cytometry (LSC) has been used to assess changes in expression of the following nuclear proteins associated with initiation of DNA replication: cyclin A, PCNA, Ki-67, p21WAF1, DNA replication factor Cdt1 and the smallest subunit of DNA polymerase δ, p12. In the present review, rather than focusing on Pol δ, we emphasize the application of LSC in these studies and outline possibilities offered by the concurrent differential analysis of DNA replication in conjunction with expression of the nuclear proteins. A more extensive analysis of the data on a correlation between rates of EdU incorporation, likely reporting DNA replication, and expression of these proteins, is presently provided. New data, specifically on the expression of cyclin D1 and cyclin E with respect to EdU incorporation as well as on a relationship between expression of cyclin A vs. p21WAF1 and Ki-67 vs. Cdt1, are also reported. Of particular interest is the observation that this approach makes it possible to assess the temporal sequence of degradation of cyclin D1, p21WAF1, Cdt1 and p12, each with respect to initiation of DNA replication and with respect to each other. Also the sequence or reappearance of these proteins in G2 after termination of DNA replication is assessed. The reviewed data provide a more comprehensive presentation of potential markers, whose presence or absence marks the DNA replicating cells. Discussed is also usefulness of these markers as indicators of proliferative activity in cancer tissues that may bear information on tumor progression and have a prognostic value.

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Section: Positive Markers Of Dna Replication: Cyclin E Cyclin a Pcnsupporting

confidence: 85%

Initiation and termination of DNA replication during S phase in relation to cyclins D1, E and A, p21WAF1, Cdt1 and the p12 subunit of DNA polymerase δ revealed in individual cells by cytometry

et al. 2015

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“…A vast literature for cell cycle models is available (Weis et al 2014), and different modelling approaches can be adopted for the description of the cell cycle at different scales of complexity. We are interested in the cell population dynamics, a higher scale level than the fine-grained study of progression through cell cycle phases and the molecular processes involved.…”

Section: Methodsmentioning

confidence: 99%

Mathematical modelling of cortical neurogenesis reveals that the founder population does not necessarily scale with neuronal output

Picco

García‐Moreno

Woolley

et al. 2017

Preprint

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The mammalian cerebral neocortex has a unique structure, composed of layers of different neuron types, interconnected in a stereotyped fashion. While the overall developmental program seems to be conserved, there are divergent developmental factors generating cortical diversity amongst mammalian species. In terms of neuronal output some of the determining factors are the size of the founder population, the duration of cortical neurogenesis, the proportion of different progenitor types, and the fine-tuned balance between self-renewing and differentiative divisions. We develop a mathematical model of neurogenesis that, accounting for these factors, aims at explaining the high diversity found across mammalian species. By framing our hypotheses in rigorous mathematical terms, we are able to identify paths of neurogenesis that match experimentally observed patterns in mouse, and to extrapolate the corresponding patterns in macaque and human. Additionally, we use the model to identify key parameters that would benefit from accurate experimental investigation. We find that the timing of switch to symmetric neurogenic divisions produces the highest . CC-BY-NC-ND 4.0 International license peer-reviewed) is the author/funder. It is made available under a The copyright holder for this preprint (which was not . http://dx.doi.org/10.1101/206045 doi: bioRxiv preprint first posted online Oct. 19, 2017; 3 variation in neuronal output. Additionally, we find that an increase in neuronal output does not necessarily reflect a larger size of founder population, and we suggest the need for further experimental quantifications to test our predictions.

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“…The goal in this paper was to review computational modelling approaches for mammalian cell cycle to see how models have facilitated our understanding of it. We briefly explained the mechanism of mammalian cell cycle regulation system by highlighting the important effect of Cyclin/Cdks as main controllers as well as their (Obeyesekere et al, 1997) G1-S (Basse et al, 2003) G1-S-G2-M (Pfeuty et al, 2008) G1-S (Gauthier & Pohl, 2011) G1-S-G2-M (Thron, 1997) G2-M (Bai et al, 2003) G1-S (Tashima et al, 2008) G1-S (Zhang et al, 2013) G2-M (Kohn, 1998) G1-S G1-S-G2-M (Iwamoto et al, 2008) G1-S (Weis et al, 2014) G1-S-G2-M (Hatzimanikatis et al, 1999) G1-S (Novak & Tyson, 2004) G1-S-G2-M (Gérard & Goldbeter, 2009) G1-S-G2-M (Zhang et al, 2014a) G2-M (Obeyesekere et al, 1999) G1-S (Alarcon et al, 2004) G1-S-G2-M (Hamada et al, 2009) G2-M (Zhang et al, 2014b) G2-M (Aguda & Tang, 1999) G1-S (Swat et al, 2004) G1-S (Alfieri et al, 2009) G1-S Table 4. Stochastic models of mammalian cell cycle.…”

Section: Discussionmentioning

confidence: 99%

A review of computational models of mammalian cell cycle

Abroudi

Samarasinghe

Kulasiri³

2015

Weber, T., McPhee, M.J. And Anderssen, R.S. (Eds) MODSIM2015, 21st International Congress on Modelling and Simulation

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Cell cycle, which comprises an ordered sequence of phases (G1, S, G2, and M) that leads to growth and division of a cell, is an essential part of life and its malfunction may cause formation of tumors and cancer. Therefore, study of cell cycle system has been the topic of many computational modelling research studies. In this paper, a thorough review of all modelling methods for mammalian cell cycle and corresponding models are presented. Due to its high complexity, mammalian cell cycle system has been less modelled than other organisms, such as yeast. Majority of models have investigated various parts of mammalian cell cycle, with few covering the whole system including all the phases. There are four main modelling types (discrete, deterministic continuous, stochastic continuous, and hybrid) that enable researchers to explore and understand system properties, such as dynamics of key regulators, oscillation behaviors, feedback loops, etc. Discrete models provide an abstract view of the system where different nodes interact with each other based on discrete logic. On the other hand, continuous models usually utilize Ordinary Differential Equations (ODEs) to incorporate continuous dynamics of the system elements (i.e., protein concentrations). The effect of noise in biological systems has been modelled through stochastic models. Hybrid models combine aforementioned modelling methods to overcome limitations of individual methods. The paper covers all the above methods highlighting their strengths and weaknesses and presents some open questions as promising future prospects for modelling cell cycle.

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A Data-Driven, Mathematical Model of Mammalian Cell Cycle Regulation

Cited by 32 publications

References 106 publications

Initiation and termination of DNA replication during S phase in relation to cyclins D1, E and A, p21WAF1, Cdt1 and the p12 subunit of DNA polymerase δ revealed in individual cells by cytometry

Initiation and termination of DNA replication during S phase in relation to cyclins D1, E and A, p21WAF1, Cdt1 and the p12 subunit of DNA polymerase δ revealed in individual cells by cytometry

Mathematical modelling of cortical neurogenesis reveals that the founder population does not necessarily scale with neuronal output

A review of computational models of mammalian cell cycle

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