Literature DB >> 24647909

Catalytic constants enable the emergence of bistability in dual phosphorylation.

Carsten Conradi1, Maya Mincheva.   

Abstract

Dual phosphorylation of proteins is a principal component of intracellular signalling. Bistability is considered an important property of such systems and its origin is not yet completely understood. Theoretical studies have established parameter values for multistationarity and bistability for many types of proteins. However, up to now no formal criterion linking multistationarity and bistability to the parameter values characterizing dual phosphorylation has been established. Deciding whether an unclassified protein has the capacity for bistability, therefore requires careful numerical studies. Here, we present two general algebraic conditions in the form of inequalities. The first employs the catalytic constants, and if satisfied guarantees multistationarity (and hence the potential for bistability). The second involves the catalytic and Michaelis constants, and if satisfied guarantees uniqueness of steady states (and hence absence of bistability). Our method also allows for the direct computation of the total concentration values such that multistationarity occurs. Applying our results yields insights into the emergence of bistability in the ERK-MEK-MKP system that previously required a delicate numerical effort. Our algebraic conditions present a practical way to determine the capacity for bistability and hence will be a useful tool for examining the origin of bistability in many models containing dual phosphorylation.

Entities:  

Keywords:  bistability; catalytic constants; dual phosphorylation; multistationarity

Mesh:

Substances:

Year:  2014        PMID: 24647909      PMCID: PMC4006255          DOI: 10.1098/rsif.2014.0158

Source DB:  PubMed          Journal:  J R Soc Interface        ISSN: 1742-5662            Impact factor:   4.118


  15 in total

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9.  Multistationarity in mass action networks with applications to ERK activation.

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  11 in total

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Review 5.  Dynamics of Posttranslational Modification Systems: Recent Progress and Future Directions.

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7.  Symmetry breaking meets multisite modification.

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8.  Core signalling motif displaying multistability through multi-state enzymes.

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9.  Kinase Inhibition Leads to Hormesis in a Dual Phosphorylation-Dephosphorylation Cycle.

Authors:  Peter Rashkov; Ian P Barrett; Robert E Beardmore; Claus Bendtsen; Ivana Gudelj
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10.  Long-term dynamics of multisite phosphorylation.

Authors:  Boris Y Rubinstein; Henry H Mattingly; Alexander M Berezhkovskii; Stanislav Y Shvartsman
Journal:  Mol Biol Cell       Date:  2016-05-25       Impact factor: 4.138

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