Principles that govern competition or co-existence in Rho-GTPase driven polarization.

dc.contributor.author

Chiou, Jian-Geng

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Ramirez, Samuel A

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Elston, Timothy C

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Witelski, Thomas P

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Schaeffer, David G

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Lew, Daniel J

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Nie, Qing

dc.date.accessioned

2018-05-01T18:16:20Z

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2018-05-01T18:16:20Z

dc.date.issued

2018-04-12

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2018-05-01T18:15:23Z

dc.description.abstract

Rho-GTPases are master regulators of polarity establishment and cell morphology. Positive feedback enables concentration of Rho-GTPases into clusters at the cell cortex, from where they regulate the cytoskeleton. Different cell types reproducibly generate either one (e.g. the front of a migrating cell) or several clusters (e.g. the multiple dendrites of a neuron), but the mechanistic basis for unipolar or multipolar outcomes is unclear. The design principles of Rho-GTPase circuits are captured by two-component reaction-diffusion models based on conserved aspects of Rho-GTPase biochemistry. Some such models display rapid winner-takes-all competition between clusters, yielding a unipolar outcome. Other models allow prolonged co-existence of clusters. We investigate the behavior of a simple class of models and show that while the timescale of competition varies enormously depending on model parameters, a single factor explains a large majority of this variation. The dominant factor concerns the degree to which the maximal active GTPase concentration in a cluster approaches a "saturation point" determined by model parameters. We suggest that both saturation and the effect of saturation on competition reflect fundamental properties of the Rho-GTPase polarity machinery, regardless of the specific feedback mechanism, which predict whether the system will generate unipolar or multipolar outcomes.

dc.identifier.issn

1553-734X

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1553-7358

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https://hdl.handle.net/10161/16662

dc.language

eng

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Public Library of Science (PLoS)

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PLoS computational biology

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10.1371/journal.pcbi.1006095

dc.title

Principles that govern competition or co-existence in Rho-GTPase driven polarization.

dc.type

Journal article

duke.contributor.orcid

Witelski, Thomas P|0000-0003-0789-9859

duke.contributor.orcid

Lew, Daniel J|0000-0001-7482-3585

pubs.issue

4

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School of Medicine

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Duke

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Duke Cancer Institute

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Institutes and Centers

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Cell Biology

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Basic Science Departments

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Molecular Genetics and Microbiology

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Pharmacology & Cancer Biology

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Trinity College of Arts & Sciences

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Mathematics

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Pratt

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Pratt School of Engineering

pubs.publication-status

Published

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14

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