Literature DB >> 23665220

Identifying network motifs that buffer front-to-back signaling in polarized neutrophils.

Yanqin Wang1, Chin-Jen Ku, Elizabeth R Zhang, Alexander B Artyukhin, Orion D Weiner, Lani F Wu, Steven J Altschuler.   

Abstract

Neutrophil polarity relies on local, mutual inhibition to segregate incompatible signaling circuits to the leading and trailing edges. Mutual inhibition alone should lead to cells having strong fronts and weak backs or vice versa. However, analysis of cell-to-cell variation in human neutrophils revealed that back polarity remains consistent despite changes in front strength. How is this buffering achieved? Pharmacological perturbations and mathematical modeling revealed a functional role for microtubules in buffering back polarity by mediating positive, long-range crosstalk from front to back; loss of microtubules inhibits buffering and results in anticorrelation between front and back signaling. Furthermore, a systematic, computational search of network topologies found that a long-range, positive front-to-back link is necessary for back buffering. Our studies suggest a design principle that can be employed by polarity networks: short-range mutual inhibition establishes distinct signaling regions, after which directed long-range activation insulates one region from variations in the other.
Copyright © 2013 The Authors. Published by Elsevier Inc. All rights reserved.

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Year:  2013        PMID: 23665220      PMCID: PMC3674638          DOI: 10.1016/j.celrep.2013.04.009

Source DB:  PubMed          Journal:  Cell Rep            Impact factor:   9.423


  48 in total

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Authors:  Jingsong Xu; Fei Wang; Alexandra Van Keymeulen; Maike Rentel; Henry R Bourne
Journal:  Proc Natl Acad Sci U S A       Date:  2005-04-28       Impact factor: 11.205

3.  Mathematical model for spatial segregation of the Rho-family GTPases based on inhibitory crosstalk.

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4.  Neutrophil polarization: spatiotemporal dynamics of RhoA activity support a self-organizing mechanism.

Authors:  Kit Wong; Olivier Pertz; Klaus Hahn; Henry Bourne
Journal:  Proc Natl Acad Sci U S A       Date:  2006-02-28       Impact factor: 11.205

5.  Adaptive-control model for neutrophil orientation in the direction of chemical gradients.

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7.  Cdc42 regulates neutrophil migration via crosstalk between WASp, CD11b, and microtubules.

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Authors:  Orion D Weiner; William A Marganski; Lani F Wu; Steven J Altschuler; Marc W Kirschner
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  20 in total

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Authors:  Alfonso Bolado-Carrancio; Oleksii S Rukhlenko; Elena Nikonova; Mikhail A Tsyganov; Anne Wheeler; Amaya Garcia-Munoz; Walter Kolch; Alex von Kriegsheim; Boris N Kholodenko
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Review 3.  The excitable signal transduction networks: movers and shapers of eukaryotic cell migration.

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4.  Simple Rho GTPase Dynamics Generate a Complex Regulatory Landscape Associated with Cell Shape.

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5.  On comparing heterogeneity across biomarkers.

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Review 6.  Excitable Signal Transduction Networks in Directed Cell Migration.

Authors:  Peter N Devreotes; Sayak Bhattacharya; Marc Edwards; Pablo A Iglesias; Thomas Lampert; Yuchuan Miao
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7.  Efficient Front-Rear Coupling in Neutrophil Chemotaxis by Dynamic Myosin II Localization.

Authors:  Tony Y-C Tsai; Sean R Collins; Caleb K Chan; Amalia Hadjitheodorou; Pui-Ying Lam; Sunny S Lou; Hee Won Yang; Julianne Jorgensen; Felix Ellett; Daniel Irimia; Michael W Davidson; Robert S Fischer; Anna Huttenlocher; Tobias Meyer; James E Ferrell; Julie A Theriot
Journal:  Dev Cell       Date:  2019-04-22       Impact factor: 12.270

8.  Chemoattractant concentration-dependent tuning of ERK signaling dynamics in migrating neutrophils.

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Review 9.  The structure of dynamic GPCR signaling networks.

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Review 10.  Envisioning migration: mathematics in both experimental analysis and modeling of cell behavior.

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