A quantitative proteomic analysis of cofilin phosphorylation in myeloid cells and its modulation using the LIM kinase inhibitor Pyr1

Renaud Prudent; Nathalie Demoncheaux; Hélène Diemer; Véronique Collin-Faure; Reuben Kapur; Fabrice Paublant; Laurence Lafanechère; Sarah Cianférani; Thierry Rabilloud

doi:https://doi.org/10.1371/journal.pone.0208979

doi.org/10.1371/journal.pone.0208979

A quantitative proteomic analysis of cofilin phosphorylation in myeloid cells and its modulation using the LIM kinase inhibitor Pyr1

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..., Thierry Rabilloud

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PLOS ONE3.70

Volume: 13, Issue: 12, Pages: e0208979 - e0208979

Published: Dec 14, 2018

Abstract

LIM kinases are located at a strategic crossroad, downstream of several signaling pathways and upstream of effectors such as microtubules and the actin cytoskeleton. Cofilin is the only LIM kinases substrate that is well described to date, and its phosphorylation on serine 3 by LIM kinases controls cofilin actin-severing activity. Consequently, LIM kinases inhibition leads to actin cytoskeleton disorganization and blockade of cell motility,...

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Paper Details

Title

A quantitative proteomic analysis of cofilin phosphorylation in myeloid cells and its modulation using the LIM kinase inhibitor Pyr1

DOI

doi.org/10.1371/journal.pone.0208979

Published Date

Dec 14, 2018

Journal

PLOS ONE

Volume

13

Issue

12

Pages

e0208979 - e0208979

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