Stimulation of cortical myosin phosphorylation by p114RhoGEF drives cell migration and tumor cell invasion.

Stimulation of cortical myosin phosphorylation by p114RhoGEF drives cell migration and tumor cell invasion.

Actinomyosin activity is an important driver of cell locomotion and has been shown to promote collective cell migration of epithelial sheets as well as single cell migration and tumor cell invasion. However, the molecular mechanisms underlying activation of cortical myosin to stimulate single cell m...

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Main Authors: Stephen J Terry, Ahmed Elbediwy, Ceniz Zihni, Andrew R Harris, Maryse Bailly, Guillaume T Charras, Maria S Balda, Karl Matter
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2012-01-01
Series:PLoS ONE
Online Access:https://www.ncbi.nlm.nih.gov/pmc/articles/pmid/23185572/?tool=EBI
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spelling doaj-1ab7cf95323a412fa97309259fa7759c2021-03-04T12:19:35ZengPublic Library of Science (PLoS)PLoS ONE1932-62032012-01-01711e5018810.1371/journal.pone.0050188Stimulation of cortical myosin phosphorylation by p114RhoGEF drives cell migration and tumor cell invasion.Stephen J TerryAhmed ElbediwyCeniz ZihniAndrew R HarrisMaryse BaillyGuillaume T CharrasMaria S BaldaKarl MatterActinomyosin activity is an important driver of cell locomotion and has been shown to promote collective cell migration of epithelial sheets as well as single cell migration and tumor cell invasion. However, the molecular mechanisms underlying activation of cortical myosin to stimulate single cell movement, and the relationship between the mechanisms that drive single cell locomotion and those that mediate collective cell migration of epithelial sheets are incompletely understood. Here, we demonstrate that p114RhoGEF, an activator of RhoA that associates with non-muscle myosin IIA, regulates collective cell migration of epithelial sheets and tumor cell invasion. Depletion of p114RhoGEF resulted in specific spatial inhibition of myosin activation at cell-cell contacts in migrating epithelial sheets and the cortex of migrating single cells, but only affected double and not single phosphorylation of myosin light chain. In agreement, overall elasticity and contractility of the cells, processes that rely on persistent and more constant forces, were not affected, suggesting that p114RhoGEF mediates process-specific myosin activation. Locomotion was p114RhoGEF-dependent on Matrigel, which favors more roundish cells and amoeboid-like actinomyosin-driven movement, but not on fibronectin, which stimulates flatter cells and lamellipodia-driven, mesenchymal-like migration. Accordingly, depletion of p114RhoGEF led to reduced RhoA, but increased Rac activity. Invasion of 3D matrices was p114RhoGEF-dependent under conditions that do not require metalloproteinase activity, supporting a role of p114RhoGEF in myosin-dependent, amoeboid-like locomotion. Our data demonstrate that p114RhoGEF drives cortical myosin activation by stimulating myosin light chain double phosphorylation and, thereby, collective cell migration of epithelial sheets and amoeboid-like motility of tumor cells.https://www.ncbi.nlm.nih.gov/pmc/articles/pmid/23185572/?tool=EBI
collection DOAJ
language English
format Article
sources DOAJ
author Stephen J Terry
Ahmed Elbediwy
Ceniz Zihni
Andrew R Harris
Maryse Bailly
Guillaume T Charras
Maria S Balda
Karl Matter
spellingShingle Stephen J Terry
Ahmed Elbediwy
Ceniz Zihni
Andrew R Harris
Maryse Bailly
Guillaume T Charras
Maria S Balda
Karl Matter
Stimulation of cortical myosin phosphorylation by p114RhoGEF drives cell migration and tumor cell invasion.
PLoS ONE
author_facet Stephen J Terry
Ahmed Elbediwy
Ceniz Zihni
Andrew R Harris
Maryse Bailly
Guillaume T Charras
Maria S Balda
Karl Matter
author_sort Stephen J Terry
title Stimulation of cortical myosin phosphorylation by p114RhoGEF drives cell migration and tumor cell invasion.
title_short Stimulation of cortical myosin phosphorylation by p114RhoGEF drives cell migration and tumor cell invasion.
title_full Stimulation of cortical myosin phosphorylation by p114RhoGEF drives cell migration and tumor cell invasion.
title_fullStr Stimulation of cortical myosin phosphorylation by p114RhoGEF drives cell migration and tumor cell invasion.
title_full_unstemmed Stimulation of cortical myosin phosphorylation by p114RhoGEF drives cell migration and tumor cell invasion.
title_sort stimulation of cortical myosin phosphorylation by p114rhogef drives cell migration and tumor cell invasion.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2012-01-01
description Actinomyosin activity is an important driver of cell locomotion and has been shown to promote collective cell migration of epithelial sheets as well as single cell migration and tumor cell invasion. However, the molecular mechanisms underlying activation of cortical myosin to stimulate single cell movement, and the relationship between the mechanisms that drive single cell locomotion and those that mediate collective cell migration of epithelial sheets are incompletely understood. Here, we demonstrate that p114RhoGEF, an activator of RhoA that associates with non-muscle myosin IIA, regulates collective cell migration of epithelial sheets and tumor cell invasion. Depletion of p114RhoGEF resulted in specific spatial inhibition of myosin activation at cell-cell contacts in migrating epithelial sheets and the cortex of migrating single cells, but only affected double and not single phosphorylation of myosin light chain. In agreement, overall elasticity and contractility of the cells, processes that rely on persistent and more constant forces, were not affected, suggesting that p114RhoGEF mediates process-specific myosin activation. Locomotion was p114RhoGEF-dependent on Matrigel, which favors more roundish cells and amoeboid-like actinomyosin-driven movement, but not on fibronectin, which stimulates flatter cells and lamellipodia-driven, mesenchymal-like migration. Accordingly, depletion of p114RhoGEF led to reduced RhoA, but increased Rac activity. Invasion of 3D matrices was p114RhoGEF-dependent under conditions that do not require metalloproteinase activity, supporting a role of p114RhoGEF in myosin-dependent, amoeboid-like locomotion. Our data demonstrate that p114RhoGEF drives cortical myosin activation by stimulating myosin light chain double phosphorylation and, thereby, collective cell migration of epithelial sheets and amoeboid-like motility of tumor cells.
url https://www.ncbi.nlm.nih.gov/pmc/articles/pmid/23185572/?tool=EBI
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