Cdc42 localization and cell polarity depend on membrane traffic

Naël Osmani; Florent Peglion; Philippe Chavrier; Sandrine Etienne-Manneville

doi:10.1083/jcb.201003091

Cdc42 localization and cell polarity depend on membrane traffic

The Journal of Cell Biology ◽

10.1083/jcb.201003091 ◽

2010 ◽

Vol 191 (7) ◽

pp. 1261-1269 ◽

Cited By ~ 113

Author(s):

Naël Osmani ◽

Florent Peglion ◽

Philippe Chavrier ◽

Sandrine Etienne-Manneville

Keyword(s):

Cell Migration ◽

Cell Polarity ◽

Membrane Trafficking ◽

Membrane Traffic ◽

Leading Edge ◽

Cell Polarization ◽

Membrane Dynamics ◽

Cell Functions ◽

Directed Cell Migration ◽

Division Cell

Cell polarity is essential for cell division, cell differentiation, and most differentiated cell functions including cell migration. The small G protein Cdc42 controls cell polarity in a wide variety of cellular contexts. Although restricted localization of active Cdc42 seems to be important for its distinct functions, mechanisms responsible for the concentration of active Cdc42 at precise cortical sites are not fully understood. In this study, we show that during directed cell migration, Cdc42 accumulation at the cell leading edge relies on membrane traffic. Cdc42 and its exchange factor βPIX localize to intracytosplasmic vesicles. Inhibition of Arf6-dependent membrane trafficking alters the dynamics of Cdc42-positive vesicles and abolishes the polarized recruitment of Cdc42 and βPIX to the leading edge. Furthermore, we show that Arf6-dependent membrane dynamics is also required for polarized recruitment of Rac and the Par6–aPKC polarity complex and for cell polarization. Our results demonstrate influence of membrane dynamics on the localization and activation of Cdc42 and consequently on directed cell migration.

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The Rac-GAP Bcr is a novel regulator of the Par complex that controls cell polarity

Molecular Biology of the Cell ◽

10.1091/mbc.e13-06-0333 ◽

2013 ◽

Vol 24 (24) ◽

pp. 3857-3868 ◽

Cited By ~ 18

Author(s):

Anjana S. Narayanan ◽

Steve B. Reyes ◽

Kyongmi Um ◽

Joseph H. McCarty ◽

Kimberley F. Tolias

Keyword(s):

Cell Migration ◽

Cell Polarity ◽

Leading Edge ◽

Cell Polarization ◽

Nucleotide Exchange ◽

Complex Activity ◽

Guanine Nucleotide Exchange ◽

Directed Cell Migration ◽

Nucleotide Exchange Factor ◽

T Lymphoma

Cell polarization is essential for many biological processes, including directed cell migration, and loss of polarity contributes to pathological conditions such as cancer. The Par complex (Par3, Par6, and PKCζ) controls cell polarity in part by recruiting the Rac-specific guanine nucleotide exchange factor T-lymphoma invasion and metastasis 1 (Tiam1) to specialized cellular sites, where Tiam1 promotes local Rac1 activation and cytoskeletal remodeling. However, the mechanisms that restrict Par-Tiam1 complex activity to the leading edge to maintain cell polarity during migration remain unclear. We identify the Rac-specific GTPase-activating protein (GAP) breakpoint cluster region protein (Bcr) as a novel regulator of the Par-Tiam1 complex. We show that Bcr interacts with members of the Par complex and inhibits both Rac1 and PKCζ signaling. Loss of Bcr results in faster, more random migration and striking polarity defects in astrocytes. These polarity defects are rescued by reducing PKCζ activity or by expressing full-length Bcr, but not an N-terminal deletion mutant or the homologous Rac-GAP, Abr, both of which fail to associate with the Par complex. These results demonstrate that Bcr is an integral member of the Par-Tiam1 complex that controls polarized cell migration by locally restricting both Rac1 and PKCζ function.

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Polarity sets the stage for cytokinesis

Molecular Biology of the Cell ◽

10.1091/mbc.e11-06-0512 ◽

2012 ◽

Vol 23 (1) ◽

pp. 7-11 ◽

Cited By ~ 16

Author(s):

Heidi Hehnly ◽

Stephen Doxsey

Keyword(s):

Cell Migration ◽

Cell Division ◽

Cell Polarity ◽

Membrane Trafficking ◽

Cell Separation ◽

Cell Polarization ◽

Separation Step ◽

Canonical Pathways

Cell polarity is important for a number of processes, from chemotaxis to embryogenesis. Recent studies suggest a new role for polarity in the orchestration of events during the final cell separation step of cell division called abscission. Abscission shares several features with cell polarization, including rearrangement of phosphatidylinositols, reorganization of microtubules, and trafficking of exocyst-associated membranes. Here we focus on how the canonical pathways for cell polarization and cell migration may play a role in spatiotemporal membrane trafficking events required for the final stages of cytokinesis.

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CaM kinase IIδ2-dependent regulation of vascular smooth muscle cell polarization and migration

AJP Cell Physiology ◽

10.1152/ajpcell.90638.2007 ◽

2008 ◽

Vol 294 (6) ◽

pp. C1465-C1475 ◽

Cited By ~ 44

Author(s):

Melissa Z. Mercure ◽

Roman Ginnan ◽

Harold A. Singer

Keyword(s):

Smooth Muscle ◽

Cell Migration ◽

Vascular Smooth Muscle ◽

Cell Monolayer ◽

Leading Edge ◽

Cell Polarization ◽

Loss Of Function ◽

Downstream Signaling ◽

Transient Activation ◽

And Migration

Previous studies indicate involvement of the multifunctional Ca2+/calmodulin-dependent protein kinase II (CaMKII) in vascular smooth muscle (VSM) cell migration. In the present study, molecular loss-of-function studies were used specifically to assess the role of the predominant CaMKIIδ2 isoform on VSM cell migration using a scratch wound healing assay. Targeted CaMKIIδ2 knockdown using siRNA or inhibition of activity by overexpressing a kinase-negative mutant resulted in attenuation of VSM cell migration. Temporal and spatial assessments of kinase autophosphorylation indicated rapid and transient activation in response to wounding, in addition to a sustained activation in the leading edge of migrating and spreading cells. Furthermore, siRNA-mediated suppression of CaMKIIδ2 resulted in the inhibition of wound-induced Rac activation and Golgi reorganization, and disruption of leading edge morphology, indicating an important function for CaMKIIδ2 in regulating VSM cell polarization. Numerous previous reports link activation of CaMKII to ERK1/2 signaling in VSM. Wound-induced ERK1/2 activation was also found to be dependent on CaMKII; however, ERK activity did not account for effects of CaMKII in regulating Golgi polarization, indicating alternative mechanisms by which CaMKII affects the complex events involved in cell migration. Wounding a VSM cell monolayer results in CaMKIIδ2 activation, which positively regulates VSM cell polarization and downstream signaling, including Rac and ERK1/2 activation, leading to cell migration.

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Paxillin-Kinase-Linker Tyrosine Phosphorylation Regulates Directional Cell Migration

Molecular Biology of the Cell ◽

10.1091/mbc.e09-07-0548 ◽

2009 ◽

Vol 20 (22) ◽

pp. 4706-4719 ◽

Cited By ~ 39

Author(s):

Jianxin A. Yu ◽

Nicholas O. Deakin ◽

Christopher E. Turner

Keyword(s):

Cell Migration ◽

Cell Adhesion ◽

Growth Factor ◽

Tyrosine Phosphorylation ◽

Wound Repair ◽

Cell Polarization ◽

Dependent Manner ◽

Directed Cell Migration ◽

Focal Adhesion Protein ◽

Directional Cell Migration

Directed cell migration requires the coordination of growth factor and cell adhesion signaling and is of fundamental importance during embryonic development, wound repair, and pathological conditions such as tumor metastasis. Herein, we demonstrate that the ArfGAP, paxillin-kinase-linker (PKL/GIT2), is tyrosine phosphorylated in response to platelet-derived growth factor (PDGF) stimulation, in an adhesion dependent manner and is necessary for directed cell migration. Using a combination of pharmacological inhibitors, knockout cells and kinase mutants, FAK, and Src family kinases were shown to mediate PDGF-dependent PKL tyrosine phosphorylation. In fibroblasts, expression of a PKL mutant lacking the principal tyrosine phosphorylation sites resulted in loss of wound-induced cell polarization as well as directional migration. PKL phosphorylation was necessary for PDGF-stimulated PKL binding to the focal adhesion protein paxillin and expression of paxillin or PKL mutants defective in their respective binding motifs recapitulated the polarization defects. RNA interference or expression of phosphorylation mutants of PKL resulted in disregulation of PDGF-stimulated Rac1 and PAK activities, reduction of Cdc42 and Erk signaling, as well as mislocalization of βPIX. Together these studies position PKL as an integral component of growth factor and cell adhesion cross-talk signaling, controlling the development of front–rear cell polarity and directional cell migration.

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Scribble, Lgl1, and myosin II form a complex in vivo to promote directed cell migration

Molecular Biology of the Cell ◽

10.1091/mbc.e19-11-0657 ◽

2020 ◽

Vol 31 (20) ◽

pp. 2234-2248

Author(s):

Maha Abedrabbo ◽

Shoshana Ravid

Keyword(s):

Cell Migration ◽

Cell Adhesion ◽

Myosin Ii ◽

Leading Edge ◽

Directed Cell Migration ◽

Lethal Giant Larvae ◽

And Migration ◽

Migrating Cells

Here we show that Scribble (Scrib), Lethal giant larvae 1 (Lgl1), and myosin II form a complex in vivo and colocalize at the cell leading edge of migrating cells, and this colocalization is interdependent. Scrib and Lgl1 are required for proper cell adhesion, polarity, and migration.

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Cell polarization mechanisms during directed cell migration

Nature Cell Biology ◽

10.1038/ncb0405-336 ◽

2005 ◽

Vol 7 (4) ◽

pp. 336-337 ◽

Cited By ~ 50

Author(s):

Anna Huttenlocher

Keyword(s):

Cell Migration ◽

Cell Polarization ◽

Directed Cell Migration

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P-cadherin promotes collective cell migration via a Cdc42-mediated increase in mechanical forces

The Journal of Cell Biology ◽

10.1083/jcb.201505105 ◽

2016 ◽

Vol 212 (2) ◽

pp. 199-217 ◽

Cited By ~ 57

Author(s):

Cédric Plutoni ◽

Elsa Bazellieres ◽

Maïlys Le Borgne-Rochet ◽

Franck Comunale ◽

Agusti Brugues ◽

...

Keyword(s):

Cell Migration ◽

Cell Polarity ◽

Cell Biology ◽

Cell Polarization ◽

Collective Cell Migration ◽

Mechanical Forces ◽

Tumor Aggressiveness ◽

And Migration ◽

Cell Cell

Collective cell migration (CCM) is essential for organism development, wound healing, and metastatic transition, the primary cause of cancer-related death, and it involves cell–cell adhesion molecules of the cadherin family. Increased P-cadherin expression levels are correlated with tumor aggressiveness in carcinoma and aggressive sarcoma; however, how P-cadherin promotes tumor malignancy remains unknown. Here, using integrated cell biology and biophysical approaches, we determined that P-cadherin specifically induces polarization and CCM through an increase in the strength and anisotropy of mechanical forces. We show that this mechanical regulation is mediated by the P-cadherin/β-PIX/Cdc42 axis; P-cadherin specifically activates Cdc42 through β-PIX, which is specifically recruited at cell–cell contacts upon CCM. This mechanism of cell polarization and migration is absent in cells expressing E- or R-cadherin. Thus, we identify a specific role of P-cadherin through β-PIX–mediated Cdc42 activation in the regulation of cell polarity and force anisotropy that drives CCM.

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Disruption of the Golgi apparatus by brefeldin A blocks cell polarization and inhibits directed cell migration.

Proceedings of the National Academy of Sciences ◽

10.1073/pnas.91.12.5686 ◽

1994 ◽

Vol 91 (12) ◽

pp. 5686-5689 ◽

Cited By ~ 79

Author(s):

A. D. Bershadsky ◽

A. H. Futerman

Keyword(s):

Cell Migration ◽

Golgi Apparatus ◽

Brefeldin A ◽

Cell Polarization ◽

Directed Cell Migration

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Mechanochemical feedback underlies coexistence of qualitatively distinct cell polarity patterns within diverse cell populations

Proceedings of the National Academy of Sciences ◽

10.1073/pnas.1700054114 ◽

2017 ◽

Vol 114 (28) ◽

pp. E5750-E5759 ◽

Cited By ~ 32

Author(s):

JinSeok Park ◽

William R. Holmes ◽

Sung Hoon Lee ◽

Hong-Nam Kim ◽

Deok-Ho Kim ◽

...

Keyword(s):

Cell Migration ◽

Cell Polarity ◽

Cell Types ◽

Small Gtpases ◽

Cell Polarization ◽

Environmental Perturbations ◽

Oscillatory Dynamic ◽

Distinct Cell ◽

Spatially Distributed ◽

Directional Cell Migration

Cell polarization and directional cell migration can display random, persistent, and oscillatory dynamic patterns. However, it is not clear whether these polarity patterns can be explained by the same underlying regulatory mechanism. Here, we show that random, persistent, and oscillatory migration accompanied by polarization can simultaneously occur in populations of melanoma cells derived from tumors with different degrees of aggressiveness. We demonstrate that all of these patterns and the probabilities of their occurrence are quantitatively accounted for by a simple mechanism involving a spatially distributed, mechanochemical feedback coupling the dynamically changing extracellular matrix (ECM)–cell contacts to the activation of signaling downstream of the Rho-family small GTPases. This mechanism is supported by a predictive mathematical model and extensive experimental validation, and can explain previously reported results for diverse cell types. In melanoma, this mechanism also accounts for the effects of genetic and environmental perturbations, including mutations linked to invasive cell spread. The resulting mechanistic understanding of cell polarity quantitatively captures the relationship between population variability and phenotypic plasticity, with the potential to account for a wide variety of cell migration states in diverse pathological and physiological conditions.

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Cdc42 Is Not Essential for Filopodium Formation, Directed Migration, Cell Polarization, and Mitosis in Fibroblastoid Cells

Molecular Biology of the Cell ◽

10.1091/mbc.e05-01-0061 ◽

2005 ◽

Vol 16 (10) ◽

pp. 4473-4484 ◽

Cited By ~ 112

Author(s):

Aleksandra Czuchra ◽

Xunwei Wu ◽

Hannelore Meyer ◽

Jolanda van Hengel ◽

Timm Schroeder ◽

...

Keyword(s):

Cell Polarity ◽

Cell Shape ◽

Cell Polarization ◽

Small Gtpase ◽

Dominant Negative ◽

Directed Migration ◽

Membrane Blebbing ◽

Directed Cell Migration ◽

Rho Family ◽

Filopodium Formation

Cdc42 is a small GTPase involved in the regulation of the cytoskeleton and cell polarity. To test whether Cdc42 has an essential role in the formation of filopodia or directed cell migration, we generated Cdc42-deficient fibroblastoid cells by conditional gene inactivation. We report here that loss of Cdc42 did not affect filopodium or lamellipodium formation and had no significant influence on the speed of directed migration nor on mitosis. Cdc42-deficient cells displayed a more elongated cell shape and had a reduced area. Furthermore, directionality during migration and reorientation of the Golgi apparatus into the direction of migration was decreased. However, expression of dominant negative Cdc42 in Cdc42-null cells resulted in strongly reduced directed migration, severely reduced single cell directionality, and complete loss of Golgi polarization and of directionality of protrusion formation toward the wound, as well as membrane blebbing. Thus, our data show that besides Cdc42 additional GTPases of the Rho-family, which share GEFs with Cdc42, are involved in the establishment and maintenance of cell polarity during directed migration.

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