RhoA/ROCK-mediated switching between Cdc42- and Rac1-dependent protrusion in MTLn3 carcinoma cells

El‐Sibai, Mirvat; Pertz, Olivier; Pang, Huan; Yip, Shu Chin; Lorenz, Michael G.; Symons, Marc; Condeelis, John S.; Hahn, Klaus M.; Backer, Jonathan M.

doi:10.1016/j.yexcr.2008.01.016

Cited by 85 publications

(88 citation statements)

References 50 publications

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“…14 However, studies examining where Rho GTPases are active in migrating cells demonstrated RhoA activity at the front as well as at the back of a variety of cell types migrating on rigid surfaces. [15][16][17][18] Our work shows for the first time that RhoA is active at the front of T cells under physiological conditions, migrating on and through the pliable EC surface.…”

Section: Rhoa Signaling At the Leading Edge Of Migrating T Cellsmentioning

confidence: 71%

“…For example, RhoA/ ROCK signaling suppresses Rac signaling at the leading edge of EGF-stimulated carcinoma cells, and inhibition of ROCK increased protrusion but reduced migration. 18 Additionally, ROCK/p-MLC is implicated in protrusive force generation at the leading edge of sarcoma cells. 24 ROCKs may drive retraction events to allow cells to reorient their direction of migration.…”

Section: A Possible Role For Rhoa In Integrin Clustersmentioning

confidence: 99%

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Multiple roles for RhoA during T cell transendothelial migration

Heasman

Ridley

2010

Small GTPases

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t cells need to cross endothelial barriers during immune surveillance and inflammation. this involves t-cell adhesion to the endothelium followed by polarization and crawling with a lamellipodium at the front and contractile uropod at the back. t cells subsequently extend lamellipodia and filopodia under the endothelium in order to transmigrate. rho Gtpases play key roles in cell migration by regulating cytoskeletal dynamics and cell adhesion. we have found that the rho Gtpase rhoa is required for efficient t-cell polarization and migration on endothelial cells as well as transendothelial migration. rhoa-depleted cells lack both lamellipodia and uropods, and instead have narrow protrusions extending from a rounded cell body. using a rhoa activity biosensor, we have shown that rhoa is active at the leading edge in lamellipodia and filopodia of crawling and transmigrating t cells, as well as in the uropod. in lamellipodia, its activity correlates with both protrusion and retraction. we predict that rhoa signals via the formin mdia1 during lamellipodial protrusion whereas it induces lamellipodial retraction via the kinase rocK and actomyosin contractility. we propose that different guanine-nucleotide exchange factors (GEfs) are responsible for coordinating rhoa activation and signaling in different regions of transmigrating t cells. IntroductionDuring inflammation leukocytes are recruited from the vasculature into tissues using a specialized migratory pathway. Rho GTPase family proteins are key regulators of cytoskeletal dynamics and cell migration, 3 and thus would be expected to contribute to the process of TEM. Most Rho GTPases cycle between an inactive, GDP-bound form and an active, GTP-bound form, which interacts with and activates downstream targets. Rho GTPases are stimulated by guanine nucleotide exchange factors (GEFs), which stimulate exchange of GDP for GTP and inactivated by GTPaseactivating proteins (GAPs), which stimulate GTP hydrolysis.In our recent paper we used an RNAi screen to identify which Rho GTPases are important for T cell TEM. 4 We found that knockdown of RhoA induced the strongest inhibition of this process and so subsequently examined the role of RhoA in detail during both T cell crawling on EC and subsequent TEM. Significantly, active RhoA was observed at both the front and back of polarized T cells as they crawled on EC and transmigrated, as well as in dynamic puncta in the basal membrane and filopodia extending beneath the endothelium of transmigrating cells ( fig. 1). Here we discuss the implications of these findings in the context of current understanding of RhoA signaling and the potential function of these cellular processes in T-cell migration. Extra View to: Heasman SJ, Carlin LM, Cox S, Ng T, Ridley AJ. Coordinated RhoA signaling at the leading edge and uropod is required for T cell transendothelial migration.

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Section: Rhoa Signaling At the Leading Edge Of Migrating T Cellsmentioning

confidence: 71%

Section: A Possible Role For Rhoa In Integrin Clustersmentioning

confidence: 99%

Multiple roles for RhoA during T cell transendothelial migration

Heasman

Ridley

2010

Small GTPases

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“…This paper also shows that RhoA should be activated at the leading edge of astrocytoma cells, as previously established for breast cancer cells (El-Sibai et al, 2008).…”

Section: Discussionsupporting

confidence: 80%

“…Even though protrusion is unaffected, the absence of focal adhesions leads to an ineffective protrusion with not enough traction force on the ECM for the cells to move forward (Gupton, & Waterman-Storer, 2006). In this system and in other systems (El-Sibai et al, 2008), we have shown that defective adhesions due to inhibition of Rac or RhoA, though they do not affect protrusion, inhibit cell motility. Hence, as we describe a need to inhibit RhoA at the tail of cells, we also confirm the newly described role of RhoA at the leading edge of cancer cells undergoing movement, contrary to the canonical distribution of RhoA activation ( Figure 7).…”

Section: Discussionmentioning

confidence: 66%

“…The role of RhoA at the edge is to allow the maturation of Rac-mediated focal complexes into focal adhesions since the absence of RhoA leads to the absence of focal adhesions and the accumulation of focal complexes (El-Sibai et al, 2008). Even though protrusion is unaffected, the absence of focal adhesions leads to an ineffective protrusion with not enough traction force on the ECM for the cells to move forward (Gupton, & Waterman-Storer, 2006).…”

Section: Discussionmentioning

confidence: 99%

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The regulation of rhoA by stard 13 in focal adhesions is essential for astrocytoma cell motility. (c2013)

Saykali¹

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Effects of ROCK inhibitor Y‐27632 on cell fusion through a microslit

Wada

Hosokawa

Ito

et al. 2015

Biotech & Bioengineering

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We previously reported a direct cytoplasmic transfer method using a microfluidic device, in which cell fusion was induced through a microslit (slit-through-fusion) by the Sendai virus envelope (HVJ-E) to prevent nuclear mixing. However, the method was impractical due to low efficiency of slit-through-fusion formation and insufficient prevention of nuclear mixing. The purpose of this study was to establish an efficient method for inducing slit-through-fusion without nuclear mixing. We hypothesized that modulation of cytoskeletal component can decrease nuclear migration through the microslit considering its functions. Here we report that supplementation with Y-27632, a specific ROCK inhibitor, significantly enhances cell fusion induction and prevention of nuclear mixing. Supplementation with Y-27632 increased the formation of slit-through-fusion efficiency by more than twofold. Disruption of F-actin by Y-27632 prevented nuclear migration between fused cells through the microslit. These two effects of Y-27632 led to promotion of the slit-through-fusion without nuclear mixing with a 16.5-fold higher frequency compared to our previous method (i.e., cell fusion induction by HVJ-E without supplementation with Y-27632). We also confirmed that mitochondria were successfully transferred to the fusion partner under conditions of Y-27632 supplementation. These findings demonstrate the practicality of our cell fusion system in producing direct cytoplasmic transfer between live cells.

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RhoA/ROCK-mediated switching between Cdc42- and Rac1-dependent protrusion in MTLn3 carcinoma cells

Cited by 85 publications

References 50 publications

Multiple roles for RhoA during T cell transendothelial migration

Multiple roles for RhoA during T cell transendothelial migration

The regulation of rhoA by stard 13 in focal adhesions is essential for astrocytoma cell motility. (c2013)

Effects of ROCK inhibitor Y‐27632 on cell fusion through a microslit

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