FMNL2 Drives Actin-Based Protrusion and Migration Downstream of Cdc42

Block, Jennifer; Breitsprecher, Dennis; Kühn, Sonja; Winterhoff, Moritz; Kage, Frieda; Geffers, Robert; Duwe, Patrick; Rohn, Jennifer L.; Baum, Buzz; Brakebusch, Cord; Geyer, Matthias; Stradal, Theresia E. B.; Faix, Jan; Rottner, Klemens

doi:10.1016/j.cub.2012.03.064

Cited by 189 publications

(286 citation statements)

References 34 publications

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“…stress fibers. This suggests that the C-terminus of FHOD1 indeed plays additional roles in FHOD1 function, potentially by augmenting actin monomer recruitment, as reported for the formins mDia1 and FMNL2 (Gould et al, 2011;Block et al, 2012). Alternatively, the sensitivity of the FHOD1 association with stress fibers to ROCK inhibition suggests that dynamic binding and unbinding of FHOD1 to stress fibers, mediated by cycles of phosphorylation and dephosphorylation, might be necessary to activate FHOD1 function fully.…”

Section: Discussionmentioning

confidence: 96%

“…Our observation that a FHOD1 mutant lacking the stress-fibertargeting GBD-FH3 domains associates more prominently with focal adhesions in steady-state conditions further supports this idea. In the lamellipodium, linear filaments are generated by mDia2 or FMNL2 (Yang et al, 2007;Tojkander et al, 2012;Block et al, 2012). Here, FHOD1 might enrich the pool of short actin filaments either by permanent or slow processive capping.…”

Section: Discussionmentioning

confidence: 99%

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FHOD1 regulates stress fiber organization by controlling transversal arc and dorsal fiber dynamics

Schulze

Graessl

Soares

et al. 2014

Journal of Cell Science

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The formin FHOD1 (formin homology 2 domain containing protein 1) can act as a capping and bundling protein in vitro. In cells, active FHOD1 stimulates the formation of ventral stress fibers. However, the cellular mechanisms by which this phenotype is produced and the physiological relevance of FHOD1 function are not currently understood. Here, we first show that FHOD1 controls the formation of two distinct stress fiber precursors differentially. On the one hand, it inhibits dorsal fiber growth, which requires the polymerization of parallel bundles of long actin filaments. On the other hand, it stimulates transverse arcs that are formed by the fusion of short antiparallel actin filaments. This combined action is crucial for the maturation of stress fibers and their spatio-temporal organization, and a lack of FHOD1 function perturbs dynamic cell behavior during cell migration. Furthermore, we show that the GTPase-binding and formin homology 3 domains (GBD and FH3) are responsible for stress fiber association and colocalization with myosin. Surprisingly, a version of FHOD1 that lacks these domains nevertheless retains its full capacity to stimulate arc and ventral stress fiber formation. Based on our findings, we propose a mechanism in which FHOD1 promotes the formation of short actin filaments and transiently associates with transverse arcs, thus providing tight temporal and spatial control of the formation and turnover of transverse arcs into mature ventral stress fibers during dynamic cell behavior.

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Section: Discussionmentioning

confidence: 96%

Section: Discussionmentioning

confidence: 99%

FHOD1 regulates stress fiber organization by controlling transversal arc and dorsal fiber dynamics

Schulze

Graessl

Soares

et al. 2014

Journal of Cell Science

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“…Through this mechanism, INF2 can regulate filament elongation rate and prevent elongation termination by capping proteins (Chesarone et al, 2010;Higgs, 2005). In cells, there is a question as to whether formins nucleate actin filaments or are elongation factors working downstream of other nucleation factors (Block et al, 2012;Quinlan, 2013;Quinlan et al, 2007). The answer to this question might depend on both the formin and the cellular context.…”

Section: Box 1 the Biochemical Properties Of Inf2mentioning

confidence: 99%

Novel roles for actin in mitochondrial fission

Hatch

Gurel

Higgs

2014

Journal of Cell Science

122

126

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Mitochondrial dynamics, including fusion, fission and translocation, are crucial to cellular homeostasis, with roles in cellular polarity, stress response and apoptosis. Mitochondrial fission has received particular attention, owing to links with several neurodegenerative diseases. A central player in fission is the cytoplasmic dynaminrelated GTPase Drp1, which oligomerizes at the fission site and hydrolyzes GTP to drive membrane ingression. Drp1 recruitment to the outer mitochondrial membrane (OMM) is a key regulatory event, which appears to require a pre-constriction step in which the endoplasmic reticulum (ER) and mitochondrion interact extensively, a process termed ERMD (ER-associated mitochondrial division). It is unclear how ER-mitochondrial contact generates the force required for pre-constriction or why pre-constriction leads to Drp1 recruitment. Recent results, however, show that ERMD might be an actin-based process in mammals that requires the ER-associated formin INF2 upstream of Drp1, and that myosin II and other actinbinding proteins might be involved. In this Commentary, we present a mechanistic model for mitochondrial fission in which actin and myosin contribute in two ways; firstly, by supplying the force for preconstriction and secondly, by serving as a coincidence detector for Drp1 binding. In addition, we discuss the possibility that multiple fission mechanisms exist in mammals.

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“…19,20 IQGAP proteins constitute another class of Rac and Cdc42 effectors that bind directly to F-actin, but their multiple functional roles are not yet fully understood. 21 Formation of actin-myosin II filaments has been suggested to determine the rigidity of the lateral and posterior cellular cortex, and to contribute to retraction of the tail during cell migration.…”

Section: A Dual Role Model For Active Rac1 In Cell Migrationmentioning

confidence: 99%