The actin cross-linker Filamin/Cheerio mediates tumor malignancy downstream of JNK signaling

Külshammer, Eva; Uhlířová, Mirka

doi:10.1242/jcs.114462

Cited by 55 publications

(104 citation statements)

References 69 publications

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“…Notably, Slit’s highly conserved human homolog (Slit2) and human Robo2 both possess human AP1 binding sites (ATGAGTCAT; three in Slit2 and nine in Robo2, data not shown), supporting that JNK-activated Slit-Robo could occur in mammals. Interestingly, in scrib + Ras V1 2 tumors, JNK upregulates the actin crosslinker Filamin/Cheerio to mediate metastasis (Külshammer and Uhlirova, 2013). Different JNK-activated actin regulators may therefore prevent or promote tumorigenesis depending on the tumor’s genetic context.…”

Section: Discussionmentioning

confidence: 99%

Slit-Robo Repulsive Signaling Extrudes Tumorigenic Cells from Epithelia

2016

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SUMMARY Cells dynamically interact throughout animal development to coordinate growth and deter disease. For example, cell-cell competition weeds out aberrant cells to enforce homeostasis. In Drosophila, tumorigenic cells mutant for the cell polarity gene scribble (scrib) are actively eliminated from epithelia when surrounded by wild-type cells. While scrib cell elimination depends critically on JNK signaling, JNK-dependent cell death cannot sufficiently explain scrib cell extirpation. Thus, how JNK executed cell elimination remained elusive. Here, we show that repulsive Slit-Robo2-Ena signaling exerts an extrusive force downstream of JNK to eliminate scrib cells from epithelia by disrupting E-cadherin. While loss of Slit-Robo2-Ena in scrib cells potentiates scrib tumor formation within the epithelium, Robo2-Ena hyperactivation surprisingly triggers luminal scrib tumor growth following excess extrusion. This extrusive signaling is amplified by a positive feedback loop between Slit-Robo2-Ena and JNK. Our observations provide a potential causal mechanism for Slit-Robo dysregulation in numerous human cancers.

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Section: Discussionmentioning

confidence: 99%

Slit-Robo Repulsive Signaling Extrudes Tumorigenic Cells from Epithelia

2016

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“…Moreover, JNK reportedly regulates actin cytoskeleton dynamics and organization of the membrane skeleton. The former effect has been linked to JNK-dependent modulation of different actin binding proteins, such as ezrin, drebrin, and filamin in epithelial cells [59, 77, 83]. The latter effect was manifested by JNK-dependent phosphorylation of adducins in tumor cells [84], and disorganization of cortical α-spectrin in cardiomyocytes [85].…”

Section: Discussionmentioning

confidence: 99%

F-actin binding protein, anillin, regulates integrity of intercellular junctions in human epithelial cells

Wang

Chadha

Feygin

et al. 2015

Cell. Mol. Life Sci.

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Tight junctions (TJ) and adherens junctions (AJ) are key morphological features of differentiated epithelial cells that regulate the integrity and permeability of tissue barriers. Structure and remodeling of epithelial junctions depends on their association with the underlying actomyosin cytoskeleton. Anillin is a unique scaffolding protein interacting with different cytoskeletal components, including actin filaments and myosin motors. Its role in the regulation of mammalian epithelial junctions remains unexplored. Downregulation of anillin expression in human prostate, colonic, and lung epithelial cells triggered AJ and TJ disassembly without altering the expression of junctional proteins. This junctional disassembly was accompanied by dramatic disorganization of the perijunctional actomyosin belt; while the general architecture of the actin cytoskeleton, and activation status of non-muscle myosin II, remained unchanged. Furthermore, loss of anillin disrupted the adducin-spectrin membrane skeleton at the areas of cell-cell contact, selectively decreased γ-adducin expression, and induced cytoplasmic aggregation of αII-spectrin. Anillin knockdown activated c-Jun N-terminal kinase (JNK), and JNK inhibition restored AJ and TJ integrity and cytoskeletal organization in anillin-depleted cells. These findings suggest a novel role for anillin in regulating intercellular adhesion in model human epithelia by mechanisms involving the suppression of JNK activity and controlling the assembly of the perijunctional cytoskeleton.

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“…However, in lgl mutant clones in the EAD, blocking JNK enhances the clonal overgrowth and leads to loss of polarity and an invasive phenotype (Grzeschik et al, 2010), and blocking JNK in scrib mutant EAD clones does not prevent, but rather enhances, the impairment of the Hippo pathway (Doggett et al, 2011). Interestingly, a recent study has revealed that, in scrib − + Ras ACT tumours, JNK activation upregulates expression of an F-actin cross-linking protein, Filamin (Cher), which acts to inhibit the Hippo pathway to promote overgrowth (Külshammer and Uhlirova, 2012). Therefore, although RhoGEF2-Rho1 + Ras ACT -mediated tumorigenesis requires JNK activation for the block to differentiation and pupation, and to promote invasion, whether JNK can also have a role in cell morphology changes or promoting proliferation via inhibition of the Hippo pathway in these tumours requires further investigation.…”

Section: Discussionmentioning

confidence: 99%

“…Whether these mechanisms contribute to the tumour growth of RhoGEF2–Rho1–Rok–Myosin-II with activated Ras in Drosophila epithelial tissues will require further analysis. Interestingly, a recent study revealed that Drosophila Filamin (Cher) binds to Myosin II and is important for activation of Myosin II activity in scrib − + Ras ACT tumours, and also that Myosin II activity is important for tumour overgrowth, via Hippo pathway inactivation, as well as invasion (Külshammer and Uhlirova, 2012). Thus, the cooperation of cell polarity mutants with oncogenic Ras might also require the RhoGEF2–Rho1–Rok–Myosin-II pathway.…”

Section: Discussionmentioning

confidence: 99%

InDrosophila, RhoGEF2 cooperates with activated Ras in tumorigenesis through a pathway involving Rho1–Rok–Myosin-II and JNK signalling

Khoo

Allan

Willoughby

et al. 2013

Disease Models &Amp; Mechanisms

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SUMMARYThe Ras oncogene contributes to ∼30% of human cancers, but alone is not sufficient for tumorigenesis. In a Drosophila screen for oncogenes that cooperate with an activated allele of Ras (RasACT) to promote tissue overgrowth and invasion, we identified the GTP exchange factor RhoGEF2, an activator of Rho-family signalling. Here, we show that RhoGEF2 also cooperates with an activated allele of a downstream effector of Ras, Raf (RafGOF). We dissect the downstream pathways through which RhoGEF2 cooperates with RasACT (and RafGOF), and show that RhoGEF2 requires Rho1, but not Rac, for tumorigenesis. Furthermore, of the Rho1 effectors, we show that RhoGEF2 + Ras (Raf)-mediated tumorigenesis requires the Rho kinase (Rok)–Myosin-II pathway, but not Diaphanous, Lim kinase or protein kinase N. The Rho1–Rok–Myosin-II pathway leads to the activation of Jun kinase (JNK), in cooperation with RasACT. Moreover, we show that activation of Rok or Myosin II, using constitutively active transgenes, is sufficient for cooperative tumorigenesis with RasACT, and together with RasACT leads to strong activation of JNK. Our results show that Rok–Myosin-II activity is necessary and sufficient for Ras-mediated tumorigenesis. Our observation that activation of Myosin II, which regulates Filamentous actin (F-actin) contractility without affecting F-actin levels, cooperates with RasACT to promote JNK activation and tumorigenesis, suggests that increased cell contractility is a key factor in tumorigenesis. Furthermore, we show that signalling via the Tumour necrosis factor (TNF; also known as Egr)-ligand–JNK pathway is most likely the predominant pathway that activates JNK upon Rok activation. Overall, our analysis highlights the need for further analysis of the Rok–Myosin-II pathway in cooperation with Ras in human cancers.

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The actin cross-linker Filamin/Cheerio mediates tumor malignancy downstream of JNK signaling

Cited by 55 publications

References 69 publications

Slit-Robo Repulsive Signaling Extrudes Tumorigenic Cells from Epithelia

Slit-Robo Repulsive Signaling Extrudes Tumorigenic Cells from Epithelia

F-actin binding protein, anillin, regulates integrity of intercellular junctions in human epithelial cells

InDrosophila, RhoGEF2 cooperates with activated Ras in tumorigenesis through a pathway involving Rho1–Rok–Myosin-II and JNK signalling

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