Slit-Robo Repulsive Signaling Extrudes Tumorigenic Cells from Epithelia

Vaughen, John; Igaki, Tatsushi

doi:10.1016/j.devcel.2016.11.015

Cited by 79 publications

(119 citation statements)

References 67 publications

(84 reference statements)

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“…One of the best known roles of Robo signaling is its effect on the cells cytoskeleton (Blockus and Chedotal, 2016; McConnell et al, 2016; Vaughen and Igaki, 2016). Results from our microarray further supported the hypothesis that Slit/Robo signaling has a wider effect on neural crest cells cytoskeleton than previously thought.…”

Section: Resultsmentioning

confidence: 99%

“…Recent findings by Vaughen and Igaki in Drosophila further supports this hypothesis. They present data that demonstrates a role for Slit/Robo via E-cadherin (E-cad) deregulation in extruding tumorigenic cells from epithelia (Vaughen and Igaki, 2016). Their findings help to explain how Slit/Robo signaling acts both as tumor suppressor and/or promoter in variety of cancers, and how this can be applied to the process of NCC becoming migratory upon delamination.…”

Section: Discussionmentioning

confidence: 99%

“…Of especial relevance is the fact that pre-migratory neural crest cells (NCC) express Slits and Robo receptor simultaneously (Giovannone et al, 2012). While we know that trunk neural crest cells are repelled by Slit molecules (Giovannone et al, 2012; Vaughen and Igaki, 2016; Zuhdi et al, 2015), and that neural crest cells over-expressing Robo1-Δ-67 do not migrate along their ventromedial pathway (Jia et al, 2005), we still do not have a clear picture among the many possible downstream pathways of Robo, which ones are involved in these responses (Blockus and Chedotal, 2016). Are Slit molecules modulating the proliferation of neural crest cells?…”

Section: Introductionmentioning

confidence: 99%

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Screen for Slit/Robo signaling in trunk neural cells reveals new players

Martinez

Zuhdi

Reyes

et al. 2018

Gene Expression Patterns

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Slits ligands and their Robo receptors are involved in quite disparate cell signaling pathways that include axon guidance, cell proliferation, cell motility and angiogenesis. Neural crest cells emerge by delamination from neural cells in the dorsal neural tube, and give rise to various components of the peripheral nervous system in vertebrates. It is well established that these cells change from a non-migratory to a highly migratory state allowing them to reach distant regions before they differentiate. However, but the mechanism controlling this delamination and subsequent migration are still not fully understood. The repulsive Slit ligand family members, have been classified also as true tumor suppressor molecules. The present study explored in further detail what possible Slit/Robo signals are at play in the trunk neural cells and neural crest cells by carrying out a microarray after Slit2 gain of function in trunk neural tubes. We found that in addition to molecules known to be downstream of Slit/Robo signaling, there were a large set of molecules known to be important in maintaining cells in non-motile, epithelia phenotype. Furthermore, we found new molecules previously not associated with Slit/Robo signaling: cell proliferation markers, Ankyrins and RAB intracellular transporters. Our findings suggest that neural crest cells use and array of different Slit/Robo pathways during their transformation from non-motile to highly motile cells.

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Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Screen for Slit/Robo signaling in trunk neural cells reveals new players

Martinez

Zuhdi

Reyes

et al. 2018

Gene Expression Patterns

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“…In flies, Slit/Robo signaling inhibits the formation of cadherin-mediated cell-cell junctions during heart development (Santiago-Martinez et al 2008). An interesting recent study in Drosophila provides evidence that Slit/Robo repellent signaling through JNK extrudes tumorigenic cells from epithelia by disrupting E-cadherin function (Vaughen and Igaki 2016). The investigators found that overexpression of Slit/Robo2 results in cells being dislocated from the epithelial surface, resulting in tumor formation within the luminal space.…”

Section: Slit-robo Regulation Of Adherens Junctionsmentioning

confidence: 99%

“…The investigators found that overexpression of Slit/Robo2 results in cells being dislocated from the epithelial surface, resulting in tumor formation within the luminal space. In contrast, loss of Slit/Robo2 signaling prevents cell extrusion, leading to tumor growth within the epithelium (Vaughen and Igaki 2016). In this way, the investigators propose that both over-and underactivation of Slit/Robo2 signaling contributes to tumorigenesis and cancer progression.…”

Section: Slit-robo Regulation Of Adherens Junctionsmentioning

confidence: 99%

Making Connections: Guidance Cues and Receptors at Nonneural Cell–Cell Junctions

Beamish

Hinck

Kennedy

2017

Cold Spring Harb Perspect Biol

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The field of axon guidance was revolutionized over the past three decades by the identification of highly conserved families of guidance cues and receptors. These proteins are essential for normal neural development and function, directing cell and axon migration, neuron-glial interactions, and synapse formation and plasticity. Many of these genes are also expressed outside the nervous system in which they influence cell migration, adhesion and proliferation. Because the nervous system develops from neural epithelium, it is perhaps not surprising that these guidance cues have significant nonneural roles in governing the specialized junctional connections between cells in polarized epithelia. The following review addresses roles for ephrins, semaphorins, netrins, slits and their receptors in regulating adherens, tight, and gap junctions in nonneural epithelia and endothelia.

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Cell competition: emerging signaling and unsolved questions

Nagata,

Igaki

2024

FEBS Letters

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Multicellular communities have an intrinsic mechanism that optimizes their structure and function via cell–cell communication. One of the driving forces for such self‐organization of the multicellular system is cell competition, the elimination of viable unfit or deleterious cells via cell–cell interaction. Studies in Drosophila and mammals have identified multiple mechanisms of cell competition caused by different types of mutations or cellular changes. Intriguingly, recent studies have found that different types of “losers” of cell competition commonly show reduced protein synthesis. In Drosophila, the reduction in protein synthesis levels in loser cells is caused by phosphorylation of the translation initiation factor eIF2α via a bZip transcription factor Xrp1. Given that a variety of cellular stresses converge on eIF2α phosphorylation and thus global inhibition of protein synthesis, cell competition may be a machinery that optimizes multicellular fitness by removing stressed cells. In this review, we summarize and discuss emerging signaling mechanisms and critical unsolved questions, as well as the role of protein synthesis in cell competition.

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Slit-Robo Repulsive Signaling Extrudes Tumorigenic Cells from Epithelia

Cited by 79 publications

References 67 publications

Screen for Slit/Robo signaling in trunk neural cells reveals new players

Screen for Slit/Robo signaling in trunk neural cells reveals new players

Making Connections: Guidance Cues and Receptors at Nonneural Cell–Cell Junctions

Cell competition: emerging signaling and unsolved questions

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