<scp>ROCK</scp>
            2 inhibition triggers the collective invasion of colorectal adenocarcinomas

Libanje, Fotine; Raingeaud, Joël; Luan, Rui; Thomas, ZoéAp; Zajac, Olivier; Veiga, Joel Paulo Russomano; Marisa, Laëtitia; Adam, Julien; Boige, Valérie; Malka, David; Goèré, Diane; Hall, Alan; Soazec, Jean-Yves; Prall, Friedrich; Gelli, Maximiliano; Dartigues, Peggy; Jaulin, Fanny

doi:10.15252/embj.201899299

Cited by 52 publications

(39 citation statements)

References 103 publications

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“…The low-contractile-force phenotype differs from the view that contractile tension increases with cell transformation in cancer (Paszek et al, 2005) and that a higher rigidity of the extracellular environment and a high-contractile-force phenotype favor cell invasiveness (Butcher et al, 2009;Kraning-Rush et al, 2012;Mierke et al, 2011). Rather, our results suggest that the relaxation of contractile forces is associated with cell scattering and migration, as it has been observed in HMECs with super-numerary centrosomes that form invasive structures in 3D cultures (Godinho et al, 2014), in cells at the front of invasive colorectal carcinomas (Libanje et al, 2019) or in metastatic osteosarcoma cells (Holenstein et al, 2019). By contrast, a high-contractile-force phenotype is more likely to promote primary tumor growth, cell survival in circulation, and at a secondary site, cell adhesion, aggregation, and the formation of a metastatic tumor (Rodriguez-Hernandez et al, 2016;Tavares et al, 2017).…”

Section: The Initiation Of Emt and Establishment Of The Intermediate contrasting

confidence: 68%

Biophysical properties of intermediate states of EMT outperform both epithelial and mesenchymal states

Margaron

Nagai

Guyon

et al. 2019

Preprint

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Potential metastatic cells can dissociate from a primary breast tumor by undergoing an epithelial-to-mesenchymal transmission (EMT). Recent work has revealed that cells in intermediate states of EMT acquire an augmented capacity for tumor-cell dissemination. These states have been characterized by molecular markers, but the structural features and the cellular mechanisms that underlie the acquisition of their invasive properties are still unknown. Using human mammary epithelial cells, we generated cells in intermediate states of EMT through the induction of a single EMT-inducing transcription factor, ZEB1, and cells in a mesenchymal state by stimulation with TGFβ. In stereotypic and spatially-defined culture conditions, the architecture, internal organization and mechanical properties of cells in the epithelial, intermediate and mesenchymal state were measured and compared. We found that the lack of intercellular cohesiveness in epithelial and mesenchymal cells can be detected early by microtubule destabilization and the repositioning of the centrosome from the cell-cell junction to the cell center. Consistent with their high migration velocities, cells in intermediate states produced low contractile forces compared with epithelial and mesenchymal cells. The high contractile forces in mesenchymal cells powered a retrograde flow pushing the nucleus away from cell adhesion to the extracellular matrix. Therefore, cells in intermediate state had structural and mechanical properties that were distinct but not necessarily intermediate between epithelial and mesenchymal cells. Based on these observations, we found that a panel of triple-negative breast cancer lines had intermediate rather than mesenchymal characteristics suggesting that the structural and mechanical properties of the intermediate state are important for understanding tumor-cell dissemination.

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Section: The Initiation Of Emt and Establishment Of The Intermediate contrasting

confidence: 68%

Biophysical properties of intermediate states of EMT outperform both epithelial and mesenchymal states

Margaron

Nagai

Guyon

et al. 2019

Preprint

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“…Our results also appear in apparent contradiction with those obtained by Vishnubhotla and collaborators who reported that ROCK-2 was highly expressed in SW620 colon cancer cells, mainly distributed in invadopodial-like structures and that its knock-down reduced the depth of invasion into a 3D-scaffold of type I collagen 61 . However, our results are in line with those recently reported by Libanje and collaborators who demonstrated that colorectal cancer cells mainly harbour a collective mode of invasion and that ROCK-2 inhibition triggers the initial induction of leader cell formation and induces collective invasion from cysts 62 . Therefore, these apparently contrasting results should probably be studied with regard to the different growing modes and environmental conditions (2D vs 3D, type and stiffness of the extracellular matrix, etc.)…”

Section: Discussionsupporting

confidence: 93%

Rock inhibition promotes NaV1.5 sodium channel-dependent SW620 colon cancer cell invasiveness

Poisson

Lopez‐Charcas

Chadet

et al. 2020

Sci Rep

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The acquisition of invasive capacities by carcinoma cells, i.e. their ability to migrate through and to remodel extracellular matrices, is a determinant process leading to their dissemination and to the development of metastases. these cancer cell properties have often been associated with an increased Rho-ROCK signalling, and ROCK inhibitors have been proposed for anticancer therapies. In this study we used the selective ROCK inhibitor, Y-27632, to address the participation of the Rho-ROCK signalling pathway in the invasive properties of SW620 human colon cancer cells. Contrarily to initial assumptions, Y-27632 induced the acquisition of a pro-migratory cell phenotype and increased cancer cell invasiveness in both 3-and 2-dimensions assays. This effect was also obtained using the other ROCK inhibitor Fasudil as well as with knocking down the expression of ROCK-1 or ROCK-2, but was prevented by the inhibition of na V 1.5 voltage-gated sodium channel activity. Indeed, ROCK inhibition enhanced the activity of the pro-invasive na V 1.5 channel through a pathway that was independent of gene expression regulation. In conclusions, our evidence identifies voltage-gated sodium channels as new targets of the ROCK signalling pathway, as well as responsible for possible deleterious effects of the use of ROCK inhibitors in the treatment of cancers.

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“…Cancer organoids have also been used to model metastatic processes, in particular to investigate the different processes of invasion [164,165]. For example, a study conducted on CRC organoids showed that inhibition of rho-associated protein kinase 2 (ROCK2) improved collective invasion in its early stages [166].…”

Section: Organoids As a Model To Study Tumorigenesismentioning

confidence: 99%

Modeling neoplastic disease with spheroids and organoids

et al. 2020

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Cancer is a complex disease in which both genetic defects and microenvironmental components contribute to the development, progression, and metastasization of disease, representing major hurdles in the identification of more effective and safer treatment regimens for patients. Three-dimensional (3D) models are changing the paradigm of preclinical cancer research as they more closely resemble the complex tissue environment and architecture found in clinical tumors than in bidimensional (2D) cell cultures. Among 3D models, spheroids and organoids represent the most versatile and promising models in that they are capable of recapitulating the heterogeneity and pathophysiology of human cancers and of filling the gap between conventional 2D in vitro testing and animal models. Such 3D systems represent a powerful tool for studying cancer biology, enabling us to model the dynamic evolution of neoplastic disease from the early stages to metastatic dissemination and the interactions with the microenvironment. Spheroids and organoids have recently been used in the field of drug discovery and personalized medicine. The combined use of 3D models could potentially improve the robustness and reliability of preclinical research data, reducing the need for animal testing and favoring their transition to clinical practice. In this review, we summarize the recent advances in the use of these 3D systems for cancer modeling, focusing on their innovative translational applications, looking at future challenges, and comparing them with most widely used animal models.

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ROCK 2 inhibition triggers the collective invasion of colorectal adenocarcinomas

Cited by 52 publications

References 103 publications

Biophysical properties of intermediate states of EMT outperform both epithelial and mesenchymal states

Biophysical properties of intermediate states of EMT outperform both epithelial and mesenchymal states

Rock inhibition promotes NaV1.5 sodium channel-dependent SW620 colon cancer cell invasiveness

Modeling neoplastic disease with spheroids and organoids

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