Literature DB >> 27347214

Snail levels control the migration mechanism of mesenchymal tumor cells.

Cristina Belgiovine1, Giulio Chiesa1, Ilaria Chiodi1, Roberta Frapolli2, Katiuscia Bonezzi3, Giulia Taraboletti3, Maurizio D'Incalci2, Chiara Mondello1.   

Abstract

Cancer cells use two major types of movement: Mesenchymal, which is typical of cells of mesenchymal origin and depends on matrix metalloproteinase (MMP) activity, and amoeboid, which is characteristic of cells with a rounded shape and relies on the activity of Rho-associated kinase (ROCK). The present authors previously demonstrated that, during neoplastic transformation, telomerase-immortalized human fibroblasts (cen3tel cells) acquired a ROCK-dependent/MMP independent mechanism of invasion, mediated by the downregulation of the ROCK cellular inhibitor Round (Rnd)3/RhoE. In the present study, cen3tel transformation was also demonstrated to be paralleled by downregulation of Snail, a major determinant of the mesenchymal movement. To test whether Snail levels could determine the type of movement adopted by mesenchymal tumor cells, Snail was ectopically expressed in tumorigenic cells. It was observed that ectopic Snail did not increase the levels of typical mesenchymal markers, but induced cells to adopt an MMP-dependent mechanism of invasion. In cells expressing ectopic Snail, invasion became sensitive to the MMP inhibitor Ro 28-2653 and insensitive to the ROCK inhibitor Y27632, suggesting that, once induced by Snail, the mesenchymal movement prevails over the amoeboid one. Snail-expressing cells had a more aggressive behavior in vivo, and exhibited increased tumor growth rate and metastatic ability. These results confirm the high plasticity of cancer cells, which can adopt different types of movement in response to changes in the expression of specific genes. Furthermore, the present findings indicate that Rnd3 and Snail are possible regulators of the type of invasion mechanism adopted by mesenchymal tumor cells.

Entities:  

Keywords:  MMP; ROCK; Rnd3/RhoE; Snail; amoeboid movement; mesenchymal movement

Year:  2016        PMID: 27347214      PMCID: PMC4907273          DOI: 10.3892/ol.2016.4642

Source DB:  PubMed          Journal:  Oncol Lett        ISSN: 1792-1074            Impact factor:   2.967


  21 in total

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4.  Dual regulation of Snail by GSK-3beta-mediated phosphorylation in control of epithelial-mesenchymal transition.

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7.  Induction of a MT1-MMP and MT2-MMP-dependent basement membrane transmigration program in cancer cells by Snail1.

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Authors:  R Grant Rowe; Xiao-Yan Li; Yuexian Hu; Thomas L Saunders; Ismo Virtanen; Antonio Garcia de Herreros; Karl-Friedrich Becker; Signe Ingvarsen; Lars H Engelholm; Guido T Bommer; Eric R Fearon; Stephen J Weiss
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9.  Compensation mechanism in tumor cell migration: mesenchymal-amoeboid transition after blocking of pericellular proteolysis.

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10.  Loss of p53 promotes RhoA-ROCK-dependent cell migration and invasion in 3D matrices.

Authors:  Gilles Gadea; Marion de Toledo; Christelle Anguille; Pierre Roux
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2.  Loss of BAP1 Results in Growth Inhibition and Enhances Mesenchymal-Epithelial Transition in Kidney Tumor Cells.

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