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Stathmin activity influences sarcoma cell shape, motility, and metastatic potential.
Publication year
2008Source
Molecular Biology of the Cell, 19, 5, (2008), pp. 2003-13ISSN
Publication type
Article / Letter to editor
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Organization
Cell Biology (UMC)
Journal title
Molecular Biology of the Cell
Volume
vol. 19
Issue
iss. 5
Page start
p. 2003
Page end
p. 13
Subject
NCMLS 2: Immune Regulation; NCMLS 2: Metabolism, transport and motion; ONCOL 3: Translational research; UMCN 1.2: Molecular diagnosis, prognosis and monitoringAbstract
The balanced activity of microtubule-stabilizing and -destabilizing proteins determines the extent of microtubule dynamics, which is implicated in many cellular processes, including adhesion, migration, and morphology. Among the destabilizing proteins, stathmin is overexpressed in different human malignancies and has been recently linked to the regulation of cell motility. The observation that stathmin was overexpressed in human recurrent and metastatic sarcomas prompted us to investigate stathmin contribution to tumor local invasiveness and distant dissemination. We found that stathmin stimulated cell motility in and through the extracellular matrix (ECM) in vitro and increased the metastatic potential of sarcoma cells in vivo. On contact with the ECM, stathmin was negatively regulated by phosphorylation. Accordingly, a less phosphorylable stathmin point mutant impaired ECM-induced microtubule stabilization and conferred a higher invasive potential, inducing a rounded cell shape coupled with amoeboid-like motility in three-dimensional matrices. Our results indicate that stathmin plays a significant role in tumor metastasis formation, a finding that could lead to exploitation of stathmin as a target of new antimetastatic drugs.
This item appears in the following Collection(s)
- Academic publications [245104]
- Electronic publications [132391]
- Faculty of Medical Sciences [93207]
- Open Access publications [106009]
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