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dc.contributor.authorBradbury, Peta
dc.contributor.authorFabry, Ben
dc.contributor.authorO’Neill, Geraldine M.
dc.date.accessioned2016-08-30
dc.date.available2016-08-30
dc.date.issued2012-09-01
dc.identifier.citationPeta Bradbury, Ben Fabry & Geraldine M. O'Neill (2012) Occupy tissue, Cell Adhesion & Migration, 6:5, 424-520, DOI: 10.4161/cam.21559en
dc.identifier.urihttp://hdl.handle.net/2123/15570
dc.description.abstractThe critical role of migration and invasion in cancer metastasis warrants new therapeutic approaches targeting the machinery regulating cell migration and invasion. While 2-dimensional (2D) models have helped identify a range of adhesion molecules, cytoskeletal components and regulators that are potentially important for cell migration, the use of models that better mimic the 3-dimensional (3D) environment has yielded new insights into the physiology of cell movement. For example, studying cells in 3D models has revealed that invading cancer cells may switch between heterogeneous invasion modes and thus evade pharmacological inhibition of invasion. Here we summarize published data in which the role of cell adhesion molecules in 2D vs. 3D migration have been directly compared and discuss mechanisms that regulate migration speed and persistence in 2D and 3D. Finally we discuss limits of 3D culture models to recapitulate the in vivo situation.en
dc.description.sponsorshipNHMRC Grant 632515en
dc.language.isoen_AUen
dc.publisherTaylor & Francisen
dc.rightsOther
dc.subjectmigrationen
dc.subjectinvasionen
dc.subjectmetastasisen
dc.subjectadhesionen
dc.subject3Den
dc.subject2Den
dc.titleOccupy tissue: the movement in cancer metastasisen
dc.typeArticleen
dc.identifier.doi10.4161/cam.21559
dc.type.pubtypeAuthor accepted manuscripten
usyd.facultyFaculty of Medicine and Health, School of Medical Sciencesen
usyd.departmentDiscipline of Pharmacologyen


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