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Inactivation of PTEN and ZFHX3 in Mammary Epithelial Cells Alters Patterns of Collective Cell Migration
Authors:Ali Dayoub  Artem I. Fokin  Maria E. Lomakina  John James  Marina Plays  Tom Jacquin  Nikita M. Novikov  Rostislav S. Vorobyov  Anastasia A. Schegoleva  Karina D. Rysenkova  Julia Gaboriaud  Sergey V. Leonov  Evgeny V. Denisov  Alexis M. Gautreau  Antonina Y. Alexandrova
Affiliation:1.N.N. Blokhin Cancer Research Center of the Ministry of Health of the Russian Federation, 115478 Moscow, Russia;2.Ecole Polytechnique, Institut Polytechnique de Paris, 91120 Palaiseau, France;3.Moscow Institute of Physics and Technology, 141700 Dolgoprudny, Russia;4.Cancer Research Institute, Tomsk National Research Medical Center, Russian Academy of Sciences, 634009 Tomsk, Russia
Abstract:Whole exome sequencing of invasive mammary carcinomas revealed the association of mutations in PTEN and ZFHX3 tumor suppressor genes (TSGs). We generated single and combined PTEN and ZFHX3 knock-outs (KOs) in the immortalized mammary epithelial cell line MCF10A to study the role of these genes and their potential synergy in migration regulation. Inactivation of PTEN, but not ZFHX3, induced the formation of large colonies in soft agar. ZFHX3 inactivation in PTEN KO, however, increased colony numbers and normalized their size. Cell migration was affected in different ways upon PTEN and ZFHX3 KO. Inactivation of PTEN enhanced coordinated cell motility and thus, the collective migration of epithelial islets and wound healing. In contrast, ZFHX3 knockout resulted in the acquisition of uncoordinated cell movement associated with the appearance of immature adhesive junctions (AJs) and the increased expression of the mesenchymal marker vimentin. Inactivation of the two TSGs thus induces different stages of partial epithelial-to-mesenchymal transitions (EMT). Upon double KO (DKO), cells displayed still another motile state, characterized by a decreased coordination in collective migration and high levels of vimentin but a restoration of mature linear AJs. This study illustrates the plasticity of migration modes of mammary cells transformed by a combination of cancer-associated genes.
Keywords:cell migration   epithelial-to-mesenchymal transition   partial EMT   vimentin   E-cadherin   adherens junctions
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