| Literature DB >> 18804435 |
Teijo Pellinen1, Saara Tuomi1, Antti Arjonen1, Maija Wolf2, Henrik Edgren2, Hannelore Meyer3, Robert Grosse4, Thomas Kitzing4, Juha K Rantala1, Olli Kallioniemi2, Reinhard Fässler3, Marko Kallio1, Johanna Ivaska5.
Abstract
Adherent cells undergo remarkable changes in shape during cell division. However, the functional interplay between cell adhesion turnover and the mitotic machinery is poorly understood. The endo/exocytic trafficking of integrins is regulated by the small GTPase Rab21, which associates with several integrin alpha subunits. Here, we show that targeted trafficking of integrins to and from the cleavage furrow is required for successful cytokinesis, and that this is regulated by Rab21. Rab21 activity, integrin-Rab21 association, and integrin endocytosis are all necessary for normal cytokinesis, which becomes impaired when integrin-mediated adhesion at the cleavage furrow fails. We also describe a chromosomal deletion and loss of Rab21 gene expression in human cancer, which leads to the accumulation of multinucleate cells. Importantly, reintroduction of Rab21 rescued this phenotype. In conclusion, Rab21-regulated integrin trafficking is essential for normal cell division, and its defects may contribute to multinucleation and genomic instability, which are hallmarks of cancer.Entities:
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Year: 2008 PMID: 18804435 DOI: 10.1016/j.devcel.2008.08.001
Source DB: PubMed Journal: Dev Cell ISSN: 1534-5807 Impact factor: 12.270