| Literature DB >> 17363900 |
Michela Zuccolo1, Annabelle Alves, Vincent Galy, Stéphanie Bolhy, Etienne Formstecher, Victor Racine, Jean-Baptiste Sibarita, Tatsuo Fukagawa, Ramin Shiekhattar, Tim Yen, Valérie Doye.
Abstract
We previously demonstrated that a fraction of the human Nup107-160 nuclear pore subcomplex is recruited to kinetochores at the onset of mitosis. However, the molecular determinants for its kinetochore targeting and the functional significance of this localization were not investigated. Here, we show that the Nup107-160 complex interacts with CENP-F, but that CENP-F only moderately contributes to its targeting to kinetochores. In addition, we show that the recruitment of the Nup107-160 complex to kinetochores mainly depends on the Ndc80 complex. We further demonstrate that efficient depletion of the Nup107-160 complex from kinetochores, achieved either by combining siRNAs targeting several of its subunits excluding Seh1, or by depleting Seh1 alone, induces a mitotic delay. Further analysis of Seh1-depleted cells revealed impaired chromosome congression, reduced kinetochore tension and kinetochore-microtubule attachment defects. Finally, we show that the presence of the Nup107-160 complex at kinetochores is required for the recruitment of Crm1 and RanGAP1-RanBP2 to these structures. Together, our data thus provide the first molecular clues underlying the function of the human Nup107-160 complex at kinetochores.Entities:
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Year: 2007 PMID: 17363900 PMCID: PMC1847668 DOI: 10.1038/sj.emboj.7601642
Source DB: PubMed Journal: EMBO J ISSN: 0261-4189 Impact factor: 11.598