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    Ingression Progression Complexes Control Extracellular Matrix Remodelling during Cytokinesis in Budding Yeast

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    Identificadores
    URI: http://hdl.handle.net/10902/10976
    DOI: 10.1371/journal.pgen.1005864
    ISSN: 1553-7390
    ISSN: 1553-7404
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    Autoría
    Foltman, MagdalenaAutoridad Unican; Molist Pérez, Iago; Arcones, Irene; Sacristán, Carlos; Filali-Mouncef Lazcano, Yasmina; Roncero, César; Sánchez Díaz, AlbertoAutoridad Unican
    Fecha
    2016
    Derechos
    © 2016 Foltman et al. This is an open access article distributed under the terms of the Creative Commons Attribution License.
    Publicado en
    PLoS Genet 12(2): e1005864
    Editorial
    Public Library of Science
    Resumen/Abstract
    Eukaryotic cells must coordinate contraction of the actomyosin ring at the division site together with ingression of the plasma membrane and remodelling of the extracellular matrix (ECM) to support cytokinesis, but the underlying mechanisms are still poorly understood. In eukaryotes, glycosyltransferases that synthesise ECM polysaccharides are emerging as key factors during cytokinesis. The budding yeast chitin synthase Chs2 makes the primary septum, a special layer of the ECM, which is an essential process during cell division. Here we isolated a group of actomyosin ring components that form complexes together with Chs2 at the cleavage site at the end of the cell cycle, which we named ‘ingression progression complexes’ (IPCs). In addition to type II myosin, the IQGAP protein Iqg1 and Chs2, IPCs contain the F-BAR protein Hof1, and the cytokinesis regulators Inn1 and Cyk3. We describe the molecular mechanism by which chitin synthase is activated by direct association of the C2 domain of Inn1, and the transglutaminase-like domain of Cyk3, with the catalytic domain of Chs2. We used an experimental system to find a previously unanticipated role for the C-terminus of Inn1 in preventing the untimely activation of Chs2 at the cleavage site until Cyk3 releases the block on Chs2 activity during late mitosis. These findings support a model for the co-ordinated regulation of cell division in budding yeast, in which IPCs play a central role.
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    UNIVERSIDAD DE CANTABRIA

    Repositorio realizado por la Biblioteca Universitaria utilizando DSpace software
    Contacto | Sugerencias
    Metadatos sujetos a:licencia de Creative Commons Reconocimiento 4.0 España