Centromeric signaling proteins boost G1 cyclin degradation and modulate cell size in budding yeast
Fecha de publicación
2018-08-06ISSN
1544-9173
Resumen
Cell size scales with ploidy in a great range of eukaryotes, but the underlying mechanisms
remain unknown. Using various orthogonal single-cell approaches, we show that cell size
increases linearly with centromere (CEN) copy number in budding yeast. This effect is due
to a G1 delay mediated by increased degradation of Cln3, the most upstream G1 cyclin acting
at Start, and specific centromeric signaling proteins, namely Mad3 and Bub3. Mad3
binds both Cln3 and Cdc4, the adaptor component of the Skp1/Cul1/F-box (SCF) complex
that targets Cln3 for degradation, these interactions being essential for the CEN-dosage
dependent effects on cell size. Our results reveal a pathway that modulates cell size as a
function of CEN number, and we speculate that, in cooperation with other CEN-independent
mechanisms, it could assist the cell to attain efficient mass/ploidy ratios
Tipo de documento
Artículo
Versión del documento
Versión aceptada
Lengua
Inglés
Materias (CDU)
61 - Medicina
Páginas
13
Publicado por
Public Library of Science
Colección
16; 8
Publicado en
PLoS Biology
Citación recomendada
Martínez-Láinez, Joan M.; Moreno, David F.; Parisi, Eva; Clotet, Josep; Aldea Malo, Martí. «Centromeric signaling proteins boost G1 cyclin degradation and modulate cell size in budding yeast». PLoS Biology, 2018, vol. 16, núm. 8, art. e2005388. Disponible en: <https://journals.plos.org/plosbiology/article?id=10.1371/journal.pbio.2005388>. Fecha de acceso: 24 oct. 2019. DOI: 10.1371/journal.pbio.2005388
Nota
Ministry of Economy and Competitiveness of Spain (grant number BFU2016-80234-R to MA and BFU 2013-44189-P to JC). JMM-L and DFM acknowledge fellowhips of the FI program of Generalitat de Catalunya. The funder had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript.
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http://creativecommons.org/licenses/by-nc-nd/4.0/
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