Competition in the chaperone-client network subordinates cell-cycle entry to growth and stress

Moreno, David F.; Parisi, Eva; Yahya, Galal; Vaggi, Federico; Csikász-Nagy, Attila; Aldea Malo, Martí

dc.contributor.author	Moreno, David F.
dc.contributor.author	Parisi, Eva
dc.contributor.author	Yahya, Galal
dc.contributor.author	Vaggi, Federico
dc.contributor.author	Csikász-Nagy, Attila
dc.contributor.author	Aldea Malo, Martí
dc.date.accessioned	2019-10-24T15:09:45Z
dc.date.available	2019-10-24T15:09:45Z
dc.date.issued	2019-04-15
dc.identifier.citation	Moreno, David F.; Parisi, Eva; Yahya, Galal; Vaggi, Federico; Csikasz-Nagy, Attila; Aldea Malo, Martí. «Competition in the chaperone-client network subordinates cell-cycle entry to growth and stress». Life Science Alliance, 2019, vol. 2, núm. 2, art. e201800277. Disponible en: <https://www.life-science-alliance.org/content/2/2/e201800277/tab-rc>. Fecha de acceso: 24 oct. 2019. DOI: 10.26508/lsa.201800277	ca
dc.identifier.issn	2575-1077	ca
dc.identifier.uri	http://hdl.handle.net/20.500.12328/1271
dc.description	We thank A Cornadó and E Rebollo for technical assistance, T Zimmermann for technical advice in FCS experiments, and B Futcher and J Skotheim for providing strains. We also thank C Rose for editing the manuscript and F Antequera, Y Barral, C Gallego, JC Igual, S Oliferenko, and F Posas for helpful comments. This work was funded by the Spanish Ministry of Science, Consolider-Ingenio 2010, and the European Union (FEDER) to M Aldea. DF Moreno received an FI fellowship from Generalitat de Catalunya.	en
dc.description.abstract	The precise coordination of growth and proliferation has a universal prevalence in cell homeostasis. As a prominent property, cell size is modulated by the coordination between these processes in bacterial, yeast, and mammalian cells, but the underlying molecular mechanisms are largely unknown. Here, we show that multifunctional chaperone systems play a concerted and limiting role in cell-cycle entry, specifically driving nuclear accumulation of the G1 Cdk–cyclin complex. Based on these findings, we establish and test a molecular competition model that recapitulates cell-cycle-entry dependence on growth rate. As key predictions at a single-cell level, we show that availability of the Ydj1 chaperone and nuclear accumulation of the G1 cyclin Cln3 are inversely dependent on growth rate and readily respond to changes in protein synthesis and stress conditions that alter protein folding requirements. Thus, chaperone workload would subordinate Start to the biosynthetic machinery and dynamically adjust proliferation to the growth potential of the cell.	ca
dc.format.extent	16	ca
dc.language.iso	eng	ca
dc.publisher	Life Science Alliance	ca
dc.relation.ispartof	Life Science Alliance	ca
dc.relation.ispartofseries	2;2
dc.rights	http://creativecommons.org/licenses/by-nc-nd/4.0/	ca
dc.rights	Attribution-NonCommercial-NoDerivatives 4.0 International	*
dc.rights.uri	http://creativecommons.org/licenses/by-nc-nd/4.0/	*
dc.subject.other	Cicle cel·lular	ca
dc.subject.other	Cell cycle	ca
dc.subject.other	Cells	ca
dc.subject.other	Cells--Growth-Molecular aspects	ca
dc.subject.other	Células	ca
dc.subject.other	Cèl·lules	ca
dc.subject.other	Cèl·lules--Creixement--Aspectes moleculars	ca
dc.title	Competition in the chaperone-client network subordinates cell-cycle entry to growth and stress	ca
dc.type	info:eu-repo/semantics/article	ca
dc.description.version	info:eu-repo/semantics/acceptedVersion	ca
dc.embargo.terms	cap	ca
dc.subject.udc	61	ca
dc.identifier.doi	https://doi.org/10.26508/lsa.201800277	ca