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Reference - PMID:32084401 - The Hydrophobic Patch Directs Cyclin B to Centrosomes to Promote Global CDK Phosphorylation at Mitosis.

Reference summary

PubMed ID
PMID:32084401
Title
The Hydrophobic Patch Directs Cyclin B to Centrosomes to Promote Global CDK Phosphorylation at Mitosis.
Authors
Basu S, Roberts EL, Jones AW, Swaffer MP, Snijders AP, Nurse P
Citation
Curr Biol 2020 Mar 09;30(5):883-892.e4
Publication year
2020
Abstract
The cyclin-dependent kinases (CDKs) are the major cell-cycle regulators that phosphorylate hundreds of substrates, controlling the onset of S phase and M phase [1-3]. However, the patterns of substrate phosphorylation increase are not uniform, as different substrates become phosphorylated at different times as cells proceed through the cell cycle [4, 5]. In fission yeast, the correct ordering of CDK substrate phosphorylation can be established by the activity of a single mitotic cyclin-CDK complex [6, 7]. Here, we investigate the substrate-docking region, the hydrophobic patch, on the fission yeast mitotic cyclin Cdc13 as a potential mechanism to correctly order CDK substrate phosphorylation. We show that the hydrophobic patch targets Cdc13 to the yeast centrosome equivalent, the spindle pole body (SPB), and disruption of this motif prevents both centrosomal localization of Cdc13 and the onset of mitosis but does not prevent S phase. CDK phosphorylation in mitosis is compromised for approximately half of all mitotic CDK substrates, with substrates affected generally being those that require the highest levels of CDK activity to become phosphorylated and those that are located at the SPB. Our experiments suggest that the hydrophobic patch of mitotic cyclins contributes to CDK substrate selection by directing the localization of Cdc13-CDK to centrosomes and that this localization of CDK contributes to the CDK substrate phosphorylation necessary to ensure proper entry into mitosis. Finally, we show that mutation of the hydrophobic patch prevents cyclin B1 localization to centrosomes in human cells, suggesting that this mechanism of cyclin-CDK spatial regulation may be conserved across eukaryotes.

Annotation

GO biological process

GO:0010971 - positive regulation of G2/M transition of mitotic cell cycle

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GO cellular component

GO:0044732 - mitotic spindle pole body

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GO molecular function

GO:0061575 - cyclin-dependent protein serine/threonine kinase activator activity

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Multi-locus phenotype

FYPO:0003246 - normal mitotic S phase progression

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Genotypes:

FYPO:0000776 - normal protein phosphorylation during vegetative growth

Genes:

Genotypes:

FYPO:0006824 - premature protein localization to mitotic spindle pole body

Genes:

Genotypes:

FYPO:0007567 - premature protein localization to mitotic spindle pole body during metaphase

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Genotypes:

Single locus phenotype

FYPO:0000446 - cell cycle arrest at mitotic G2/M phase transition

Genes:

Genotypes:

FYPO:0002822 - decreased protein localization to mitotic spindle pole body during mitosis

Genes:

Genotypes:

FYPO:0007475 - delayed onset of protein localization to mitotic spindle pole body

Genes:

Genotypes:

FYPO:0002061 - inviable vegetative cell population

Genes:

Genotypes:

FYPO:0003246 - normal mitotic S phase progression

Genes:

Genotypes:

FYPO:0000776 - normal protein phosphorylation during vegetative growth

Genes:

Genotypes:

FYPO:0001357 - normal vegetative cell population growth

Genes:

Genotypes:

FYPO:0002516 - premature mitotic G2/M phase transition

Genes:

Genotypes: