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Reference - PMID:22660415 - MPS1/Mph1 phosphorylates the kinetochore protein KNL1/Spc7 to recruit SAC components.

Reference summary

PubMed ID
PMID:22660415
Title
MPS1/Mph1 phosphorylates the kinetochore protein KNL1/Spc7 to recruit SAC components.
Authors
Yamagishi Y, Yang CH, Tanno Y, Watanabe Y
Citation
Nat Cell Biol 2012 Jun 03;14(7):746-52
Publication year
2012
Abstract
The genomic stability of all organisms depends on the precise partition of chromosomes to daughter cells. The spindle assembly checkpoint (SAC) senses unattached kinetochores and prevents premature entry to anaphase, thus ensuring that all chromosomes attach to opposite spindle poles (bi-orientation) during mitosis. MPS1 is an evolutionarily conserved protein kinase required for the SAC and chromosome bi-orientation. Yet, its primary cellular substrate has remained elusive. We show that fission yeast Mph1 (MPS1 homologue) phosphorylates the kinetochore protein Spc7 (KNL1/Blinkin homologue) at the MELT repeat sequences. This phosphorylation promotes the in vitro binding to the Bub1-Bub3 complex, which is required for kinetochore-based SAC activation (Mad1-Mad2-Mad3 localization) and chromosome alignment. Accordingly, a non-phosphorylatable spc7-12A mutation abolishes kinetochore targeting of Bub1-Bub3, whereas a phospho-mimetic spc7-12E mutation forces them to localize at kinetochores throughout the entire cell cycle, even in the absence of Mph1. Thus, MPS1/Mph1 kinase locating at the unattached kinetochores initially creates a mark, which is crucial for SAC activation and chromosome bi-orientation. This mechanism seems to be conserved in human cells.

Annotation

GO biological process

GO:0007094 - mitotic spindle assembly checkpoint signaling

Genes:

GO:0090266 - regulation of mitotic cell cycle spindle assembly checkpoint

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GO cellular component

GO:0000776 - kinetochore

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GO:0005634 - nucleus

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GO molecular function

GO:0004674 - protein serine/threonine kinase activity

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Modification

MOD:00047 - O-phospho-L-threonine

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Multi-locus phenotype

FYPO:0000141 - abnormal mitotic sister chromatid segregation

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Genotypes:

FYPO:0007174 - abnormal protein localization to kinetochore during mitotic interphase

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Genotypes:

FYPO:0004318 - abolished mitotic spindle assembly checkpoint

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Genotypes:

FYPO:0008166 - abolished protein localization to kinetochore during mitotic prometaphase

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Genotypes:

FYPO:0005780 - decreased response to mitotic spindle assembly checkpoint signaling

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Genotypes:

FYPO:0007399 - normal protein localization to kinetochore during mitotic interphase

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Genotypes:

FYPO:0001357 - normal vegetative cell population growth

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Genotypes:

FYPO:0000091 - sensitive to thiabendazole

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Single locus phenotype

FYPO:0000141 - abnormal mitotic sister chromatid segregation

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Genotypes:

FYPO:0003591 - abnormal protein complex binding

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Genotypes:

FYPO:0007174 - abnormal protein localization to kinetochore during mitotic interphase

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Genotypes:

FYPO:0008164 - abnormal protein localization to kinetochore during mitotic M phase

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FYPO:0001268 - abnormal protein localization to kinetochore during vegetative growth

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Genotypes:

FYPO:0008166 - abolished protein localization to kinetochore during mitotic prometaphase

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FYPO:0002678 - abolished protein phosphorylation

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FYPO:0000705 - abolished protein-protein interaction

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Genotypes:

FYPO:0008165 - decreased protein localization to kinetochore during mitotic prometaphase

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Genotypes:

FYPO:0005780 - decreased response to mitotic spindle assembly checkpoint signaling

Genes:

Genotypes:

FYPO:0001355 - decreased vegetative cell population growth

Genes:

Genotypes:

FYPO:0002638 - increased activation of mitotic spindle assembly checkpoint

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Genotypes:

FYPO:0005232 - normal protein complex binding

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Genotypes:

FYPO:0005042 - normal protein localization to kinetochore

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Genotypes:

FYPO:0005212 - normal protein localization to kinetochore during mitotic prometaphase

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Genotypes:

FYPO:0000091 - sensitive to thiabendazole

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Genotypes: