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Reference - PMID:16483313 - Securin can have a separase cleavage site by substitution mutations in the domain required for stabilization and inhibition of separase.

Reference summary

PubMed ID
PMID:16483313
Title
Securin can have a separase cleavage site by substitution mutations in the domain required for stabilization and inhibition of separase.
Authors
Nagao K, Yanagida M
Citation
Genes Cells 2006 Mar;11(3):247-60
Publication year
2006
Abstract
Securin-separase complex is required for sister chromatid separation. Securin degrades in an APC/cyclosome dependent manner. Separase is activated on the destruction of securin and cleaves cohesin. Fission yeast securin/Cut2 required for proper separase localization has the motifs for destruction and separase-binding at the N- and C-termini, respectively. We report here the third essential domain, which becomes toxic when the 76-amino acid fragment (81-156) in the middle is overproduced. The fragment inhibits separase, while separase is recruited normally and securin is destroyed. It may interfere with separase activation after destruction of securin. If the 127DIE129 stretch is substituted for AIA, the fragment toxicity and the full-length function are abolished. Interestingly, Cut2 is cleaved in a separase dependent manner if the cleavage consensus is introduced following the DIE sequence. This finding is consistent with the proposed model that the DIE region may mimic the cleavage site of separase and inhibit the activation of separase. Evidence for physical interaction between the fragment and separase is provided. A temperature sensitive mutation cut1-K73 isolated by its specific resistance to the fragment toxicity resides in the superhelical region of separase, suggesting that the catalytic site and the helical region in separase may cooperate for activation.

Annotation

Multi-locus phenotype

FYPO:0002061 - inviable vegetative cell population

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FYPO:0001513 - normal mitotic sister chromatid segregation

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FYPO:0001357 - normal vegetative cell population growth

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Single locus phenotype

FYPO:0000620 - abnormal cell cycle arrest in mitotic metaphase

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FYPO:0004481 - abolished cell population growth at high temperature

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FYPO:0005377 - abolished proteolysis during vegetative growth

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FYPO:0003165 - cut with abnormal chromosome segregation

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Genotypes:

FYPO:0002061 - inviable vegetative cell population

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FYPO:0003758 - mitotic spindle elongation without chromosome separation

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FYPO:0005410 - normal protein degradation during mitosis

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FYPO:0002966 - normal protein localization to mitotic spindle

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FYPO:0001357 - normal vegetative cell population growth

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Genotypes: