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Reference - PMID:1706223 - mik1 and wee1 cooperate in the inhibitory tyrosine phosphorylation of cdc2.

Reference summary

PubMed ID
PMID:1706223
Title
mik1 and wee1 cooperate in the inhibitory tyrosine phosphorylation of cdc2.
Authors
Lundgren K, Walworth N, Booher R, Dembski M, Kirschner M, Beach D
Citation
Cell 1991 Mar 22;64(6):1111-22
Publication year
1991
Abstract
wee1 acts antagonistically to cdc25 in the tyrosine dephosphorylation and activation of cdc2, yet biochemical evidence suggests that wee1 is not required for tyrosine phosphorylation and its role is obscure. We show here that a related 66 kd kinase, called mik1, acts redundantly with wee1 in the negative regulation of cdc2 in S. pombe. A null allele of mik1 has no discernible phenotype, but a mik1 wee1 double mutant is hypermitotically lethal: all normal M phase checkpoints are bypassed, including the requirement for initiation of cell cycle "start," completion of S phase, and function of the cdc25+ mitotic activator. In the absence of mik1 and wee1 activity, cdc2 rapidly loses phosphate on tyrosine, both in strains undergoing mitotic lethality and in those that are viable owing to a compensating mutation within cdc2. The data suggest that mik1 and wee1 act cooperatively on cdc2, either directly as the inhibitory tyrosine kinase or as essential activators of that kinase.

Annotation

GO biological process

GO:0010972 - negative regulation of G2/M transition of mitotic cell cycle

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Single locus phenotype

FYPO:0001929 - normal cell cycle regulation during cellular response to hydroxyurea

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FYPO:0001492 - viable elongated vegetative cell

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FYPO:0002060 - viable vegetative cell population

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FYPO:0002177 - viable vegetative cell with normal cell morphology

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