| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 2039248 | Cell Reports | 2016 | 14 Pages |
•Cks2 regulates the phosphorylation of Wee1A by Cdk1 in a biphasic manner•This biphasic regulation accounts for Cks overexpression phenotypes•Cks2 changes the balance in the mutual inhibition of Cdk1 and Wee1A
SummaryPrevious work has shown that Suc1/Cks proteins can promote the hyperphosphorylation of primed Cdk1 substrates through the formation of ternary Cdk1-Cks-phosphosubstrate complexes. This raises the possibility that Cks proteins might be able to both facilitate and interfere with hyperphosphorylation through a mechanism analogous to the prozone effect in antigen-antibody interactions, with substoichiometric Cks promoting the formation of Cdk1-Cks-phosphosubstrate complexes and suprastoichiometric Cks instead promoting the formation of Cdk1-Cks and Cks-phosphosubstrate complexes. We tested this hypothesis through a combination of theory, proof-of-principle experiments with oligonucleotide annealing, and experiments on the interaction of Xenopus cyclin B1-Cdk1-Cks2 with Wee1A in vitro and in Xenopus extracts. Our findings help explain why both Cks under-expression and overexpression interfere with cell-cycle progression and provide insight into the regulation of the Cdk1 system.
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