Proteomics

Dataset Information

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Positively charged specificity site in cyclin B1 is essential for mitotic fidelity


ABSTRACT: Phosphorylation of substrates by cyclin-dependent kinases (CDKs) is the driving force of cell cycle progression. Several CDK-activating cyclins are involved, yet how they contribute to substrate specificity is still poorly understood. Here, we discovered that a positively charged pocket in cyclin B1, which is exclusively conserved within B-type cyclins and binds phosphorylated serine- or threonine-residues as well as acidic side chains, is essential for correct execution of mitosis. HeLa cells expressing pocket mutant cyclin B1 are strongly delayed in anaphase onset due to multiple defects in mitotic spindle function and timely activation of the E3-ligase APC/C. Non-functional pocket results in decreased APC/C phosphorylation at non-consensus CDK1 sites, compromised in vitro ubiquitylation activity, and reduced binding of the E2-enzyme UBE2S. Our results support a model in which cyclin B1’s pocket serves as specificity factor for sequential substrate phosphorylations involving initial priming events facilitating subsequent pocket-dependent phosphorylations at non-consensus CDK1 motifs.

INSTRUMENT(S):

ORGANISM(S): Homo Sapiens (human)

TISSUE(S): Cell Culture

SUBMITTER: Florian Stengel  

LAB HEAD: Prof Dr Florian Stengel

PROVIDER: PXD048838 | Pride | 2025-05-06

REPOSITORIES: Pride

Dataset's files

Source:
Action DRS
20231124_101448_PH_B1human_new2.sne Other
210907_swissprot_UP000005640.fasta Fasta
Q2108_heidpe_153.raw Raw
Q2108_heidpe_154.raw Raw
Q2108_heidpe_156.raw Raw
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Publications

Positively charged specificity site in cyclin B1 is essential for mitotic fidelity.

Heinzle Christian C   Höfler Anna A   Yu Jun J   Heid Peter P   Kremer Nora N   Schunk Rebecca R   Stengel Florian F   Bange Tanja T   Boland Andreas A   Mayer Thomas U TU  

Nature communications 20250120 1


Phosphorylation of substrates by cyclin-dependent kinases (CDKs) is the driving force of cell cycle progression. Several CDK-activating cyclins are involved, yet how they contribute to substrate specificity is still poorly understood. Here, we discover that a positively charged pocket in cyclin B1, which is exclusively conserved within B-type cyclins and binds phosphorylated serine- or threonine-residues, is essential for correct execution of mitosis. HeLa cells expressing pocket mutant cyclin B  ...[more]

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