Proteomics

Dataset Information

0

The Eyes Absent family members EYA4 and EYA1 promote PLK1 activation and successful mitosis through tyrosine dephosphorylation: siEYA4 pY IP-MS

ABSTRACT: The Eyes Absent family of proteins (EYA1-4) are a biochemically unique group of tyrosine phosphatases known to be tumour promoting across a range of cancer types. To date, the molecular targets of EYA phosphatase activity remain largely uncharacterised. Here, we identify Polo-like kinase 1 (PLK1) as a direct interactor and phosphatase substrate of both EYA4 and EYA1, with pY445 on PLK1 being the primary target site. EYA-mediated dephosphorylation of PLK1 in the G2 phase of the cell cycle is required for centrosome maturation, PLK1 localization to centrosomes, and polo-box domain (PBD) dependent interactions between PLK1 and the PLK1-activating proteins BORA and CEP192. Molecular dynamics simulations support the rationale that pY445 confers a structural impairment to PBD-substrate interactions that is relieved by EYA-mediated dephosphorylation. Depletion of EYA4 or EYA1, or chemical inhibition of EYA phosphatase activity, dramatically reduces PLK1 activation, causing mitotic defects and cell death. Overall, we have characterized a novel phosphotyrosine signalling network governing PLK1 and mitosis. This work provides a mechanism of cell killing for EYA phosphatase inhibitors with important therapeutic implications.

INSTRUMENT(S): Q Exactive

ORGANISM(S): Homo Sapiens (human)

SUBMITTER: Christopher Nelson  

LAB HEAD: Hilda Amelia Pickett

PROVIDER: PXD036430 | Pride | 2024-02-26

REPOSITORIES: Pride

Json Xml

Dataset's files

Source:
Action DRS
20190328_QEPLUS2_CN_B8.raw Raw
20190419_QEPLUS_CN_B10.raw Raw
20190419_QEPLUS_CN_B9.raw Raw
20190419_QEPLUS_CN_C8.raw Raw
20190419_QEPLUS_CN_C9.raw Raw
Items per page:
1 - 5 of 7
altmetric image

Publications

The Eyes Absent proteins (EYA1-4) are a biochemically unique group of tyrosine phosphatases known to be tumour-promoting across a range of cancer types. To date, the targets of EYA phosphatase activity remain largely uncharacterised. Here, we identify Polo-like kinase 1 (PLK1) as an interactor and phosphatase substrate of EYA4 and EYA1, with pY445 on PLK1 being the primary target site. Dephosphorylation of pY445 in the G2 phase of the cell cycle is required for centrosome maturation, PLK1 locali  ...[more]

Similar Datasets

Proteomics The Eyes Absent family members EYA4 and EYA1 promote PLK1 activation and successful mitosis through tyrosine dephosphorylation: EYA4 BioID
2024-02-26 | PXD036405 | Pride
Proteomics The Eyes Absent family members EYA4 and EYA1 promote PLK1 activation and successful mitosis through tyrosine dephosphorylation: PLK1 PRM
2024-02-26 | PXD037064 | Pride
Proteomics Global assessment of Plk1 network dynamics identifies inhibition of PP6 as a mechanism to promote Aurora A activity
2018-03-09 | MSV000082147 | MassIVE
Transcriptomics PDK1 Signaling Towards PLK1-Myc Activation Confers Oncogenic Transformation and Tumor Initiating Cell Activation and Resistance to mTOR-targeted Therapy.
2013-07-31 | E-GEOD-30669 | biostudies-arrayexpress
Transcriptomics Role of PLK1 in epithelial-mesenchymal transition in human melanoma
2024-01-01 | GSE237385 | GEO
Proteomics PLK1 phosphorylation of Epstein-Barr virus nuclear antigen 2
2021-08-22 | PXD022970 | Pride
Other Genetic enhancers of partial PLK1 inhibition reveal hypersensitivity to kinetochore perturbations
2023-10-02 | GSE228155 | GEO
Transcriptomics Single-cell analysis identifies PLK1 as a driver of immunosuppressive tumor microenvironment in LUAD
2024-05-28 | GSE264739 | GEO
Transcriptomics Centrosomal Localization of DNAJ-PKAc Fusion Heightens PLK1 Inhibitor Sensitivity in Fibrolamellar Cancer
2023-12-19 | GSE250059 | GEO
Transcriptomics PDK1 Signaling Towards PLK1-Myc Activation Confers Oncogenic Transformation and Tumor Initiating Cell Activation and Resistance to mTOR-targeted Therapy.
2013-07-31 | GSE30669 | GEO