PXD056514

PXD056514 is an original dataset announced via ProteomeXchange.

Dataset Summary

Title	Phosphoproteomics identifies determinants of PAK inhibitor sensitivity in AML cells
Description	Background The p21 activated kinases (PAK) are frequently dysregulated in cancer and have central roles in oncogenic signalling, prompting the development of PAK inhibitors (PAKi) as anticancer agents. However, such compounds have not reached clinical use because, at least partially, there is a limited mechanistic understanding of their mode of action. Here, we aimed to characterize functional and molecular responses to PAK inhibitors (PF-3758309, FRAX-486 and IPA-3) in multiple AML models to gain mechanistic insights on how these inhibitors work in this disease and identify determinants of response in patient samples. Methods We used proteomics and phosphoproteomics to profile PAKi impact on protein phosphorylation and expression and kinase activity in P31/Fuj and MV4-11 AML cells, and primary cells from 8 AML patients. We also integrated gene dependency data with phosphoproteomics and proteomics to identify which proteins targeted by PAKi are necessary for the proliferation of AML. We studied the effect PAKi on cell cycle progression, proliferation, differentiation and apoptosis. Finally, we used phosphoproteomics data as input for machine learning models that predicted “ex vivo” response of primary AML cells to PF-3758309 and identify markers of response. Results PF-3758309 was the most effective PAKi in reducing proliferation and inducing apoptosis in AML. PF-3758309 inhibited PAK, AMPK and PKCA activities in all AML cell lines and primary cells tested. This compound reduced the phosphorylation and expression of c-MYC and multiple ribosomal proteins in both cell lines and targeted the FLT3 pathway in FLT3-ITD mutated cells. In primary cells, PF-3758309 reduced STAT5 phosphorylation at Y699 in models with high phosphorylation on this site. Functionally, PF-3758309 reduced cell-growth, induced apoptosis, blocked the cell cycle progression and promoted differentiation in a model-dependent manner. ML modelling accurately classified primary AML samples as sensitive or resistant to PF-3758309 “ex vivo” treatment. Analysis of the models highlighted phosphorylation of PFH2 at Ser705 as a potential biomarker of response to PF-3758309. Conclusions In summary, our data define the proteomic, molecular and functional response of AML cells to PF-3758309 and suggest a route to personalise treatments in AML based on PAK inhibitors.
HostingRepository	PRIDE
AnnounceDate	2025-05-07
AnnouncementXML	Submission_2025-05-07_04:19:36.827.xml
DigitalObjectIdentifier	https://dx.doi.org/10.6019/PXD056514
ReviewLevel	Peer-reviewed dataset
DatasetOrigin	Original dataset
RepositorySupport	Supported dataset by repository
PrimarySubmitter	Pedro Casado-Izquierdo
SpeciesList	scientific name: Homo sapiens (Human); NCBI TaxID: 9606;
ModificationList	2-pyrrolidone-5-carboxylic acid (Glu); phosphorylated residue; monohydroxylated residue; iodoacetamide derivatized residue
Instrument	Q Exactive; LTQ Orbitrap

Dataset History

Revision	Datetime	Status	ChangeLog Entry
0	2024-10-04 12:08:22	ID requested
⏵ 1	2025-05-07 04:19:37	announced

Publication List

10.6019/PXD056514;
10.1186/s12964-025-02107-0;
Casado P, Marfa S, Hadi MM, Gerdes H, Martin-Guerrero SM, Miraki-Moud F, Rajeeve V, Cutillas PR, Phosphoproteomics identifies determinants of PAK inhibitor sensitivity in leukaemia cells. Cell Commun Signal, 23(1):135(2025) [pubmed]

10.6019/PXD056514;

10.1186/s12964-025-02107-0;

Casado P, Marfa S, Hadi MM, Gerdes H, Martin-Guerrero SM, Miraki-Moud F, Rajeeve V, Cutillas PR, Phosphoproteomics identifies determinants of PAK inhibitor sensitivity in leukaemia cells. Cell Commun Signal, 23(1):135(2025) [pubmed]

Keyword List

submitter keyword: Acute Myeloid Leukaemia, Phosphoproteomics, Machine Learning, kinase inhibitors, PAK inhibitors, target therapy, PF-3758309, Proteomics, Biomarkers,Cancer

submitter keyword: Acute Myeloid Leukaemia, Phosphoproteomics, Machine Learning, kinase inhibitors, PAK inhibitors, target therapy, PF-3758309, Proteomics, Biomarkers,Cancer

Contact List

Pedro R. Cutillas
contact affiliation	Centre for Genomics and Computational Biology, Barts Cancer Institute, Queen Mary University of London
contact email	p.cutillas@qmul.ac.uk
lab head
Pedro Casado-Izquierdo
contact affiliation	Cell Signalling
contact email	p.m.casado-izquierdo@qmul.ac.uk
dataset submitter

Full Dataset Link List

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PRIDE project URI

Dataset FTP location
NOTE: Most web browsers have now discontinued native support for FTP access within the browser window. But you can usually install another FTP app (we recommend FileZilla) and configure your browser to launch the external application when you click on this FTP link. Or otherwise, launch an app that supports FTP (like FileZilla) and use this address: ftp://ftp.pride.ebi.ac.uk/pride/data/archive/2025/05/PXD056514

PRIDE project URI

Repository Record List

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