Phosphoproteomics of primary AML patient samples reveals rationale for AKT combination therapy and p53 context to overcome selinexor resistance

Kristina B. Emdal; Nicolàs Palacio-Escat; Caroline Wigerup; Akihiro Eguchi; Helén Nilsson; Dorte B. Bekker-Jensen; Lars Rönnstrand; Julhash U. Kazi; Alexandre Puissant; Raphaël Itzykson; Julio Saez-Rodriguez; Kristina Masson; Peter Blume-Jensen; Jesper V. Olsen

doi:10.1016/j.celrep.2022.111177

Phosphoproteomics of primary AML patient samples reveals rationale for AKT combination therapy and p53 context to overcome selinexor resistance

Kristina B. Emdal, Nicolàs Palacio-Escat, Caroline Wigerup, Akihiro Eguchi, Helén Nilsson, Dorte B. Bekker-Jensen, Lars Rönnstrand, Julhash U. Kazi, Alexandre Puissant, Raphaël Itzykson, Julio Saez-Rodriguez, Kristina Masson, Peter Blume-Jensen, Jesper V. Olsen

Research output: Contribution to journal › Article › peer-review

Abstract

Acute myeloid leukemia (AML) is a heterogeneous disease with variable patient responses to therapy. Selinexor, an inhibitor of nuclear export, has shown promising clinical activity for AML. To identify the molecular context for monotherapy sensitivity as well as rational drug combinations, we profile selinexor signaling responses using phosphoproteomics in primary AML patient samples and cell lines. Functional phosphosite scoring reveals that p53 function is required for selinexor sensitivity consistent with enhanced efficacy of selinexor in combination with the MDM2 inhibitor nutlin-3a. Moreover, combining selinexor with the AKT inhibitor MK-2206 overcomes dysregulated AKT-FOXO3 signaling in resistant cells, resulting in synergistic anti-proliferative effects. Using high-throughput spatial proteomics to profile subcellular compartments, we measure global proteome and phospho-proteome dynamics, providing direct evidence of nuclear translocation of FOXO3 upon combination treatment. Our data demonstrate the potential of phosphoproteomics and functional phosphorylation site scoring to successfully pinpoint key targetable signaling hubs for rational drug combinations.

Original language	English
Article number	111177
Journal	Cell Reports
Volume	40
Issue number	6
DOIs	https://doi.org/10.1016/j.celrep.2022.111177
Publication status	Published - 2022 Aug 9

Subject classification (UKÄ)

Cell and Molecular Biology

Free keywords

acute myeloid leukemia
combination therapy
CP: Cancer
CP: Molecular biology
drug resistance
functional scoring
mass spectrometry
MK-2206
nutlin-3a
phosphoproteomics
selinexor
subcellular proteomics

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1016/j.celrep.2022.111177Licence: CC BY

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Emdal, K. B., Palacio-Escat, N., Wigerup, C., Eguchi, A., Nilsson, H., Bekker-Jensen, D. B., Rönnstrand, L., Kazi, J. U., Puissant, A., Itzykson, R., Saez-Rodriguez, J., Masson, K., Blume-Jensen, P., & Olsen, J. V. (2022). Phosphoproteomics of primary AML patient samples reveals rationale for AKT combination therapy and p53 context to overcome selinexor resistance. Cell Reports, 40(6), Article 111177. https://doi.org/10.1016/j.celrep.2022.111177

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title = "Phosphoproteomics of primary AML patient samples reveals rationale for AKT combination therapy and p53 context to overcome selinexor resistance",

abstract = "Acute myeloid leukemia (AML) is a heterogeneous disease with variable patient responses to therapy. Selinexor, an inhibitor of nuclear export, has shown promising clinical activity for AML. To identify the molecular context for monotherapy sensitivity as well as rational drug combinations, we profile selinexor signaling responses using phosphoproteomics in primary AML patient samples and cell lines. Functional phosphosite scoring reveals that p53 function is required for selinexor sensitivity consistent with enhanced efficacy of selinexor in combination with the MDM2 inhibitor nutlin-3a. Moreover, combining selinexor with the AKT inhibitor MK-2206 overcomes dysregulated AKT-FOXO3 signaling in resistant cells, resulting in synergistic anti-proliferative effects. Using high-throughput spatial proteomics to profile subcellular compartments, we measure global proteome and phospho-proteome dynamics, providing direct evidence of nuclear translocation of FOXO3 upon combination treatment. Our data demonstrate the potential of phosphoproteomics and functional phosphorylation site scoring to successfully pinpoint key targetable signaling hubs for rational drug combinations.",

keywords = "acute myeloid leukemia, combination therapy, CP: Cancer, CP: Molecular biology, drug resistance, functional scoring, mass spectrometry, MK-2206, nutlin-3a, phosphoproteomics, selinexor, subcellular proteomics",

author = "Emdal, {Kristina B.} and Nicol{\`a}s Palacio-Escat and Caroline Wigerup and Akihiro Eguchi and Hel{\'e}n Nilsson and Bekker-Jensen, {Dorte B.} and Lars R{\"o}nnstrand and Kazi, {Julhash U.} and Alexandre Puissant and Rapha{\"e}l Itzykson and Julio Saez-Rodriguez and Kristina Masson and Peter Blume-Jensen and Olsen, {Jesper V.}",

year = "2022",

month = aug,

day = "9",

doi = "10.1016/j.celrep.2022.111177",

language = "English",

volume = "40",

journal = "Cell Reports",

issn = "2211-1247",

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Emdal, KB, Palacio-Escat, N, Wigerup, C, Eguchi, A, Nilsson, H, Bekker-Jensen, DB, Rönnstrand, L , Kazi, JU, Puissant, A, Itzykson, R, Saez-Rodriguez, J, Masson, K, Blume-Jensen, P & Olsen, JV 2022, 'Phosphoproteomics of primary AML patient samples reveals rationale for AKT combination therapy and p53 context to overcome selinexor resistance', Cell Reports, vol. 40, no. 6, 111177. https://doi.org/10.1016/j.celrep.2022.111177

TY - JOUR

T1 - Phosphoproteomics of primary AML patient samples reveals rationale for AKT combination therapy and p53 context to overcome selinexor resistance

AU - Emdal, Kristina B.

AU - Palacio-Escat, Nicolàs

AU - Wigerup, Caroline

AU - Eguchi, Akihiro

AU - Nilsson, Helén

AU - Bekker-Jensen, Dorte B.

AU - Rönnstrand, Lars

AU - Kazi, Julhash U.

AU - Puissant, Alexandre

AU - Itzykson, Raphaël

AU - Saez-Rodriguez, Julio

AU - Masson, Kristina

AU - Blume-Jensen, Peter

AU - Olsen, Jesper V.

PY - 2022/8/9

Y1 - 2022/8/9

N2 - Acute myeloid leukemia (AML) is a heterogeneous disease with variable patient responses to therapy. Selinexor, an inhibitor of nuclear export, has shown promising clinical activity for AML. To identify the molecular context for monotherapy sensitivity as well as rational drug combinations, we profile selinexor signaling responses using phosphoproteomics in primary AML patient samples and cell lines. Functional phosphosite scoring reveals that p53 function is required for selinexor sensitivity consistent with enhanced efficacy of selinexor in combination with the MDM2 inhibitor nutlin-3a. Moreover, combining selinexor with the AKT inhibitor MK-2206 overcomes dysregulated AKT-FOXO3 signaling in resistant cells, resulting in synergistic anti-proliferative effects. Using high-throughput spatial proteomics to profile subcellular compartments, we measure global proteome and phospho-proteome dynamics, providing direct evidence of nuclear translocation of FOXO3 upon combination treatment. Our data demonstrate the potential of phosphoproteomics and functional phosphorylation site scoring to successfully pinpoint key targetable signaling hubs for rational drug combinations.

AB - Acute myeloid leukemia (AML) is a heterogeneous disease with variable patient responses to therapy. Selinexor, an inhibitor of nuclear export, has shown promising clinical activity for AML. To identify the molecular context for monotherapy sensitivity as well as rational drug combinations, we profile selinexor signaling responses using phosphoproteomics in primary AML patient samples and cell lines. Functional phosphosite scoring reveals that p53 function is required for selinexor sensitivity consistent with enhanced efficacy of selinexor in combination with the MDM2 inhibitor nutlin-3a. Moreover, combining selinexor with the AKT inhibitor MK-2206 overcomes dysregulated AKT-FOXO3 signaling in resistant cells, resulting in synergistic anti-proliferative effects. Using high-throughput spatial proteomics to profile subcellular compartments, we measure global proteome and phospho-proteome dynamics, providing direct evidence of nuclear translocation of FOXO3 upon combination treatment. Our data demonstrate the potential of phosphoproteomics and functional phosphorylation site scoring to successfully pinpoint key targetable signaling hubs for rational drug combinations.

KW - acute myeloid leukemia

KW - combination therapy

KW - CP: Cancer

KW - CP: Molecular biology

KW - drug resistance

KW - functional scoring

KW - mass spectrometry

KW - MK-2206

KW - nutlin-3a

KW - phosphoproteomics

KW - selinexor

KW - subcellular proteomics

U2 - 10.1016/j.celrep.2022.111177

DO - 10.1016/j.celrep.2022.111177

M3 - Article

C2 - 35947955

AN - SCOPUS:85135711058

SN - 2211-1247

VL - 40

JO - Cell Reports

JF - Cell Reports

IS - 6

M1 - 111177

ER -

Phosphoproteomics of primary AML patient samples reveals rationale for AKT combination therapy and p53 context to overcome selinexor resistance

Abstract

Subject classification (UKÄ)

Free keywords

UN SDGs

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