Phosphoproteomic profiling of T cell acute lymphoblastic leukemia reveals targetable kinases and combination treatment strategies.

Valentina Cordo; Mariska Meijer; Rico Hagelaar; Richard R de Goeij-de Haas; Vera Poort; Alex A Henneman; Sander R Piersma; Thang V Pham; Koichi Oshima; Adolfo A Ferrando; Guido J R Zaman; Connie R Jimenez; Jules Meijerink

Phosphoproteomic profiling of T cell acute lymphoblastic leukemia reveals targetable kinases and combination treatment strategies.

Valentina Cordo, Mariska Meijer, Rico Hagelaar, Richard R de Goeij-de Haas, Vera Poort, Alex A Henneman, Sander R Piersma, Thang V Pham, Koichi Oshima, Adolfo A Ferrando, Guido J R Zaman, Connie R Jimenez, Jules Meijerink

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20 Citations (Scopus)

Abstract

Protein kinase inhibitors are amongst the most successful cancer treatments, but targetable kinases activated by genomic abnormalities are rare in T cell acute lymphoblastic leukemia. Nevertheless, kinases can be activated in the absence of genetic defects. Thus, phosphoproteomics can provide information on pathway activation and signaling networks that offer opportunities for targeted therapy. Here, we describe a mass spectrometry-based global phosphoproteomic profiling of 11 T cell acute lymphoblastic leukemia cell lines to identify targetable kinases. We report a comprehensive dataset consisting of 21,000 phosphosites on 4,896 phosphoproteins, including 217 kinases. We identify active Src-family kinases signaling as well as active cyclin-dependent kinases. We validate putative targets for therapy ex vivo and identify potential combination treatments, such as the inhibition of the INSR/IGF-1R axis to increase the sensitivity to dasatinib treatment. Ex vivo validation of selected drug combinations using patient-derived xenografts provides a proof-of-concept for phosphoproteomics-guided design of personalized treatments.

Original language	English
Article number	1048
Journal	Nature communications
Volume	13
Issue number	1
Publication status	Published - 25 Feb 2022

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https://www.nature.com/articles/s41467-022-28682-1

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Cordo, V., Meijer, M., Hagelaar, R., de Goeij-de Haas, R. R., Poort, V., Henneman, A. A., Piersma, S. R., Pham, T. V., Oshima, K., Ferrando, A. A., Zaman, G. J. R., Jimenez, C. R., & Meijerink, J. (2022). Phosphoproteomic profiling of T cell acute lymphoblastic leukemia reveals targetable kinases and combination treatment strategies. Nature communications, 13(1), Article 1048. https://www.nature.com/articles/s41467-022-28682-1

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title = "Phosphoproteomic profiling of T cell acute lymphoblastic leukemia reveals targetable kinases and combination treatment strategies.",

abstract = "Protein kinase inhibitors are amongst the most successful cancer treatments, but targetable kinases activated by genomic abnormalities are rare in T cell acute lymphoblastic leukemia. Nevertheless, kinases can be activated in the absence of genetic defects. Thus, phosphoproteomics can provide information on pathway activation and signaling networks that offer opportunities for targeted therapy. Here, we describe a mass spectrometry-based global phosphoproteomic profiling of 11 T cell acute lymphoblastic leukemia cell lines to identify targetable kinases. We report a comprehensive dataset consisting of 21,000 phosphosites on 4,896 phosphoproteins, including 217 kinases. We identify active Src-family kinases signaling as well as active cyclin-dependent kinases. We validate putative targets for therapy ex vivo and identify potential combination treatments, such as the inhibition of the INSR/IGF-1R axis to increase the sensitivity to dasatinib treatment. Ex vivo validation of selected drug combinations using patient-derived xenografts provides a proof-of-concept for phosphoproteomics-guided design of personalized treatments.",

author = "Valentina Cordo and Mariska Meijer and Rico Hagelaar and \{de Goeij-de Haas\}, \{Richard R\} and Vera Poort and Henneman, \{Alex A\} and Piersma, \{Sander R\} and Pham, \{Thang V\} and Koichi Oshima and Ferrando, \{Adolfo A\} and Zaman, \{Guido J R\} and Jimenez, \{Connie R\} and Jules Meijerink",

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Cordo, V, Meijer, M, Hagelaar, R, de Goeij-de Haas, RR, Poort, V, Henneman, AA, Piersma, SR, Pham, TV, Oshima, K, Ferrando, AA, Zaman, GJR, Jimenez, CR & Meijerink, J 2022, 'Phosphoproteomic profiling of T cell acute lymphoblastic leukemia reveals targetable kinases and combination treatment strategies.', Nature communications, vol. 13, no. 1, 1048. <https://www.nature.com/articles/s41467-022-28682-1>

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AU - Meijer, Mariska

AU - Hagelaar, Rico

AU - de Goeij-de Haas, Richard R

AU - Poort, Vera

AU - Henneman, Alex A

AU - Piersma, Sander R

AU - Pham, Thang V

AU - Oshima, Koichi

AU - Ferrando, Adolfo A

AU - Zaman, Guido J R

AU - Jimenez, Connie R

AU - Meijerink, Jules

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AB - Protein kinase inhibitors are amongst the most successful cancer treatments, but targetable kinases activated by genomic abnormalities are rare in T cell acute lymphoblastic leukemia. Nevertheless, kinases can be activated in the absence of genetic defects. Thus, phosphoproteomics can provide information on pathway activation and signaling networks that offer opportunities for targeted therapy. Here, we describe a mass spectrometry-based global phosphoproteomic profiling of 11 T cell acute lymphoblastic leukemia cell lines to identify targetable kinases. We report a comprehensive dataset consisting of 21,000 phosphosites on 4,896 phosphoproteins, including 217 kinases. We identify active Src-family kinases signaling as well as active cyclin-dependent kinases. We validate putative targets for therapy ex vivo and identify potential combination treatments, such as the inhibition of the INSR/IGF-1R axis to increase the sensitivity to dasatinib treatment. Ex vivo validation of selected drug combinations using patient-derived xenografts provides a proof-of-concept for phosphoproteomics-guided design of personalized treatments.

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Phosphoproteomic profiling of T cell acute lymphoblastic leukemia reveals targetable kinases and combination treatment strategies.

Abstract

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