PP2A methylesterase PME-1 suppresses anoikis and is associated with therapy relapse of PTEN-deficient prostate cancers

Anna Aakula; Aleksi Isomursu; Christian Rupp; Andrew Erickson; Nikhil Gupta; Otto Kauko; Pragya Shah; Artur Padzik; Yuba Raj Pokharel; Amanpreet Kaur; Song Ping Li; Lloyd Trotman; Pekka Taimen; Antti Rannikko; Jan Lammerding; Ilkka Paatero; Tuomas Mirtti; Johanna Ivaska; Jukka Westermarck

doi:10.1002/1878-0261.13353

PP2A methylesterase PME-1 suppresses anoikis and is associated with therapy relapse of PTEN-deficient prostate cancers

Anna Aakula, Aleksi Isomursu, Christian Rupp, Andrew Erickson, Nikhil Gupta, Otto Kauko, Pragya Shah, Artur Padzik, Yuba Raj Pokharel, Amanpreet Kaur, Song Ping Li, Lloyd Trotman, Pekka Taimen, Antti Rannikko, Jan Lammerding, Ilkka Paatero, Tuomas Mirtti, Johanna Ivaska, Jukka Westermarck^*

^*Corresponding author for this work

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Abstract

While organ-confined prostate cancer (PCa) is mostly therapeutically manageable, metastatic progression of PCa remains an unmet clinical challenge. Resistance to anoikis, a form of cell death initiated by cell detachment from the surrounding extracellular matrix, is one of the cellular processes critical for PCa progression towards aggressive disease. Therefore, further understanding of anoikis regulation in PCa might provide therapeutic opportunities. Here, we discover that PCa tumours with concomitant inhibition of two tumour suppressor phosphatases, PP2A and PTEN, are particularly aggressive, having < 50% 5-year secondary-therapy-free patient survival. Functionally, overexpression of PME-1, a methylesterase for the catalytic PP2A-C subunit, inhibits anoikis in PTEN-deficient PCa cells. In vivo, PME-1 inhibition increased apoptosis in in ovo PCa tumour xenografts, and attenuated PCa cell survival in zebrafish circulation. Molecularly, PME-1-deficient PC3 cells display increased trimethylation at lysines 9 and 27 of histone H3 (H3K9me3 and H3K27me3), a phenotype known to correlate with increased apoptosis sensitivity. In summary, our results demonstrate that PME-1 supports anoikis resistance in PTEN-deficient PCa cells. Clinically, these results identify PME-1 as a candidate biomarker for a subset of particularly aggressive PTEN-deficient PCa.

Original language	English
Pages (from-to)	1007-1023
Number of pages	17
Journal	Molecular Oncology
Volume	17
Issue number	6
DOIs	https://doi.org/10.1002/1878-0261.13353
Publication status	Published - Jun 2023
MoE publication type	A1 Journal article-refereed

Keywords

anoikis
integrin
LAP2A/B
nuclear lamina
PP2A-C methylation
PPME1

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10.1002/1878-0261.13353

Molecular Oncology - 2022 - Aakula - PP2A methylesterase PME‐1 suppresses anoikis and is associated with therapy relapse ofFinal published version, 2.02 MBLicence: CC BY

https://urn.fi/URN:NBN:fi-fe202402136923

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Aakula, A., Isomursu, A., Rupp, C., Erickson, A., Gupta, N., Kauko, O., Shah, P., Padzik, A., Pokharel, Y. R., Kaur, A., Li, S. P., Trotman, L., Taimen, P., Rannikko, A., Lammerding, J., Paatero, I., Mirtti, T., Ivaska, J., & Westermarck, J. (2023). PP2A methylesterase PME-1 suppresses anoikis and is associated with therapy relapse of PTEN-deficient prostate cancers. Molecular Oncology, 17(6), 1007-1023. https://doi.org/10.1002/1878-0261.13353

@article{f35534ecc4ed4ff9886d8fc0310e0ff6,

title = "PP2A methylesterase PME-1 suppresses anoikis and is associated with therapy relapse of PTEN-deficient prostate cancers",

abstract = "While organ-confined prostate cancer (PCa) is mostly therapeutically manageable, metastatic progression of PCa remains an unmet clinical challenge. Resistance to anoikis, a form of cell death initiated by cell detachment from the surrounding extracellular matrix, is one of the cellular processes critical for PCa progression towards aggressive disease. Therefore, further understanding of anoikis regulation in PCa might provide therapeutic opportunities. Here, we discover that PCa tumours with concomitant inhibition of two tumour suppressor phosphatases, PP2A and PTEN, are particularly aggressive, having < 50% 5-year secondary-therapy-free patient survival. Functionally, overexpression of PME-1, a methylesterase for the catalytic PP2A-C subunit, inhibits anoikis in PTEN-deficient PCa cells. In vivo, PME-1 inhibition increased apoptosis in in ovo PCa tumour xenografts, and attenuated PCa cell survival in zebrafish circulation. Molecularly, PME-1-deficient PC3 cells display increased trimethylation at lysines 9 and 27 of histone H3 (H3K9me3 and H3K27me3), a phenotype known to correlate with increased apoptosis sensitivity. In summary, our results demonstrate that PME-1 supports anoikis resistance in PTEN-deficient PCa cells. Clinically, these results identify PME-1 as a candidate biomarker for a subset of particularly aggressive PTEN-deficient PCa.",

keywords = "anoikis, integrin, LAP2A/B, nuclear lamina, PP2A-C methylation, PPME1",

author = "Anna Aakula and Aleksi Isomursu and Christian Rupp and Andrew Erickson and Nikhil Gupta and Otto Kauko and Pragya Shah and Artur Padzik and Pokharel, {Yuba Raj} and Amanpreet Kaur and Li, {Song Ping} and Lloyd Trotman and Pekka Taimen and Antti Rannikko and Jan Lammerding and Ilkka Paatero and Tuomas Mirtti and Johanna Ivaska and Jukka Westermarck",

note = "Publisher Copyright: {\textcopyright} 2022 The Authors. Molecular Oncology published by John Wiley & Sons Ltd on behalf of Federation of European Biochemical Societies.",

year = "2023",

month = jun,

doi = "10.1002/1878-0261.13353",

language = "English",

volume = "17",

pages = "1007--1023",

journal = "Molecular Oncology",

issn = "1574-7891",

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Aakula, A, Isomursu, A, Rupp, C, Erickson, A, Gupta, N, Kauko, O, Shah, P, Padzik, A, Pokharel, YR, Kaur, A, Li, SP, Trotman, L, Taimen, P, Rannikko, A, Lammerding, J, Paatero, I, Mirtti, T, Ivaska, J & Westermarck, J 2023, 'PP2A methylesterase PME-1 suppresses anoikis and is associated with therapy relapse of PTEN-deficient prostate cancers', Molecular Oncology, vol. 17, no. 6, pp. 1007-1023. https://doi.org/10.1002/1878-0261.13353

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T1 - PP2A methylesterase PME-1 suppresses anoikis and is associated with therapy relapse of PTEN-deficient prostate cancers

AU - Aakula, Anna

AU - Isomursu, Aleksi

AU - Rupp, Christian

AU - Erickson, Andrew

AU - Gupta, Nikhil

AU - Kauko, Otto

AU - Shah, Pragya

AU - Padzik, Artur

AU - Pokharel, Yuba Raj

AU - Kaur, Amanpreet

AU - Li, Song Ping

AU - Trotman, Lloyd

AU - Taimen, Pekka

AU - Rannikko, Antti

AU - Lammerding, Jan

AU - Paatero, Ilkka

AU - Mirtti, Tuomas

AU - Ivaska, Johanna

AU - Westermarck, Jukka

PY - 2023/6

Y1 - 2023/6

N2 - While organ-confined prostate cancer (PCa) is mostly therapeutically manageable, metastatic progression of PCa remains an unmet clinical challenge. Resistance to anoikis, a form of cell death initiated by cell detachment from the surrounding extracellular matrix, is one of the cellular processes critical for PCa progression towards aggressive disease. Therefore, further understanding of anoikis regulation in PCa might provide therapeutic opportunities. Here, we discover that PCa tumours with concomitant inhibition of two tumour suppressor phosphatases, PP2A and PTEN, are particularly aggressive, having < 50% 5-year secondary-therapy-free patient survival. Functionally, overexpression of PME-1, a methylesterase for the catalytic PP2A-C subunit, inhibits anoikis in PTEN-deficient PCa cells. In vivo, PME-1 inhibition increased apoptosis in in ovo PCa tumour xenografts, and attenuated PCa cell survival in zebrafish circulation. Molecularly, PME-1-deficient PC3 cells display increased trimethylation at lysines 9 and 27 of histone H3 (H3K9me3 and H3K27me3), a phenotype known to correlate with increased apoptosis sensitivity. In summary, our results demonstrate that PME-1 supports anoikis resistance in PTEN-deficient PCa cells. Clinically, these results identify PME-1 as a candidate biomarker for a subset of particularly aggressive PTEN-deficient PCa.

AB - While organ-confined prostate cancer (PCa) is mostly therapeutically manageable, metastatic progression of PCa remains an unmet clinical challenge. Resistance to anoikis, a form of cell death initiated by cell detachment from the surrounding extracellular matrix, is one of the cellular processes critical for PCa progression towards aggressive disease. Therefore, further understanding of anoikis regulation in PCa might provide therapeutic opportunities. Here, we discover that PCa tumours with concomitant inhibition of two tumour suppressor phosphatases, PP2A and PTEN, are particularly aggressive, having < 50% 5-year secondary-therapy-free patient survival. Functionally, overexpression of PME-1, a methylesterase for the catalytic PP2A-C subunit, inhibits anoikis in PTEN-deficient PCa cells. In vivo, PME-1 inhibition increased apoptosis in in ovo PCa tumour xenografts, and attenuated PCa cell survival in zebrafish circulation. Molecularly, PME-1-deficient PC3 cells display increased trimethylation at lysines 9 and 27 of histone H3 (H3K9me3 and H3K27me3), a phenotype known to correlate with increased apoptosis sensitivity. In summary, our results demonstrate that PME-1 supports anoikis resistance in PTEN-deficient PCa cells. Clinically, these results identify PME-1 as a candidate biomarker for a subset of particularly aggressive PTEN-deficient PCa.

KW - anoikis

KW - integrin

KW - LAP2A/B

KW - nuclear lamina

KW - PP2A-C methylation

KW - PPME1

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U2 - 10.1002/1878-0261.13353

DO - 10.1002/1878-0261.13353

M3 - Article

C2 - 36461911

AN - SCOPUS:85153206254

SN - 1574-7891

VL - 17

SP - 1007

EP - 1023

JO - Molecular Oncology

JF - Molecular Oncology

IS - 6

ER -

PP2A methylesterase PME-1 suppresses anoikis and is associated with therapy relapse of PTEN-deficient prostate cancers

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