WIP1 Phosphatase as a Potential Therapeutic Target in Neuroblastoma

The wild-type p53-induced phosphatase 1 (WIP1) is a serine/threonine phosphatase that negatively regulates multiple proteins involved in DNA damage response including p53, CHK2, Histone H2AX, and ATM, and it has been shown to be overexpressed or amplified in human cancers including breast and ovaria...

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Autores principales: Richter, Mark, Dayaram, Tajhal, Gilmartin, Aidan G., Ganji, Gopinath, Pemmasani, Sandhya Kiran, Van Der Key, Harjeet, Shohet, Jason M., Donehower, Lawrence A., Kumar, Rakesh
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2015
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4319922/
https://www.ncbi.nlm.nih.gov/pubmed/25658463
http://dx.doi.org/10.1371/journal.pone.0115635
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author Richter, Mark
Dayaram, Tajhal
Gilmartin, Aidan G.
Ganji, Gopinath
Pemmasani, Sandhya Kiran
Van Der Key, Harjeet
Shohet, Jason M.
Donehower, Lawrence A.
Kumar, Rakesh
author_facet Richter, Mark
Dayaram, Tajhal
Gilmartin, Aidan G.
Ganji, Gopinath
Pemmasani, Sandhya Kiran
Van Der Key, Harjeet
Shohet, Jason M.
Donehower, Lawrence A.
Kumar, Rakesh
author_sort Richter, Mark
collection PubMed
description The wild-type p53-induced phosphatase 1 (WIP1) is a serine/threonine phosphatase that negatively regulates multiple proteins involved in DNA damage response including p53, CHK2, Histone H2AX, and ATM, and it has been shown to be overexpressed or amplified in human cancers including breast and ovarian cancers. We examined WIP1 mRNA levels across multiple tumor types and found the highest levels in breast cancer, leukemia, medulloblastoma and neuroblastoma. Neuroblastoma is an exclusively TP53 wild type tumor at diagnosis and inhibition of p53 is required for tumorigenesis. Neuroblastomas in particular have previously been shown to have 17q amplification, harboring the WIP1 (PPM1D) gene and associated with poor clinical outcome. We therefore sought to determine whether inhibiting WIP1 with a selective antagonist, GSK2830371, can attenuate neuroblastoma cell growth through reactivation of p53 mediated tumor suppression. Neuroblastoma cell lines with wild-type TP53 alleles were highly sensitive to GSK2830371 treatment, while cell lines with mutant TP53 were resistant to GSK2830371. The majority of tested neuroblastoma cell lines with copy number gains of the PPM1D locus were also TP53 wild-type and sensitive to GSK2830371A; in contrast cell lines with no copy gain of PPM1D were mixed in their sensitivity to WIP1 inhibition, with the primary determinant being TP53 mutational status. Since WIP1 is involved in the cellular response to DNA damage and drugs used in neuroblastoma treatment induce apoptosis through DNA damage, we sought to determine whether GSK2830371 could act synergistically with standard of care chemotherapeutics. Treatment of wild-type TP53 neuroblastoma cell lines with both GSK2830371 and either doxorubicin or carboplatin resulted in enhanced cell death, mediated through caspase 3/7 induction, as compared to either agent alone. Our data suggests that WIP1 inhibition represents a novel therapeutic approach to neuroblastoma that could be integrated with current chemotherapeutic approaches.
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spelling pubmed-43199222015-02-18 WIP1 Phosphatase as a Potential Therapeutic Target in Neuroblastoma Richter, Mark Dayaram, Tajhal Gilmartin, Aidan G. Ganji, Gopinath Pemmasani, Sandhya Kiran Van Der Key, Harjeet Shohet, Jason M. Donehower, Lawrence A. Kumar, Rakesh PLoS One Research Article The wild-type p53-induced phosphatase 1 (WIP1) is a serine/threonine phosphatase that negatively regulates multiple proteins involved in DNA damage response including p53, CHK2, Histone H2AX, and ATM, and it has been shown to be overexpressed or amplified in human cancers including breast and ovarian cancers. We examined WIP1 mRNA levels across multiple tumor types and found the highest levels in breast cancer, leukemia, medulloblastoma and neuroblastoma. Neuroblastoma is an exclusively TP53 wild type tumor at diagnosis and inhibition of p53 is required for tumorigenesis. Neuroblastomas in particular have previously been shown to have 17q amplification, harboring the WIP1 (PPM1D) gene and associated with poor clinical outcome. We therefore sought to determine whether inhibiting WIP1 with a selective antagonist, GSK2830371, can attenuate neuroblastoma cell growth through reactivation of p53 mediated tumor suppression. Neuroblastoma cell lines with wild-type TP53 alleles were highly sensitive to GSK2830371 treatment, while cell lines with mutant TP53 were resistant to GSK2830371. The majority of tested neuroblastoma cell lines with copy number gains of the PPM1D locus were also TP53 wild-type and sensitive to GSK2830371A; in contrast cell lines with no copy gain of PPM1D were mixed in their sensitivity to WIP1 inhibition, with the primary determinant being TP53 mutational status. Since WIP1 is involved in the cellular response to DNA damage and drugs used in neuroblastoma treatment induce apoptosis through DNA damage, we sought to determine whether GSK2830371 could act synergistically with standard of care chemotherapeutics. Treatment of wild-type TP53 neuroblastoma cell lines with both GSK2830371 and either doxorubicin or carboplatin resulted in enhanced cell death, mediated through caspase 3/7 induction, as compared to either agent alone. Our data suggests that WIP1 inhibition represents a novel therapeutic approach to neuroblastoma that could be integrated with current chemotherapeutic approaches. Public Library of Science 2015-02-06 /pmc/articles/PMC4319922/ /pubmed/25658463 http://dx.doi.org/10.1371/journal.pone.0115635 Text en © 2015 Richter et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Richter, Mark
Dayaram, Tajhal
Gilmartin, Aidan G.
Ganji, Gopinath
Pemmasani, Sandhya Kiran
Van Der Key, Harjeet
Shohet, Jason M.
Donehower, Lawrence A.
Kumar, Rakesh
WIP1 Phosphatase as a Potential Therapeutic Target in Neuroblastoma
title WIP1 Phosphatase as a Potential Therapeutic Target in Neuroblastoma
title_full WIP1 Phosphatase as a Potential Therapeutic Target in Neuroblastoma
title_fullStr WIP1 Phosphatase as a Potential Therapeutic Target in Neuroblastoma
title_full_unstemmed WIP1 Phosphatase as a Potential Therapeutic Target in Neuroblastoma
title_short WIP1 Phosphatase as a Potential Therapeutic Target in Neuroblastoma
title_sort wip1 phosphatase as a potential therapeutic target in neuroblastoma
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4319922/
https://www.ncbi.nlm.nih.gov/pubmed/25658463
http://dx.doi.org/10.1371/journal.pone.0115635
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