Inhibition of PI3K-AKT-mTOR pathway sensitizes endometrial cancer cell lines to PARP inhibitors

Inhibition of PI3K-AKT-mTOR pathway sensitizes endometrial cancer cell lines to PARP inhibitors

Abstract Background Phosphatase and Tensin homolog (PTEN) is a tumor suppressor gene. Loss of its function is the most frequent genetic alteration in endometrioid endometrial cancers (70–80%) and high grade tumors (90%). We assessed the sensitivity of endometrial cancer cell lines to PARP inhibitors...

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Main Authors: Charles-André Philip, Ido Laskov, Marie-Claude Beauchamp, Maud Marques, Oreekha Amin, Joanna Bitharas, Roy Kessous, Liron Kogan, Tahira Baloch, Walter H. Gotlieb, Amber Yasmeen
Format: Article
Language:English
Published: BMC 2017-09-01
Series:BMC Cancer
Subjects:
Endometrial cancer
PTEN
PI3K/mTOR pathway
PARP inhibitor
DNA repair pathway
RAD51
Online Access:http://link.springer.com/article/10.1186/s12885-017-3639-0
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spelling doaj-921f99facb7e4ba981e9e6deacfbde8f2020-11-24T21:11:58ZengBMCBMC Cancer1471-24072017-09-0117111110.1186/s12885-017-3639-0Inhibition of PI3K-AKT-mTOR pathway sensitizes endometrial cancer cell lines to PARP inhibitorsCharles-André Philip0Ido Laskov1Marie-Claude Beauchamp2Maud Marques3Oreekha Amin4Joanna Bitharas5Roy Kessous6Liron Kogan7Tahira Baloch8Walter H. Gotlieb9Amber Yasmeen10Segal Cancer Center, Lady Davis Institute of Medical Research, McGill UniversityDivision of Gynecologic Oncology, Jewish General Hospital, McGill UniversityDivision of Gynecologic Oncology, Jewish General Hospital, McGill UniversitySegal Cancer Center, Lady Davis Institute of Medical Research, McGill UniversitySegal Cancer Center, Lady Davis Institute of Medical Research, McGill UniversitySegal Cancer Center, Lady Davis Institute of Medical Research, McGill UniversityDivision of Gynecologic Oncology, Jewish General Hospital, McGill UniversityDivision of Gynecologic Oncology, Jewish General Hospital, McGill UniversitySegal Cancer Center, Lady Davis Institute of Medical Research, McGill UniversityDivision of Gynecologic Oncology, Jewish General Hospital, McGill UniversityDivision of Gynecologic Oncology, Jewish General Hospital, McGill UniversityAbstract Background Phosphatase and Tensin homolog (PTEN) is a tumor suppressor gene. Loss of its function is the most frequent genetic alteration in endometrioid endometrial cancers (70–80%) and high grade tumors (90%). We assessed the sensitivity of endometrial cancer cell lines to PARP inhibitors (olaparib and BMN-673) and a PI3K inhibitor (BKM-120), alone or in combination, in the context of their PTEN mutation status. We also highlighted a direct pathway linking PTEN to DNA repair. Methods Using endometrial cancer cellular models with known PTEN status, we evaluated their homologous recombination (HR) functionality by RAD51 foci formation assay. The 50% Inhibitory concentration (IC50) of PI3K and PARP inhibitors in these cells was assessed, and western blotting was performed to determine the expression of proteins involved in the PI3K/mTOR pathway. Moreover, we explored the interaction between RAD51 and PI3K/mTOR by immunofluorescence. Next, the combination effect of PI3K and PARP inhibitors on cell proliferation was evaluated by a clonogenic assay. Results Cells with mutated PTEN showed over-activation of the PI3K/mTOR pathway. These cells were more sensitive to PARP inhibition compared to PTEN wild-type cells. In addition, PI3K inhibitor treatment reduced RAD51 foci formation in PTEN mutated cells, and sensitized these cells to PARP inhibitor. Conclusion Targeting both PARP and PI3K might lead to improved personalized therapeutic approaches in endometrial cancer patients with PTEN mutations. Understanding the complex interaction of PTEN mutations with DNA repair in endometrial cancer will help to better select patients that are likely to respond to some of the new and costly targeted therapies.http://link.springer.com/article/10.1186/s12885-017-3639-0Endometrial cancerPTENPI3K/mTOR pathwayPARP inhibitorDNA repair pathwayRAD51
collection DOAJ
language English
format Article
sources DOAJ
author Charles-André Philip
Ido Laskov
Marie-Claude Beauchamp
Maud Marques
Oreekha Amin
Joanna Bitharas
Roy Kessous
Liron Kogan
Tahira Baloch
Walter H. Gotlieb
Amber Yasmeen
spellingShingle Charles-André Philip
Ido Laskov
Marie-Claude Beauchamp
Maud Marques
Oreekha Amin
Joanna Bitharas
Roy Kessous
Liron Kogan
Tahira Baloch
Walter H. Gotlieb
Amber Yasmeen
Inhibition of PI3K-AKT-mTOR pathway sensitizes endometrial cancer cell lines to PARP inhibitors
BMC Cancer
Endometrial cancer
PTEN
PI3K/mTOR pathway
PARP inhibitor
DNA repair pathway
RAD51
author_facet Charles-André Philip
Ido Laskov
Marie-Claude Beauchamp
Maud Marques
Oreekha Amin
Joanna Bitharas
Roy Kessous
Liron Kogan
Tahira Baloch
Walter H. Gotlieb
Amber Yasmeen
author_sort Charles-André Philip
title Inhibition of PI3K-AKT-mTOR pathway sensitizes endometrial cancer cell lines to PARP inhibitors
title_short Inhibition of PI3K-AKT-mTOR pathway sensitizes endometrial cancer cell lines to PARP inhibitors
title_full Inhibition of PI3K-AKT-mTOR pathway sensitizes endometrial cancer cell lines to PARP inhibitors
title_fullStr Inhibition of PI3K-AKT-mTOR pathway sensitizes endometrial cancer cell lines to PARP inhibitors
title_full_unstemmed Inhibition of PI3K-AKT-mTOR pathway sensitizes endometrial cancer cell lines to PARP inhibitors
title_sort inhibition of pi3k-akt-mtor pathway sensitizes endometrial cancer cell lines to parp inhibitors
publisher BMC
series BMC Cancer
issn 1471-2407
publishDate 2017-09-01
description Abstract Background Phosphatase and Tensin homolog (PTEN) is a tumor suppressor gene. Loss of its function is the most frequent genetic alteration in endometrioid endometrial cancers (70–80%) and high grade tumors (90%). We assessed the sensitivity of endometrial cancer cell lines to PARP inhibitors (olaparib and BMN-673) and a PI3K inhibitor (BKM-120), alone or in combination, in the context of their PTEN mutation status. We also highlighted a direct pathway linking PTEN to DNA repair. Methods Using endometrial cancer cellular models with known PTEN status, we evaluated their homologous recombination (HR) functionality by RAD51 foci formation assay. The 50% Inhibitory concentration (IC50) of PI3K and PARP inhibitors in these cells was assessed, and western blotting was performed to determine the expression of proteins involved in the PI3K/mTOR pathway. Moreover, we explored the interaction between RAD51 and PI3K/mTOR by immunofluorescence. Next, the combination effect of PI3K and PARP inhibitors on cell proliferation was evaluated by a clonogenic assay. Results Cells with mutated PTEN showed over-activation of the PI3K/mTOR pathway. These cells were more sensitive to PARP inhibition compared to PTEN wild-type cells. In addition, PI3K inhibitor treatment reduced RAD51 foci formation in PTEN mutated cells, and sensitized these cells to PARP inhibitor. Conclusion Targeting both PARP and PI3K might lead to improved personalized therapeutic approaches in endometrial cancer patients with PTEN mutations. Understanding the complex interaction of PTEN mutations with DNA repair in endometrial cancer will help to better select patients that are likely to respond to some of the new and costly targeted therapies.
topic Endometrial cancer
PTEN
PI3K/mTOR pathway
PARP inhibitor
DNA repair pathway
RAD51
url http://link.springer.com/article/10.1186/s12885-017-3639-0
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