Inactivation of BRCA2 in human cancer cells identifies a subset of tumors with enhanced sensitivity towards death receptormediated apoptosis

PURPOSE: DNA repair defects due to detrimental BRCA2-mutations confer increased susceptibility towards DNA interstrand-crosslinking (ICL) agents and define patient subpopulations for individualized genotype-based cancer therapy. However, due to the side effects of these drugs, there is a need to ide...

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Autores principales: De Toni, Enrico N., Ziesch, Andreas, Rizzani, Antonia, Török, Helga-Paula, Hocke, Sandra, Lü, Shuai, Wang, Shao-Chun, Hucl, Tomas, Göke, Burkhard, Bruns, Christiane, Gallmeier, Eike
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2016
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Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4891053/
https://www.ncbi.nlm.nih.gov/pubmed/26843614
http://dx.doi.org/10.18632/oncotarget.7053
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author De Toni, Enrico N.
Ziesch, Andreas
Rizzani, Antonia
Török, Helga-Paula
Hocke, Sandra
Lü, Shuai
Wang, Shao-Chun
Hucl, Tomas
Göke, Burkhard
Bruns, Christiane
Gallmeier, Eike
author_facet De Toni, Enrico N.
Ziesch, Andreas
Rizzani, Antonia
Török, Helga-Paula
Hocke, Sandra
Lü, Shuai
Wang, Shao-Chun
Hucl, Tomas
Göke, Burkhard
Bruns, Christiane
Gallmeier, Eike
author_sort De Toni, Enrico N.
collection PubMed
description PURPOSE: DNA repair defects due to detrimental BRCA2-mutations confer increased susceptibility towards DNA interstrand-crosslinking (ICL) agents and define patient subpopulations for individualized genotype-based cancer therapy. However, due to the side effects of these drugs, there is a need to identify additional agents, which could be used alone or in combination with ICL-agents. Therefore, we investigated whether BRCA2-mutations might also increase the sensitivity towards TRAIL-receptors (TRAIL-R)-targeting compounds. EXPERIMENTAL DESIGN: Two independent model systems were applied: a BRCA2 gene knockout and a BRCA2 gene complementation model. The effects of TRAIL-R-targeting compounds and ICL-agents on cell viability, apoptosis and cell cycle distribution were compared in BRCA2-proficient versus-deficient cancer cells in vitro. In addition, the effects of the TRAIL-R2-targeting antibody LBY135 were assessed in vivo using a murine tumor xenograft model. RESULTS: BRCA2-deficient cancer cells displayed an increased sensitivity towards TRAIL-R-targeting agents. These effects exceeded and were mechanistically distinguishable from the well-established effects of ICL-agents. In vitro, ICL-agents expectedly induced an early cell cycle arrest followed by delayed apoptosis, whereas TRAIL-R-targeting compounds caused early apoptosis without prior cell cycle arrest. In vivo, treatment with LBY135 significantly reduced the tumor growth of BRCA2-deficient cancer cells in a xenograft model. CONCLUSIONS: BRCA2 mutations strongly increase the in vitro- and in vivo-sensitivity of cancer cells towards TRAIL-R-mediated apoptosis. This effect is mechanistically distinguishable from the well-established ICL-hypersensitivity of BRCA2-deficient cells. Our study thus defines a new genetic subpopulation of cancers susceptible towards TRAIL-R-targeting compounds, which could facilitate novel therapeutic approaches for patients with BRCA2-deficient tumors.
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spelling pubmed-48910532016-06-20 Inactivation of BRCA2 in human cancer cells identifies a subset of tumors with enhanced sensitivity towards death receptormediated apoptosis De Toni, Enrico N. Ziesch, Andreas Rizzani, Antonia Török, Helga-Paula Hocke, Sandra Lü, Shuai Wang, Shao-Chun Hucl, Tomas Göke, Burkhard Bruns, Christiane Gallmeier, Eike Oncotarget Research Paper PURPOSE: DNA repair defects due to detrimental BRCA2-mutations confer increased susceptibility towards DNA interstrand-crosslinking (ICL) agents and define patient subpopulations for individualized genotype-based cancer therapy. However, due to the side effects of these drugs, there is a need to identify additional agents, which could be used alone or in combination with ICL-agents. Therefore, we investigated whether BRCA2-mutations might also increase the sensitivity towards TRAIL-receptors (TRAIL-R)-targeting compounds. EXPERIMENTAL DESIGN: Two independent model systems were applied: a BRCA2 gene knockout and a BRCA2 gene complementation model. The effects of TRAIL-R-targeting compounds and ICL-agents on cell viability, apoptosis and cell cycle distribution were compared in BRCA2-proficient versus-deficient cancer cells in vitro. In addition, the effects of the TRAIL-R2-targeting antibody LBY135 were assessed in vivo using a murine tumor xenograft model. RESULTS: BRCA2-deficient cancer cells displayed an increased sensitivity towards TRAIL-R-targeting agents. These effects exceeded and were mechanistically distinguishable from the well-established effects of ICL-agents. In vitro, ICL-agents expectedly induced an early cell cycle arrest followed by delayed apoptosis, whereas TRAIL-R-targeting compounds caused early apoptosis without prior cell cycle arrest. In vivo, treatment with LBY135 significantly reduced the tumor growth of BRCA2-deficient cancer cells in a xenograft model. CONCLUSIONS: BRCA2 mutations strongly increase the in vitro- and in vivo-sensitivity of cancer cells towards TRAIL-R-mediated apoptosis. This effect is mechanistically distinguishable from the well-established ICL-hypersensitivity of BRCA2-deficient cells. Our study thus defines a new genetic subpopulation of cancers susceptible towards TRAIL-R-targeting compounds, which could facilitate novel therapeutic approaches for patients with BRCA2-deficient tumors. Impact Journals LLC 2016-01-28 /pmc/articles/PMC4891053/ /pubmed/26843614 http://dx.doi.org/10.18632/oncotarget.7053 Text en Copyright: © 2016 De Toni et al. http://creativecommons.org/licenses/by/2.5/ 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 credited.
spellingShingle Research Paper
De Toni, Enrico N.
Ziesch, Andreas
Rizzani, Antonia
Török, Helga-Paula
Hocke, Sandra
Lü, Shuai
Wang, Shao-Chun
Hucl, Tomas
Göke, Burkhard
Bruns, Christiane
Gallmeier, Eike
Inactivation of BRCA2 in human cancer cells identifies a subset of tumors with enhanced sensitivity towards death receptormediated apoptosis
title Inactivation of BRCA2 in human cancer cells identifies a subset of tumors with enhanced sensitivity towards death receptormediated apoptosis
title_full Inactivation of BRCA2 in human cancer cells identifies a subset of tumors with enhanced sensitivity towards death receptormediated apoptosis
title_fullStr Inactivation of BRCA2 in human cancer cells identifies a subset of tumors with enhanced sensitivity towards death receptormediated apoptosis
title_full_unstemmed Inactivation of BRCA2 in human cancer cells identifies a subset of tumors with enhanced sensitivity towards death receptormediated apoptosis
title_short Inactivation of BRCA2 in human cancer cells identifies a subset of tumors with enhanced sensitivity towards death receptormediated apoptosis
title_sort inactivation of brca2 in human cancer cells identifies a subset of tumors with enhanced sensitivity towards death receptormediated apoptosis
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4891053/
https://www.ncbi.nlm.nih.gov/pubmed/26843614
http://dx.doi.org/10.18632/oncotarget.7053
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