Radiosensitization of HNSCC cells by EGFR inhibition depends on the induction of cell cycle arrests

The increase in cellular radiosensitivity by EGF receptor (EGFR) inhibition has been shown to be attributable to the induction of a G1-arrest in p53-proficient cells. Because EGFR targeting in combination with radiotherapy is used to treat head and neck squamous cell carcinomas (HNSCC) which are pre...

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Autores principales: Kriegs, Malte, Kasten-Pisula, Ulla, Riepen, Britta, Hoffer, Konstantin, Struve, Nina, Myllynen, Laura, Braig, Friederike, Binder, Mascha, Rieckmann, Thorsten, Grénman, Reidar, Petersen, Cordula, Dikomey, Ekkehard, Rothkamm, Kai
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2016
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5216710/
https://www.ncbi.nlm.nih.gov/pubmed/27281611
http://dx.doi.org/10.18632/oncotarget.9161
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author Kriegs, Malte
Kasten-Pisula, Ulla
Riepen, Britta
Hoffer, Konstantin
Struve, Nina
Myllynen, Laura
Braig, Friederike
Binder, Mascha
Rieckmann, Thorsten
Grénman, Reidar
Petersen, Cordula
Dikomey, Ekkehard
Rothkamm, Kai
author_facet Kriegs, Malte
Kasten-Pisula, Ulla
Riepen, Britta
Hoffer, Konstantin
Struve, Nina
Myllynen, Laura
Braig, Friederike
Binder, Mascha
Rieckmann, Thorsten
Grénman, Reidar
Petersen, Cordula
Dikomey, Ekkehard
Rothkamm, Kai
author_sort Kriegs, Malte
collection PubMed
description The increase in cellular radiosensitivity by EGF receptor (EGFR) inhibition has been shown to be attributable to the induction of a G1-arrest in p53-proficient cells. Because EGFR targeting in combination with radiotherapy is used to treat head and neck squamous cell carcinomas (HNSCC) which are predominantly p53 mutated, we tested the effects of EGFR targeting on cellular radiosensitivity, proliferation, apoptosis, DNA repair and cell cycle control using a large panel of HNSCC cell lines. In these experiments EGFR targeting inhibited signal transduction, blocked proliferation and induced radiosensitization but only in some cell lines and only under normal (pre-plating) conditions. This sensitization was not associated with impaired DNA repair (53BP1 foci) or induction of apoptosis. However, it was associated with the induction of a lasting G2-arrest. Both, the radiosensitization and the G2-arrest were abrogated if the cells were re-stimulated (delayed plating) with actually no radiosensitization being detectable in any of the 14 tested cell lines. Therefore we conclude that EGFR targeting can induce a reversible G2 arrest in p53 deficient HNSCC cells, which does not consequently result in a robust cellular radiosensitization. Together with recent animal and clinical studies our data indicate that EGFR inhibition is no effective strategy to increase the radiosensitivity of HNSCC cells.
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spelling pubmed-52167102017-01-15 Radiosensitization of HNSCC cells by EGFR inhibition depends on the induction of cell cycle arrests Kriegs, Malte Kasten-Pisula, Ulla Riepen, Britta Hoffer, Konstantin Struve, Nina Myllynen, Laura Braig, Friederike Binder, Mascha Rieckmann, Thorsten Grénman, Reidar Petersen, Cordula Dikomey, Ekkehard Rothkamm, Kai Oncotarget Research Paper The increase in cellular radiosensitivity by EGF receptor (EGFR) inhibition has been shown to be attributable to the induction of a G1-arrest in p53-proficient cells. Because EGFR targeting in combination with radiotherapy is used to treat head and neck squamous cell carcinomas (HNSCC) which are predominantly p53 mutated, we tested the effects of EGFR targeting on cellular radiosensitivity, proliferation, apoptosis, DNA repair and cell cycle control using a large panel of HNSCC cell lines. In these experiments EGFR targeting inhibited signal transduction, blocked proliferation and induced radiosensitization but only in some cell lines and only under normal (pre-plating) conditions. This sensitization was not associated with impaired DNA repair (53BP1 foci) or induction of apoptosis. However, it was associated with the induction of a lasting G2-arrest. Both, the radiosensitization and the G2-arrest were abrogated if the cells were re-stimulated (delayed plating) with actually no radiosensitization being detectable in any of the 14 tested cell lines. Therefore we conclude that EGFR targeting can induce a reversible G2 arrest in p53 deficient HNSCC cells, which does not consequently result in a robust cellular radiosensitization. Together with recent animal and clinical studies our data indicate that EGFR inhibition is no effective strategy to increase the radiosensitivity of HNSCC cells. Impact Journals LLC 2016-05-04 /pmc/articles/PMC5216710/ /pubmed/27281611 http://dx.doi.org/10.18632/oncotarget.9161 Text en Copyright: © 2016 Kriegs 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
Kriegs, Malte
Kasten-Pisula, Ulla
Riepen, Britta
Hoffer, Konstantin
Struve, Nina
Myllynen, Laura
Braig, Friederike
Binder, Mascha
Rieckmann, Thorsten
Grénman, Reidar
Petersen, Cordula
Dikomey, Ekkehard
Rothkamm, Kai
Radiosensitization of HNSCC cells by EGFR inhibition depends on the induction of cell cycle arrests
title Radiosensitization of HNSCC cells by EGFR inhibition depends on the induction of cell cycle arrests
title_full Radiosensitization of HNSCC cells by EGFR inhibition depends on the induction of cell cycle arrests
title_fullStr Radiosensitization of HNSCC cells by EGFR inhibition depends on the induction of cell cycle arrests
title_full_unstemmed Radiosensitization of HNSCC cells by EGFR inhibition depends on the induction of cell cycle arrests
title_short Radiosensitization of HNSCC cells by EGFR inhibition depends on the induction of cell cycle arrests
title_sort radiosensitization of hnscc cells by egfr inhibition depends on the induction of cell cycle arrests
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5216710/
https://www.ncbi.nlm.nih.gov/pubmed/27281611
http://dx.doi.org/10.18632/oncotarget.9161
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