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Neoplastic human embryonic stem cells as a model of radiation resistance of human cancer stem cells

Studies have implicated that a small sub-population of cells within a tumour, termed cancer stem cells (CSCs), have an enhanced capacity for tumour formation in multiple cancers and may be responsible for recurrence of the disease after treatment, including radiation. Although comparisons have been...

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Autores principales: Dingwall, Steve, Lee, Jung Bok, Guezguez, Borhane, Fiebig, Aline, McNicol, Jamie, Boreham, Douglas, Collins, Tony J., Bhatia, Mick
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2015
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4673161/
https://www.ncbi.nlm.nih.gov/pubmed/26082437
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author Dingwall, Steve
Lee, Jung Bok
Guezguez, Borhane
Fiebig, Aline
McNicol, Jamie
Boreham, Douglas
Collins, Tony J.
Bhatia, Mick
author_facet Dingwall, Steve
Lee, Jung Bok
Guezguez, Borhane
Fiebig, Aline
McNicol, Jamie
Boreham, Douglas
Collins, Tony J.
Bhatia, Mick
author_sort Dingwall, Steve
collection PubMed
description Studies have implicated that a small sub-population of cells within a tumour, termed cancer stem cells (CSCs), have an enhanced capacity for tumour formation in multiple cancers and may be responsible for recurrence of the disease after treatment, including radiation. Although comparisons have been made between CSCs and bulk-tumour, the more important comparison with respect to therapy is between tumour-sustaining CSC versus normal stem cells that maintain the healthy tissue. However, the absence of normal known counterparts for many CSCs has made it difficult to compare the radiation responses of CSCs with the normal stem cells required for post-radiotherapy tissue regeneration and the maintenance of tissue homeostasis. Here we demonstrate that transformed human embryonic stem cells (t-hESCs), showing features of neoplastic progression produce tumours resistant to radiation relative to their normal counterpart upon injection into immune compromised mice. We reveal that t-hESCs have a reduced capacity for radiation induced cell death via apoptosis and exhibit altered cell cycle arrest relative to hESCs in vitro. t-hESCs have an increased expression of BclXL in comparison to their normal counterparts and re-sensitization of t-hESCs to radiation upon addition of BH3-only mimetic ABT737, suggesting that overexpression of BclXL underpins t-hESC radiation insensitivity. Using this novel discovery platform to investigate radiation resistance in human CSCs, our study indicates that chemotherapy targeting Bcl2-family members may prove to be an adjuvant to radiotherapy capable of targeting CSCs.
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spelling pubmed-46731612015-12-23 Neoplastic human embryonic stem cells as a model of radiation resistance of human cancer stem cells Dingwall, Steve Lee, Jung Bok Guezguez, Borhane Fiebig, Aline McNicol, Jamie Boreham, Douglas Collins, Tony J. Bhatia, Mick Oncotarget Research Paper Studies have implicated that a small sub-population of cells within a tumour, termed cancer stem cells (CSCs), have an enhanced capacity for tumour formation in multiple cancers and may be responsible for recurrence of the disease after treatment, including radiation. Although comparisons have been made between CSCs and bulk-tumour, the more important comparison with respect to therapy is between tumour-sustaining CSC versus normal stem cells that maintain the healthy tissue. However, the absence of normal known counterparts for many CSCs has made it difficult to compare the radiation responses of CSCs with the normal stem cells required for post-radiotherapy tissue regeneration and the maintenance of tissue homeostasis. Here we demonstrate that transformed human embryonic stem cells (t-hESCs), showing features of neoplastic progression produce tumours resistant to radiation relative to their normal counterpart upon injection into immune compromised mice. We reveal that t-hESCs have a reduced capacity for radiation induced cell death via apoptosis and exhibit altered cell cycle arrest relative to hESCs in vitro. t-hESCs have an increased expression of BclXL in comparison to their normal counterparts and re-sensitization of t-hESCs to radiation upon addition of BH3-only mimetic ABT737, suggesting that overexpression of BclXL underpins t-hESC radiation insensitivity. Using this novel discovery platform to investigate radiation resistance in human CSCs, our study indicates that chemotherapy targeting Bcl2-family members may prove to be an adjuvant to radiotherapy capable of targeting CSCs. Impact Journals LLC 2015-06-13 /pmc/articles/PMC4673161/ /pubmed/26082437 Text en Copyright: © 2015 Dingwall 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
Dingwall, Steve
Lee, Jung Bok
Guezguez, Borhane
Fiebig, Aline
McNicol, Jamie
Boreham, Douglas
Collins, Tony J.
Bhatia, Mick
Neoplastic human embryonic stem cells as a model of radiation resistance of human cancer stem cells
title Neoplastic human embryonic stem cells as a model of radiation resistance of human cancer stem cells
title_full Neoplastic human embryonic stem cells as a model of radiation resistance of human cancer stem cells
title_fullStr Neoplastic human embryonic stem cells as a model of radiation resistance of human cancer stem cells
title_full_unstemmed Neoplastic human embryonic stem cells as a model of radiation resistance of human cancer stem cells
title_short Neoplastic human embryonic stem cells as a model of radiation resistance of human cancer stem cells
title_sort neoplastic human embryonic stem cells as a model of radiation resistance of human cancer stem cells
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4673161/
https://www.ncbi.nlm.nih.gov/pubmed/26082437
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