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Chemosensitivity profiling of osteosarcoma tumour cell lines identifies a model of BRCAness

Chemosensitivity profiling of osteosarcoma tumour cell lines identifies a model of BRCAness
Chemosensitivity profiling of osteosarcoma tumour cell lines identifies a model of BRCAness
Osteosarcoma (OS) is an aggressive sarcoma, where novel treatment approaches are required. Genomic studies suggest that a subset of OS, including OS tumour cell lines (TCLs), exhibit genomic loss of heterozygosity (LOH) patterns reminiscent of BRCA1 or BRCA2 mutant tumours. This raises the possibility that PARP inhibitors (PARPi), used to treat BRCA1/2 mutant cancers, could be used to target OS. Using high-throughput drug sensitivity screening we generated chemosensitivity profiles for 79 small molecule inhibitors, including three clinical PARPi. Drug screening was performed in 88 tumour cell lines, including 18 OS TCLs. This identified known sensitivity effects in OS TCLs, such as sensitivity to FGFR inhibitors. When compared to BRCA1/2 mutant TCLs, OS TCLs, with the exception of LM7, were PARPi resistant, including those with previously determined BRCAness LoH profiles. Post-screen validation experiments confirmed PARPi sensitivity in LM7 cells as well as a defect in the ability to form nuclear RAD51 foci in response to DNA damage. LM7 provides one OS model for the study of PARPi sensitivity through a potential defect in RAD51-mediated DNA repair. The drug sensitivity dataset we generated in 88 TCLs could also serve as a resource for the study of drug sensitivity effects in OS.
bone cancer, predictive markers
2045-2322
Holme, Harriett
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Gulati, Aditi
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Brough, Rachel
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Fleuren, Emmy D. G.
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Bajrami, Ilirjana
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Campbell, James
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Chong, Irene Y.
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Costa-Cabral, Sara
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Elliott, Richard
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Fenton, Tim R.
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Frankum, Jessica
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Jones, Samuel E.
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Menon, Malini
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Miller, Rowan
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Selfe, Joanna L.
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Kriegsheim, Alex von
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Munoz, Amaya Garcia
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Rodriguez, Javier
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Graaf, Winette T. A. van der
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Williamson, Chris T.
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Ryan, Colm J.
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Pettitt, Stephen
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Ashworth, Alan
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Strauss, Sandra J.
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Lord, Christopher J.
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Holme, Harriett
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Gulati, Aditi
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Brough, Rachel
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Campbell, James
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Elliott, Richard
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Fenton, Tim R.
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Frankum, Jessica
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Jones, Samuel E.
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Menon, Malini
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Selfe, Joanna L.
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Kriegsheim, Alex von
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Munoz, Amaya Garcia
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Rodriguez, Javier
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Shipley, Janet
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Graaf, Winette T. A. van der
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Williamson, Chris T.
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Ryan, Colm J.
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Pettitt, Stephen
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Ashworth, Alan
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Strauss, Sandra J.
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Lord, Christopher J.
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Holme, Harriett, Gulati, Aditi, Brough, Rachel, Fleuren, Emmy D. G., Bajrami, Ilirjana, Campbell, James, Chong, Irene Y., Costa-Cabral, Sara, Elliott, Richard, Fenton, Tim R., Frankum, Jessica, Jones, Samuel E., Menon, Malini, Miller, Rowan, Pemberton, Helen N., Postel-Vinay, Sophie, Rafiq, Rumana, Selfe, Joanna L., Kriegsheim, Alex von, Munoz, Amaya Garcia, Rodriguez, Javier, Shipley, Janet, Graaf, Winette T. A. van der, Williamson, Chris T., Ryan, Colm J., Pettitt, Stephen, Ashworth, Alan, Strauss, Sandra J. and Lord, Christopher J. (2018) Chemosensitivity profiling of osteosarcoma tumour cell lines identifies a model of BRCAness. Scientific Reports, 8 (1), [10614]. (doi:10.1038/s41598-018-29043-z).

Record type: Article

Abstract

Osteosarcoma (OS) is an aggressive sarcoma, where novel treatment approaches are required. Genomic studies suggest that a subset of OS, including OS tumour cell lines (TCLs), exhibit genomic loss of heterozygosity (LOH) patterns reminiscent of BRCA1 or BRCA2 mutant tumours. This raises the possibility that PARP inhibitors (PARPi), used to treat BRCA1/2 mutant cancers, could be used to target OS. Using high-throughput drug sensitivity screening we generated chemosensitivity profiles for 79 small molecule inhibitors, including three clinical PARPi. Drug screening was performed in 88 tumour cell lines, including 18 OS TCLs. This identified known sensitivity effects in OS TCLs, such as sensitivity to FGFR inhibitors. When compared to BRCA1/2 mutant TCLs, OS TCLs, with the exception of LM7, were PARPi resistant, including those with previously determined BRCAness LoH profiles. Post-screen validation experiments confirmed PARPi sensitivity in LM7 cells as well as a defect in the ability to form nuclear RAD51 foci in response to DNA damage. LM7 provides one OS model for the study of PARPi sensitivity through a potential defect in RAD51-mediated DNA repair. The drug sensitivity dataset we generated in 88 TCLs could also serve as a resource for the study of drug sensitivity effects in OS.

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s41598-018-29043-z - Version of Record
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Published date: 1 July 2018
Keywords: bone cancer, predictive markers

Identifiers

Local EPrints ID: 456244
URI: http://eprints.soton.ac.uk/id/eprint/456244
DOI: doi:10.1038/s41598-018-29043-z
ISSN: 2045-2322
PURE UUID: 55c50d7f-939a-4bca-8167-97e296c8cec6
ORCID for Tim R. Fenton: ORCID iD orcid.org/0000-0002-4737-8233

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Date deposited: 26 Apr 2022 21:22
Last modified: 17 Mar 2024 04:11

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Contributors

Author: Harriett Holme
Author: Aditi Gulati
Author: Rachel Brough
Author: Emmy D. G. Fleuren
Author: Ilirjana Bajrami
Author: James Campbell
Author: Irene Y. Chong
Author: Sara Costa-Cabral
Author: Richard Elliott
Author: Tim R. Fenton ORCID iD
Author: Jessica Frankum
Author: Samuel E. Jones
Author: Malini Menon
Author: Rowan Miller
Author: Helen N. Pemberton
Author: Sophie Postel-Vinay
Author: Rumana Rafiq
Author: Joanna L. Selfe
Author: Alex von Kriegsheim
Author: Amaya Garcia Munoz
Author: Javier Rodriguez
Author: Janet Shipley
Author: Winette T. A. van der Graaf
Author: Chris T. Williamson
Author: Colm J. Ryan
Author: Stephen Pettitt
Author: Alan Ashworth
Author: Sandra J. Strauss
Author: Christopher J. Lord

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