Glioblastoma adaptation traced through decline of an IDH1 clonal driver and macro-evolution of a double-minute chromosome

BACKGROUND: Glioblastoma (GBM) is the most common malignant brain cancer occurring in adults, and is associated with dismal outcome and few therapeutic options. GBM has been shown to predominantly disrupt three core pathways through somatic aberrations, rendering it ideal for precision medicine appr...

Descripción completa

Detalles Bibliográficos
Autores principales: Favero, F., McGranahan, N., Salm, M., Birkbak, N. J., Sanborn, J. Z., Benz, S. C., Becq, J., Peden, J. F., Kingsbury, Z., Grocok, R. J., Humphray, S., Bentley, D., Spencer-Dene, B., Gutteridge, A., Brada, M., Roger, S., Dietrich, P.-Y., Forshew, T., Gerlinger, M., Rowan, A., Stamp, G., Eklund, A. C., Szallasi, Z., Swanton, C.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2015
Materias:
Original Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4405282/
https://www.ncbi.nlm.nih.gov/pubmed/25732040
http://dx.doi.org/10.1093/annonc/mdv127
_version_ 1782367615504613376
author Favero, F.
McGranahan, N.
Salm, M.
Birkbak, N. J.
Sanborn, J. Z.
Benz, S. C.
Becq, J.
Peden, J. F.
Kingsbury, Z.
Grocok, R. J.
Humphray, S.
Bentley, D.
Spencer-Dene, B.
Gutteridge, A.
Brada, M.
Roger, S.
Dietrich, P.-Y.
Forshew, T.
Gerlinger, M.
Rowan, A.
Stamp, G.
Eklund, A. C.
Szallasi, Z.
Swanton, C.
author_facet Favero, F.
McGranahan, N.
Salm, M.
Birkbak, N. J.
Sanborn, J. Z.
Benz, S. C.
Becq, J.
Peden, J. F.
Kingsbury, Z.
Grocok, R. J.
Humphray, S.
Bentley, D.
Spencer-Dene, B.
Gutteridge, A.
Brada, M.
Roger, S.
Dietrich, P.-Y.
Forshew, T.
Gerlinger, M.
Rowan, A.
Stamp, G.
Eklund, A. C.
Szallasi, Z.
Swanton, C.
author_sort Favero, F.
collection PubMed
description BACKGROUND: Glioblastoma (GBM) is the most common malignant brain cancer occurring in adults, and is associated with dismal outcome and few therapeutic options. GBM has been shown to predominantly disrupt three core pathways through somatic aberrations, rendering it ideal for precision medicine approaches. METHODS: We describe a 35-year-old female patient with recurrent GBM following surgical removal of the primary tumour, adjuvant treatment with temozolomide and a 3-year disease-free period. Rapid whole-genome sequencing (WGS) of three separate tumour regions at recurrence was carried out and interpreted relative to WGS of two regions of the primary tumour. RESULTS: We found extensive mutational and copy-number heterogeneity within the primary tumour. We identified a TP53 mutation and two focal amplifications involving PDGFRA, KIT and CDK4, on chromosomes 4 and 12. A clonal IDH1 R132H mutation in the primary, a known GBM driver event, was detectable at only very low frequency in the recurrent tumour. After sub-clonal diversification, evidence was found for a whole-genome doubling event and a translocation between the amplified regions of PDGFRA, KIT and CDK4, encoded within a double-minute chromosome also incorporating miR26a-2. The WGS analysis uncovered progressive evolution of the double-minute chromosome converging on the KIT/PDGFRA/PI3K/mTOR axis, superseding the IDH1 mutation in dominance in a mutually exclusive manner at recurrence, consequently the patient was treated with imatinib. Despite rapid sequencing and cancer genome-guided therapy against amplified oncogenes, the disease progressed, and the patient died shortly after. CONCLUSION: This case sheds light on the dynamic evolution of a GBM tumour, defining the origins of the lethal sub-clone, the macro-evolutionary genomic events dominating the disease at recurrence and the loss of a clonal driver. Even in the era of rapid WGS analysis, cases such as this illustrate the significant hurdles for precision medicine success.
format Online
Article
Text
id pubmed-4405282
institution National Center for Biotechnology Information
language English
publishDate 2015
publisher Oxford University Press
record_format MEDLINE/PubMed
spelling pubmed-44052822015-04-23 Glioblastoma adaptation traced through decline of an IDH1 clonal driver and macro-evolution of a double-minute chromosome Favero, F. McGranahan, N. Salm, M. Birkbak, N. J. Sanborn, J. Z. Benz, S. C. Becq, J. Peden, J. F. Kingsbury, Z. Grocok, R. J. Humphray, S. Bentley, D. Spencer-Dene, B. Gutteridge, A. Brada, M. Roger, S. Dietrich, P.-Y. Forshew, T. Gerlinger, M. Rowan, A. Stamp, G. Eklund, A. C. Szallasi, Z. Swanton, C. Ann Oncol Original Articles BACKGROUND: Glioblastoma (GBM) is the most common malignant brain cancer occurring in adults, and is associated with dismal outcome and few therapeutic options. GBM has been shown to predominantly disrupt three core pathways through somatic aberrations, rendering it ideal for precision medicine approaches. METHODS: We describe a 35-year-old female patient with recurrent GBM following surgical removal of the primary tumour, adjuvant treatment with temozolomide and a 3-year disease-free period. Rapid whole-genome sequencing (WGS) of three separate tumour regions at recurrence was carried out and interpreted relative to WGS of two regions of the primary tumour. RESULTS: We found extensive mutational and copy-number heterogeneity within the primary tumour. We identified a TP53 mutation and two focal amplifications involving PDGFRA, KIT and CDK4, on chromosomes 4 and 12. A clonal IDH1 R132H mutation in the primary, a known GBM driver event, was detectable at only very low frequency in the recurrent tumour. After sub-clonal diversification, evidence was found for a whole-genome doubling event and a translocation between the amplified regions of PDGFRA, KIT and CDK4, encoded within a double-minute chromosome also incorporating miR26a-2. The WGS analysis uncovered progressive evolution of the double-minute chromosome converging on the KIT/PDGFRA/PI3K/mTOR axis, superseding the IDH1 mutation in dominance in a mutually exclusive manner at recurrence, consequently the patient was treated with imatinib. Despite rapid sequencing and cancer genome-guided therapy against amplified oncogenes, the disease progressed, and the patient died shortly after. CONCLUSION: This case sheds light on the dynamic evolution of a GBM tumour, defining the origins of the lethal sub-clone, the macro-evolutionary genomic events dominating the disease at recurrence and the loss of a clonal driver. Even in the era of rapid WGS analysis, cases such as this illustrate the significant hurdles for precision medicine success. Oxford University Press 2015-05 2015-03-02 /pmc/articles/PMC4405282/ /pubmed/25732040 http://dx.doi.org/10.1093/annonc/mdv127 Text en © The Author 2015. Published by Oxford University Press on behalf of the European Society for Medical Oncology. http://creativecommons.org/licenses/by-nc/4.0/ This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License (http://creativecommons.org/licenses/by-nc/4.0/), which permits non-commercial re-use, distribution, and reproduction in any medium, provided the original work is properly cited. For commercial re-use, please contact journals.permissions@oup.com
spellingShingle Original Articles
Favero, F.
McGranahan, N.
Salm, M.
Birkbak, N. J.
Sanborn, J. Z.
Benz, S. C.
Becq, J.
Peden, J. F.
Kingsbury, Z.
Grocok, R. J.
Humphray, S.
Bentley, D.
Spencer-Dene, B.
Gutteridge, A.
Brada, M.
Roger, S.
Dietrich, P.-Y.
Forshew, T.
Gerlinger, M.
Rowan, A.
Stamp, G.
Eklund, A. C.
Szallasi, Z.
Swanton, C.
Glioblastoma adaptation traced through decline of an IDH1 clonal driver and macro-evolution of a double-minute chromosome
title Glioblastoma adaptation traced through decline of an IDH1 clonal driver and macro-evolution of a double-minute chromosome
title_full Glioblastoma adaptation traced through decline of an IDH1 clonal driver and macro-evolution of a double-minute chromosome
title_fullStr Glioblastoma adaptation traced through decline of an IDH1 clonal driver and macro-evolution of a double-minute chromosome
title_full_unstemmed Glioblastoma adaptation traced through decline of an IDH1 clonal driver and macro-evolution of a double-minute chromosome
title_short Glioblastoma adaptation traced through decline of an IDH1 clonal driver and macro-evolution of a double-minute chromosome
title_sort glioblastoma adaptation traced through decline of an idh1 clonal driver and macro-evolution of a double-minute chromosome
topic Original Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4405282/
https://www.ncbi.nlm.nih.gov/pubmed/25732040
http://dx.doi.org/10.1093/annonc/mdv127
work_keys_str_mv AT faverof glioblastomaadaptationtracedthroughdeclineofanidh1clonaldriverandmacroevolutionofadoubleminutechromosome
AT mcgranahann glioblastomaadaptationtracedthroughdeclineofanidh1clonaldriverandmacroevolutionofadoubleminutechromosome
AT salmm glioblastomaadaptationtracedthroughdeclineofanidh1clonaldriverandmacroevolutionofadoubleminutechromosome
AT birkbaknj glioblastomaadaptationtracedthroughdeclineofanidh1clonaldriverandmacroevolutionofadoubleminutechromosome
AT sanbornjz glioblastomaadaptationtracedthroughdeclineofanidh1clonaldriverandmacroevolutionofadoubleminutechromosome
AT benzsc glioblastomaadaptationtracedthroughdeclineofanidh1clonaldriverandmacroevolutionofadoubleminutechromosome
AT becqj glioblastomaadaptationtracedthroughdeclineofanidh1clonaldriverandmacroevolutionofadoubleminutechromosome
AT pedenjf glioblastomaadaptationtracedthroughdeclineofanidh1clonaldriverandmacroevolutionofadoubleminutechromosome
AT kingsburyz glioblastomaadaptationtracedthroughdeclineofanidh1clonaldriverandmacroevolutionofadoubleminutechromosome
AT grocokrj glioblastomaadaptationtracedthroughdeclineofanidh1clonaldriverandmacroevolutionofadoubleminutechromosome
AT humphrays glioblastomaadaptationtracedthroughdeclineofanidh1clonaldriverandmacroevolutionofadoubleminutechromosome
AT bentleyd glioblastomaadaptationtracedthroughdeclineofanidh1clonaldriverandmacroevolutionofadoubleminutechromosome
AT spencerdeneb glioblastomaadaptationtracedthroughdeclineofanidh1clonaldriverandmacroevolutionofadoubleminutechromosome
AT gutteridgea glioblastomaadaptationtracedthroughdeclineofanidh1clonaldriverandmacroevolutionofadoubleminutechromosome
AT bradam glioblastomaadaptationtracedthroughdeclineofanidh1clonaldriverandmacroevolutionofadoubleminutechromosome
AT rogers glioblastomaadaptationtracedthroughdeclineofanidh1clonaldriverandmacroevolutionofadoubleminutechromosome
AT dietrichpy glioblastomaadaptationtracedthroughdeclineofanidh1clonaldriverandmacroevolutionofadoubleminutechromosome
AT forshewt glioblastomaadaptationtracedthroughdeclineofanidh1clonaldriverandmacroevolutionofadoubleminutechromosome
AT gerlingerm glioblastomaadaptationtracedthroughdeclineofanidh1clonaldriverandmacroevolutionofadoubleminutechromosome
AT rowana glioblastomaadaptationtracedthroughdeclineofanidh1clonaldriverandmacroevolutionofadoubleminutechromosome
AT stampg glioblastomaadaptationtracedthroughdeclineofanidh1clonaldriverandmacroevolutionofadoubleminutechromosome
AT eklundac glioblastomaadaptationtracedthroughdeclineofanidh1clonaldriverandmacroevolutionofadoubleminutechromosome
AT szallasiz glioblastomaadaptationtracedthroughdeclineofanidh1clonaldriverandmacroevolutionofadoubleminutechromosome
AT swantonc glioblastomaadaptationtracedthroughdeclineofanidh1clonaldriverandmacroevolutionofadoubleminutechromosome

Ejemplares similares