Intratumour diversity of chromosome copy numbers in neuroblastoma mediated by on-going chromosome loss from a polyploid state.

Intratumour diversity of chromosome copy numbers in neuroblastoma mediated by on-going chromosome loss from a polyploid state.

Neuroblastomas (NBs) are tumours of the sympathetic nervous system accounting for 8-10% of paediatric cancers. NBs exhibit extensive intertumour genetic heterogeneity, but their extent of intratumour genetic diversity has remained unexplored. We aimed to assess intratumour genetic variation in NBs w...

Full description

Bibliographic Details
Main Authors: Gisela Lundberg, Yuesheng Jin, Daniel Sehic, Ingrid Øra, Rogier Versteeg, David Gisselsson
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2013-01-01
Series:PLoS ONE
Online Access:https://www.ncbi.nlm.nih.gov/pmc/articles/pmid/23555645/?tool=EBI
id doaj-4a7c17f326f54da09dbb2a3e5bae2ba5
record_format Article
spelling doaj-4a7c17f326f54da09dbb2a3e5bae2ba52021-03-03T23:33:37ZengPublic Library of Science (PLoS)PLoS ONE1932-62032013-01-0183e5926810.1371/journal.pone.0059268Intratumour diversity of chromosome copy numbers in neuroblastoma mediated by on-going chromosome loss from a polyploid state.Gisela LundbergYuesheng JinDaniel SehicIngrid ØraRogier VersteegDavid GisselssonNeuroblastomas (NBs) are tumours of the sympathetic nervous system accounting for 8-10% of paediatric cancers. NBs exhibit extensive intertumour genetic heterogeneity, but their extent of intratumour genetic diversity has remained unexplored. We aimed to assess intratumour genetic variation in NBs with a focus on whole chromosome changes and their underlying mechanism. Allelic ratios obtained by SNP-array data from 30 aneuploid primary NBs and NB cell lines were used to quantify the size of clones harbouring specific genomic imbalances. In 13 cases, this was supplemented by fluorescence in situ hybridisation to assess copy number diversity in detail. Computer simulations of different mitotic segregation errors, single cell cloning, analysis of mitotic figures, and time lapse imaging of dividing NB cells were used to infer the most likely mechanism behind intratumour variation in chromosome number. Combined SNP array and FISH analyses showed that all cases exhibited higher inter-cellular copy number variation than non-neoplastic control tissue, with up to 75% of tumour cells showing non-modal chromosome copy numbers. Comparisons of copy number profiles, resulting from simulations of different segregation errors to genomic profiles of 120 NBs indicated that loss of chromosomes from a tetraploid state was more likely than other mechanisms to explain numerical aberrations in NB. This was supported by a high frequency of lagging chromosomes at anaphase and polyploidisation events in growing NB cells. The dynamic nature of numerical aberrations was corroborated further by detecting substantial copy number diversity in cell populations grown from single NB cells. We conclude that aneuploid NBs typically show extensive intratumour chromosome copy number diversity, and that this phenomenon is most likely explained by continuous loss of chromosomes from a polyploid state.https://www.ncbi.nlm.nih.gov/pmc/articles/pmid/23555645/?tool=EBI
collection DOAJ
language English
format Article
sources DOAJ
author Gisela Lundberg
Yuesheng Jin
Daniel Sehic
Ingrid Øra
Rogier Versteeg
David Gisselsson
spellingShingle Gisela Lundberg
Yuesheng Jin
Daniel Sehic
Ingrid Øra
Rogier Versteeg
David Gisselsson
Intratumour diversity of chromosome copy numbers in neuroblastoma mediated by on-going chromosome loss from a polyploid state.
PLoS ONE
author_facet Gisela Lundberg
Yuesheng Jin
Daniel Sehic
Ingrid Øra
Rogier Versteeg
David Gisselsson
author_sort Gisela Lundberg
title Intratumour diversity of chromosome copy numbers in neuroblastoma mediated by on-going chromosome loss from a polyploid state.
title_short Intratumour diversity of chromosome copy numbers in neuroblastoma mediated by on-going chromosome loss from a polyploid state.
title_full Intratumour diversity of chromosome copy numbers in neuroblastoma mediated by on-going chromosome loss from a polyploid state.
title_fullStr Intratumour diversity of chromosome copy numbers in neuroblastoma mediated by on-going chromosome loss from a polyploid state.
title_full_unstemmed Intratumour diversity of chromosome copy numbers in neuroblastoma mediated by on-going chromosome loss from a polyploid state.
title_sort intratumour diversity of chromosome copy numbers in neuroblastoma mediated by on-going chromosome loss from a polyploid state.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2013-01-01
description Neuroblastomas (NBs) are tumours of the sympathetic nervous system accounting for 8-10% of paediatric cancers. NBs exhibit extensive intertumour genetic heterogeneity, but their extent of intratumour genetic diversity has remained unexplored. We aimed to assess intratumour genetic variation in NBs with a focus on whole chromosome changes and their underlying mechanism. Allelic ratios obtained by SNP-array data from 30 aneuploid primary NBs and NB cell lines were used to quantify the size of clones harbouring specific genomic imbalances. In 13 cases, this was supplemented by fluorescence in situ hybridisation to assess copy number diversity in detail. Computer simulations of different mitotic segregation errors, single cell cloning, analysis of mitotic figures, and time lapse imaging of dividing NB cells were used to infer the most likely mechanism behind intratumour variation in chromosome number. Combined SNP array and FISH analyses showed that all cases exhibited higher inter-cellular copy number variation than non-neoplastic control tissue, with up to 75% of tumour cells showing non-modal chromosome copy numbers. Comparisons of copy number profiles, resulting from simulations of different segregation errors to genomic profiles of 120 NBs indicated that loss of chromosomes from a tetraploid state was more likely than other mechanisms to explain numerical aberrations in NB. This was supported by a high frequency of lagging chromosomes at anaphase and polyploidisation events in growing NB cells. The dynamic nature of numerical aberrations was corroborated further by detecting substantial copy number diversity in cell populations grown from single NB cells. We conclude that aneuploid NBs typically show extensive intratumour chromosome copy number diversity, and that this phenomenon is most likely explained by continuous loss of chromosomes from a polyploid state.
url https://www.ncbi.nlm.nih.gov/pmc/articles/pmid/23555645/?tool=EBI
work_keys_str_mv AT giselalundberg intratumourdiversityofchromosomecopynumbersinneuroblastomamediatedbyongoingchromosomelossfromapolyploidstate
AT yueshengjin intratumourdiversityofchromosomecopynumbersinneuroblastomamediatedbyongoingchromosomelossfromapolyploidstate
AT danielsehic intratumourdiversityofchromosomecopynumbersinneuroblastomamediatedbyongoingchromosomelossfromapolyploidstate
AT ingridøra intratumourdiversityofchromosomecopynumbersinneuroblastomamediatedbyongoingchromosomelossfromapolyploidstate
AT rogierversteeg intratumourdiversityofchromosomecopynumbersinneuroblastomamediatedbyongoingchromosomelossfromapolyploidstate
AT davidgisselsson intratumourdiversityofchromosomecopynumbersinneuroblastomamediatedbyongoingchromosomelossfromapolyploidstate
_version_ 1714811424558022656

Similar Items