Genome-Wide Analysis of Interchromosomal Interaction Probabilities Reveals Chained Translocations and Overrepresentation of Translocation Breakpoints in Genes in a Cutaneous T-Cell Lymphoma Cell Line

In classical models of tumorigenesis, the accumulation of tumor promoting chromosomal aberrations is described as a gradual process. Next-generation sequencing-based methods have recently revealed complex patterns of chromosomal aberrations, which are beyond explanation by these classical models of...

Descripción completa

Detalles Bibliográficos
Autores principales: Steininger, Anne, Ebert, Grit, Becker, Benjamin V., Assaf, Chalid, Möbs, Markus, Schmidt, Christian A., Grabarczyk, Piotr, Jensen, Lars R., Przybylski, Grzegorz K., Port, Matthias, Kuss, Andreas W., Ullmann, Reinhard
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2018
Materias:
Oncology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5988852/
https://www.ncbi.nlm.nih.gov/pubmed/29900125
http://dx.doi.org/10.3389/fonc.2018.00183
_version_ 1783329363055345664
author Steininger, Anne
Ebert, Grit
Becker, Benjamin V.
Assaf, Chalid
Möbs, Markus
Schmidt, Christian A.
Grabarczyk, Piotr
Jensen, Lars R.
Przybylski, Grzegorz K.
Port, Matthias
Kuss, Andreas W.
Ullmann, Reinhard
author_facet Steininger, Anne
Ebert, Grit
Becker, Benjamin V.
Assaf, Chalid
Möbs, Markus
Schmidt, Christian A.
Grabarczyk, Piotr
Jensen, Lars R.
Przybylski, Grzegorz K.
Port, Matthias
Kuss, Andreas W.
Ullmann, Reinhard
author_sort Steininger, Anne
collection PubMed
description In classical models of tumorigenesis, the accumulation of tumor promoting chromosomal aberrations is described as a gradual process. Next-generation sequencing-based methods have recently revealed complex patterns of chromosomal aberrations, which are beyond explanation by these classical models of karyotypic evolution of tumor genomes. Thus, the term chromothripsis has been introduced to describe a phenomenon, where temporarily and spatially confined genomic instability results in dramatic chromosomal rearrangements limited to segments of one or a few chromosomes. Simultaneously arising and misrepaired DNA double-strand breaks are also the cause of another phenomenon called chromoplexy, which is characterized by the presence of chained translocations and interlinking deletion bridges involving several chromosomes. In this study, we demonstrate the genome-wide identification of chromosomal translocations based on the analysis of translocation-associated changes in spatial proximities of chromosome territories on the example of the cutaneous T-cell lymphoma cell line Se-Ax. We have used alterations of intra- and interchromosomal interaction probabilities as detected by genome-wide chromosome conformation capture (Hi-C) to infer the presence of translocations and to fine-map their breakpoints. The outcome of this analysis was subsequently compared to datasets on DNA copy number alterations and gene expression. The presence of chained translocations within the Se-Ax genome, partly connected by intervening deletion bridges, indicates a role of chromoplexy in the etiology of this cutaneous T-cell lymphoma. Notably, translocation breakpoints were significantly overrepresented in genes, which highlight gene-associated biological processes like transcription or other gene characteristics as a possible cause of the observed complex rearrangements. Given the relevance of chromosomal aberrations for basic and translational research, genome-wide high-resolution analysis of structural chromosomal aberrations will gain increasing importance.
format Online
Article
Text
id pubmed-5988852
institution National Center for Biotechnology Information
language English
publishDate 2018
publisher Frontiers Media S.A.
record_format MEDLINE/PubMed
spelling pubmed-59888522018-06-13 Genome-Wide Analysis of Interchromosomal Interaction Probabilities Reveals Chained Translocations and Overrepresentation of Translocation Breakpoints in Genes in a Cutaneous T-Cell Lymphoma Cell Line Steininger, Anne Ebert, Grit Becker, Benjamin V. Assaf, Chalid Möbs, Markus Schmidt, Christian A. Grabarczyk, Piotr Jensen, Lars R. Przybylski, Grzegorz K. Port, Matthias Kuss, Andreas W. Ullmann, Reinhard Front Oncol Oncology In classical models of tumorigenesis, the accumulation of tumor promoting chromosomal aberrations is described as a gradual process. Next-generation sequencing-based methods have recently revealed complex patterns of chromosomal aberrations, which are beyond explanation by these classical models of karyotypic evolution of tumor genomes. Thus, the term chromothripsis has been introduced to describe a phenomenon, where temporarily and spatially confined genomic instability results in dramatic chromosomal rearrangements limited to segments of one or a few chromosomes. Simultaneously arising and misrepaired DNA double-strand breaks are also the cause of another phenomenon called chromoplexy, which is characterized by the presence of chained translocations and interlinking deletion bridges involving several chromosomes. In this study, we demonstrate the genome-wide identification of chromosomal translocations based on the analysis of translocation-associated changes in spatial proximities of chromosome territories on the example of the cutaneous T-cell lymphoma cell line Se-Ax. We have used alterations of intra- and interchromosomal interaction probabilities as detected by genome-wide chromosome conformation capture (Hi-C) to infer the presence of translocations and to fine-map their breakpoints. The outcome of this analysis was subsequently compared to datasets on DNA copy number alterations and gene expression. The presence of chained translocations within the Se-Ax genome, partly connected by intervening deletion bridges, indicates a role of chromoplexy in the etiology of this cutaneous T-cell lymphoma. Notably, translocation breakpoints were significantly overrepresented in genes, which highlight gene-associated biological processes like transcription or other gene characteristics as a possible cause of the observed complex rearrangements. Given the relevance of chromosomal aberrations for basic and translational research, genome-wide high-resolution analysis of structural chromosomal aberrations will gain increasing importance. Frontiers Media S.A. 2018-05-30 /pmc/articles/PMC5988852/ /pubmed/29900125 http://dx.doi.org/10.3389/fonc.2018.00183 Text en Copyright © 2018 Steininger, Ebert, Becker, Assaf, Möbs, Schmidt, Grabarczyk, Jensen, Przybylski, Port, Kuss and Ullmann. https://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Oncology
Steininger, Anne
Ebert, Grit
Becker, Benjamin V.
Assaf, Chalid
Möbs, Markus
Schmidt, Christian A.
Grabarczyk, Piotr
Jensen, Lars R.
Przybylski, Grzegorz K.
Port, Matthias
Kuss, Andreas W.
Ullmann, Reinhard
Genome-Wide Analysis of Interchromosomal Interaction Probabilities Reveals Chained Translocations and Overrepresentation of Translocation Breakpoints in Genes in a Cutaneous T-Cell Lymphoma Cell Line
title Genome-Wide Analysis of Interchromosomal Interaction Probabilities Reveals Chained Translocations and Overrepresentation of Translocation Breakpoints in Genes in a Cutaneous T-Cell Lymphoma Cell Line
title_full Genome-Wide Analysis of Interchromosomal Interaction Probabilities Reveals Chained Translocations and Overrepresentation of Translocation Breakpoints in Genes in a Cutaneous T-Cell Lymphoma Cell Line
title_fullStr Genome-Wide Analysis of Interchromosomal Interaction Probabilities Reveals Chained Translocations and Overrepresentation of Translocation Breakpoints in Genes in a Cutaneous T-Cell Lymphoma Cell Line
title_full_unstemmed Genome-Wide Analysis of Interchromosomal Interaction Probabilities Reveals Chained Translocations and Overrepresentation of Translocation Breakpoints in Genes in a Cutaneous T-Cell Lymphoma Cell Line
title_short Genome-Wide Analysis of Interchromosomal Interaction Probabilities Reveals Chained Translocations and Overrepresentation of Translocation Breakpoints in Genes in a Cutaneous T-Cell Lymphoma Cell Line
title_sort genome-wide analysis of interchromosomal interaction probabilities reveals chained translocations and overrepresentation of translocation breakpoints in genes in a cutaneous t-cell lymphoma cell line
topic Oncology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5988852/
https://www.ncbi.nlm.nih.gov/pubmed/29900125
http://dx.doi.org/10.3389/fonc.2018.00183
work_keys_str_mv AT steiningeranne genomewideanalysisofinterchromosomalinteractionprobabilitiesrevealschainedtranslocationsandoverrepresentationoftranslocationbreakpointsingenesinacutaneoustcelllymphomacellline
AT ebertgrit genomewideanalysisofinterchromosomalinteractionprobabilitiesrevealschainedtranslocationsandoverrepresentationoftranslocationbreakpointsingenesinacutaneoustcelllymphomacellline
AT beckerbenjaminv genomewideanalysisofinterchromosomalinteractionprobabilitiesrevealschainedtranslocationsandoverrepresentationoftranslocationbreakpointsingenesinacutaneoustcelllymphomacellline
AT assafchalid genomewideanalysisofinterchromosomalinteractionprobabilitiesrevealschainedtranslocationsandoverrepresentationoftranslocationbreakpointsingenesinacutaneoustcelllymphomacellline
AT mobsmarkus genomewideanalysisofinterchromosomalinteractionprobabilitiesrevealschainedtranslocationsandoverrepresentationoftranslocationbreakpointsingenesinacutaneoustcelllymphomacellline
AT schmidtchristiana genomewideanalysisofinterchromosomalinteractionprobabilitiesrevealschainedtranslocationsandoverrepresentationoftranslocationbreakpointsingenesinacutaneoustcelllymphomacellline
AT grabarczykpiotr genomewideanalysisofinterchromosomalinteractionprobabilitiesrevealschainedtranslocationsandoverrepresentationoftranslocationbreakpointsingenesinacutaneoustcelllymphomacellline
AT jensenlarsr genomewideanalysisofinterchromosomalinteractionprobabilitiesrevealschainedtranslocationsandoverrepresentationoftranslocationbreakpointsingenesinacutaneoustcelllymphomacellline
AT przybylskigrzegorzk genomewideanalysisofinterchromosomalinteractionprobabilitiesrevealschainedtranslocationsandoverrepresentationoftranslocationbreakpointsingenesinacutaneoustcelllymphomacellline
AT portmatthias genomewideanalysisofinterchromosomalinteractionprobabilitiesrevealschainedtranslocationsandoverrepresentationoftranslocationbreakpointsingenesinacutaneoustcelllymphomacellline
AT kussandreasw genomewideanalysisofinterchromosomalinteractionprobabilitiesrevealschainedtranslocationsandoverrepresentationoftranslocationbreakpointsingenesinacutaneoustcelllymphomacellline
AT ullmannreinhard genomewideanalysisofinterchromosomalinteractionprobabilitiesrevealschainedtranslocationsandoverrepresentationoftranslocationbreakpointsingenesinacutaneoustcelllymphomacellline

Ejemplares similares