Major Chromosomal Breakpoint Intervals in Breast Cancer Co-Localize with Differentially Methylated Regions

Solid tumors exhibit chromosomal rearrangements resulting in gain or loss of multiple chromosomal loci (copy number variation, or CNV), and translocations that occasionally result in the creation of novel chimeric genes. In the case of breast cancer, although most individual tumors each have unique...

Descripción completa

Detalles Bibliográficos
Autores principales: Eric Tang, Man-Hung, Varadan, Vinay, Kamalakaran, Sitharthan, Zhang, Michael Q., Dimitrova, Nevenka, Hicks, James
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2012
Materias:
Oncology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3530719/
https://www.ncbi.nlm.nih.gov/pubmed/23293768
http://dx.doi.org/10.3389/fonc.2012.00197
_version_ 1782254053968838656
author Eric Tang, Man-Hung
Varadan, Vinay
Kamalakaran, Sitharthan
Zhang, Michael Q.
Dimitrova, Nevenka
Hicks, James
author_facet Eric Tang, Man-Hung
Varadan, Vinay
Kamalakaran, Sitharthan
Zhang, Michael Q.
Dimitrova, Nevenka
Hicks, James
author_sort Eric Tang, Man-Hung
collection PubMed
description Solid tumors exhibit chromosomal rearrangements resulting in gain or loss of multiple chromosomal loci (copy number variation, or CNV), and translocations that occasionally result in the creation of novel chimeric genes. In the case of breast cancer, although most individual tumors each have unique CNV landscape, the breakpoints, as measured over large datasets, appear to be non-randomly distributed in the genome. Breakpoints show a significant regional concentration at genomic loci spanning perhaps several megabases. The proximal cause of these breakpoint concentrations is a subject of speculation, but is, as yet, largely unknown. To shed light on this issue, we have performed a bio-statistical analysis on our previously published data for a set of 119 breast tumors and normal controls (Wiedswang et al., 2003), where each sample has both high-resolution CNV and methylation data. The method examined the distribution of closeness of breakpoint regions with differentially methylated regions (DMR), coupled with additional genomic parameters, such as repeat elements and designated “fragile sites” in the reference genome. Through this analysis, we have identified a set of 93 regional loci called breakpoint enriched DMR (BEDMRs) characterized by altered DNA methylation in cancer compared to normal cells that are associated with frequent breakpoint concentrations within a distance of 1 Mb. BEDMR loci are further associated with local hypomethylation (66%), concentrations of the Alu SINE repeats within 3 Mb (35% of the cases), and tend to occur near a number of cancer related genes such as the protocadherins, AKT1, DUB3, GAB2. Furthermore, BEDMRs seem to deregulate members of the histone gene family and chromatin remodeling factors, e.g., JMJD1B, which might affect the chromatin structure and disrupt coordinate signaling and repair. From this analysis we propose that preference for chromosomal breakpoints is related to genome structure coupled with alterations in DNA methylation and hence, chromatin structure, associated with tumorigenesis.
format Online
Article
Text
id pubmed-3530719
institution National Center for Biotechnology Information
language English
publishDate 2012
publisher Frontiers Media S.A.
record_format MEDLINE/PubMed
spelling pubmed-35307192013-01-04 Major Chromosomal Breakpoint Intervals in Breast Cancer Co-Localize with Differentially Methylated Regions Eric Tang, Man-Hung Varadan, Vinay Kamalakaran, Sitharthan Zhang, Michael Q. Dimitrova, Nevenka Hicks, James Front Oncol Oncology Solid tumors exhibit chromosomal rearrangements resulting in gain or loss of multiple chromosomal loci (copy number variation, or CNV), and translocations that occasionally result in the creation of novel chimeric genes. In the case of breast cancer, although most individual tumors each have unique CNV landscape, the breakpoints, as measured over large datasets, appear to be non-randomly distributed in the genome. Breakpoints show a significant regional concentration at genomic loci spanning perhaps several megabases. The proximal cause of these breakpoint concentrations is a subject of speculation, but is, as yet, largely unknown. To shed light on this issue, we have performed a bio-statistical analysis on our previously published data for a set of 119 breast tumors and normal controls (Wiedswang et al., 2003), where each sample has both high-resolution CNV and methylation data. The method examined the distribution of closeness of breakpoint regions with differentially methylated regions (DMR), coupled with additional genomic parameters, such as repeat elements and designated “fragile sites” in the reference genome. Through this analysis, we have identified a set of 93 regional loci called breakpoint enriched DMR (BEDMRs) characterized by altered DNA methylation in cancer compared to normal cells that are associated with frequent breakpoint concentrations within a distance of 1 Mb. BEDMR loci are further associated with local hypomethylation (66%), concentrations of the Alu SINE repeats within 3 Mb (35% of the cases), and tend to occur near a number of cancer related genes such as the protocadherins, AKT1, DUB3, GAB2. Furthermore, BEDMRs seem to deregulate members of the histone gene family and chromatin remodeling factors, e.g., JMJD1B, which might affect the chromatin structure and disrupt coordinate signaling and repair. From this analysis we propose that preference for chromosomal breakpoints is related to genome structure coupled with alterations in DNA methylation and hence, chromatin structure, associated with tumorigenesis. Frontiers Media S.A. 2012-12-27 /pmc/articles/PMC3530719/ /pubmed/23293768 http://dx.doi.org/10.3389/fonc.2012.00197 Text en Copyright © 2012 Tang, Varadan, Kamalakaran, Zhang, Dimitrova and Hicks. http://creativecommons.org/licenses/by/3.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits use, distribution and reproduction in other forums, provided the original authors and source are credited and subject to any copyright notices concerning any third-party graphics etc.
spellingShingle Oncology
Eric Tang, Man-Hung
Varadan, Vinay
Kamalakaran, Sitharthan
Zhang, Michael Q.
Dimitrova, Nevenka
Hicks, James
Major Chromosomal Breakpoint Intervals in Breast Cancer Co-Localize with Differentially Methylated Regions
title Major Chromosomal Breakpoint Intervals in Breast Cancer Co-Localize with Differentially Methylated Regions
title_full Major Chromosomal Breakpoint Intervals in Breast Cancer Co-Localize with Differentially Methylated Regions
title_fullStr Major Chromosomal Breakpoint Intervals in Breast Cancer Co-Localize with Differentially Methylated Regions
title_full_unstemmed Major Chromosomal Breakpoint Intervals in Breast Cancer Co-Localize with Differentially Methylated Regions
title_short Major Chromosomal Breakpoint Intervals in Breast Cancer Co-Localize with Differentially Methylated Regions
title_sort major chromosomal breakpoint intervals in breast cancer co-localize with differentially methylated regions
topic Oncology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3530719/
https://www.ncbi.nlm.nih.gov/pubmed/23293768
http://dx.doi.org/10.3389/fonc.2012.00197
work_keys_str_mv AT erictangmanhung majorchromosomalbreakpointintervalsinbreastcancercolocalizewithdifferentiallymethylatedregions
AT varadanvinay majorchromosomalbreakpointintervalsinbreastcancercolocalizewithdifferentiallymethylatedregions
AT kamalakaransitharthan majorchromosomalbreakpointintervalsinbreastcancercolocalizewithdifferentiallymethylatedregions
AT zhangmichaelq majorchromosomalbreakpointintervalsinbreastcancercolocalizewithdifferentiallymethylatedregions
AT dimitrovanevenka majorchromosomalbreakpointintervalsinbreastcancercolocalizewithdifferentiallymethylatedregions
AT hicksjames majorchromosomalbreakpointintervalsinbreastcancercolocalizewithdifferentiallymethylatedregions

Ejemplares similares