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Subtype-specific CpG island shore methylation and mutation patterns in 30 breast cancer cell lines

Authors
Chae, HeejoonLee, SangseonNephew, Kenneth P.Kim, Sun
Issue Date
Dec-2016
Publisher
BMC
Keywords
Breast cancer; Subtype; DNA methylation; CpGI shore; Mutation
Citation
BMC SYSTEMS BIOLOGY, v.10, pp 433 - 443
Pages
11
Journal Title
BMC SYSTEMS BIOLOGY
Volume
10
Start Page
433
End Page
443
URI
https://scholarworks.sookmyung.ac.kr/handle/2020.sw.sookmyung/3144
DOI
10.1186/s12918-016-0356-2
ISSN
1752-0509
1752-0509
Abstract
Background: Aberrant epigenetic modifications, including DNA methylation, are key regulators of gene activity in tumorigenesis. Breast cancer is a heterogeneous disease, and large-scale analyses indicate that tumor from normal and benign tissues, as well as molecular subtypes of breast cancer, can be distinguished based on their distinct genomic, transcriptomic, and epigenomic profiles. In this study, we used affinity-based methylation sequencing data in 30 breast cancer cell lines representing functionally distinct cancer subtypes to investigate methylation and mutation patterns at the whole genome level. Results: Our analysis revealed significant differences in CpG island (CpGI) shore methylation and mutation patterns among breast cancer subtypes. In particular, the basal-like B type, a highly aggressive form of the disease, displayed distinct CpGI shore hypomethylation patterns that were significantly associated with downstream gene regulation. We determined that mutation rates at CpG sites were highly correlated with DNA methylation status and observed distinct mutation rates among the breast cancer subtypes. These findings were validated by using targeted bisulfite sequencing of differentially expressed genes (n=85) among the cell lines. Conclusions: Our results suggest that alterations in DNA methylation play critical roles in gene regulatory process as well as cytosine substitution rates at CpG sites in molecular subtypes of breast cancer. © 2016 The Author(s).
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공과대학 (소프트웨어학부(첨단))
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