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Gene Expression Profiling of Breast Cancer Brain Metastasisopen access

Authors
Lee, Ji YunPark, KyungheeLee, EunjinAhn, TaeJinJung, Hae HyunLim, Sung HeeHong, MineuiDo, In-GuCho, Eun YoonKim, Duk-HwanKim, Ji-YeonAhn, Jin SeokIm, Young-HyuckPark, Yeon Hee
Issue Date
Jun-2016
Publisher
NATURE PUBLISHING GROUP
Citation
SCIENTIFIC REPORTS, v.6
Journal Title
SCIENTIFIC REPORTS
Volume
6
URI
https://scholarworks.bwise.kr/cau/handle/2019.sw.cau/69727
DOI
10.1038/srep28623
ISSN
2045-2322
Abstract
The biology of breast cancer brain metastasis (BCBM) is poorly understood. We aimed to explore genes that are implicated in the process of brain metastasis of primary breast cancer (BC). NanoString nCounter Analysis covering 252 target genes was used for comparison of gene expression levels between 20 primary BCs that relapsed to brain and 41 BCBM samples. PAM50-based intrinsic subtypes such as HER2-enriched and basal-like were clearly over-represented in BCBM. A panel of 22 genes was found to be significantly differentially expressed between primary BC and BCBM. Five of these genes, CXCL12, MMP2, MMP11, VCAM1, and MME, which have previously been associated with tumor progression, angiogenesis, and metastasis, clearly discriminated between primary BC and BCBM. Notably, the five genes were significantly upregulated in primary BC compared to BCBM. Conversely, SOX2 and OLIG2 genes were upregulated in BCBM. These genes may participate in metastatic colonization but not in primary tumor development. Among patient-matched paired samples (n = 17), a PAM50 molecular subtype conversion was observed in eight cases (47.1%), with a trend toward unfavorable subtypes in patients with the distinct gene expression. Our findings, although not conclusive, reveal differentially expressed genes that might mediate the brain metastasis process.
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