Please use this identifier to cite or link to this item: https://doi.org/10.1038/s41523-018-0070-x
Title: Elucidating therapeutic molecular targets in premenopausal Asian women with recurrent breast cancers
Authors: Yap, Y.-S
Singh, A.P
Lim, J.H.C
Ahn, J.-H
Jung, K.-H
Kim, J
Dent, R.A 
Ng, R.C.H 
Kim, S.-B
Chiang, D.Y
Keywords: BRCA1 associated ring domain protein 1
cyclin D1
cyclin dependent kinase inhibitor 1B
epidermal growth factor receptor 2
hormone receptor
hypoxia inducible factor 1alpha
MutL protein homolog 1
Myc protein
protein kinase LKB1
protein mcl 1
protein MDMX
protein p53
tetratricopeptide repeat protein
transcription factor GATA 3
adult
Article
Asian
breast cancer
BRIP1 gene
cancer recurrence
CCND1 gene
CDKN1B gene
cell cycle
cohort analysis
controlled study
ERBB2 gene
female
GATA3 gene
gene amplification
gene frequency
gene mutation
human
human epidermal growth factor receptor 2 positive breast cancer
KMT2C gene
KMT2D gene
major clinical study
MCL1 gene
MDM4 gene
MLH1 gene
molecular biology
oncogene c myc
overall survival
PCDH15 gene
PIK3CA gene
prediction
premenopause
prevalence
priority journal
PRKAR1A gene
PRKDC gene
signal transduction
STK11 gene
TPR gene
tumor suppressor gene
Issue Date: 2018
Citation: Yap, Y.-S, Singh, A.P, Lim, J.H.C, Ahn, J.-H, Jung, K.-H, Kim, J, Dent, R.A, Ng, R.C.H, Kim, S.-B, Chiang, D.Y (2018). Elucidating therapeutic molecular targets in premenopausal Asian women with recurrent breast cancers. npj Breast Cancer 4 (1) : 19. ScholarBank@NUS Repository. https://doi.org/10.1038/s41523-018-0070-x
Rights: Attribution 4.0 International
Abstract: Breast cancer is an increasing problem in Asia, with a higher proportion of premenopausal patients who are at higher risk of recurrence. Targeted sequencing was performed on DNA extracted from primary tumor specimens of 63 premenopausal Asian patients who relapsed after initial diagnosis of non-metastatic breast cancer. The most prevalent alterations included: TP53 (65%); PIK3CA (32%); GATA3 (29%); ERBB2 (27%); MYC (25%); KMT2C (21%); MCL1 (17%); PRKDC, TPR, BRIP1 (14%); MDM4, PCDH15, PRKAR1A, CDKN1B (13%); CCND1, KMT2D, STK11, and MLH1 (11%). Sixty of the 63 patients (95%) had at least one genetic alteration in a signaling pathway related to cell cycle or p53 signaling. The presence of MCL1 amplification, HIF-1-alpha transcription factor network pathway alterations, and direct p53 effectors pathway alterations were independent predictors of inferior overall survival from initial diagnosis. Comparison with non-Asian premenopausal tumors in The Cancer Genome Atlas (TCGA) revealed a higher prevalence of TP53 mutations among HER2-positive cancers, and more frequent TP53, TET2, and CDK12 mutations among hormone receptor-positive HER2-negative cancers in our cohort. Given the limited number of non-Asian premenopausal breast cancers that had relapsed in TCGA, we compared the frequency of mutations in our cohort with 43 premenopausal specimens from both TCGA and International Cancer Genome Consortium that had relapsed. There was a trend toward higher prevalence of TP53 mutations in our cohort. Certain genomic aberrations may be enriched in tumors of poor-prognosis premenopausal Asian breast cancers. The development of novel therapies targeting these aberrations merit further research. © 2018, The Author(s).
Source Title: npj Breast Cancer
URI: https://scholarbank.nus.edu.sg/handle/10635/182065
ISSN: 23744677
DOI: 10.1038/s41523-018-0070-x
Rights: Attribution 4.0 International
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