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miR-374a-5p promotes tumor progression by targeting ARRB1 in triple negative breast cancer

Authors
Son, DasomKim, YesolLim, SeraKang, Hyeok-GuKim, Da-HyunPark, Jee WonCheong, WoosungKong, Hyun KyungHan, WonshikPark, Woong-YangChun, Kyung-HeePark, Jong Hoon
Issue Date
Jul-2019
Publisher
ELSEVIER IRELAND LTD
Keywords
miR-374a-5p; Triple negative breast cancer; Arrestin beta 1; AMPK alpha
Citation
CANCER LETTERS, v.454, pp 224 - 233
Pages
10
Journal Title
CANCER LETTERS
Volume
454
Start Page
224
End Page
233
URI
https://scholarworks.sookmyung.ac.kr/handle/2020.sw.sookmyung/2958
DOI
10.1016/j.canlet.2019.04.006
ISSN
0304-3835
1872-7980
Abstract
Triple negative breast cancer (TNBC) has higher aggressiveness and poorer outcomes compared with other subtypes of breast cancer. However, the genomic and molecular aberrations of TNBC are largely unknown. In this study, miR-374a-5p was discovered as a novel TNBC-specific miRNA and its functions and the molecular mechanisms involved were investigated. Combined gene expression profiling of miRNA-microarray and human transcriptome dataset analysis revealed that miR-374a-5p is specifically upregulated in TNBC patients. Functional studies using in vitro and in vivo models indicated that upregulated miR-374a-5p promotes tumor progression in TNBC. miR-374a-5p was also found to directly target arrestin beta 1 (ARRB1) that is specifically downregulated in TNBC patients in several human genomic datasets. Overexpressed ARRB1 reduced TNBC cell growth and migration, and the ARRB1 expression level is inversely correlated with the histological grade of the breast cancer and positively associated with TNBC patient survival, suggestive of a tumor-suppressive function of ARRB1 in breast cancer. Interestingly, increased ARRB1 activates AMPK in TNBC cells, associated with the expression of miR-374a-5p. Taken together, the findings suggest that miR-374a-5p is a potential prognostic marker of TNBC.
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