| Literature DB >> 30720865 |
Wei Sun1,2,3, Xiaoen Xu1,2,3, Yizhou Jiang1,2,3, Xi Jin1,2,3, Ping Zhou4, Yirong Liu1,2,3, Yajie Guo1,2,3, Ding Ma1,2,3, Wenjia Zuo1,2,3, Shenglin Huang3,5, Xianghuo He3,5, Zhiming Shao1,2,3,6.
Abstract
Luminal breast cancer (BC) has a sustained risk of late disease recurrence and death. Considerable numbers of patients suffer from antiendocrine therapy resistance. Here, we identified a novel lncRNA whose expression is high in breast cancer and especially higher in luminal breast cancer, dubbed LOL (lncRNA of luminal), that acts as a natural sponge for let-7 microRNAs to regulate tumor growth and tamoxifen resistance. LOL overexpression in parental MCF-7 cells exhibited a proliferative advantage in the addition of tamoxifen than negative control. Knocking down LOL in TamR MCF-7 cells, recovered the sensitivity of cells to tamoxifen. Strikingly, we demonstrated that LOL is transcribed from a genomic locus of an enhancer to maintain its high expression in luminal BC and that it is extremely sensitive to enhancer-regulating factors, such as ZMYND8 and BRD4. Estrogen deprivation or ERα signaling pathway blockage can further stimulate LOL expression, which can promote tumor progression. Clinical analysis of 374 luminal breast cancer samples indicated that LOL is an independent prognostic factor for poor survival in luminal BC. In conclusion, targeting LOL using preclinical/clinical drugs, such as BRD4 inhibitors, may represent a promising approach to inhibit luminal breast cancer progression and tamoxifen resistance.Entities:
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Year: 2019 PMID: 30720865 DOI: 10.1002/ijc.32185
Source DB: PubMed Journal: Int J Cancer ISSN: 0020-7136 Impact factor: 7.396