Proliferation-associated long noncoding RNA,TMPO-AS1, is a potential therapeutic target for triple-negative breast cancer

被引:30
|
作者
Mitobe, Yuichi [1 ]
Ikeda, Kazuhiro [1 ]
Sato, Wataru [1 ]
Kodama, Yukinobu [2 ]
Naito, Mitsuru [3 ]
Gotoh, Noriko [4 ]
Miyata, Kanjiro [5 ]
Kataoka, Kazunori [6 ,7 ]
Sasaki, Hitoshi [2 ]
Horie-Inoue, Kuniko [1 ]
Inoue, Satoshi [1 ,8 ]
机构
[1] Saitama Med Univ, Res Ctr Genom Med, Div Gene Regulat & Signal Transduct, Saitama, Japan
[2] Nagasaki Univ Hosp, Dept Hosp Pharm, Nagasaki, Japan
[3] Univ Tokyo, Ctr Dis Biol & Integrat Med, Grad Sch Med, Tokyo, Japan
[4] Kanazawa Univ, Canc Res Inst, Div Canc Cell Biol, Kanazawa, Ishikawa, Japan
[5] Univ Tokyo, Grad Sch Engn, Dept Mat Engn, Tokyo, Japan
[6] Univ Tokyo, Inst Future Initiat, Tokyo, Japan
[7] Kawasaki Inst Ind Promot, Innovat Ctr Nanomed, Kawasaki, Kanagawa, Japan
[8] Tokyo Metropolitan Inst Gerontol, Dept Syst Aging Sci & Med, Tokyo, Japan
基金
日本学术振兴会;
关键词
breast cancer; DDS; lncRNA; TMPO-AS1; TNBC; POLY-L-LYSINE; OPEN PLATFORM; BETA; RNA; EXPRESSION; SIRNA; DELIVERY; CELLS; MICELLES; DISEASE;
D O I
10.1111/cas.14498
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Triple-negative breast cancer (TNBC) is an aggressive subtype of breast cancer compared with luminal or epidermal growth factor receptor 2 subtypes, thus effective therapeutic options for TNBC are yet to be developed. Nowadays, oncogenic long noncoding RNAs (lncRNAs) are applied to cancer management as a new class of therapeutic targets. We previously showed that thymopoietin antisense transcript 1 (TMPO-AS1) is a proliferation-associated lncRNA that contributes to hormone-dependent breast cancer progression by stabilizing estrogen receptor-alpha mRNA. We here showed thatTMPO-AS1is abundantly expressed in basal-like breast cancer subtype based on the transcriptomic data in The Cancer Genome Atlas as well as in TNBC cell lines and patient-derived cells. Small interfering RNA-based loss-of-function analyses showed thatTMPO-AS1knockdown substantially represses the proliferation and migration of TNBC cells. Expression microarray analysis showed thatTMPO-AS1alters gene signatures related to transforming growth factor-beta signaling in addition to proliferative E2F signaling pathways.TMPO-AS1-targeted siRNA treatment through engineered drug delivery systems using cancer-targeted polyion complex micelle or nanoball technology significantly impaired the in vivo growth of primary and metastatic TNBC xenograft tumors. Our findings suggest thatTMPO-AS1plays a key role in TNBC pathophysiology and could be a potential therapeutic target for TNBC.
引用
收藏
页码:2440 / 2450
页数:11
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