RNA-sequence-based microRNA expression signature in breast cancer: tumor-suppressive miR-101-5p regulates molecular pathogenesis.

IF 5 2区 医学 Q1 ONCOLOGY Molecular Oncology Pub Date : 2020-02-01 Epub Date: 2019-12-29 DOI:10.1002/1878-0261.12602
Hiroko Toda, Naohiko Seki, Sasagu Kurozumi, Yoshiaki Shinden, Yasutaka Yamada, Nijiro Nohata, Shogo Moriya, Tetsuya Idichi, Kosei Maemura, Takaaki Fujii, Jun Horiguchi, Yuko Kijima, Shoji Natsugoe
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Abstract

Aberrantly expressed microRNA (miRNA) are known to disrupt intracellular RNA networks in cancer cells. Exploring miRNA-dependent molecular networks is a major challenge in cancer research. In this study, we performed RNA-sequencing of breast cancer (BrCa) clinical specimens to identify tumor-suppressive miRNA in BrCa. In total, 64 miRNA were identified as candidate tumor-suppressive miRNA in BrCa cells. Analysis of our BrCa signature revealed that several miRNA duplexes (guide strand/passenger strand) derived from pre-miRNA were downregulated in BrCa tissues (e.g. miR-99a-5p/-3p, miR-101-5p/-3p, miR-126-5p/-3p, miR-143-5p/-3p, and miR-144-5p/-3p). Among these miRNA, we focused on miR-101-5p, the passenger strand of pre-miR-101, and investigated its tumor-suppressive roles and oncogenic targets in BrCa cells. Low expression of miR-101-5p predicted poor prognosis in patients with BrCa (overall survival rate: P = 0.0316). Ectopic expression of miR-101-5p attenuated aggressive phenotypes, e.g. proliferation, migration, and invasion, in BrCa cells. Finally, we identified seven putative oncogenic genes (i.e. High Mobility Group Box 3, Epithelial splicing regulatory protein 1, GINS complex subunit 1 (GINS1), Tumor Protein D52, Serine/Arginine-Rich Splicing Factor Kinase 1, Vang-like protein 1, and Mago Homolog B) regulated by miR-101-5p in BrCa cells. The expression of these target genes was associated with the molecular pathogenesis of BrCa. Furthermore, we explored the oncogenic roles of GINS1, whose function had not been previously elucidated, in BrCa cells. Aberrant expression of GINS1 mRNA and protein was observed in BrCa clinical specimens, and high GINS1 expression significantly predicted poor prognosis in patients with BrCa (overall survival rate: P = 0.0126). Knockdown of GINS1 inhibited the malignant features of BrCa cells. Thus, identification of tumor-suppressive miRNA and molecular networks controlled by these miRNA in BrCa cells may be an effective strategy for elucidation of the molecular pathogenesis of this disease.

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基于RNA序列的microRNA在乳腺癌中的表达特征:肿瘤抑制miR - 101 - 5p调控分子发病机制
已知异常表达的microRNA (miRNA)会破坏癌细胞的细胞内RNA网络。探索miRNA依赖的分子网络是癌症研究的主要挑战。在这项研究中,我们对乳腺癌(BrCa)临床标本进行了RNA测序,以鉴定BrCa中的肿瘤抑制miRNA。总共有64个miRNA在BrCa细胞中被鉴定为候选的肿瘤抑制miRNA。我们的BrCa特征分析显示,BrCa组织中源自前miRNA的几种miRNA双链(引导链/客链)下调(例如miR‐99a‐5p/‐3p、miR‐101‐5p/‐3p、miR‐126‐5p/‐3p、miR‐143‐5p/‐3p和miR‐144‐5p/‐3p)。在这些miRNA中,我们重点研究了miR - 101 - 5p, miR - 101 pre - 101的客运链,并研究了其在BrCa细胞中的肿瘤抑制作用和致癌靶点。miR - 101 - 5p低表达预示BrCa患者预后不良(总生存率:P = 0.0316)。miR - 101 - 5p的异位表达减弱了BrCa细胞的侵袭性表型,如增殖、迁移和侵袭。最后,我们确定了BrCa细胞中miR‐101‐5p调控的7个推定的致癌基因(即高迁移率组盒3、上皮剪接调节蛋白1、GINS复合体亚基1 (GINS1)、肿瘤蛋白D52、丝氨酸/精氨酸丰富剪接因子激酶1、Vang‐like蛋白1和Mago同源基因B)。这些靶基因的表达与BrCa的分子发病机制有关。此外,我们探索了GINS1在BrCa细胞中的致癌作用,其功能以前未被阐明。GINS1 mRNA和蛋白在BrCa临床标本中表达异常,GINS1高表达可显著预测BrCa患者预后不良(总生存率:P = 0.0126)。GINS1的敲低抑制了BrCa细胞的恶性特征。因此,在BrCa细胞中鉴定肿瘤抑制miRNA和由这些miRNA控制的分子网络可能是阐明该疾病分子发病机制的有效策略。
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来源期刊
Molecular Oncology
Molecular Oncology 医学-肿瘤学
CiteScore
12.60
自引率
1.50%
发文量
203
审稿时长
6-12 weeks
期刊介绍: Molecular Oncology highlights new discoveries, approaches, and technical developments, in basic, clinical and discovery-driven translational cancer research. It publishes research articles, reviews (by invitation only), and timely science policy articles. The journal is now fully Open Access with all articles published over the past 10 years freely available.
期刊最新文献
Hypoxia-induced miR-210-3p expression in lung adenocarcinoma potentiates tumor development by regulating CCL2 mediated monocyte infiltration. Kinase activities in pancreatic ductal adenocarcinoma with prognostic and therapeutic avenues. Issue Information Issue Information Issue Information
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