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长链非编码RNA LINC01207促进肺腺癌的增殖。

The long noncoding RNA LINC01207 promotes proliferation of lung adenocarcinoma.

作者信息

Wang Gongchao, Chen Hongbo, Liu Jun

机构信息

Department of Surgery, School of Nursing, Shandong University Jinan 250012, China.

出版信息

Am J Cancer Res. 2015 Sep 15;5(10):3162-73. eCollection 2015.

Abstract

Lung adenocarcinoma (LAD) and lung squamous cell cancer (LSCC) are two most common histological types of lung cancer, while they differ in many aspects. Recent evidence shows that long non-coding RNAs (lncRNAs) play an important role in the process of cancer initiation and progression. Thus, characterization of LAD and LSCC associated lncRNAs may help understand the difference between LAD and LSCC. Here, we analyzed three sets of RNA-seq data, including LAD RNA-seq data from TCGA project. We identified a novel lncRNA, long intergenic non-protein coding RNA 1207 (LINC01207) which was significantly up-regulated in LAD tissues compared with paired non-tumor tissues (5.78 fold increase, P<0.05), while there was no significant differences between LSCC tissues and adjacent non-tumor tissues. The expression level of LINC01207 was associated with TNM stage of LAD patients, and higher LINC01207 level indicated advanced TNM stage (P<0.05) and shorter survival (HR=2.53, P<0.05). By small interfering RNA (siRNA) mediated knockdown of LINC01207, we determined the biological function of LINC01207 in A549 cell line. After knockdown of LINC01207, cell proliferation ability was inhibited. Further analysis showed that after silence of LINC01207, the percentage of apoptotic cells significantly increased. By RNA immunoprecipitation and Chromatin immunoprecipitation assay, we demonstrated that LINC01207 could bind with EZH2 and mediated trimethylation of histone 3 lysine 27 at the promoter region of Bad, an important pro-apoptotic gene. Finally, we developed xenograft tumor models in nude mice and xenograft tumors derived from A549 cells transfected with siRNA-LINC01207 had significantly lower tumor weight and smaller tumor volume. In summary, the novel lncRNA, LINC01207 is specifically up-regulated in LAD but not in LSCC; and LINC01207 could promote LAD cell growth both in vivo and in vitro.

摘要

肺腺癌(LAD)和肺鳞状细胞癌(LSCC)是肺癌两种最常见的组织学类型,然而它们在许多方面存在差异。最近的证据表明,长链非编码RNA(lncRNAs)在癌症发生和发展过程中发挥着重要作用。因此,对与LAD和LSCC相关的lncRNAs进行表征可能有助于理解LAD和LSCC之间的差异。在此,我们分析了三组RNA测序数据,包括来自TCGA项目的LAD RNA测序数据。我们鉴定出一种新型lncRNA,长链基因间非编码RNA 1207(LINC01207),与配对的非肿瘤组织相比,其在LAD组织中显著上调(增加5.78倍,P<0.05),而在LSCC组织和相邻非肿瘤组织之间没有显著差异。LINC01207的表达水平与LAD患者的TNM分期相关,LINC01207水平越高表明TNM分期越晚(P<0.05)且生存期越短(HR=2.53,P<0.05)。通过小干扰RNA(siRNA)介导的LINC01207敲低,我们确定了LINC01207在A549细胞系中的生物学功能。敲低LINC01207后,细胞增殖能力受到抑制。进一步分析表明,沉默LINC01207后,凋亡细胞的百分比显著增加。通过RNA免疫沉淀和染色质免疫沉淀试验,我们证明LINC01207可以与EZH2结合,并介导重要促凋亡基因Bad启动子区域组蛋白3赖氨酸27的三甲基化。最后,我们在裸鼠中建立了异种移植肿瘤模型,源自用siRNA-LINC01207转染的A549细胞的异种移植肿瘤的肿瘤重量显著降低,肿瘤体积更小。总之,新型lncRNA LINC01207在LAD中特异性上调,但在LSCC中未上调;并且LINC01207在体内和体外均可促进LAD细胞生长。

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