miR-342 的下调与他莫昔芬耐药的乳腺癌肿瘤有关。
Downregulation of miR-342 is associated with tamoxifen resistant breast tumors.
机构信息
Department of Pathology, University of Colorado Denver, School of Medicine, Aurora, Colorado 80045, USA.
出版信息
Mol Cancer. 2010 Dec 20;9:317. doi: 10.1186/1476-4598-9-317.
BACKGROUND
Tumor resistance to the selective estrogen receptor modulator tamoxifen remains a serious clinical problem especially in patients with tumors that also overexpress HER2. We have recently demonstrated that the clinically important isoform of HER2, HERΔ16, promotes therapeutically refractory breast cancer including resistance to endocrine therapy. Likewise additional breast tumor cell models of tamoxifen resistance have been developed that do not involve HER2 overexpression. However, a unifying molecular mechanism of tamoxifen resistance has remained elusive.
RESULTS
Here we analyzed multiple cell models of tamoxifen resistance derived from MCF-7 cells to examine the influence of microRNAs (miRNAs) on tamoxifen resistance. We compared miRNA expression profiles of tamoxifen sensitive MCF-7 cells and tamoxifen resistant MCF-7/HER2Δ16 cells. We observed significant and dramatic downregulation of miR-342 in the MCF-7/HER2Δ16 cell line as well as the HER2 negative but tamoxifen resistant MCF-7 variants TAMR1 and LCC2. Restoring miR-342 expression in the MCF-7/HER2Δ16 and TAMR1 cell lines sensitized these cells to tamoxifen-induced apoptosis with a dramatic reduction in cell growth. Expression of miR-342 was also reduced in a panel of tamoxifen refractory human breast tumors, underscoring the potential clinical importance of miR-342 downregulation. Towards the goal of identifying direct and indirect targets of miR-342 we restored miR-342 expression in MCF-7/HER2Δ16 cells and analyzed changes in global gene expression by microarray. The impact of miR-342 on gene expression in MCF-7/HER2Δ16 cells was not limited to miR-342 in silica predicted targets. Ingenuity Pathways Analysis of the dataset revealed a significant influence of miR-342 on multiple tumor cell cycle regulators.
CONCLUSIONS
Our findings suggest that miR-342 regulates tamoxifen response in breast tumor cell lines and our clinical data indicates a trend towards reduced miR-342 expression and tamoxifen resistance. In addition, our results suggest that miR-342 regulates expression of genes involved in tamoxifen mediated tumor cell apoptosis and cell cycle progression. Restoring miR-342 expression may represent a novel therapeutic approach to sensitizing and suppressing the growth of tamoxifen refractory breast tumors.
背景
肿瘤对选择性雌激素受体调节剂他莫昔芬的耐药性仍然是一个严重的临床问题,尤其是在肿瘤同时过表达 HER2 的患者中。我们最近证明,HER2 的临床重要同工型 HERΔ16 促进了治疗上难治性乳腺癌,包括对内分泌治疗的耐药性。同样,已经开发出了其他不涉及 HER2 过表达的他莫昔芬耐药性的乳腺癌细胞模型。然而,他莫昔芬耐药性的统一分子机制仍然难以捉摸。
结果
在这里,我们分析了来自 MCF-7 细胞的多种他莫昔芬耐药细胞模型,以研究 microRNAs(miRNAs)对他莫昔芬耐药性的影响。我们比较了他莫昔芬敏感的 MCF-7 细胞和他莫昔芬耐药的 MCF-7/HER2Δ16 细胞的 miRNA 表达谱。我们观察到 miR-342 在 MCF-7/HER2Δ16 细胞系以及 HER2 阴性但他莫昔芬耐药的 MCF-7 变体 TAMR1 和 LCC2 中显著而显著地下调。在 MCF-7/HER2Δ16 和 TAMR1 细胞系中恢复 miR-342 的表达使这些细胞对他莫昔芬诱导的细胞凋亡敏感,细胞生长显著减少。miR-342 的表达在一组他莫昔芬耐药的人类乳腺癌肿瘤中也降低,强调了 miR-342 下调的潜在临床重要性。为了确定 miR-342 的直接和间接靶标,我们在 MCF-7/HER2Δ16 细胞中恢复了 miR-342 的表达,并通过微阵列分析了全局基因表达的变化。miR-342 对 MCF-7/HER2Δ16 细胞中基因表达的影响不仅限于 miR-342 在硅中的预测靶标。数据集的 Ingenuity 通路分析显示,miR-342 对多个肿瘤细胞周期调节剂有显著影响。
结论
我们的研究结果表明,miR-342 调节乳腺癌细胞系中他莫昔芬的反应,我们的临床数据表明 miR-342 表达降低与他莫昔芬耐药性之间存在趋势。此外,我们的结果表明,miR-342 调节参与他莫昔芬介导的肿瘤细胞凋亡和细胞周期进程的基因的表达。恢复 miR-342 的表达可能代表一种新的治疗方法,可用于敏化和抑制他莫昔芬耐药性乳腺癌肿瘤的生长。
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