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mRNA expression profiles show differential regulatory effects of microRNAs between estrogen receptor-positive and estrogen receptor-negative breast cancer

机译:mRNA表达谱显示microRNA在雌激素受体阳性和雌激素受体阴性乳腺癌之间的不同调节作用

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ABSTRACT: BACKGROUND: Recent studies have shown that the regulatory effect of microRNAs can be investigated by examining expression changes of their target genes. Given this, it is useful to define an overall metric of regulatory effect for a specific microRNA and see how this changes across different conditions. RESULTS: Here, we define a regulatory effect score (RE-score) to measure the inhibitory effect of a microRNA in a sample, essentially the average difference in expression of its targets versus non-targets. Then we compare the RE-scores of various microRNAs between two breast cancer subtypes: estrogen receptor positive (ER+) and negative (ER-). We applied this approach to five microarray breast cancer datasets and found that the expression of target genes of most microRNAs was more repressed in ER- than ER+; that is, microRNAs appear to have higher RE-scores in ER- breast cancer. These results are robust to the microRNA target prediction method. To interpret these findings, we analyzed the level of microRNA expression in previous studies and found that higher microRNA expression was not always accompanied by higher inhibitory effects. However, several key microRNA processing genes, especially Ago2 and Dicer, were differentially expressed between ER- and ER+ breast cancer, which may explain the different regulatory effects of microRNAs in these two breast cancer subtypes. CONCLUSIONS: The RE-score is a promising indicator to measure microRNAs' inhibitory effects. Most microRNAs exhibit higher RE-scores in ER- than in ER+ samples, suggesting that they have stronger inhibitory effects in ER- breast cancers.
机译:摘要:背景:最近的研究表明,microRNA的调节作用可以通过检查其靶基因的表达变化来研究。鉴于此,定义特定microRNA调控效果的总体指标并查看其在不同条件下如何变化非常有用。结果:在这里,我们定义了一个调节效果评分(RE评分),用于测量样品中microRNA的抑制效果,本质上是其靶标与非靶标表达的平均差异。然后,我们比较两种乳腺癌亚型之间的各种microRNA的RE得分:雌激素受体阳性(ER +)和阴性(ER-)。我们将这种方法应用于五个微阵列乳腺癌数据集,发现大多数microRNA的靶基因在ER-中的表达比ER +受到更多的抑制。也就是说,在ER乳腺癌中,microRNA的RE得分更高。这些结果对于microRNA靶标预测方法是可靠的。为了解释这些发现,我们分析了先前研究中microRNA的表达水平,发现较高的microRNA表达并不总是伴随较高的抑制作用。但是,在ER-和ER +乳腺癌之间差异表达了几个关键的microRNA加工基因,尤其是Ago2和Dicer,这可能解释了microRNA在这两种乳腺癌亚型中的不同调控作用。结论:RE分数是测量microRNA抑制作用的有前途的指标。与ER +样品相比,大多数microRNA在ER-中的RE得分更高,表明它们在ER-乳腺癌中具有更强的抑制作用。

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