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Identification of microRNA targets.

机译:鉴定microRNA靶标。

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摘要

microRNAs (miRNAs) are a recently discovered class of small non-coding RNAs. Their mature form is 20-25 nucleotides (nt) long, and is derived from a longer hairpin precursor. Almost 700 miRNAs are currently known in human. miRNAs regulate their target genes by blocking their translation into protein, or by compromising the stability of a messenger RNA (mRNA), leading to its degradation. To understand the biological function of microRNAs it is crucial to identify their target genes. miRNAs and mRNAs interact through partial Watson-Crick complementarity, and it is known that binding sites of conserved miRNAs are often conserved themselves. It is believed that several miRNAs can regulate the same gene simultaneously. Taking into account the characteristics of miRNA::mRNA interaction, we designed a probabilistic sequence model that enables us to estimate the likelihood for each gene in the data set to be a target of a given set of miRNAs. By requiring the presence of some number of binding sites conserved in related species, we are applying a filter that keeps the false positive predictions number at an acceptable level. We used the method to predict targets of all human, worm and fruit fly miRNAs, and many predictions were later confirmed by experiments. Perhaps surprisingly, our data predicted that a single miRNA regulated the expression of hundreds of mRNAs and that altogether thousands of human genes are regulated by miRNAs. This prediction has by now been widely accepted. Among other predictions, we found that a mouse gene Myothrophin is predicted to be coordinately targeted by three miRNAs, and this was experimentally confirmed in cell lines. In order to discover the sequence motifs that are mediating the effect of miRNAs on their targets, we analyzed the genome-wide expression data obtained by miRNAs. Using an iterative linear regression model, we could select the motifs that best explain the genome-wide changes in expression imposed by the activity of miRNAs. In the end, we apply both methods to analyze experiments performed on B cells (immune system), and were able to in part uncover the role of miRNAs in B cell development.
机译:microRNA(miRNA)是最近发现的一类小型非编码RNA。它们的成熟形式为20-25个核苷酸(nt)长,并衍生自更长的发夹前体。目前人类已知近700种miRNA。 miRNA通过阻止其翻译成蛋白质或破坏信使RNA(mRNA)的稳定性(从而导致其降解)来调节其靶基因。要了解microRNA的生物学功能,至关重要的是确定其靶基因。 miRNA和mRNA通过部分Watson-Crick互补性相互作用,并且众所周知,保守的miRNA的结合位点通常是保守的。据信几种miRNA可以同时调节同一基因。考虑到miRNA :: mRNA相互作用的特征,我们设计了一个概率序列模型,该模型使我们能够估计数据集中每个基因成为给定miRNA集的目标的可能性。通过要求存在一些在相关物种中保守的结合位点,我们应用了将假阳性预测数保持在可接受水平的过滤器。我们使用该方法预测所有人类,蠕虫和果蝇miRNA的靶标,许多预测后来被实验证实。也许令人惊讶的是,我们的数据预测单个miRNA可以调节数百种mRNA的表达,而总共数千种人类基因都可以被miRNA调节。到目前为止,这一预测已被广泛接受。除其他预测外,我们还发现小鼠基因Mythrophin被预测为三个miRNA的协同靶点,并且在细胞系中得到了实验证实。为了发现介导miRNA对其靶标作用的序列基序,我们分析了miRNA获得的全基因组表达数据。使用迭代线性回归模型,我们可以选择最能解释由miRNA活性引起的全基因组表达变化的基序。最后,我们使用这两种方法来分析对B细胞(免疫系统)进行的实验,并且能够部分揭示miRNA在B细胞发育中的作用。

著录项

  • 作者

    Krek, Azra.;

  • 作者单位

    New York University.;

  • 授予单位 New York University.;
  • 学科 Biology Bioinformatics.;Biophysics General.
  • 学位 Ph.D.
  • 年度 2009
  • 页码 92 p.
  • 总页数 92
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 生物物理学;
  • 关键词

  • 入库时间 2022-08-17 11:38:06

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