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A Least Angle Regression Model for the Prediction of Canonical and Non-Canonical miRNA-mRNA Interactions

机译:最小角度回归模型,用于预测规范和非规范的miRNA-mRNA相互作用

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摘要

microRNAs (miRNAs) are short non-coding RNAs with regulatory functions in various biological processes including cell differentiation, development and oncogenic transformation. They can bind to mRNA transcripts of protein-coding genes and repress their translation or lead to mRNA degradation. Conversely, the transcription of miRNAs is regulated by proteins including transcription factors, co-factors, and messenger molecules in signaling pathways, yielding a bidirectional regulatory network of gene and miRNA expression. We describe here a least angle regression approach for uncovering the functional interplay of gene and miRNA regulation based on paired gene and miRNA expression profiles. First, we show that gene expression profiles can indeed be reconstructed from the expression profiles of miRNAs predicted to be regulating the specific gene. Second, we propose a two-step model where in the first step, sequence information is used to constrain the possible set of regulating miRNAs and in the second step, this constraint is relaxed to find regulating miRNAs that do not rely on perfect seed binding. Finally, a bidirectional network comprised of miRNAs regulating genes and genes regulating miRNAs is built from our previous regulatory predictions. After applying the method to a human cancer cell line data set, an analysis of the underlying network reveals miRNAs known to be associated with cancer when dysregulated are predictors of genes with functions in apoptosis. Among the predicted and newly identified targets that lack a classical miRNA seed binding site of a specific oncomir, miR-19b-1, we found an over-representation of genes with functions in apoptosis, which is in accordance with the previous finding that this miRNA is the key oncogenic factor in the mir-17-92 cluster. In addition, we found genes involved in DNA recombination and repair that underline its importance in maintaining the integrity of the cell.
机译:microRNA(miRNA)是短的非编码RNA,在包括细胞分化,发育和致癌转化在内的各种生物过程中具有调节功能。它们可以与蛋白质编码基因的mRNA转录物结合并抑制其翻译或导致mRNA降解。相反,miRNA的转录受信号通路中包括转录因子,辅因子和信使分子的蛋白质调控,从而产生基因和miRNA表达的双向调控网络。我们在这里描述了一种最小角度回归方法,用于基于配对的基因和miRNA表达谱揭示基因和miRNA调控的功能相互作用。首先,我们证明确实可以从预测调控特定基因的miRNA的表达谱中重建基因表达谱。其次,我们提出了一个两步模型,其中第一步是使用序列信息来约束可能的调节miRNA集,第二步是放宽此约束以找到不依赖完美种子结合的调节miRNA。最后,根据我们以前的调控预测,构建了一个由调控miRNA和调控miRNA的基因组成的双向网络。在将该方法应用于人类癌细胞系数据集之后,对基础网络的分析显示,失调时已知与癌症相关的miRNA是具有凋亡功能的基因的预测因子。在预测的和新发现的靶标中,该靶标缺乏特定的癌基因miR-19b-1的经典miRNA种子结合位点,我们发现了具有凋亡功能的基因的过度表达,这与先前的发现相符。是mir-17-92簇中的关键致癌因子。此外,我们发现参与DNA重组和修复的基因突显了其在维持细胞完整性方面的重要性。

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