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Transcription Factor Centric Discovery of Regulatory Elements in Mammalian Genomes Using Alignment-Independent Conservation Maps

机译:使用对齐独立的保护图,转录因子在哺乳动物基因组中的监管元素发现

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The computational identification of DNA binding sites that have high affinity for a specific transcription factor is an important problem that has only been partially addressed in prokaryotes and lower eukaryotes. Given the higher length of regulatory regions and the relative low complexity of DNA binding signature, however, methods to address this problem in higher order eukaryotes are lacking. In this paper, we propose a novel computational framework, which combines cellular network reverse engineering, integrative genomics, and comparative genomic approaches, to address this problem for a set of human transcription factors. Specifically, we study the regulatory regions of putative orthologous targets of a given transcription factor, obtained by reverse engineering methods, in several mammalian genomes. Highly conserved regions are identified by pattern discovery. Finally DNA binding sites are inferred from these regions using a standard Position Weight Matrices (PWM) discovery algorithm. By framing the identification of the PWM as an optimization problem over the two parameters of the method, we are able to discover known binding sites for several genes and to propose reasonable signatures for genes that have not been previously characterized.
机译:对特定转录因子具有高亲和力的DNA结合位点的计算鉴定是仅在原核生物和下真核生物中部分地寻址的重要问题。然而,考虑到更高长度的调节区域和DNA结合特征的相对低的复杂性,缺乏在高阶的真核中解决这个问题的方法。在本文中,我们提出了一种新颖的计算框架,其结合了蜂窝网络逆向工程,综合基因组学和比较基因组方法,以解决一组人的转录因子。具体而言,我们研究了几种哺乳动物基因组的逆向工程方法获得的给定转录因子的推定正交靶标推定的正交靶点。通过模式发现来确定高度保守的区域。最后,使用标准位置权重矩阵(PWM)发现算法从这些区域推断DNA结合位点。通过绘制PWM的鉴定作为该方法的两个参数的优化问题,我们能够发现几种基因的已知结合位点,并提出尚未表征的基因的合理签名。

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