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Identification of Lineage-Specific Cis-Regulatory Modules Associated with Variation in Transcription Factor Binding and Chromatin Activity Using Ornstein–Uhlenbeck Models

机译:使用Ornstein–Uhlenbeck模型鉴定与转录因子结合和染色质活性变化相关的特定于谱系的顺式调控模块

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摘要

Scoring the impact of noncoding variation on the function of cis-regulatory regions, on their chromatin state, and on the qualitative and quantitative expression levels of target genes is a fundamental problem in evolutionary genomics. A particular challenge is how to model the divergence of quantitative traits and to identify relationships between the changes across the different levels of the genome, the chromatin activity landscape, and the transcriptome. Here, we examine the use of the Ornstein–Uhlenbeck (OU) model to infer selection at the level of predicted cis-regulatory modules (CRMs), and link these with changes in transcription factor binding and chromatin activity. Using publicly available cross-species ChIP-Seq and STARR-Seq data we show how OU can be applied genome-wide to identify candidate transcription factors for which binding site and CRM turnover is correlated with changes in regulatory activity. Next, we profile open chromatin in the developing eye across three Drosophila species. We identify the recognition motifs of the chromatin remodelers, Trithorax-like and Grainyhead as mostly correlating with species-specific changes in open chromatin. In conclusion, we show in this study that CRM scores can be used as quantitative traits and that motif discovery approaches can be extended towards more complex models of divergence.
机译:评估非编码变异对顺式调控区功能,其染色质状态以及靶基因的定性和定量表达水平的影响,是进化基因组学中的一个基本问题。一个特殊的挑战是如何对定量性状的差异进行建模,以及如何确定基因组不同水平,染色质活性图谱和转录组之间变化之间的关系。在这里,我们研究了使用Ornstein-Uhlenbeck(OU)模型在预测的顺式调控模块(CRM)水平上推断选择,并将其与转录因子结合和染色质活性的变化联系在一起。使用公开提供的跨物种ChIP-Seq和STARR-Seq数据,我们展示了OU如何在全基因组范围内应用,以识别候选转录因子,其结合位点和CRM营业额与调节活性的变化相关。接下来,我们在三种果蝇物种的发育中的眼睛中剖析开放的染色质。我们确定染色质重塑剂,Trithorax样和Grainyhead的识别基序与开放染色质中的物种特异性变化最相关。总而言之,我们在这项研究中表明,CRM分数可以用作定量特征,并且主题发现方法可以扩展到更复杂的差异模型。

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