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Identification of significant chromatin contacts from HiChIP data by FitHiChIP

机译:通过FitHiChIP从HiChIP数据中识别重要的染色质接触

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摘要

HiChIP/PLAC-seq is increasingly becoming popular for profiling 3D chromatin contacts among regulatory elements and for annotating functions of genetic variants. Here we describe FitHiChIP, a computational method for loop calling from HiChIP/PLAC-seq data, which jointly models the non-uniform coverage and genomic distance scaling of contact counts to compute statistical significance estimates. We also develop a technique to filter putative bystander loops that can be explained by stronger adjacent loops. Compared to existing methods, FitHiChIP performs better in recovering contacts reported by Hi-C, promoter capture Hi-C and ChIA-PET experiments and in capturing previously validated promoter-enhancer interactions. FitHiChIP loop calls are reproducible among replicates and are consistent across different experimental settings. Our work also provides a framework for differential HiChIP analysis with an option to utilize ChIP-seq data for further characterizing differential loops. Even though designed for HiChIP, FitHiChIP is also applicable to other conformation capture assays.
机译:HiChIP / PLAC-seq在分析调控元件之间的3D染色质接触以及注释遗传变异功能方面正变得越来越流行。在这里,我们描述FitHiChIP,这是一种从HiChIP / PLAC-seq数据进行循环调用的计算方法,该方法联合建模接触计数的不均匀覆盖率和基因组距离缩放以计算统计显着性估计。我们还开发了一种过滤假定的旁观者循环的技术,可以用更强的相邻循环来解释。与现有方法相比,FitHiChIP在恢复Hi-C报告的接触,启动子捕获Hi-C和ChIA-PET实验以及捕获先前已验证的启动子-增强子相互作用方面表现更好。 FitHiChIP循环调用在复制之间可重现,并且在不同的实验设置下保持一致。我们的工作还为差分HiChIP分析提供了框架,并提供了利用ChIP-seq数据进一步表征差分回路的选项。即使是为HiChIP设计的,FitHiChIP也适用于其他构象捕获测定。

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