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ABC: a tool to identify SNVs causing allele-specific transcription factor binding from ChIP-Seq experiments

机译:ABC:一种从ChIP-Seq实验中识别引起等位基因特异性转录因子结合的SNV的工具

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摘要

>Motivation: Detection of allelic imbalances in ChIP-Seq reads is a powerful approach to identify functional non-coding single nucleotide variants (SNVs), either polymorphisms or mutations, which modulate the affinity of transcription factors for chromatin. We present ABC, a computational tool that identifies allele-specific binding of transcription factors from aligned ChIP-Seq reads at heterozygous SNVs. ABC controls for potential false positives resulting from biases introduced by the use of short sequencing reads in ChIP-Seq and can efficiently process a large number of heterozygous SNVs.>Results: ABC successfully identifies previously characterized functional SNVs, such as the rs4784227 breast cancer risk associated SNP that modulates the affinity of FOXA1 for the chromatin.>Availability and implementation: The code is open-source under an Artistic-2.0 license and versioned on GitHub (). ABC is written in PERL and can be run on any platform with both PERL (≥5.18.1) and R (≥3.1.1) installed. The script requires the PERL Statistics::R module.>Contact: >Supplementary information: are available at Bioinformatics online.
机译:>动机:检测ChIP-Seq读物中的等位基因失衡是一种功能强大的方法,可识别功能性非编码单核苷酸变体(SNV),即多态性或突变,其可调节转录因子对染色质的亲和力。我们提出了ABC,一种计算工具,可从杂合SNV处的对齐的ChIP-Seq读取中识别转录因子的等位基因特异性结合。 ABC可以控制由于在ChIP-Seq中使用短测序读取而导致的偏倚所导致的潜在假阳性,并可以有效地处理大量杂合SNV。>结果:ABC成功地识别了先前表征的功能性SNV,例如因为rs4784227与乳腺癌风险相关的SNP会调节FOXA1对染色质的亲和力。>可用性和实现:该代码在Artistic-2.0许可下是开源的,并在GitHub上进行了版本化。 ABC用PERL编写,可以在安装了PERL(≥5.18.1)和R(≥3.1.1)的任何平台上运行。该脚本需要PERL Statistics :: R模块。>联系方式: >补充信息:可从Bioinformatics在线获得。

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