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ChIP-seq 阴性对照信号噪声模型的显著性分析

A signal-noise model for significance analysis of ChIP-seq with negative control.

机构信息

Genome Institute of Singapore, Singapore.

出版信息

Bioinformatics. 2010 May 1;26(9):1199-204. doi: 10.1093/bioinformatics/btq128. Epub 2010 Apr 5.

Abstract

MOTIVATION

ChIP-seq is becoming the main approach to the genome-wide study of protein-DNA interactions and histone modifications. Existing informatics tools perform well to extract strong ChIP-enriched sites. However, two questions remain to be answered: (i) to which extent is a ChIP-seq experiment able to reveal the weak ChIP-enriched sites? (ii) are the weak sites biologically meaningful? To answer these questions, it is necessary to identify the weak ChIP signals from background noise.

RESULTS

We propose a linear signal-noise model, in which a noise rate was introduced to represent the fraction of noise in a ChIP library. We developed an iterative algorithm to estimate the noise rate using a control library, and derived a library-swapping strategy for the false discovery rate estimation. These approaches were integrated in a general-purpose framework, named CCAT (Control-based ChIP-seq Analysis Tool), for the significance analysis of ChIP-seq. Applications to H3K4me3 and H3K36me3 datasets showed that CCAT predicted significantly more ChIP-enriched sites that the previous methods did. With the high sensitivity of CCAT prediction, we revealed distinct chromatin features associated to the strong and weak H3K4me3 sites.

AVAILABILITY

http://cmb.gis.a-star.edu.sg/ChIPSeq/tools.htm.

摘要

动机

ChIP-seq 正成为研究蛋白质-DNA 相互作用和组蛋白修饰的全基因组的主要方法。现有的信息学工具在提取强 ChIP 富集位点方面表现良好。然而,仍有两个问题有待回答:(i)ChIP-seq 实验在多大程度上能够揭示弱 ChIP 富集的位点?(ii)这些弱位点是否具有生物学意义?为了回答这些问题,有必要从背景噪声中识别出弱的 ChIP 信号。

结果

我们提出了一种线性信号-噪声模型,其中引入了噪声率来表示 ChIP 文库中噪声的分数。我们开发了一种使用对照文库估计噪声率的迭代算法,并为假发现率估计推导了一种文库交换策略。这些方法被整合到一个名为 CCAT(基于对照的 ChIP-seq 分析工具)的通用框架中,用于 ChIP-seq 的显著性分析。应用于 H3K4me3 和 H3K36me3 数据集的结果表明,CCAT 预测的 ChIP 富集位点比以前的方法多。CCAT 预测具有较高的灵敏度,我们揭示了与强和弱 H3K4me3 位点相关的独特染色质特征。

可用性

http://cmb.gis.a-star.edu.sg/ChIPSeq/tools.htm。

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