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HMCan-diff: a method to detect changes in histone modifications in cells with different genetic characteristics

机译:HMCan-diff:一种检测具有不同遗传特征的细胞中组蛋白修饰变化的方法

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摘要

Comparing histone modification profiles between cancer and normal states, or across different tumor samples, can provide insights into understanding cancer initiation, progression and response to therapy. ChIP-seq histone modification data of cancer samples are distorted by copy number variation innate to any cancer cell. We present HMCan-diff, the first method designed to analyze ChIP-seq data to detect changes in histone modifications between two cancer samples of different genetic backgrounds, or between a cancer sample and a normal control. HMCan-diff explicitly corrects for copy number bias, and for other biases in the ChIP-seq data, which significantly improves prediction accuracy compared to methods that do not consider such corrections. On in silico simulated ChIP-seq data generated using genomes with differences in copy number profiles, HMCan-diff shows a much better performance compared to other methods that have no correction for copy number bias. Additionally, we benchmarked HMCan-diff on four experimental datasets, characterizing two histone marks in two different scenarios. We correlated changes in histone modifications between a cancer and a normal control sample with changes in gene expression. On all experimental datasets, HMCan-diff demonstrated better performance compared to the other methods.
机译:比较癌症和正常状态之间或不同肿瘤样品之间的组蛋白修饰谱,可以提供了解癌症起始,进展和对治疗的反应的见解。癌症样品的ChIP-seq组蛋白修饰数据因任何癌细胞固有的拷贝数变化而失真。我们介绍了HMCan-diff,这是第一种设计用于分析ChIP-seq数据以检测具有不同遗传背景的两个癌症样品之间或癌症样品与正常对照之间的组蛋白修饰变化的方法。 HMCan-diff显式校正了拷贝数偏差以及ChIP-seq数据中的其他偏差,与不考虑此类校正的方法相比,这可以显着提高预测准确性。在使用具有拷贝数分布差异的基因组生成的计算机模拟的ChIP-seq数据上,与不对拷贝数偏差进行校正的其他方法相比,HMCan-diff显示出更好的性能。此外,我们在四个实验数据集上对HMCan-diff进行了基准测试,在两种不同情况下表征了两个组蛋白标记。我们将癌症和正常对照样品之间的组蛋白修饰变化与基因表达变化相关联。在所有实验数据集上,HMCan-diff与其他方法相比表现出更好的性能。

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