A test for detecting differential indirect trans effects between two groups of samples.

Pub Date : 2018-07-31 DOI:10.1515/sagmb-2017-0058
Nimisha Chaturvedi, Renée X de Menezes, Jelle J Goeman, Wessel van Wieringen
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Abstract

Integrative analysis of copy number and gene expression data can help in understanding the cis and trans effect of copy number aberrations on transcription levels of genes involved in a pathway. To analyse how these copy number mediated gene-gene interactions differ between groups of samples we propose a new method, named dNET. Our method uses ridge regression to model the network topology involving one gene's expression level, its gene dosage and the expression levels of other genes in the network. The interaction parameters are estimated by fitting the model per gene for all samples together. However, instead of testing for differential network topology per gene, dNET tests for an overall difference in estimated parameters between two groups of samples and produces a single p-value. With the help of several simulation studies, we show that dNET can detect differential network nodes with high accuracy and low rate of false positives even in the presence of differential cis effects. We also apply dNET to publicly available TCGA cancer datasets and identify pathways where copy number mediated gene-gene interactions differ between samples with cancer stage lower than stage 3 and samples with cancer stage 3 or above.

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一种检测两组样本间差异间接反效应的检验。
拷贝数和基因表达数据的综合分析有助于理解拷贝数畸变对通路相关基因转录水平的顺式和反式影响。为了分析这些拷贝数介导的基因相互作用在不同样本组之间的差异,我们提出了一种名为dNET的新方法。我们的方法使用脊回归来建模网络拓扑,包括一个基因的表达水平,它的基因剂量和网络中其他基因的表达水平。通过对所有样本的每个基因模型进行拟合来估计相互作用参数。然而,dNET不是测试每个基因的差异网络拓扑结构,而是测试两组样本之间估计参数的总体差异,并产生单个p值。通过一些仿真研究,我们证明了即使在存在差分顺式效应的情况下,dNET也能以高精度和低误报率检测差分网络节点。我们还将dNET应用于公开可用的TCGA癌症数据集,并确定拷贝数介导的基因相互作用在癌症阶段低于3期和癌症阶段3或以上的样本之间的不同途径。
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