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Identification of cis-regulatory mutations generating de novo edges in personalized cancer gene regulatory networks

Zeynep Kalender Atak, Hana Imrichova, Dmitry Svetlichnyy, Gert Hulselmans, Valerie Christiaens, Joke Reumers, Hugo Ceulemans, Stein Aerts
doi: https://doi.org/10.1101/130641
Zeynep Kalender Atak
1Laboratory of Computational Biology, Center for Human Genetics, University of Leuven, Leuven, Belgium
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Hana Imrichova
1Laboratory of Computational Biology, Center for Human Genetics, University of Leuven, Leuven, Belgium
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Dmitry Svetlichnyy
1Laboratory of Computational Biology, Center for Human Genetics, University of Leuven, Leuven, Belgium
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Gert Hulselmans
1Laboratory of Computational Biology, Center for Human Genetics, University of Leuven, Leuven, Belgium
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Valerie Christiaens
1Laboratory of Computational Biology, Center for Human Genetics, University of Leuven, Leuven, Belgium
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Joke Reumers
2Janssen Pharmaceutica NV, a Belgian company with registered offices at Turnhoutseweg 30, 2340 Beerse
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Hugo Ceulemans
2Janssen Pharmaceutica NV, a Belgian company with registered offices at Turnhoutseweg 30, 2340 Beerse
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Stein Aerts
1Laboratory of Computational Biology, Center for Human Genetics, University of Leuven, Leuven, Belgium
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Abstract

The identification of functional non-coding mutations is a key challenge in the field of genomics, where whole-genome re-sequencing can swiftly generate a set of all genomic variants in a sample, such as a tumor biopsy. The size of the human regulatory landscape places a challenge on finding recurrent cis-regulatory mutations across samples of the same cancer type. Therefore, powerful computational approaches are required to sift through the tens of thousands of non-coding variants, to identify potentially functional variants that have an impact on the gene expression profile of the sample. Here we introduce an integrative analysis pipeline, called μ- cisTarget, to filter, annotate and prioritize non-coding variants based on their putative effect on the underlying 'personal' gene regulatory network. We first validate μ-cisTarget by re-analyzing three cases of oncogenic non-coding mutations, namely the TAL1 and LMO1 enhancer mutations in T-ALL, and the TERT promoter mutation in melanoma. Next, we re-sequenced the full genome of ten cancer cell lines of six different cancer types, and used matched transcriptome data and motif discovery to infer master regulators for each sample. We identified candidate functional non-coding mutations that generate de novo binding sites for these master regulators, and that result in the up-regulation of nearby oncogenic drivers. We finally validated the predictions using tertiary data including matched epigenome data. Our approach is generally applicable to re-sequenced cancer genomes, or other genomes, when a disease- or sample-specific gene signature is available for network inference. μ-cisTarget is available from http://mucistarget.aertslab.org.

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Posted April 25, 2017.
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Identification of cis-regulatory mutations generating de novo edges in personalized cancer gene regulatory networks
Zeynep Kalender Atak, Hana Imrichova, Dmitry Svetlichnyy, Gert Hulselmans, Valerie Christiaens, Joke Reumers, Hugo Ceulemans, Stein Aerts
bioRxiv 130641; doi: https://doi.org/10.1101/130641
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Identification of cis-regulatory mutations generating de novo edges in personalized cancer gene regulatory networks
Zeynep Kalender Atak, Hana Imrichova, Dmitry Svetlichnyy, Gert Hulselmans, Valerie Christiaens, Joke Reumers, Hugo Ceulemans, Stein Aerts
bioRxiv 130641; doi: https://doi.org/10.1101/130641

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