Integrative inference of subclonal tumour evolution from single-cell and bulk sequencing data

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作者
Salem Malikic
Katharina Jahn
Jack Kuipers
S. Cenk Sahinalp
Niko Beerenwinkel
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[1] Simon Fraser University,School of Computing Science
[2] Vancouver Prostate Centre,Department of Computer Science
[3] Department of Biosystems Science and Engineering,undefined
[4] ETH Zurich,undefined
[5] Swiss Institute of Bioinformatics,undefined
[6] Indiana University,undefined
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Understanding the clonal architecture and evolutionary history of a tumour poses one of the key challenges to overcome treatment failure due to resistant cell populations. Previously, studies on subclonal tumour evolution have been primarily based on bulk sequencing and in some recent cases on single-cell sequencing data. Either data type alone has shortcomings with regard to this task, but methods integrating both data types have been lacking. Here, we present B-SCITE, the first computational approach that infers tumour phylogenies from combined single-cell and bulk sequencing data. Using a comprehensive set of simulated data, we show that B-SCITE systematically outperforms existing methods with respect to tree reconstruction accuracy and subclone identification. B-SCITE provides high-fidelity reconstructions even with a modest number of single cells and in cases where bulk allele frequencies are affected by copy number changes. On real tumour data, B-SCITE generated mutation histories show high concordance with expert generated trees.
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