Cardelino: computational integration of somatic clonal substructure and single-cell transcriptomes

被引:0
|
作者
Davis J. McCarthy
Raghd Rostom
Yuanhua Huang
Daniel J. Kunz
Petr Danecek
Marc Jan Bonder
Tzachi Hagai
Ruqian Lyu
Wenyi Wang
Daniel J. Gaffney
Benjamin D. Simons
Oliver Stegle
Sarah A. Teichmann
机构
[1] Wellcome Genome Campus,European Molecular Biology Laboratory, European Bioinformatics Institute
[2] St Vincent’s Institute of Medical Research,Melbourne Integrative Genomics, School of Mathematics and Statistics/School of Biosciences
[3] University of Melbourne,Wellcome Sanger Institute
[4] Wellcome Genome Campus,Department of Clinical Neurosciences
[5] University of Cambridge,Department of Physics
[6] Cavendish Laboratory,The Wellcome Trust/Cancer Research UK Gurdon Institute
[7] University of Cambridge,School of Molecular Cell Biology and Biotechnology, George S Wise Faculty of Life Sciences
[8] Tel Aviv University,Department of Bioinformatics and Computational Biology
[9] The University of Texas MD Anderson Cancer Center,The Wellcome Trust/Medical Research Council Stem Cell Institute
[10] University of Cambridge,European Molecular Biology Laboratory
[11] Genome Biology Unit,Division of Computational Genomics and Systems Genetics
[12] German Cancer Research Center,Wellcome Genome Campus
[13] Wellcome Trust Sanger Institute,UCL Great Ormond Street Institute of Child Health
[14] University College London,Department of Medical Statistics
[15] University Medical Center Göttingen,Centre for Gene Regulation & Expression, School of Life Sciences
[16] University of Dundee,Department of Haematology
[17] University of Cambridge,Centre for Stem Cells & Regenerative Medicine, King’s College London, Tower Wing
[18] Guy’s Hospital,Wellcome Trust and MRC Cambridge Stem Cell Institute and Biomedical, Research Centre, Anne McLaren Laboratory
[19] Great Maze Pond,NHS Blood and Transplant
[20] University of Cambridge,Department of Genetics
[21] Cambridge Biomedical Campus,undefined
[22] University of Cambridge,undefined
来源
Nature Methods | 2020年 / 17卷
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摘要
Bulk and single-cell DNA sequencing has enabled reconstructing clonal substructures of somatic tissues from frequency and cooccurrence patterns of somatic variants. However, approaches to characterize phenotypic variations between clones are not established. Here we present cardelino (https://github.com/single-cell-genetics/cardelino), a computational method for inferring the clonal tree configuration and the clone of origin of individual cells assayed using single-cell RNA-seq (scRNA-seq). Cardelino flexibly integrates information from imperfect clonal trees inferred based on bulk exome-seq data, and sparse variant alleles expressed in scRNA-seq data. We apply cardelino to a published cancer dataset and to newly generated matched scRNA-seq and exome-seq data from 32 human dermal fibroblast lines, identifying hundreds of differentially expressed genes between cells from different somatic clones. These genes are frequently enriched for cell cycle and proliferation pathways, indicating a role for cell division genes in somatic evolution in healthy skin.
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页码:414 / 421
页数:7
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