Linked-read analysis identifies mutations in single-cell DNA-sequencing data

Craig L. Bohrson,Allison R. Barton,Michael A. Lodato,Rachel E. Rodin,Vinay V. Viswanadham,Doga Can Gulhan,Isidro Cortes,Maxwell A. Sherman,Lovelace J. Luquette,Minseok Kwon,Michael E. Coulter,Christopher A. Walsh,Peter J. Park

Linked-read analysis identifies mutations in single-cell DNA-sequencing data

2019

Craig L. Bohrson
Allison R. Barton
Michael A. Lodato
Rachel E. Rodin
Vinay V. Viswanadham
Doga Can Gulhan
Isidro Cortes
Maxwell A. Sherman
Lovelace J. Luquette
Minseok Kwon
Michael E. Coulter
Christopher A. Walsh
Peter J. Park

Whole-genome sequencing of DNA from single cells has the potential to reshape our understanding of mutational heterogeneity in normal and diseased tissues. However, a major difficulty is distinguishing amplification artifacts from biologically derived somatic mutations. Here, we describe linked-read analysis (LiRA), a method that accurately identifies somatic single-nucleotide variants (sSNVs) by using read-level phasing with nearby germline heterozygous polymorphisms, thereby enabling the characterization of mutational signatures and estimation of somatic mutation rates in single cells.

Keywords:

Genetics
DNA sequencing
Cell
Germline
DNA
Molecular biology
Somatic cell
Germline mutation
COLD-PCR
Biology
DNA extraction
Bioinformatics

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