Single duplex DNA sequencing with CODEC detects mutations with high sensitivity

Author:

Bae Jin H.ORCID,Liu RuolinORCID,Roberts Eugenia,Nguyen Erica,Tabrizi ShervinORCID,Rhoades Justin,Blewett Timothy,Xiong Kan,Gydush Gregory,Shea Douglas,An Zhenyi,Patel Sahil,Cheng Ju,Sridhar Sainetra,Liu Mei Hong,Lassen EmilieORCID,Skytte Anne-BineORCID,Grońska-Pęski MartaORCID,Shoag Jonathan E.,Evrony Gilad D.,Parsons Heather A.ORCID,Mayer Erica L.,Makrigiorgos G. Mike,Golub Todd R.ORCID,Adalsteinsson Viktor A.ORCID

Abstract

AbstractDetecting mutations from single DNA molecules is crucial in many fields but challenging. Next-generation sequencing (NGS) affords tremendous throughput but cannot directly sequence double-stranded DNA molecules (‘single duplexes’) to discern the true mutations on both strands. Here we present Concatenating Original Duplex for Error Correction (CODEC), which confers single duplex resolution to NGS. CODEC affords 1,000-fold higher accuracy than NGS, using up to 100-fold fewer reads than duplex sequencing. CODEC revealed mutation frequencies of 2.72 × 10−8 in sperm of a 39-year-old individual, and somatic mutations acquired with age in blood cells. CODEC detected genome-wide, clonal hematopoiesis mutations from single DNA molecules, single mutated duplexes from tumor genomes and liquid biopsies, microsatellite instability with 10-fold greater sensitivity and mutational signatures, and specific tumor mutations with up to 100-fold fewer reads. CODEC enables more precise genetic testing and reveals biologically significant mutations, which are commonly obscured by NGS errors.

Funder

Gerstner Family Foundation

Conquer Cancer Foundation

Prostate Cancer Foundation

U.S. Department of Health & Human Services | National Institutes of Health

Damon Runyon Cancer Research Foundation

Sontag Foundation

Breast Cancer Research Foundation

Susan G. Komen

Publisher

Springer Science and Business Media LLC

Subject

Genetics

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