MAESTRO affords ‘breadth and depth’ for mutation testing

Author:

Gydush Gregory,Nguyen Erica,Bae Jin H.,Rhoades Justin,Reed Sarah C.,Shea Douglas,Xiong Kan,Liu Ruolin,Blewett Timothy,Yu Fangyan,Leong Ka Wai,Choudhury Atish D.,Stover Daniel G.ORCID,Tolaney Sara M.,Krop Ian E.,Love J. ChristopherORCID,Parsons Heather A.,Makrigiorgos G. Mike,Golub Todd R.,Adalsteinsson Viktor A.

Abstract

AbstractThe ability to assay large numbers of low-abundance mutations is crucial in biomedicine. Yet, the technical hurdles of sequencing multiple mutations at extremely high depth and accuracy remain daunting. For sequencing low-level mutations, it’s either ‘depth or breadth’ but not both. Here, we report a simple and powerful approach to accurately track thousands of distinct mutations with minimal reads. Our technique called MAESTRO (minor allele enriched sequencing through recognition oligonucleotides) employs massively-parallel mutation enrichment to empower duplex sequencing—one of the most accurate methods—to track up to 10,000 low-frequency mutations with up to 100-fold less sequencing. In example use cases, we show that MAESTRO could enable mutation validation from cancer genome sequencing studies. We also show that it could track thousands of mutations from a patient’s tumor in cell-free DNA, which may improve detection of minimal residual disease from liquid biopsies. In all, MAESTRO improves the breadth, depth, accuracy, and efficiency of mutation testing.

Publisher

Cold Spring Harbor Laboratory

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