Clinically actionable mutation profiles in patients with cancer identified by whole-genome sequencing

Author:

Schuh AnnaORCID,Dreau HeleneORCID,Knight Samantha J.L.ORCID,Ridout KateORCID,Mizani Tuba,Vavoulis DimitrisORCID,Colling RichardORCID,Antoniou PavlosORCID,Kvikstad Erika M.ORCID,Pentony Melissa M.ORCID,Hamblin Angela,Protheroe AndrewORCID,Parton Marina,Shah Ketan A.ORCID,Orosz Zsolt,Athanasou Nick,Hassan Bass,Flanagan Adrienne M.,Ahmed Ahmed,Winter Stuart,Harris Adrian,Tomlinson IanORCID,Popitsch Niko,Church David,Taylor Jenny C.

Abstract

Next-generation sequencing (NGS) efforts have established catalogs of mutations relevant to cancer development. However, the clinical utility of this information remains largely unexplored. Here, we present the results of the first eight patients recruited into a clinical whole-genome sequencing (WGS) program in the United Kingdom. We performed PCR-free WGS of fresh frozen tumors and germline DNA at 75× and 30×, respectively, using the HiSeq2500 HTv4. Subtracted tumor VCFs and paired germlines were subjected to comprehensive analysis of coding and noncoding regions, integration of germline with somatically acquired variants, and global mutation signatures and pathway analyses. Results were classified into tiers and presented to a multidisciplinary tumor board. WGS results helped to clarify an uncertain histopathological diagnosis in one case, led to informed or supported prognosis in two cases, leading to de-escalation of therapy in one, and indicated potential treatments in all eight. Overall 26 different tier 1 potentially clinically actionable findings were identified using WGS compared with six SNVs/indels using routine targeted NGS. These initial results demonstrate the potential of WGS to inform future diagnosis, prognosis, and treatment choice in cancer and justify the systematic evaluation of the clinical utility of WGS in larger cohorts of patients with cancer.

Publisher

Cold Spring Harbor Laboratory

Subject

General Medicine

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