Sensitive detection of MYCN amplified neuroblastoma in blood samples with structural variants using whole genome sequencing

MYCN high amplification in neuroblastoma indicates a high-risk diagnosis. Although this feature is routinely detected using tumor whole genome sequencing followed by copy number analysis, it remains unclear whether MYCN amplification can be detected in blood samples. Leveraging on recent progress in the error profiling of structural alterations (SVs), we hypothesize that copy number analysis coupled with SV detection can enable sensitive detection of MYCN amplification in blood samples. By using childhood neuroblastoma cohorts from three institutions, we demonstrate that standard whole genome sequencing (30-100X) of blood samples enables detection of MYCN amplification in 64% of cases with limit of detection as low as 0.01% and SV markers are superior to conventional copy number markers. Further, we demonstrate that buccal samples collected at diagnosis are less affected by circulating tumor DNAs for MYCN amplified neuroblastoma. Together, our findings indicate the power of SV analysis in liquid biopsies to ascertain high risk MYCN amplified neuroblastoma.

• Type: Other
• Archive: European Genome-phenome Archive (EGA)