Whole genome, transcriptome and methylome profiling enhances actionable target discovery in high-risk pediatric cancer.
Marie WongChelsea MayohLoretta M S LauDong Anh K Khoung-QuangMark PineseAmit KumarPaulette BarahonaEmilie E WilkiePatricia SullivanRachel Bowen-JamesMustafa H SyedIñigo MartincorenaFederico AbascalAlexandra SherstyukNoemi Auxiliadora Fuentes BolanosJonathan BaberPeter PriestleyM Emmy M DolmanEmmy D G FleurenMarie-Emilie GauthierEmily V A MouldVelimir GayevskiyAndrew J GiffordDylan Grebert-WadePatrick A StrongElodie ManouvrierMeera WarbyDavid M ThomasJudy KirkKatherine TuckerTracey O'BrienFrank AlvaroGeoffry B McCowageLuciano Dalla-PozzaNicholas G GottardoHeather TappPaul WoodSeong-Lin KhawJordan R HansfordAndrew S MooreMurray D NorrisToby N TrahairRichard B LockVanessa TyrrellMichelle HaberGlenn M MarshallDavid S ZieglerPaul G EkertMark J CowleyPublished in: Nature medicine (2020)
The Zero Childhood Cancer Program is a precision medicine program to benefit children with poor-outcome, rare, relapsed or refractory cancer. Using tumor and germline whole genome sequencing (WGS) and RNA sequencing (RNAseq) across 252 tumors from high-risk pediatric patients with cancer, we identified 968 reportable molecular aberrations (39.9% in WGS and RNAseq, 35.1% in WGS only and 25.0% in RNAseq only). Of these patients, 93.7% had at least one germline or somatic aberration, 71.4% had therapeutic targets and 5.2% had a change in diagnosis. WGS identified pathogenic cancer-predisposing variants in 16.2% of patients. In 76 central nervous system tumors, methylome analysis confirmed diagnosis in 71.1% of patients and contributed to a change of diagnosis in two patients (2.6%). To date, 43 patients have received a recommended therapy, 38 of whom could be evaluated, with 31% showing objective evidence of clinical benefit. Comprehensive molecular profiling resolved the molecular basis of virtually all high-risk cancers, leading to clinical benefit in some patients.