Feasibility of whole genome and transcriptome profiling in pediatric and young adult cancers.
N ShuklaMax Fine LevineGunes GundemD DomenicoB SpitzerN BouvierJ E Arango-OssaD GlodzikJ S Medina-MartínezUmeshkumar K BhanotJ Gutiérrez-AbrilY ZhouE FialaE StockfischS LiM I Rodriguez-SanchezT O'DonohueCassidy CobbsMichael H A RoehrlJamal K BenhamidaF Iglesias CardenasM OrtizM KinnamanS RobertsM LadanyiS ModakS Farouk-SaitE SlotkinMatthias A KarajannisF Dela CruzJulia L Glade BenderAhmet ZehirA VialeMichael F WalshAndrew L KungElli PapaemmanuilPublished in: Nature communications (2022)
The utility of cancer whole genome and transcriptome sequencing (cWGTS) in oncology is increasingly recognized. However, implementation of cWGTS is challenged by the need to deliver results within clinically relevant timeframes, concerns about assay sensitivity, reporting and prioritization of findings. In a prospective research study we develop a workflow that reports comprehensive cWGTS results in 9 days. Comparison of cWGTS to diagnostic panel assays demonstrates the potential of cWGTS to capture all clinically reported mutations with comparable sensitivity in a single workflow. Benchmarking identifies a minimum of 80× as optimal depth for clinical WGS sequencing. Integration of germline, somatic DNA and RNA-seq data enable data-driven variant prioritization and reporting, with oncogenic findings reported in 54% more patients than standard of care. These results establish key technical considerations for the implementation of cWGTS as an integrated test in clinical oncology.
Keyphrases
- single cell
- rna seq
- high throughput
- palliative care
- healthcare
- electronic health record
- adverse drug
- end stage renal disease
- quality improvement
- young adults
- primary care
- newly diagnosed
- chronic kidney disease
- ejection fraction
- genome wide
- childhood cancer
- emergency department
- big data
- single molecule
- pain management
- squamous cell