Systematic discovery of gene fusions in pediatric cancer by integrating RNA-seq and WGS.

Ianthe A E M van BelzenCasey CaiMarc van TuilShashi BadloeEric StrengmanAlex JanseEugène T P VerwielDouwe F M van der LeestLennart KesterJan J MolenaarJules MeijerinkJarno DrostWeng Chuan PengHindrik H D KerstensBastiaan B J TopsFrank C P HolstegePatrick KemmerenJayne Y Hehir-Kwa

Published in: BMC cancer (2023)

Our results indicate how clinically relevant and potentially pathogenic gene fusions can be identified and their functional effects investigated by combining WGS and RNA-seq. Integrating RNA fusion predictions with underlying SVs advances fusion detection beyond extensive manual filtering. Taken together, we developed a method for identifying candidate gene fusions that is suitable for precision oncology applications. Our method provides multi-omics evidence for assessing the pathogenicity of tumor-specific gene fusions for future clinical decision making.

Keyphrases

rna seq
single cell
copy number
genome wide
decision making
genome wide identification
high throughput
palliative care
small molecule
dna methylation
staphylococcus aureus
transcription factor
mass spectrometry
cystic fibrosis
papillary thyroid
escherichia coli
lymph node metastasis
high speed