Origin of second malignancies in children

Pediatric cancers are rare diseases, and children without known germline predisposing conditions who develop a second malignancy during developmental ages are extremely rare. We present four such clinical cases and through whole-genome and error-correcting ultra-deep duplex sequencing of tumor and normal samples, we explored the origin of the second malignancy in four children, uncovering different routes of development. The exposure to cytotoxic therapies was linked to the emergence of a secondary AML. A common somatic mutation acquired early during embryonic development was the driver of two solid malignancies in another child. In two cases, the two tumors developed from completely independent clones diverging during embryogenesis. Importantly, we demonstrate that platinum-based therapies contributed at least in one order of magnitude more mutations per day of exposure than aging to normal tissues in these children.

Type: Whole Genome Sequencing
Archiver: European Genome-Phenome Archive (EGA)

4 Datasets

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Dataset ID	Description	Technology	Samples
EGAD50000000237	Whole Genome Sequencing (120X) of the two tumors and blood from 4 pediatric cases with second malignancies (12 WGS)	Illumina NovaSeq X	12
EGAD50000000238	Whole Genome Sequencing of normal tissues from case 3 (9 WGS 120X), including parents blood Whole Genome Sequencing (2 WGS 30X).	Illumina NovaSeq X	11
EGAD50000000239	Duplex Sequencing of normal and tumor tissues from case 2 and case 3 (10 DS)	Illumina NovaSeq X	10
EGAD50000000240	Whole Genome Sequencing of 2 expanded clones from a cell line derived from the rhabdoid tumor case 3 (2 WGS 20X)	Illumina NovaSeq X	2