Copy number signatures and mutational processes in ovarian carcinoma

Geoff Macintyre,Teodora Goranova,Dilrini De Silva,Darren Ennis,Anna M. Piskorz,Matthew Eldridge,Daoud Sie,Liz-Anne Lewsley,Aishah Hanif,Cheryl Wilson,Suzanne Dowson,Rosalind M. Glasspool,Michelle Lockley,Elly Brockbank,Ana Montes,Axel Walther,Sudha Sundar,Richard J. Edmondson,Geoff Hall,Andrew R Clamp,Charlie Gourley,Marcia Hall,Christina Fotopoulou,Hani Gabra,James Paul,Anna Supernat,David Millan,Aoisha Hoyle,Gareth Bryson,Craig Nourse,Laura Mincarelli,Luis Navarro Sanchez,Bauke Ylstra,Mercedes Jiménez Liñán,Luiza Moore,Oliver Hofmann,Florian Markowetz,Iain A. McNeish,James D. Brenton

Copy number signatures and mutational processes in ovarian carcinoma

2018

The genomic complexity of profound copy number aberrations has prevented effective molecular stratification of ovarian cancers. Here, to decode this complexity, we derived copy number signatures from shallow whole-genome sequencing of 117 high-grade serous ovarian cancer (HGSOC) cases, which were validated on 527 independent cases. We show that HGSOC comprises a continuum of genomes shaped by multiple mutational processes that result in known patterns of genomic aberration. Copy number signature exposures at diagnosis predict both overall survival and the probability of platinum-resistant relapse. Measurement of signature exposures provides a rational framework to choose combination treatments that target multiple mutational processes.

Keywords:

Ovarian cancer
Carcinoma
Genetics
Genome
Biology
mutator phenotype
Serous fluid
Pathogenesis
Bioinformatics
overall survival
tp53 mutation
ovarian carcinoma
SNP

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