Molecular landscape and functional characterization of centrosome amplification in ovarian cancer

Author:

Sauer Carolin M.ORCID,Hall James A.ORCID,Couturier Dominique-LaurentORCID,Bradley ThomasORCID,Piskorz Anna M.,Griffiths Jacob,Sawle AshleyORCID,Eldridge Matthew D.ORCID,Smith PhilipORCID,Hosking Karen,Reinius Marika A. V.ORCID,Morrill Gavarró LenaORCID,Mes-Masson Anne-MarieORCID,Ennis Darren,Millan David,Hoyle AoishaORCID,McNeish Iain A.ORCID,Jimenez-Linan Mercedes,Martins Filipe CorreiaORCID,Tischer Julia,Vias Maria,Brenton James D.ORCID

Abstract

AbstractHigh-grade serous ovarian carcinoma (HGSOC) is characterised by poor outcome and extreme chromosome instability (CIN). Therapies targeting centrosome amplification (CA), a key mediator of chromosome missegregation, may have significant clinical utility in HGSOC. However, the prevalence of CA in HGSOC, its relationship to genomic biomarkers of CIN and its potential impact on therapeutic response have not been defined. Using high-throughput multi-regional microscopy on 287 clinical HGSOC tissues and 73 cell lines models, here we show that CA through centriole overduplication is a highly recurrent and heterogeneous feature of HGSOC and strongly associated with CIN and genome subclonality. Cell-based studies showed that high-prevalence CA is phenocopied in ovarian cancer cell lines, and that high CA is associated with increased multi-treatment resistance; most notably to paclitaxel, the commonest treatment used in HGSOC. CA in HGSOC may therefore present a potential driver of tumour evolution and a powerful biomarker for response to standard-of-care treatment.

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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