Whole-genome analysis of Nigerian patients with breast cancer reveals ethnic-driven somatic evolution and distinct genomic subtypes

Author:

Ansari-Pour NaserORCID,Zheng YonglanORCID,Yoshimatsu Toshio F.ORCID,Sanni Ayodele,Ajani MustaphaORCID,Reynier Jean-Baptiste,Tapinos Avraam,Pitt Jason J.,Dentro Stefan,Woodard Anna,Rajagopal Padma Sheila,Fitzgerald Dominic,Gruber Andreas J.,Odetunde Abayomi,Popoola Abiodun,Falusi Adeyinka G.,Babalola Chinedum PeaceORCID,Ogundiran Temidayo,Ibrahim Nasiru,Barretina JordiORCID,Van Loo PeterORCID,Chen MengjieORCID,White Kevin P.,Ojengbede Oladosu,Obafunwa John,Huo DezhengORCID,Wedge David C.ORCID,Olopade Olufunmilayo I.ORCID

Abstract

AbstractBlack women across the African diaspora experience more aggressive breast cancer with higher mortality rates than white women of European ancestry. Although inter-ethnic germline variation is known, differential somatic evolution has not been investigated in detail. Analysis of deep whole genomes of 97 breast cancers, with RNA-seq in a subset, from women in Nigeria in comparison with The Cancer Genome Atlas (n = 76) reveal a higher rate of genomic instability and increased intra-tumoral heterogeneity as well as a unique genomic subtype defined by early clonal GATA3 mutations with a 10.5-year younger age at diagnosis. We also find non-coding mutations in bona fide drivers (ZNF217 and SYPL1) and a previously unreported INDEL signature strongly associated with African ancestry proportion, underscoring the need to expand inclusion of diverse populations in biomedical research. Finally, we demonstrate that characterizing tumors for homologous recombination deficiency has significant clinical relevance in stratifying patients for potentially life-saving therapies.

Publisher

Springer Science and Business Media LLC

Subject

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

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