Tumor sequencing of African ancestry reveals differences in clinically relevant alterations across common cancers
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Elsevier Inc
Abstract
Cancer genomes from patients with African (AFR) ancestry have been poorly studied in clinical research. We
leverage two large genomic cohorts to investigate the relationship between genomic alterations and AFR
ancestry in six common cancers. Cross-cancer type associations, such as an enrichment of MYC amplificance with AFR ancestry in lung, breast, and prostate cancers, and depletion of BRAF alterations, are observed
in colorectal and pancreatic cancers. There are differences in actionable alterations, such as depletion of
KRAS G12C and EGFR L858R, and enrichment of ROS1 fusion with AFR ancestry in lung cancers. Interestingly, in lung cancer, KRAS mutations are less common in both smokers and non-smokers with AFR ancestry.
whereas the association of TP53 mutations with AFR ancestry is only seen in smokers, suggesting an
ancestry-environment interaction that modifies driver rates. Our study highlights the need to increase the representation of patients with AFR ancestry in drug development and biomarker development.
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Research Article