Disease areas:
  • cancer and other tissue growths
Last updated:
Author(s):
Rodrigo A S Barreiro, Tatiana F de Almeida, Catarina Gomes, Frederico Monfardini, Allysson A de Farias, Gabriela C Tunes, Gabriel M de Souza, Etienne Duim, Jaqueline de Sá Correia, Antonio V Campos Coelho, Marcel P Caraciolo, Yeda A Oliveira Duarte, Mayana Zatz, Edson Amaro, João B Oliveira, Bárbara D Bitarello, Helena Brentani, Michel S Naslavsky
Publish date:
6 July 2024
Journal:
Journal of Molecular Diagnostics
PubMed ID:
38972593

Abstract

Polygenic risk scores (PRSs) for breast cancer have a clear clinical utility in risk prediction. PRS transferability across populations and ancestry groups is hampered by population-specific factors, ultimately leading to differences in variant effects, such as linkage disequilibrium and differences in variant frequency (allele frequency differences). Thus, locally sourced population-based phenotypic and genomic data sets are essential to assess the validity of PRSs derived from signals detected across populations. This study assesses the transferability of a breast cancer PRS composed of 313 risk variants (313-PRS) in a Brazilian trihybrid admixed ancestries (European, African, and Native American) whole-genome sequenced cohort, the Rare Genomes Project. 313-PRS was computed in the Rare Genomes Project (n = 853) using the UK Biobank (UKBB; n = 264,307) as reference. The Brazilian cohorts have a high European ancestry (EA) component, with allele frequency differences and to a lesser extent linkage disequilibrium patterns similar to those found in EA populations. The 313-PRS distribution was found to be inflated when compared with that of the UKBB, leading to potential overestimation of PRS-based risk if EA is taken as a standard. However, case controls lead to equivalent predictive power when compared with UKBB-EA samples with area under the receiver operating characteristic curve values of 0.66 to 0.62 compared with 0.63 for UKBB.

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