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Within-Family Analysis of Prs313: Insights Into Breast Cancer Risk Prediction Publisher



Lanjanian H ; Tehranifateh ST ; Akbarzadeh M ; Moazzamjazi M ; Zarkesh M ; Masjoudi S ; Zahedi AS ; Najdhassanbonab L ; Asgarian S ; Moghaddas MR ; Guity K ; Shalbafan B ; Momenan A ; Khalili D Show All Authors
Authors
  1. Lanjanian H
  2. Tehranifateh ST
  3. Akbarzadeh M
  4. Moazzamjazi M
  5. Zarkesh M
  6. Masjoudi S
  7. Zahedi AS
  8. Najdhassanbonab L
  9. Asgarian S
  10. Moghaddas MR
  11. Guity K
  12. Shalbafan B
  13. Momenan A
  14. Khalili D
  15. Tehrani FR
  16. Hedayati M
  17. Azizi F
  18. Daneshpour MS

Source: Journal of Genetic Engineering and Biotechnology Published:2025


Abstract

Polygenic risk scores (PRS) incorporate numerous genetic variants, each with a small impact on cancer pathogenesis, to provide personalized risk assessments. This study investigated, the applicability of PRS313 for breast cancer risk both in the general population and within families (patients vs different groups of their relatives) from the Tehran Cardiometabolic Genetic Study (TCGS)cohort. The cohort included 72 breast cancer cases and 2,603 controls. PRS313 showed no significant difference between cases and controls, and logistic regression indicated no significant association between PRS313 and breast cancer risk (OR: 1.24, 95 % CI: 1.002–1.54). However, PRS differences between patients and their first- and second-degree relatives showed strong statistical significance. The monogenic variant analysis identified 21 loss-of-function (LOF) variants in the cohort, but only one (BRCA2 9976A > T) was common among breast cancer cases. Our findings highlight the importance of within-family analysis of PRS and the challenges of applying European-derived PRS models to diverse populations. © 2025 Elsevier B.V., All rights reserved.
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