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Polygenic risk scores for prostate cancer: Comparative evaluations in UK and Australian cohorts.

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HGG advances 2025 Vol.6(4) p. 100477
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출처

Tanha HM, Law MH, Ingold N, Ly P, Olsen CM, Pandeya N

📝 환자 설명용 한 줄

Risk-based approaches offer promise for enhancing early detection of prostate cancer.

🔬 핵심 임상 통계 (초록에서 자동 추출 — 원문 검증 권장)
  • 표본수 (n) 184,010
  • 연구 설계 Cohort Study

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↓ .bib ↓ .ris
APA Tanha HM, Law MH, et al. (2025). Polygenic risk scores for prostate cancer: Comparative evaluations in UK and Australian cohorts.. HGG advances, 6(4), 100477. https://doi.org/10.1016/j.xhgg.2025.100477
MLA Tanha HM, et al.. "Polygenic risk scores for prostate cancer: Comparative evaluations in UK and Australian cohorts.." HGG advances, vol. 6, no. 4, 2025, pp. 100477.
PMID 40629691 ↗

Abstract

Risk-based approaches offer promise for enhancing early detection of prostate cancer. Polygenic risk scores (PGSs) have emerged as a potential approach for risk stratification, though their performance varies by population. We evaluated nine PGSs (four existing, five new) for predicting 5-year prostate cancer risk across three international population-based prospective cohorts: UK Biobank (UKB), the Australian QSkin Sun and Health Study (QSkin), and Melbourne Collaborative Cohort Study (MCCS). We analyzed UKB European-ancestry (n = 184,010), South-Asian-ancestry (n = 5,097), and African-ancestry (n = 3,193), QSkin European-ancestry (n = 6,791), and MCCS European-ancestry (n = 1,809) male participants. We estimated age-specific 5-year prostate cancer risks (from population data) and PGS-adjusted risks (age-specific risks multiplied by PGS-based relative risks). Predictive performance was assessed using discrimination (AUC) and calibration. PGS significantly enhanced 5-year risk prediction over age alone, particularly for European ancestry (AUC increase 0.05-0.12, p < 10). PGS performance was consistent across European-ancestry men in Australian and UK cohorts, and by pre-baseline prostate-specific antigen tests and family history in UKB. No single PGS outperformed others across all cohorts and ancestry groups. As an illustrative example for potential risk stratification, for a leading PGS in both Australian cohorts, we estimated the population-average 5-year risk at age 50 was reached 5 years earlier by individuals with 20% highest PGS451 and 5 years later by those with 20% lowest PGS451. In conclusion, rigorous analyses with consistent results from international cohorts support the potential of PGS to improve 5-year prostate cancer risk prediction. In the future, PGS may be improved further to enhance performance in diverse populations.

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