Population‐specific validation and comparison of the performance of 77‐ and 313‐variant polygenic risk scores for breast cancer risk prediction

Author:

Hovhannisyan Milena1,Zemankova Petra12,Nehasil Petr123,Matejkova Katerina14,Borecka Marianna1,Cerna Marta1,Dolezalova Tatana1,Dvorakova Lenka3,Foretova Lenka5,Horackova Klara1,Jelinkova Sandra1,Just Pavel1,Kalousova Marta1,Kral Jan16,Machackova Eva5,Nemcova Barbora1,Safarikova Marketa1,Springer Drahomira1,Stastna Barbora17,Tavandzis Spiros8,Vocka Michal9,Zima Tomas1,Soukupova Jana1,Kleiblova Petra110,Ernst Corinna11ORCID,Kleibl Zdenek12ORCID,Janatova Marketa1ORCID

Affiliation:

1. Institute of Medical Biochemistry and Laboratory Diagnostics First Faculty of Medicine Charles University and General University Hospital in Prague Prague Czech Republic

2. Institute of Pathological Physiology First Faculty of Medicine Charles University Prague Czech Republic

3. Department of Paediatrics and Inherited Metabolic Disorders First Faculty of Medicine Charles University and General University Hospital in Prague Prague Czech Republic

4. Department of Genetics and Microbiology Faculty of Science Charles University in Prague Prague Czech Republic

5. Department of Cancer Epidemiology and Genetics Masaryk Memorial Cancer Institute Brno Czech Republic

6. Centre for Medical Genetics and Reproductive Medicine GENNET Prague Czech Republic

7. Department of Biochemistry Faculty of Science Charles University Prague Czech Republic

8. Department of Medical Genetics AGEL Research and Training Institute AGEL Laboratories Novy Jicin Czech Republic

9. Department of Oncology First Faculty of Medicine Charles University and General University Hospital in Prague Prague Czech Republic

10. Institute of Biology and Medical Genetics First Faculty of Medicine Charles University and General University Hospital in Prague Prague Czech Republic

11. Centre for Familial Breast and Ovarian Cancer Center for Integrated Oncology Medical Faculty University of Cologne and University Hospital Cologne Cologne Germany

Abstract

AbstractBackgroundThe polygenic risk score (PRS) allows the quantification of the polygenic effect of many low‐penetrance alleles on the risk of breast cancer (BC). This study aimed to evaluate the performance of two sets comprising 77 or 313 low‐penetrance loci (PRS77 and PRS313) in patients with BC in the Czech population.MethodsIn a retrospective case‐control study, variants were genotyped from both the PRS77 and PRS313 sets in 1329 patients with BC and 1324 noncancer controls, all women without germline pathogenic variants in BC predisposition genes. Odds ratios (ORs) were calculated according to the categorical PRS in individual deciles. Weighted Cox regression analysis was used to estimate the hazard ratio (HR) per standard deviation (SD) increase in PRS.ResultsThe distributions of standardized PRSs in patients and controls were significantly different (p < 2.2 × 10−16) with both sets. PRS313 outperformed PRS77 in categorical and continuous PRS analyses. For patients in the highest 2.5% of PRS313, the risk reached an OR of 3.05 (95% CI, 1.66–5.89; p = 1.76 × 10−4). The continuous risk was estimated as an HRper SD of 1.64 (95% CI, 1.49–1.81; p < 2.0 × 10−16), which resulted in an absolute risk of 21.03% at age 80 years for individuals in the 95th percentile of PRS313. Discordant categorization into PRS deciles was observed in 248 individuals (9.3%).ConclusionsBoth PRS77 and PRS313 are able to stratify individuals according to their BC risk in the Czech population. PRS313 shows better discriminatory ability. The results support the potential clinical utility of using PRS313 in individualized BC risk prediction.

Publisher

Wiley

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