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Polygenic risk score model for renal cell carcinoma in the Korean population and relationship with lifestyle-associated factors

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Authors

Hong, Joo Young; Han, Jang Hee; Jeong, Seung Hwan; Kwak, Cheol; Kim, Hyeon Hoe; Jeong, Chang wook

Issue Date
2024-01-10
Publisher
BMC
Citation
BMC Genomics, Vol.25, no.46
Keywords
Polygenic risk scoreGenome-wide association studyRenal cell carcinomaKorean populationNon-coding variantEpigeneticsLifestyle-associated factor
Abstract
Background The polygenic risk score (PRS) is used to predict the risk of developing common complex diseases
or cancers using genetic markers. Although PRS is used in clinical practice to predict breast cancer risk, it is more
accurate for Europeans than for non-Europeans because of the sample size of training genome-wide association
studies (GWAS). To address this disparity, we constructed a PRS model for predicting the risk of renal cell carcinoma
(RCC) in the Korean population.
Results Using GWAS analysis, we identified 43 Korean-specific variants and calculated the PRS. Subsequent to
plotting receiver operating characteristic (ROC) curves, we selected the 31 best-performing variants to construct an
optimal PRS model. The resultant PRS model with 31 variants demonstrated a prediction rate of 77.4%. The pathway
analysis indicated that the identified non-coding variants are involved in regulating the expression of genes related to
cancer initiation and progression. Notably, favorable lifestyle habits, such as avoiding tobacco and alcohol, mitigated
the risk of RCC across PRS strata expressing genetic risk.
Conclusion A Korean-specific PRS model was established to predict the risk of RCC in the underrepresented Korean
population. Our findings suggest that lifestyle-associated factors influencing RCC risk are associated with acquired risk
factors indirectly through epigenetic modification, even among individuals in the higher PRS category.
Keywords Polygenic risk score, Genome-wide association study, Renal cell carcinoma, Korean population, Noncoding variant, Epigenetics, Lifestyle-associated factor
ISSN
1471-2164
Language
English
URI
https://hdl.handle.net/10371/198867
DOI
https://doi.org/10.1186/s12864-024-09974-w
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