Détail du document
Identifiant

doi:10.1186/s12894-024-01524-6...

Auteur
Hsieh, Ai-Ru Luo, Yi-Ling Bao, Bo-Ying Chou, Tzu-Chieh
Langue
en
Editeur

BioMed Central

Catégorie

Urology

Année

2024

Date de référencement

03/07/2024

Mots clés
genetic risk score genome-wide association study prostate cancer cancer models prostate bcr risk grs genetic data
Métrique

Résumé

Background In recent years, Genome-Wide Association Studies (GWAS) has identified risk variants related to complex diseases, but most genetic variants have less impact on phenotypes.

To solve the above problems, methods that can use variants with low genetic effects, such as genetic risk score (GRS), have been developed to predict disease risk.

Methods As the GRS model with the most incredible prediction power for complex diseases has not been determined, our study used simulation data and prostate cancer data to explore the disease prediction power of three GRS models, including the simple count genetic risk score (SC-GRS), the direct logistic regression genetic risk score (DL-GRS), and the explained variance weighted GRS based on directed logistic regression (EVDL-GRS).

Results and Conclusions We used 26 SNPs to establish GRS models to predict the risk of biochemical recurrence (BCR) after radical prostatectomy.

Combining clinical variables such as age at diagnosis, body mass index, prostate-specific antigen, Gleason score, pathologic T stage, and surgical margin and GRS models has better predictive power for BCR.

The results of simulation data (statistical power = 0.707) and prostate cancer data (area under curve = 0.8462) show that DL-GRS has the best prediction performance.

The rs455192 was the most relevant locus for BCR ( p  = 2.496 × 10^–6) in our study.

Hsieh, Ai-Ru,Luo, Yi-Ling,Bao, Bo-Ying,Chou, Tzu-Chieh, 2024, Comparative analysis of genetic risk scores for predicting biochemical recurrence in prostate cancer patients after radical prostatectomy, BioMed Central

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