The Clinical Utility of the BMD-related comprehensive Genome-wide polygenic score in identifying individuals with a high risk of osteoporotic fractures

Xiao, Xiangxue; Wu, Qing

doi:10.1101/2022.11.16.22282416

Cited by 1 publication

(7 citation statements)

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“…Implementing individual-level genome-wide PGSs summarizing the underlying genetic predisposition of certain diseases in the clinical setting holds excellent promise. Previously, we developed and internally validated two genome-wide BMD-related PGSs using data from the UKB cohort [ 17 ]. Our findings indicated that both PGSs were significantly associated with incident fractures, even after being adjusted for FRAX clinical risk factors [ 17 ].…”

Section: Discussionmentioning

confidence: 99%

“…Previously, we developed and internally validated two genome-wide BMD-related PGSs using data from the UKB cohort [ 17 ]. Our findings indicated that both PGSs were significantly associated with incident fractures, even after being adjusted for FRAX clinical risk factors [ 17 ]. In the current study, we replicated the two BMD-associated PGSs from previous work [ 17 ] and additionally derived a third PGS—metaPGS combining the effect of the two established PGSs and evaluated their predictive effect in an independent WHI postmenopausal women sample.…”

Section: Discussionmentioning

confidence: 99%

“…PGS _ FNBMD ldpred and PGS _ TBBMD ldpred were quantified using LDpred2 with optimal hyperparameters determined previously [ 17 ]. For femoral neck BMD and total body BMD, ρ thresholds of 0.03 and 0.13, respectively, were used to derive the genome-wide PGSs for each individual in the WHI cohort.…”

Section: Methodsmentioning

confidence: 99%

“…Moreover, extensive cohort resources have enabled the genetic prediction of such heritable clinical risk factors from genotypes through polygenic scores (PGS), which capture information from many single nucleotide polymorphisms (SNPs) assayed from genome-wide genotyping. We previously developed and validated two genome-wide PGSs related to the femoral neck ( PGS _ FNBMD ldpred ) and total body BMD ( PGS _ TBBMD ldpred ) in the UK Biobank (UKB) cohort [ 17 ]. Both genome-wide PGS was proven to be significantly associated with incident fracture risk, even after accounting for FRAX clinical risk factors [ 17 ] However, the UKB participants were generally younger and healthier than the general population.…”

Section: Introductionmentioning

confidence: 99%

“…We previously developed and validated two genome-wide PGSs related to the femoral neck ( PGS _ FNBMD ldpred ) and total body BMD ( PGS _ TBBMD ldpred ) in the UK Biobank (UKB) cohort [ 17 ]. Both genome-wide PGS was proven to be significantly associated with incident fracture risk, even after accounting for FRAX clinical risk factors [ 17 ] However, the UKB participants were generally younger and healthier than the general population. Our prior findings thus lack generalizability outside of the UKB cohort.…”

Section: Introductionmentioning

confidence: 99%

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Validation of a genome-wide polygenic score in improving fracture risk assessment beyond the FRAX tool in the Women’s Health Initiative study

Xiao

2023

PLoS ONE

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Background Previous study has established two polygenic scores (PGSs) related to femoral neck bone mineral density (BMD) (PGS_FNBMDldpred) and total body BMD (PGS_TBBMDldpred) that are associated with fracture risk. However, these findings have not yet been externally validated in an independent cohort. Objectives This study aimed to validate the predictive performance of the two established PGSs and to investigate whether adding PGSs to the Fracture Risk Assessment Tool (FRAX) improves the predictive ability of FRAX in identifying women at high risk of major osteoporotic fracture (MOF) and hip fractures (HF). Methods The study used the Women’s Health Initiative (WHI) cohort of 9,000 postmenopausal women of European ancestry. Cox Proportional Hazard Models were used to assess the association between each PGS and MOF/HF risk. Four models were formulated to investigate the effect of adding PGSs to the FRAX risk factors: (1) Base model: FRAX risk factors; (2) Base model + PGS_FNBMDldpred; (3) Base model + PGS_TBBMDldpred; (4) Base model + metaPGS. The reclassification ability of models with PGS was further assessed using the Net Reclassification Improvement (NRI) and the Integrated discrimination improvement (IDI). Results The study found that the PGSs were not significantly associated with MOF or HF after adjusting for FRAX risk factors. The FRAX base model showed moderate discrimination of MOF and HF, with a C-index of 0.623 (95% CI, 0.609 to 0.641) and 0.702 (95% CI, 0.609 to 0.718), respectively. Adding PGSs to the base FRAX model did not improve the ability to discriminate MOF or HF. Reclassification analysis showed that compared to the model without PGS, the model with PGS_TBBMDldpred (1.2%, p = 0.04) and metaPGS (1.7%, p = 0.05) improve the reclassification of HF, but not MOF. Conclusions The findings suggested that incorporating genetic information into the FRAX tool has minimal improvement in predicting HF risk for elderly Caucasian women. These results highlight the need for further research to identify other factors that may contribute to fracture risk in elderly Caucasian women.

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Section: Discussionmentioning

confidence: 99%