Polygenic Risk Score Improves Prediction of Primary Open Angle Glaucoma Onset in the Ocular Hypertension Treatment Study

Author:

Singh Rishabh K.,Zhao Yan,Elze Tobias,Fingert John,Gordon Mae,Kass Michael A.,Luo Yuyang,Pasquale Louis R.,Scheetz Todd,Segrè Ayellet V.,Wiggs Janey L.,Zebardast Nazlee

Abstract

AbstractObjective or PurposePrimary open-angle glaucoma (POAG) is a highly heritable disease with 127 identified risk loci. Polygenic risks score (PRS) offers a measure of aggregate genetic burden. In this study, we assess whether PRS improves risk stratification in patients with ocular hypertension.DesignA post-hoc analysis of the Ocular Hypertension Treatment Study (OHTS) data.Setting, Participants, and/or Controls1636 participants were followed from 1994 to 2020 across 22 sites. The PRS was computed for 1009 OHTS participants using summary statistics from largest cross-ancestry POAG metanalysis with weights trained using 8,813,496 variants from 488,395 participants in the UK Biobank.Methods, Interventions, or TestingSurvival regression analysis, with endpoint as development of POAG, predicted disease onset from PRS incorporating baseline covariates.Main Outcomes and MeasuresOutcome measures were hazard ratios for POAG onset. Concordance index and time-dependent AUC were used to compare the predictive performance of multivariable Cox-Proportional Hazards models.ResultsMean PRS was significantly higher for POAG-converters (0.24 ± 0.95) than for non-converters (- 0.12 ± 1.00) (p < 0.01). POAG risk increased 1.36% with each higher PRS decile, with conversion ranging from 9.5% in the lowest PRS decile to 21.8% in the highest decile. Comparison of low-and high-risk PRS tertiles showed a 1.8-fold increase in 20-year POAG risk for participants of European and African ancestries (p<0.01). In the subgroup randomized to delayed treatment, each increase in PRS decile was associated with a 0.52-year decrease in age at diagnosis, (p=0.05). No significant linear relationship between PRS and age at POAG diagnosis was present in the early treatment group. Prediction models significantly improved with the addition of PRS as a covariate (C-index = 0.77) compared to OHTS baseline model (C-index=0.75) (p<0.01). One standard deviation higher PRS conferred a mean hazard ratio of 1.25 (CI=[1.13, 1.44]) for POAG onset.ConclusionsHigher PRS is associated with increased risk for, and earlier development of POAG in patients with ocular hypertension. Early treatment may mitigate the risk from high genetic burden, delaying clinically detectable disease by up to 5.2 years. The inclusion of a PRS improves the prediction of POAG onset.

Publisher

Cold Spring Harbor Laboratory

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