Selection, optimization and validation of ten chronic disease polygenic risk scores for clinical implementation in diverse US populations.
Niall J LennonLeah C KottyanChristopher KachulisNoura S Abul-HusnJoshua AriasGillian BelbinJennifer E BelowSonja I BerndtWendy K ChungJames J CiminoEllen Wright ClaytonJohn J ConnollyDavid R CrosslinOzan DikilitasDigna R Velez EdwardsQiPing FengMarissa FisherRobert R FreimuthTian Genull nullnull nullJoseph T GlessnerAdam S GordonCandace PattersonHakon H HakonarsonMaegan V HardenMargaret HarrJoel N HirschhornClive HoggartLi HsuMarguerite R IrvinGail P JarvikElizabeth W KarlsonAtlas KhanAmit KheraKrzysztof KirylukIftikhar J KulloKatie LarkinNita LimdiJodell E LinderRuth J F LoosYuan LuoEdyta MalolepszaTeri A ManolioLisa J MartinLi McCarthyElizabeth M McNallyJames B MeigsTesfaye B MershaJonathan D MosleyAnjene M AddingtonBahram NamjouNihal PaiLorenzo L PesceUlrike PetersJosh F PetersonCynthia A ProwsMegan J PuckelwartzMichael J BamshadDan M RodenElisabeth A RosenthalRobb RowleyKonrad Teodor SawickiDaniel J SchaidRoelof A J SmitJohanna L SmithJordan W SmollerMinta ThomasHemant TiwariDiana M ToledoNataraja Sarma VaitinadinDavid VeenstraTheresa L WalunasZhe WangWei-Qi WeiChunhua WengGeorgia L WiesnerXianyong YinEimear E KennyPublished in: Nature medicine (2024)
Polygenic risk scores (PRSs) have improved in predictive performance, but several challenges remain to be addressed before PRSs can be implemented in the clinic, including reduced predictive performance of PRSs in diverse populations, and the interpretation and communication of genetic results to both providers and patients. To address these challenges, the National Human Genome Research Institute-funded Electronic Medical Records and Genomics (eMERGE) Network has developed a framework and pipeline for return of a PRS-based genome-informed risk assessment to 25,000 diverse adults and children as part of a clinical study. From an initial list of 23 conditions, ten were selected for implementation based on PRS performance, medical actionability and potential clinical utility, including cardiometabolic diseases and cancer. Standardized metrics were considered in the selection process, with additional consideration given to strength of evidence in African and Hispanic populations. We then developed a pipeline for clinical PRS implementation (score transfer to a clinical laboratory, validation and verification of score performance), and used genetic ancestry to calibrate PRS mean and variance, utilizing genetically diverse data from 13,475 participants of the All of Us Research Program cohort to train and test model parameters. Finally, we created a framework for regulatory compliance and developed a PRS clinical report for return to providers and for inclusion in an additional genome-informed risk assessment. The initial experience from eMERGE can inform the approach needed to implement PRS-based testing in diverse clinical settings.