Monogenic and Polygenic Contributions to QTc Prolongation in the Population

Nauffal, Victor; Morrill, Valerie N.; Jurgens, Sean J.; Choi, Seung Hoan; Hall, Amelia Weber; Weng, Lu‐Chen; Halford, Jennifer L; Austin‐Tse, Christina; Haggerty, Christopher M.; Harris, Stephanie; Wong, Eugene; Alonso, Álvaro; Arking, Dan E.; Benjamin, Emelia J.; Boerwinkle, Eric; Min, Yuan‐I; Correa, Adolfo; Fornwalt, Brandon K.; Heckbert, Susan R.; Kooperberg, Charles; Lin, Henry J.; Loos, Ruth J.F.; Rice, Kenneth; Gupta, Namrata; Blackwell, Thomas W.; Mitchell, Braxton D.; Morrison, Alanna C.; Psaty, Bruce M.; Post, Wendy S.; Redline, Susan; Rehm, Heidi L.; Rich, Stephen S.; Rotter, Jerome I.; Soliman, Elsayed Z.; Sotoodehnia, Nona; Lunetta, Kathryn L.; Ellinor, Patrick T.; Lubitz, Steven A.

doi:10.1161/circulationaha.121.057261

Cited by 17 publications

(15 citation statements)

References 34 publications

(45 reference statements)

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“…23 SNPs with low imputation quality (R 2 <0.3) were filtered. We applied the QTc PRS developed by Nauffal et al 24 using the score function in PLINK to calculate the PRS from the imputed genetic data.…”

Section: Methodsmentioning

confidence: 99%

Detection of distant familial relatedness in biobanks for identification of undiagnosed carriers of a Mendelian disease variant: application to Long QT syndrome

Lancaster

Chen

Shoemaker

et al. 2023

Preprint

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Importance: The diagnosis and study of rare genetic disease is often limited to referral populations, leading to underdiagnosis and a biased assessment of penetrance and phenotype. Objective: To develop a generalizable method of genotype inference based on distant relatedness and to deploy this to identify undiagnosed Type 5 Long QT Syndrome (LQT5) rare variant carriers in a non-referral population. Participants: We identified 9 LQT5 probands and 3 first-degree relatives referred to a single Genetic Arrhythmia clinic, each carrying D76N (p.Asp76Asn), the most common variant implicated in LQT5. The non-referral population consisted of 69,879 ancestry-matched subjects in BioVU, a large biobank that links electronic health records to dense array data. Participants were enrolled from 2007-2022. Data analysis was performed in 2022. Exposures: We developed and applied a novel approach to genotype inference (Distant Relatedness for Identification and Variant Evaluation, or DRIVE) to identify shared, identical-by-descent (IBD) large chromosomal segments in array data. Main Outcomes and Measures: We sought to establish genetic relatedness among the probands and to use genomic segments underlying D76N to identify other potential carriers in BioVU. We then further studied the role of D76N in LQT5 pathogenesis. Results: Genetic reconstruction of pedigrees and distant relatedness detection among clinic probands using DRIVE revealed shared recent common ancestry and identified a single long shared haplotype. Interrogation of the non-referral population in BioVU identified a further 23 subjects sharing this haplotype, and sequencing confirmed D76N carrier status in 22, all previously undiagnosed with LQT5. The QTc was prolonged in D76N carriers compared to BioVU controls, with 40% penetrance of QTc ≥ 480 msec. Among D76N carriers, a QTc polygenic score was additively associated with QTc prolongation. Conclusions and Relevance: Detection of IBD shared chromosomal segments around D76N enabled identification of distantly related and previously undiagnosed rare-variant carriers, demonstrated the contribution of polygenic risk to monogenic disease penetrance, and further established LQT5 as a primary arrhythmia disorder. Analysis of shared chromosomal regions spanning disease-causing mutations can identify undiagnosed cases of genetic diseases.

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Section: Methodsmentioning

confidence: 99%

Detection of distant familial relatedness in biobanks for identification of undiagnosed carriers of a Mendelian disease variant: application to Long QT syndrome

Lancaster

Chen

Shoemaker

et al. 2023

Preprint

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“…HAGS for all genes across different cell types using H3K27ac HiChIP interactions are calculated. Interestingly, two risk genes (NOS1AP and KCNH2) reported in ( 35–37 ) were ranked 1st and 12th in HAEC heart cell line, respectively. In contrast, NOS1AP ranked 3rd while KCNH2 ranked 11 729th in PAEC lung cell line, NOS1AP and KCNH2 all ranked 4179th in HARA lung cell line due to no overlapped HiChIP interactions.…”

Section: Database Featuresmentioning

confidence: 99%

“…A QT interval duration study ( 35 ) is taken as an illustrative example. HAGS for all genes across different cell types using H3K27ac HiChIP interactions are calculated.…”

Section: Database Featuresmentioning

confidence: 99%

HiChIPdb: a comprehensive database of HiChIP regulatory interactions

Zeng

Yin

et al. 2022

Nucleic Acids Research

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Elucidating the role of 3D architecture of DNA in gene regulation is crucial for understanding cell differentiation, tissue homeostasis and disease development. Among various chromatin conformation capture methods, HiChIP has received increasing attention for its significant improvement over other methods in profiling of regulatory (e.g. H3K27ac) and structural (e.g. cohesin) interactions. To facilitate the studies of 3D regulatory interactions, we developed a HiChIP interactions database, HiChIPdb (http://health.tsinghua.edu.cn/hichipdb/). The current version of HiChIPdb contains ∼262M annotated HiChIP interactions from 200 high-throughput HiChIP samples across 108 cell types. The functionalities of HiChIPdb include: (i) standardized categorization of HiChIP interactions in a hierarchical structure based on organ, tissue and cell line and (ii) comprehensive annotations of HiChIP interactions with regulatory genes and GWAS Catalog SNPs. To the best of our knowledge, HiChIPdb is the first comprehensive database that utilizes a unified pipeline to map the functional interactions across diverse cell types and tissues in different resolutions. We believe this database has the potential to advance cutting-edge research in regulatory mechanisms in development and disease by removing the barrier in data aggregation, preprocessing, and analysis.

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“…LQTS is an inherited cardiac arrhythmia with congenital and drug-induced presentations defined by a prolongation of the corrected QT interval on an electrocardiogram. 1, 2 The QT interval, corrected for heart rate (QTc), is 30-40% heritable, 3, 4 with narrow-sense, autosomal common single nucleotide polymorphisms (SNP) contribution estimated around 20%; 5, 6 the SNP contribution to LQTS is similar, around 15%. 7 Until recently, LQTS had been thought of as largely a monogenic disorder with approximately 75% of congenital LQTS probands carrying a variant in one of three cardiac ion channel genes: KCNQ1 , KCNH2 , and SCN5A .…”

Section: Introductionmentioning

confidence: 99%

Generation of human induced pluripotent stem cell (hiPSC) lines from patients with extreme high and low polygenic scores for QT interval

Mitchell,

Ullah,

Vanags

et al. 2023

Preprint

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Long QT syndrome (LQTS) is an inherited cardiac arrhythmia syndrome with congenital and drug-induced presentations and known monogenic and polygenic contributions. LQTS represents a significant clinical challenge due to its complex genetic underpinning and propensity for fatal arrhythmias. In this study, we generated induced pluripotent stem cells (iPSCs) reprogrammed from peripheral blood mononuclear cells (PBMCs) of six patients with extreme polygenic scores for short and long corrected QT intervals. iPSC lines were rigorously validated for genomic integrity through karyotyping and targeted mutation analysis specific to a lengthened or shortened QT interval. Pluripotency was confirmed by expression of key markers TRA 1-60, TRA 1-81, SOX2, OCT4, NANOG, and REX1 via quantitative PCR and immunofluorescence. Subsequent cardiac induction successfully generated cardiomyocytes that were further characterized. This patient-specific approach will enable us to better understand variable expressivity and penetrance of LQTS. Rigorously validated iPSC lines serve as a vital resource for elucidating the molecular mechanisms underlying LQTS. Our study provides a robust and clinically relevant resource to facilitate our understanding the genetic and cellular complexity of LQTS.

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Monogenic and Polygenic Contributions to QTc Prolongation in the Population

Cited by 17 publications

References 34 publications

Detection of distant familial relatedness in biobanks for identification of undiagnosed carriers of a Mendelian disease variant: application to Long QT syndrome

Detection of distant familial relatedness in biobanks for identification of undiagnosed carriers of a Mendelian disease variant: application to Long QT syndrome

HiChIPdb: a comprehensive database of HiChIP regulatory interactions

Generation of human induced pluripotent stem cell (hiPSC) lines from patients with extreme high and low polygenic scores for QT interval

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