Estimating the Posttest Probability of Long QT Syndrome Diagnosis for Rare KCNH2 Variants

Krystian Kozek; Yuko Wada; Luca Sala; Isabelle Denjoy; Christian Egly; Matthew J O'Neill; Takeshi Aiba; Wataru Shimizu; Naomasa Makita; Taisuke Ishikawa; Lia Crotti; Carla Spazzolini; Maria-Christina Kotta; Federica Dagradi; Silvia Castelletti; Matteo Pedrazzini; Massimiliano Gnecchi; Antoine Leenhardt; Joe-Elie Salem; Seiko Ohno; Yi Zuo; Andrew M Glazer; Jonathan D Mosley; Dan M Roden; Bjorn C Knollmann; Jeffrey D Blume; Fabrice Extramiana; Peter J Schwartz; Minoru Horie; Brett M Kroncke

doi:10.1161/CIRCGEN.120.003289

Estimating the Posttest Probability of Long QT Syndrome Diagnosis for Rare KCNH2 Variants

Circ Genom Precis Med. 2021 Aug;14(4):e003289. doi: 10.1161/CIRCGEN.120.003289. Epub 2021 Jul 26.

Authors

Krystian Kozek¹, Yuko Wada^{1

2}, Luca Sala³, Isabelle Denjoy⁴, Christian Egly¹, Matthew J O'Neill¹, Takeshi Aiba⁵, Wataru Shimizu⁶, Naomasa Makita^{5

7}, Taisuke Ishikawa⁷, Lia Crotti^{3

8

9

10}, Carla Spazzolini⁹, Maria-Christina Kotta, Federica Dagradi⁹, Silvia Castelletti⁹, Matteo Pedrazzini³, Massimiliano Gnecchi^{11

12}, Antoine Leenhardt^{4

13}, Joe-Elie Salem^{14

15}, Seiko Ohno^{2

5}, Yi Zuo¹⁶, Andrew M Glazer¹, Jonathan D Mosley^{1

16

17}, Dan M Roden^{1

16}, Bjorn C Knollmann¹, Jeffrey D Blume, Fabrice Extramiana^{4

13}, Peter J Schwartz^{3

9}, Minoru Horie², Brett M Kroncke¹

Affiliations

¹ Vanderbilt Center for Arrhythmia Research and Therapeutics (VanCART), Departments of Medicine & Pharmacology (K.K., Y.W., C.E., M.J.O., A.M.G., J.D.M., D.M.R., B.C.K., B.M.K.), Vanderbilt University Medical Center, Nashville, TN.
² Department of Cardiovascular Medicine, Shiga University of Medical Science, Otsu, Japan (Y.W., S.O., M.H.).
³ Laboratory of Cardiovascular Genetics, Istituto Auxologico Italiano IRCCS, Cusano Milanino, Italy (L.S., L.C., C.K., M.P., P.J.S.).
⁴ CNMR Maladies Cardiaques Héréditaires Rares, AP-HP, Hôpital Bichat, Paris, France (I.D., A.L., F.E.).
⁵ Department of Cardiovascular Medicine (T.A., N.M., S.O.), National Cerebral and Cardiovascular Center, Suita.
⁶ Department of Cardiovascular Medicine, Graduate School of Medicine, Nippon Medical School, Tokyo, Japan (W.S.).
⁷ 7Omics Research Center (N.M., T.I.), National Cerebral and Cardiovascular Center, Suita.
⁸ Department of Cardiovascular, Neural & Metabolic Sciences, San Luca Hospital (L.C.), Istituto Auxologico Italiano IRCCS.
⁹ Center for Cardiac Arrhythmias of Genetic Origin (L.C., C.S., F.D., S.C., P.J.S.), Istituto Auxologico Italiano IRCCS.
¹⁰ Department of Medicine and Surgery, University Milano Bicocca, Milan (L.C.).
¹¹ Department of Molecular Medicine, Unit of Cardiology, University of Pavia (M.G.).
¹² Intensive Cardiac Care Unit and Lab of Experimental Cardiology for Cell and Molecular Therapy, Fondazione IRCCS Policlinico San Matteo, Pavia, Italy (M.G.).
¹³ University de Paris (A.L., F.E.).
¹⁴ Division of Cardiovascular Medicine, Cardio-oncology Program (J.-E.S.), Vanderbilt University Medical Center, Nashville, TN.
¹⁵ Sorbonne Université, INSERM CIC-1901, AP-HP, Department of Pharmacology, Regional Pharmacovigilance Center, Pitié-Salpêtrière Hospital, Paris, France (J.-E.S.).
¹⁶ Department of Biostatistics (Y.Z., J.D.M., D.M.R.), Vanderbilt University, Nashville, TN.
¹⁷ Biomedical Informatics (J.D.M.), Vanderbilt University, Nashville, TN.

Abstract

Background: The proliferation of genetic profiling has revealed many associations between genetic variations and disease. However, large-scale phenotyping efforts in largely healthy populations, coupled with DNA sequencing, suggest variants currently annotated as pathogenic are more common in healthy populations than previously thought. In addition, novel and rare variants are frequently observed in genes associated with disease both in healthy individuals and those under suspicion of disease. This raises the question of whether these variants can be useful predictors of disease. To answer this question, we assessed the degree to which the presence of a variant in the cardiac potassium channel gene KCNH2 was diagnostically predictive for the autosomal dominant long QT syndrome.

Methods: We estimated the probability of a long QT diagnosis given the presence of each KCNH2 variant using Bayesian methods that incorporated variant features such as changes in variant function, protein structure, and in silico predictions. We call this estimate the posttest probability of disease. Our method was applied to over 4000 individuals heterozygous for 871 missense or in-frame insertion/deletion variants in KCNH2 and validated against a separate international cohort of 933 individuals heterozygous for 266 missense or in-frame insertion/deletion variants.

Results: Our method was well-calibrated for the observed fraction of heterozygotes diagnosed with long QT syndrome. Heuristically, we found that the innate diagnostic information one learns about a variant from 3-dimensional variant location, in vitro functional data, and in silico predictors is equivalent to the diagnostic information one learns about that same variant by clinically phenotyping 10 heterozygotes. Most importantly, these data can be obtained in the absence of any clinical observations.

Conclusions: We show how variant-specific features can inform a prior probability of disease for rare variants even in the absence of clinically phenotyped heterozygotes.

Keywords: genetic variation; heterozygotes; ion channel; long QT syndrome; phenotype.

Publication types

Research Support, N.I.H., Extramural
Research Support, Non-U.S. Gov't

MeSH terms

ERG1 Potassium Channel*
Heterozygote*
Humans
INDEL Mutation*
Long QT Syndrome* / diagnosis
Long QT Syndrome* / genetics
Mutation, Missense*

Substances

ERG1 Potassium Channel
KCNH2 protein, human

Abstract

Publication types

MeSH terms

Substances

Grants and funding