Multi-Ethnic Genome-Wide Association Study of Decomposed Cardioelectric Phenotypes Illustrates Strategies to Identify and Characterize Evidence of Shared Genetic Effects for Complex Traits

Antoine R. Baldassari; Colleen M. Sitlani; Heather M. Highland; Dan E. Arking; Steve Buyske; Dawood Darbar; Rahul Gondalia; Misa Graff; Xiuqing Guo; Susan R. Heckbert; Lucia A. Hindorff; Chani J. Hodonsky; Yii Der Ida Chen; Robert C. Kaplan; Ulrike Peters; Wendy Post; Alex P. Reiner; Jerome I. Rotter; Ralph V. Shohet; Amanda A. Seyerle; Nona Sotoodehnia; Ran Tao; Kent D. Taylor; Genevieve L. Wojcik; Jie Yao; Eimear E. Kenny; Henry J. Lin; Elsayed Z. Soliman; Eric A. Whitsel; Kari E. North; Charles Kooperberg; Christy L. Avery

doi:10.1161/CIRCGEN.119.002680

Multi-Ethnic Genome-Wide Association Study of Decomposed Cardioelectric Phenotypes Illustrates Strategies to Identify and Characterize Evidence of Shared Genetic Effects for Complex Traits

Antoine R. Baldassari, Colleen M. Sitlani, Heather M. Highland, Dan E. Arking, Steve Buyske, Dawood Darbar, Rahul Gondalia, Misa Graff, Xiuqing Guo, Susan R. Heckbert, Lucia A. Hindorff, Chani J. Hodonsky, Yii Der Ida Chen, Robert C. Kaplan, Ulrike Peters, Wendy Post, Alex P. Reiner, Jerome I. Rotter, Ralph V. Shohet, Amanda A. SeyerleNona Sotoodehnia, Ran Tao, Kent D. Taylor, Genevieve L. Wojcik, Jie Yao, Eimear E. Kenny, Henry J. Lin, Elsayed Z. Soliman, Eric A. Whitsel, Kari E. North, Charles Kooperberg, Christy L. Avery

Epidemiology & Population Health

Research output: Contribution to journal › Article › peer-review

3 Scopus citations

Abstract

Background: We examined how expanding electrocardiographic trait genome-wide association studies to include ancestrally diverse populations, prioritize more precise phenotypic measures, and evaluate evidence for shared genetic effects enabled the detection and characterization of loci. Methods: We decomposed 10 seconds, 12-lead electrocardiograms from 34 668 multi-ethnic participants (15% Black; 30% Hispanic/Latino) into 6 contiguous, physiologically distinct (P wave, PR segment, QRS interval, ST segment, T wave, and TP segment) and 2 composite, conventional (PR interval and QT interval) interval scale traits and conducted multivariable-adjusted, trait-specific univariate genome-wide association studies using 1000-G imputed single-nucleotide polymorphisms. Evidence of shared genetic effects was evaluated by aggregating meta-analyzed univariate results across the 6 continuous electrocardiographic traits using the combined phenotype adaptive sum of powered scores test. Results: We identified 6 novels (CD36, PITX2, EMB, ZNF592, YPEL2, and BC043580) and 87 known loci (adaptive sum of powered score test P<5×10^-9). Lead single-nucleotide polymorphism rs3211938 at CD36 was common in Blacks (minor allele frequency=10%), near monomorphic in European Americans, and had effects on the QT interval and TP segment that ranked among the largest reported to date for common variants. The other 5 novel loci were observed when evaluating the contiguous but not the composite electrocardiographic traits. Combined phenotype testing did not identify novel electrocardiographic loci unapparent using traditional univariate approaches, although this approach did assist with the characterization of known loci. Conclusions: Despite including one-third as many participants as published electrocardiographic trait genome-wide association studies, our study identified 6 novel loci, emphasizing the importance of ancestral diversity and phenotype resolution in this era of ever-growing genome-wide association studies.

Original language	English (US)
Pages (from-to)	E002680
Journal	Circulation. Genomic and precision medicine
Volume	13
Issue number	4
DOIs	https://doi.org/10.1161/CIRCGEN.119.002680
State	Published - Aug 1 2020

Keywords

cardiovascular diseases
electrophysiology
epidemiology
genome-wide association study
population

ASJC Scopus subject areas

Genetics
Cardiology and Cardiovascular Medicine
Genetics(clinical)

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1161/CIRCGEN.119.002680

Cite this

Baldassari, A. R., Sitlani, C. M., Highland, H. M., Arking, D. E., Buyske, S., Darbar, D., Gondalia, R., Graff, M., Guo, X., Heckbert, S. R., Hindorff, L. A., Hodonsky, C. J., Ida Chen, Y. D., Kaplan, R. C., Peters, U., Post, W., Reiner, A. P., Rotter, J. I., Shohet, R. V., ... Avery, C. L. (2020). Multi-Ethnic Genome-Wide Association Study of Decomposed Cardioelectric Phenotypes Illustrates Strategies to Identify and Characterize Evidence of Shared Genetic Effects for Complex Traits. Circulation. Genomic and precision medicine, 13(4), E002680. https://doi.org/10.1161/CIRCGEN.119.002680

Multi-Ethnic Genome-Wide Association Study of Decomposed Cardioelectric Phenotypes Illustrates Strategies to Identify and Characterize Evidence of Shared Genetic Effects for Complex Traits. / Baldassari, Antoine R.; Sitlani, Colleen M.; Highland, Heather M. et al.
In: Circulation. Genomic and precision medicine, Vol. 13, No. 4, 01.08.2020, p. E002680.

Research output: Contribution to journal › Article › peer-review

Baldassari, AR, Sitlani, CM, Highland, HM, Arking, DE, Buyske, S, Darbar, D, Gondalia, R, Graff, M, Guo, X, Heckbert, SR, Hindorff, LA, Hodonsky, CJ, Ida Chen, YD, Kaplan, RC, Peters, U, Post, W, Reiner, AP, Rotter, JI, Shohet, RV, Seyerle, AA, Sotoodehnia, N, Tao, R, Taylor, KD, Wojcik, GL, Yao, J, Kenny, EE, Lin, HJ, Soliman, EZ, Whitsel, EA, North, KE, Kooperberg, C & Avery, CL 2020, 'Multi-Ethnic Genome-Wide Association Study of Decomposed Cardioelectric Phenotypes Illustrates Strategies to Identify and Characterize Evidence of Shared Genetic Effects for Complex Traits', Circulation. Genomic and precision medicine, vol. 13, no. 4, pp. E002680. https://doi.org/10.1161/CIRCGEN.119.002680

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title = "Multi-Ethnic Genome-Wide Association Study of Decomposed Cardioelectric Phenotypes Illustrates Strategies to Identify and Characterize Evidence of Shared Genetic Effects for Complex Traits",

abstract = "Background: We examined how expanding electrocardiographic trait genome-wide association studies to include ancestrally diverse populations, prioritize more precise phenotypic measures, and evaluate evidence for shared genetic effects enabled the detection and characterization of loci. Methods: We decomposed 10 seconds, 12-lead electrocardiograms from 34 668 multi-ethnic participants (15% Black; 30% Hispanic/Latino) into 6 contiguous, physiologically distinct (P wave, PR segment, QRS interval, ST segment, T wave, and TP segment) and 2 composite, conventional (PR interval and QT interval) interval scale traits and conducted multivariable-adjusted, trait-specific univariate genome-wide association studies using 1000-G imputed single-nucleotide polymorphisms. Evidence of shared genetic effects was evaluated by aggregating meta-analyzed univariate results across the 6 continuous electrocardiographic traits using the combined phenotype adaptive sum of powered scores test. Results: We identified 6 novels (CD36, PITX2, EMB, ZNF592, YPEL2, and BC043580) and 87 known loci (adaptive sum of powered score test P<5×10-9). Lead single-nucleotide polymorphism rs3211938 at CD36 was common in Blacks (minor allele frequency=10%), near monomorphic in European Americans, and had effects on the QT interval and TP segment that ranked among the largest reported to date for common variants. The other 5 novel loci were observed when evaluating the contiguous but not the composite electrocardiographic traits. Combined phenotype testing did not identify novel electrocardiographic loci unapparent using traditional univariate approaches, although this approach did assist with the characterization of known loci. Conclusions: Despite including one-third as many participants as published electrocardiographic trait genome-wide association studies, our study identified 6 novel loci, emphasizing the importance of ancestral diversity and phenotype resolution in this era of ever-growing genome-wide association studies.",

keywords = "cardiovascular diseases, electrophysiology, epidemiology, genome-wide association study, population",

author = "Baldassari, {Antoine R.} and Sitlani, {Colleen M.} and Highland, {Heather M.} and Arking, {Dan E.} and Steve Buyske and Dawood Darbar and Rahul Gondalia and Misa Graff and Xiuqing Guo and Heckbert, {Susan R.} and Hindorff, {Lucia A.} and Hodonsky, {Chani J.} and {Ida Chen}, {Yii Der} and Kaplan, {Robert C.} and Ulrike Peters and Wendy Post and Reiner, {Alex P.} and Rotter, {Jerome I.} and Shohet, {Ralph V.} and Seyerle, {Amanda A.} and Nona Sotoodehnia and Ran Tao and Taylor, {Kent D.} and Wojcik, {Genevieve L.} and Jie Yao and Kenny, {Eimear E.} and Lin, {Henry J.} and Soliman, {Elsayed Z.} and Whitsel, {Eric A.} and North, {Kari E.} and Charles Kooperberg and Avery, {Christy L.}",

year = "2020",

month = aug,

day = "1",

doi = "10.1161/CIRCGEN.119.002680",

language = "English (US)",

volume = "13",

pages = "E002680",

journal = "Circulation. Genomic and precision medicine",

issn = "1942-325X",

publisher = "Lippincott Williams and Wilkins Ltd.",

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T1 - Multi-Ethnic Genome-Wide Association Study of Decomposed Cardioelectric Phenotypes Illustrates Strategies to Identify and Characterize Evidence of Shared Genetic Effects for Complex Traits

AU - Baldassari, Antoine R.

AU - Sitlani, Colleen M.

AU - Highland, Heather M.

AU - Arking, Dan E.

AU - Buyske, Steve

AU - Darbar, Dawood

AU - Gondalia, Rahul

AU - Graff, Misa

AU - Guo, Xiuqing

AU - Heckbert, Susan R.

AU - Hindorff, Lucia A.

AU - Hodonsky, Chani J.

AU - Ida Chen, Yii Der

AU - Kaplan, Robert C.

AU - Peters, Ulrike

AU - Post, Wendy

AU - Reiner, Alex P.

AU - Rotter, Jerome I.

AU - Shohet, Ralph V.

AU - Seyerle, Amanda A.

AU - Sotoodehnia, Nona

AU - Tao, Ran

AU - Taylor, Kent D.

AU - Wojcik, Genevieve L.

AU - Yao, Jie

AU - Kenny, Eimear E.

AU - Lin, Henry J.

AU - Soliman, Elsayed Z.

AU - Whitsel, Eric A.

AU - North, Kari E.

AU - Kooperberg, Charles

AU - Avery, Christy L.

PY - 2020/8/1

Y1 - 2020/8/1

N2 - Background: We examined how expanding electrocardiographic trait genome-wide association studies to include ancestrally diverse populations, prioritize more precise phenotypic measures, and evaluate evidence for shared genetic effects enabled the detection and characterization of loci. Methods: We decomposed 10 seconds, 12-lead electrocardiograms from 34 668 multi-ethnic participants (15% Black; 30% Hispanic/Latino) into 6 contiguous, physiologically distinct (P wave, PR segment, QRS interval, ST segment, T wave, and TP segment) and 2 composite, conventional (PR interval and QT interval) interval scale traits and conducted multivariable-adjusted, trait-specific univariate genome-wide association studies using 1000-G imputed single-nucleotide polymorphisms. Evidence of shared genetic effects was evaluated by aggregating meta-analyzed univariate results across the 6 continuous electrocardiographic traits using the combined phenotype adaptive sum of powered scores test. Results: We identified 6 novels (CD36, PITX2, EMB, ZNF592, YPEL2, and BC043580) and 87 known loci (adaptive sum of powered score test P<5×10-9). Lead single-nucleotide polymorphism rs3211938 at CD36 was common in Blacks (minor allele frequency=10%), near monomorphic in European Americans, and had effects on the QT interval and TP segment that ranked among the largest reported to date for common variants. The other 5 novel loci were observed when evaluating the contiguous but not the composite electrocardiographic traits. Combined phenotype testing did not identify novel electrocardiographic loci unapparent using traditional univariate approaches, although this approach did assist with the characterization of known loci. Conclusions: Despite including one-third as many participants as published electrocardiographic trait genome-wide association studies, our study identified 6 novel loci, emphasizing the importance of ancestral diversity and phenotype resolution in this era of ever-growing genome-wide association studies.

AB - Background: We examined how expanding electrocardiographic trait genome-wide association studies to include ancestrally diverse populations, prioritize more precise phenotypic measures, and evaluate evidence for shared genetic effects enabled the detection and characterization of loci. Methods: We decomposed 10 seconds, 12-lead electrocardiograms from 34 668 multi-ethnic participants (15% Black; 30% Hispanic/Latino) into 6 contiguous, physiologically distinct (P wave, PR segment, QRS interval, ST segment, T wave, and TP segment) and 2 composite, conventional (PR interval and QT interval) interval scale traits and conducted multivariable-adjusted, trait-specific univariate genome-wide association studies using 1000-G imputed single-nucleotide polymorphisms. Evidence of shared genetic effects was evaluated by aggregating meta-analyzed univariate results across the 6 continuous electrocardiographic traits using the combined phenotype adaptive sum of powered scores test. Results: We identified 6 novels (CD36, PITX2, EMB, ZNF592, YPEL2, and BC043580) and 87 known loci (adaptive sum of powered score test P<5×10-9). Lead single-nucleotide polymorphism rs3211938 at CD36 was common in Blacks (minor allele frequency=10%), near monomorphic in European Americans, and had effects on the QT interval and TP segment that ranked among the largest reported to date for common variants. The other 5 novel loci were observed when evaluating the contiguous but not the composite electrocardiographic traits. Combined phenotype testing did not identify novel electrocardiographic loci unapparent using traditional univariate approaches, although this approach did assist with the characterization of known loci. Conclusions: Despite including one-third as many participants as published electrocardiographic trait genome-wide association studies, our study identified 6 novel loci, emphasizing the importance of ancestral diversity and phenotype resolution in this era of ever-growing genome-wide association studies.

KW - cardiovascular diseases

KW - electrophysiology

KW - epidemiology

KW - genome-wide association study

KW - population

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JO - Circulation. Genomic and precision medicine

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Multi-Ethnic Genome-Wide Association Study of Decomposed Cardioelectric Phenotypes Illustrates Strategies to Identify and Characterize Evidence of Shared Genetic Effects for Complex Traits

Abstract

Keywords

ASJC Scopus subject areas

UN SDGs

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