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Genome-wide association study of heart rate and its variability in Hispanic/Latino cohorts.

Citation
Kerr, K. F., et al. “Genome-Wide Association Study Of Heart Rate And Its Variability In Hispanic/Latino Cohorts.”. Heart Rhythm, pp. 1675-1684.
Center UCSD-UCLA
Author Kathleen F Kerr, Christy L Avery, Henry J Lin, Laura M Raffield, Qian S Zhang, Brian L Browning, Sharon R Browning, Matthew P Conomos, Stephanie M Gogarten, Cathy C Laurie, Tamar Sofer, Timothy A Thornton, Chancellor Hohensee, Rebecca D Jackson, Charles Kooperberg, Yun Li, Raúl Méndez-Giráldez, Marco Perez V, Ulrike Peters, Alexander P Reiner, Zhu-Ming Zhang, Jie Yao, Nona Sotoodehnia, Kent D Taylor, Xiuqing Guo, Leslie A Lange, Elsayed Z Soliman, James G Wilson, Jerome I Rotter, Susan R Heckbert, Deepti Jain, Eric A Whitsel
Keywords Autonomic nervous system, Electrocardiogram, Epidemiology, Genetic association studies, Ion channels/membrane transport
Abstract

BACKGROUND: Although time-domain measures of heart rate variability (HRV) are used to estimate cardiac autonomic tone and disease risk in multiethnic populations, the genetic epidemiology of HRV in Hispanics/Latinos has not been characterized.

OBJECTIVE: The purpose of this study was to conduct a genome-wide association study of heart rate (HR) and its variability in the Hispanic Community Health Study/Study of Latinos, Multi-Ethnic Study of Atherosclerosis, and Women's Health Initiative Hispanic SNP-Health Association Resource project (n = 13,767).

METHODS: We estimated HR (bpm), standard deviation of normal-to-normal interbeat intervals (SDNN, ms), and root mean squared difference in successive, normal-to-normal interbeat intervals (RMSSD, ms) from resting, standard 12-lead ECGs. We estimated associations between each phenotype and 17 million genotyped or imputed single nucleotide polymorphisms (SNPs), accounting for relatedness and adjusting for age, sex, study site, and ancestry. Cohort-specific estimates were combined using fixed-effects, inverse-variance meta-analysis. We investigated replication for select SNPs exceeding genome-wide (P <5 × 10) or suggestive (P <10) significance thresholds.

RESULTS: Two genome-wide significant SNPs replicated in a European ancestry cohort, 1 one for RMSSD (rs4963772; chromosome 12) and another for SDNN (rs12982903; chromosome 19). A suggestive SNP for HR (rs236352; chromosome 6) replicated in an African-American cohort. Functional annotation of replicated SNPs in cardiac and neuronal tissues identified potentially causal variants and mechanisms.

CONCLUSION: This first genome-wide association study of HRV and HR in Hispanics/Latinos underscores the potential for even modestly sized samples of non-European ancestry to inform the genetic epidemiology of complex traits.

Year of Publication
2017
Journal
Heart rhythm
Volume
14
Issue
11
Number of Pages
1675-1684
Date Published
12/2017
ISSN Number
1556-3871
DOI
10.1016/j.hrthm.2017.06.018
Alternate Journal
Heart Rhythm
PMID
28610988
PMCID
PMC5671896
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