Genomic Autopsy of Sudden Deaths in Young Individuals

医学 尸检 猝死 队列 基因检测 心源性猝死 死因 年轻人 内科学 疾病
作者
Gregory Webster,Megan J. Puckelwartz,Lorenzo L. Pesce,Lisa Dellefave-Castillo,Carlos G. Vanoye,Franck Potet,Patrick Page,Samuel Kearns,Tess D. Pottinger,Steven M. White,Ponni Arunkumar,Rachael Olson,Amber Kofman,Nora Ibrahim,Alexander Ing,Casey Brew,Kai Lee Yap,Sabah Kadri,Alfred L. George,Elizabeth M. McNally
出处
期刊:JAMA Cardiology [American Medical Association]
卷期号:6 (11): 1247-1247 被引量:15
标识
DOI:10.1001/jamacardio.2021.2789
摘要

Postmortem genetic testing of young individuals with sudden death has previously identified pathogenic gene variants. However, prior studies primarily considered highly penetrant monogenic variants, often without detailed decedent and family clinical information.To assess genotype and phenotype risk in a diverse cohort of young decedents with sudden death and their families.Pathological and whole-genome sequence analysis was conducted in a cohort referred from a national network of medical examiners. Cases were accrued prospectively from May 2015 to March 2019 across 24 US states. Analysis began September 2016 and ended November 2020.Evaluation of autopsy and clinical data integrated with whole-genome sequence data and family member evaluation.A total of 103 decedents (mean [SD] age at death, 23.7 [11.9] years; age range, 1-44 years), their surviving family members, and 140 sex- and genetic ancestry-matched controls were analyzed. Among 103 decedents, autopsy and clinical data review categorized 36 decedents with postmortem diagnoses, 23 decedents with findings of uncertain significance, and 44 with sudden unexplained death. Pathogenic/likely pathogenic (P/LP) genetic variants in arrhythmia or cardiomyopathy genes were identified in 13 decedents (12.6%). A multivariable analysis including decedent phenotype, ancestry, and sex demonstrated that younger decedents had a higher burden of P/LP variants and select variants of uncertain significance (effect size, -1.64; P = .001). These select, curated variants of uncertain significance in cardiac genes were more common in decedents than controls (83 of 103 decedents [86%] vs 100 of 140 controls [71%]; P = .005), and decedents harbored more rare cardiac variants than controls (2.3 variants per individual vs 1.8 in controls; P = .006). Genetic testing of 31 parent-decedent trios and 14 parent-decedent dyads revealed 8 transmitted P/LP variants and 1 de novo P/LP variant. Incomplete penetrance was present in 6 of 8 parents who transmitted a P/LP variant.Whole-genome sequencing effectively identified P/LP variants in cases of sudden death in young individuals, implicating both arrhythmia and cardiomyopathy genes. Genomic analyses and familial phenotype association suggest potentially additive, oligogenic risk mechanisms for sudden death in this cohort.

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