December 20, 2021Open Access

De novo mutations in childhood cases of sudden unexplained death that disrupt intracellular Ca 2+ regulation

Q: What is the clinical evidence from this study?

Study design: Case-Control. Population: Sudden unexplained death in childhood (SUDC) (n=124). Intervention: Whole-exome sequencing for de novo mutations vs. Healthy external control trios and internal control trios. Primary outcome: Enrichment of nonsynonymous de novo mutations in genes associated with cardiac and seizure disorders (OR 9.76, p=2.15 × 10^-4).

Key Result

Nonsynonymous de novo mutations in genes associated with cardiac and seizure disorders were significantly enriched in children with sudden unexplained death compared to controls (OR 9.76).

Study Design

Type

Case-Control (n=124)

Multicenter

Yes

Structured PICO

What genetic risk factors contribute to sudden unexplained death in children?

Population

124 'trios' (decedent child and living parents) of childhood cases of sudden unexplained death (children ≥1 year of age)

Intervention

Whole-exome sequencing

Comparator

Controls

Outcome

Identification of genetic risk factors (de novo mutations)

De novo mutations in genes regulating calcium-related excitability in cardiomyocytes and neurons contribute to approximately 9% of sudden unexplained deaths in children over 1 year of age.

Main Result

Effect estimate: OR 9.76

p-value: p=2.15 × 10^-4

Limitations

Case ascertainment was not population-based, relying on referrals from bereaved parents, clinicians, or medical examiners.
Focus exclusively on unexplained deaths may limit comparability to recent population-based studies of sudden death.
De novo mutation calling pipeline relied on hard call QC thresholds and may have missed real contributory mutations.
Mosaicism analysis was primarily limited to DNA from blood rather than multiple organs.

Abstract

Significance Approximately 400 United States children 1 y of age and older die suddenly from unexplained causes annually. We studied whole-exome sequence data from 124 “trios” (decedent child and living parents) to identify genetic risk factors. Nonsynonymous mutations, mostly de novo (present in child but absent in both biological parents), were highly enriched in genes associated with cardiac and seizure disorders relative to controls, and contributed to 9% of deaths. We found significant overtransmission of loss-of-function or pathogenic missense variants in cardiac and seizure disorder genes. Most pathogenic variants were de novo in origin, highlighting the importance of trio studies. Many of these pathogenic de novo mutations altered a protein network regulating calcium-related excitability at submembrane junctions in cardiomyocytes and neurons.

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Cite This Study

Halvorsen et al. (Mon,) conducted a case-control in Sudden unexplained death in childhood (SUDC) (n=124). Whole-exome sequencing for de novo mutations vs. Healthy external control trios and internal control trios was evaluated on Enrichment of nonsynonymous de novo mutations in genes associated with cardiac and seizure disorders (OR 9.76, p=2.15 × 10^-4). Nonsynonymous de novo mutations in genes associated with cardiac and seizure disorders were significantly enriched in children with sudden unexplained death compared to controls (OR 9.76).

synapsesocial.com/papers/6a125389bb918b6e5b6714bd https://doi.org/https://doi.org/10.1073/pnas.2115140118

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