Genetic variant burden and adverse outcomes in pediatric cardiomyopathy

Background Previous genetic research in pediatric cardiomyopathy (CM) has focused on pathogenic variants for diagnostic purposes, with limited data evaluating genotype-outcome correlations. We explored whether greater genetic variant burden (pathogenic or variants of unknown significance, VUS) corre...

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Bibliographic Details
Published in:Pediatric research 2021-05, Vol.89 (6), p.1470-1476
Main Authors: Burstein, Danielle S., Gaynor, J. William, Griffis, Heather, Ritter, Alyssa, Connor, Matthew J. O’, Rossano, Joseph W., Lin, Kimberly Y., Ahrens-Nicklas, Rebecca C.
Format: Article
Language:English
Subjects:
Adolescent
Cardiomyopathies - genetics
Cardiomyopathy
Child
Child, Preschool
Clinical outcomes
Clinical Research Article
Female
Genetic Predisposition to Disease
Genotype
Humans
Infant
Infant, Newborn
Male
Medicine
Medicine & Public Health
Pediatric Surgery
Pediatrics
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Summary:Background Previous genetic research in pediatric cardiomyopathy (CM) has focused on pathogenic variants for diagnostic purposes, with limited data evaluating genotype-outcome correlations. We explored whether greater genetic variant burden (pathogenic or variants of unknown significance, VUS) correlates with worse outcomes. Methods Children with dilated CM (DCM) and hypertrophic CM (HCM) who underwent multigene testing between 2010 and 2018 were included. Composite endpoint was freedom from major adverse cardiac event (MACE). Results Three hundred and thirty-eight subjects were included [49% DCM, median age 5.7 (interquartile range (IQR) 0.2–13.4) years, 51% HCM, median age 3.0 (IQR 0.1–12.5) years]. Pathogenic variants alone were not associated with MACE in either cohort (DCM p  = 0.44; HCM p  = 0.46). In DCM, VUS alone [odds ratio (OR) 4.0, 95% confidence interval (CI) 1.9–8.3] and in addition to pathogenic variants (OR 5.2, 95% CI 1.7–15.9) was associated with MACE. The presence of VUS alone or in addition to pathogenic variants were not associated with MACE in HCM ( p  = 0.22 and p  = 0.33, respectively). Conclusion Increased genetic variant burden (pathogenic variants and VUS) is associated with worse clinical outcomes in DCM but not HCM. Genomic variants that influence DCM onset may be distinct from those driving disease progression, highlighting the potential value of universal genetic testing to improve risk stratification. Impact In pediatric CM, inconsistent findings historically have been shown between genotype and phenotype severity when only pathogenic variants have been considered. Increased genetic variant burden (including both pathogenic variants and VUS) is associated with worse clinical outcomes in DCM but not HCM. Genomic variants that influence CM onset may be distinct from those variants that drive disease progression and influence outcomes in phenotype-positive individuals. Incorporation of both pathogenic variants and VUS may improve risk stratification models in pediatric CM.
ISSN:0031-3998
1530-0447
DOI:10.1038/s41390-020-1101-5