Further exploration of cardiac channelopathy and cardiomyopathy genes in stillbirth

Author:

Merc Maja Dolanc1ORCID,Kotnik Urška23,Peterlin Borut23,Lovrecic Luca23

Affiliation:

1. Division of Gynecology and Obstetrics Department of Perinatology University Medical Centre Ljubljana Ljubljana Slovenia

2. Clinical Institute for Genomic Medicine University Medical Centre Ljubljana Ljubljana Slovenia

3. Faculty of Medicine University of Ljubljana Ljubljana Slovenia

Abstract

AbstractObjectiveTo explore genetic variation including whole genome copy number variation and sequence analysis of 98 genes associated with pediatric or adult cardiomyopathies, cardiac channelopathies, and sudden death in an unexplained intrauterine fetal death cohort.MethodsThe study population included 55 stillbirth cases that remained unexplained after thorough postmortem examination, excluding maternal, fetal, and placental causes of stillbirth. Molecular karyotyping was performed in 55 cases and the trio exome sequencing approach was applied in 19 cases.ResultsThe analysis revealed six rare variants with predicted effects on protein function in six genes (CASQ2, DSC2, KCNE1, LDB3, MYH6, and SCN5A) previously reported in cases of stillbirth or severe early onset pediatric cardiac related phenotypes. When applying strict American College of Genetics and Genomics classification guidelines, these are still variants of uncertain significance.ConclusionsSeveral potentially stillbirth‐related genetic variants were detected in our cohort, adding to the growing literature on cardiac phenotype gene variation in stillbirth. However, the mechanisms of action, gene‐gene interaction, and contribution of the uterine environment are still to be deciphered. In order to advance our knowledge of the genetics of unexplained fetal death, there is an evident need for international collaboration and field standardization.

Publisher

Wiley

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