2013
DOI: 10.1161/circep.113.000618
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Arrhythmia Phenotype During Fetal Life Suggests Long-QT Syndrome Genotype

Abstract: Background Fetal arrhythmias characteristic of long QT syndrome (LQTS) include torsades de pointes (TdP) and/or 2° atrioventricular block (AVB), but sinus bradycardia, defined as fetal heart rate <3% for gestational age, is most common. We hypothesized that prenatal rhythm phenotype might predict LQTS genotype and facilitate improved risk stratification and management. Method and Results Records of subjects exhibiting LQTS fetal arrhythmias were reviewed. Fetal echocardiograms, neonatal ECG, and genetic test… Show more

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Cited by 60 publications
(56 citation statements)
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“…Regarding phenotype, our data reveal that the mean third trimester intrauterine heart rates of LQT1 fetuses correlate with neonatal heart rate, as well as show association with postnatal cardiac phenotype (QTc and arrhythmia). Importantly, although sinus bradycardia is often described as a rather benign manifestation, with a favorable outcome when treated with β-blockers, [13][14][15]25 it is evident from the present study that isolated sinus bradycardia may also be the presenting symptom of a most severe form of LQTS (ie, double mutation carriage), Figure 6. Mean third trimester heart rates, stratified by specific genotype, and phenotype indicated by marker shapes (minus sign, no symptoms; ×, arrhythmia symptoms), related to different cutoffs (horizontal lines) representing obstetric standard for bradycardia (<110 beats per minute), reduced fetal heart rate (110-120 beats per minute), and the discussed cut-off for long-QT syndrome (LQTS) suspicion (≤133 beats per minute, ie, mean noncarrier heart rate −2 SD).…”
Section: Discussionmentioning
confidence: 67%
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“…Regarding phenotype, our data reveal that the mean third trimester intrauterine heart rates of LQT1 fetuses correlate with neonatal heart rate, as well as show association with postnatal cardiac phenotype (QTc and arrhythmia). Importantly, although sinus bradycardia is often described as a rather benign manifestation, with a favorable outcome when treated with β-blockers, [13][14][15]25 it is evident from the present study that isolated sinus bradycardia may also be the presenting symptom of a most severe form of LQTS (ie, double mutation carriage), Figure 6. Mean third trimester heart rates, stratified by specific genotype, and phenotype indicated by marker shapes (minus sign, no symptoms; ×, arrhythmia symptoms), related to different cutoffs (horizontal lines) representing obstetric standard for bradycardia (<110 beats per minute), reduced fetal heart rate (110-120 beats per minute), and the discussed cut-off for long-QT syndrome (LQTS) suspicion (≤133 beats per minute, ie, mean noncarrier heart rate −2 SD).…”
Section: Discussionmentioning
confidence: 67%
“…15 In a later study on the same cohort, 21/32 fetal cases presenting with isolated sinus bradycardia (defined as fetal heart rate less than the third percentile for gestational age and absence of atrioventricular block or ventricular tachycardia) were reported to be of LQT1 genotype. 13 In this present study including 110 mutation carriers from 2 LQT1 founder populations, fetal heart rate manifestations were clearly genotype dependent, ranging from mild in single mutation carriers to pronounced in double mutation carriers. Even within the single-mutations group, carriers of the p.R518X nonsense mutation (associated with a 50% KCNQ1 function-loss in vitro 23 ) presented with a tendency toward milder heart rate reduction and QTc prolongation than carriers of the dominant negative p.Y111C mutation (associated with >75% KCNQ1 function-loss in vitro 24 ).…”
Section: Genotype-phenotype Correlations In Fetal Lqt1mentioning
confidence: 58%
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