28 July 2016: Articles 
A Neonate with Susceptibility to Long QT Syndrome Type 6 who Presented with Ventricular Fibrillation and Sudden Unexpected Infant Death
Challenging differential diagnosis, Rare disease, Educational Purpose (only if useful for a systematic review or synthesis)
Charles W. Sauer AEF , Krishelle L. Marc-Aurele AEFDOI: 10.12659/AJCR.898327
Am J Case Rep 2016; 17:544-548
Abstract
BACKGROUND: This is a case of a neonate with susceptibility to long QT syndrome (LQTS) who presented with a sudden unexpected infant death. Experts continue to debate whether universal electrocardiogram (ECG) screening of all newborns is feasible, practical, and cost-effective.
CASE REPORT: A 19-day-old neonate was found unresponsive by her mother. ECG showed ventricular fibrillation and a combination of a lidocaine drip plus multiple defibrillations converted the rhythm to normal sinus. Unfortunately, MRI brain imaging showed multiple infarcts and EEG showed burst suppression pattern with frequent seizures; life supportive treatment was stopped and the infant died. Genetic testing revealed two mutations in the KCNE2 gene consistent with susceptibility to LQTS type 6.
CONCLUSIONS: We believe this case is the first to demonstrate both a precipitating electrocardiographic and genetic cause of death for an infant with LQTS, showing a cause-and-effect relationship between LQTS mutation, ventricular arrhythmia, and death. We wonder whether universal ECG newborn screening to prevent LQTS death could have saved this baby.
Keywords: Echocardiography, DNA Mutational Analysis, DNA - genetics, Electrocardiography, Genetic Predisposition to Disease, genetic testing, Heart Conduction System - physiopathology, Infant, Newborn, Long QT Syndrome - genetics, Mutation, Potassium Channels, Voltage-Gated - metabolism, Sudden Infant Death - etiology, Ventricular Fibrillation - genetics
Background
This case describes a neonate who presented with sudden unexpected infant death due to long QT syndrome (LQTS) and raises the question: “Is it now time for universal electrocardiogram (ECG) screening for all newborns?”
Case Report
A female neonate who had otherwise been healthy was found by her mother to be unresponsive on day of life 19. The infant was rushed to the emergency department and found to be in pulseless cardiac arrest with ventricular fibrillation. Cardiac defibrillation converted the rhythm back to normal sinus rhythm (Figure 1). A lidocaine drip was started but the patient continued to go in and out of ventricular fibrillation a total of 21 times. With each defibrillation, she quickly converted back to normal sinus rhythm. Eventually her rhythm stabilized.
An echocardiogram was performed which revealed no gross abnormalities. An ECG showed a prolonged QT interval of 465 milliseconds (msec) (Figure 2). Even though an acute cardiac event can lead to a prolonged QT, genetic testing and work-up for LQTS was undertaken. There was no history of sudden death or syncope in the family. ECGs from the available family members were normal and blood from the baby was obtained for LQTS gene panel testing. The FAMILION Genetic Test for LQTS from the Transgenomic Lab (New Haven, Connecticut, USA) sequenced the complete open reading frame, splice junctions, and flanking regions of the genes KCNQ1, KCNH2, SCN5a, KCNE1, and KCNE2. The test returned positive for two different mutations in gene KCNE2 (Ile 20 Asn and Arg 27 His), a gene associated with LQTS type 6. These mutations were classified as Class II or possible deleterious mutations. According to the test result, approximately 5% of patients without LQTS will exhibit Class II mutations.
A magnetic resonance image (MRI) of the patient’s brain showed restricted diffusion in the posterior parietal lobes and occipital lobes bilaterally and possibly restricted diffusion in the left cerebellar hemisphere, consistent with multiple infarcts (Figures 3, 4), and the baby was severely encephalopathic with a burst suppression pattern on EEG and extremely frequent electrographic seizures. Therefore, life supportive treatment was discontinued. We recommended that the baby’s family obtain genetic testing for LQTS. The father declined genetic testing despite encouragement. The mother obtained genetic testing which was positive for one of the infant’s deleterious mutations (KCNE2 Arg 27 His). We recommended testing for other maternal family members. Unfortunately, the mother’s family has not undergone genetic testing at the time of this case report.
Discussion
To our knowledge, this is the first case demonstrating evidence of both a lethal arrhythmia as a precipitating event and a genetic diagnosis indicating susceptibility to LQTS for an infant who might have otherwise died of sudden infant death syndrome (SIDS) [1–5]. The infant tested positive for two LQTS mutations in gene KCNE2 and had a prolonged QT interval of 465 msec.
LQTS is an electrophysiologic cardiac disorder characterized by QT interval prolongation. A mutation in one or more of 15 genes are known to be associated with LQTS; however, approximately 20% of families with a firm clinical diagnosis of LQTS do not have a defect in any of those 15 genes. [6] It is estimated that 60–75% of LQTS cases will have a mutation in the KCNQ1, KCNH2, or SCN5A genes (LQTS type 1, 2, and 3). Mutations in the other 12 genes only make up about 1% of LQTS cases. Long QT syndrome type 6 is associated with a mutation in the KCNE2 gene located at the 21q22.11 chromosome locus, and is associated with a potassium voltage gated channel [6]. In about 4–10% of individuals with LQTS, two pathogenic variations are found (digenic/biallelic inheritance). These individuals have a more severe phenotype [6]. LQTS, including type 6, is typically inherited in an autosomal dominant manner. Therefore, once a diagnosis is made, it is important to offer testing to first-degree relatives and extended relatives as indicated. The mother of this infant tested positive for one of the infant’s mutations on the KCNE2 gene. Since the father declined genetic testing, we do not know whether the other mutation was inherited from him or
The most common symptom in an individual with LQTS is syncope, but only 50% or fewer of untreated individuals with a variant in one of the 15 genes will exhibit symptoms [6]. In some instances, LQTS will lead to ventricular fibrillation, cardiac arrest, and sudden death [6]. The life threatening arrhythmias are most likely to occur in persons under the age of 15 [7]. Beta-blocker medication is the primary treatment for LQTS, but in some cases an implantable cardioverter-defibrillator (ICD) and/or left cardiac sympathetic denervation is needed. ICD therapy should be considered for asymptomatic individuals with two or more pathogenic variants on molecular testing [6]. Another high-risk group includes infants who suffer a cardiac arrest during the first year of life. They are poorly responsive to beta-blocker therapy and may be difficult to save without an ICD [7]. Treatment has profoundly reduced mortality. In the 1980s, mortality was nearly 50% in untreated LQTS syncopal patients, but with current management the mortality is now less than 1% [7,8].
We wonder whether universal ECG newborn screening to prevent LQTS death could have saved the baby in this case report. While the baby’s death cannot be assigned as a SIDS death because the infant was evaluated by an emergency room team who promptly recognized ventricular fibrillation, the infant would have likely died at home without explanation. Sudden infant death syndrome is assigned to infant deaths that cannot be explained after a thorough case investigation, including a scene investigation, autopsy, and review of the clinical history [9]. The incidence of SIDS has been decreasing since the back-to-sleep campaign, but has now stabilized at about 0.5–0.6 per 1,000 live births in the United States [10]. For the sake of discussion, we will review the association of prolonged QT interval and SIDS. After evaluating 34,442 Italian newborns from 1976 to 1994, Schwartz et al. reported a significant association with a prolonged mean corrected QT interval (QTc) and SIDS [11]. The mean QTc, measured on the third or fourth day of life, of infants who eventually died of SIDS, was statistically longer than that of infants who survived to one year of age (435±45 msec
A flurry of responses from leading experts ensued. They argued that because prior studies had not shown ventricular arrhythmias prior to SIDS, we could not “assume that a cause-and-effect relationship between prolonged QT interval and SIDS exists” [12–14]. Furthermore, experts argued that several studies and at least one large study of 7,254 infants contradicted the Italian data [15–17]. Schwartz et al. countered, however, that “even though [the authors of the study of 7,254 infants] concluded that there was no significant difference between victims of SIDS and controls, 6 of the 15 infants who died of SIDS (40 percent) had a QTc exceeding the 90th percentile for the study population” [11]. Opponents of neonatal screening with ECG argued that the variability of QTc within the first week of life, errors in QTc measurement, an anticipated high false positive rate depending on the QTc cutoff, practical barriers of reimbursement, availability of equipment, and appropriate professional workforce, in addition to cost for screening and genetic testing, made screening “neither prudent nor practical” [17–24]. In a 2010 survey of North American pediatric cardiologists, only 10% would agree to a mandate for ECG screening [25].
Despite the controversy, Japan now has universal ECG screening of students in 1st, 7th, and 10th grades [26]. Furthermore, the Italian Ministry of Health funded a prospective “pilot” ECG study of 50,000 infants to assess the feasibility and outcome of nationwide neonatal ECG screening [27]. From 2001 to 2006, Schwartz et al. enrolled newborns in 18 Italian maternity hospitals for ECG screening between the 15th and 25th day of life [28]. Using a cutoff of >450 msec, 236 out of 44,596 infants were identified for repeat ECG testing within one to two weeks. Using a cutoff of >470 msec initially, then later >460 msec, 59 of 236 infants were identified for genetic testing. Among genotyped infants, disease-causing mutations were found in 43% (12/28) of infants with QTc >470 and 29% (4/14) of infants with a QTc between 461 and 470 msec. These results provided the first direct evidence of the prevalence of LQTS and supported neonatal ECG screening with guided molecular testing. The project also identified 15 undiagnosed parents as well as 42 other undiagnosed family members with LQTS. At least 31 infants were treated with 2 mg/kg/day propranolol with no reported side effects and no reported symptoms of LQTS, such as neonatal death.
Several groups have since supported ECG screening in infancy to prevent LQTS-related death [7,8,29–32]. The estimated prevalence of LQTS is 1:2,000 [28]. Using ECG screening to guide genetic testing, 80% of individuals with LQTS could be identified, and many other family members could subsequently be diagnosed once the proband is identified. ECG screening would also identify other infants at risk for death, including those with coarctation of the aorta and anomalous origin of the left coronary artery from the pulmonary artery, diagnoses which can escape the first medical visit [27]. Treatment is extremely effective with minimal side effects [33]. Looking specifically at LQTS patients, screening can increase their expected survival by 7.6 years, making screening more cost-effective than previously estimated [19,27]. Experts now report that “it is advisable to genotype newborns in LQTS families and newborns found to have a clear QT prolongation during an ECG screening” [34].
Conclusions
We believe that our case is the first to demonstrate both a precipitating electrocardiographic and genetic cause of death for an infant with susceptibility to LQTS, showing a cause-and-effect relationship between LQTS mutation, ventricular arrhythmia, and death. We wonder whether universal ECG newborn screening to prevent LQTS death could have saved this baby.
References:
1.. Southall DP, Arrowsmith WA, Oakley JR, Prolonged QT interval and cardiac arrhythmias in two neonates: sudden infant death syndrome in one case: Arch Dis Child, 1979; 54(10); 776-79, pmid: 507901
2.. Schwartz PJ, Priori SG, Bloise R, Molecular diagnosis in a child with sudden infant death syndrome: Lancet, 2001; 358(9290); 1342-43, pmid: 11684219
3.. Theeuws C, Nuyens D, Gewillig M, Foetal presentation of long QT syndrome: Acta Cardiol, 2013; 68(3); 331-34, pmid: 23882882
4.. Moltedo JM, Benjamin MN, Olmedo J, [An apparent life threatening secondary to long Qt syndrome]: Medicina (B Aires), 2013; 73(2); 153-54, pmid: 23570766 [in Spanish]
5.. Christiansen M, Tonder N, Larsen LA, Mutations in the HERG K+-ion channel: A novel link between long QT syndrome and sudden infant death syndrome: Am J Cardiol, 2005; 95(3); 433-34, pmid: 15670565
6.. Alders M, Christiaans I, Long QT Syndrome 2003 Feb 20 [Updated 2015 Jun 18 ]; 1993-2016, Seattle (WA), University of Washington, Seattle
7.. Saul JP, Schwartz PJ, Ackerman MJ, Triedman JK, Rationale and objectives for ECG screening in infancy: Heart Rhythm, 2014; 11(12); 2316-21, pmid: 25239430
8.. Tristani-Firouzi M, Revisiting the challenges of universal screening for long QT syndrome: J Electrocardiol, 2015; 48(6); 1053-57, pmid: 26355713
9.. , SIDS and other sleep-related infant deaths: Expansion of recommendations for a safe infant sleeping environment: Pediatrics, 2011; 128(5); 1030-39, pmid: 22007004
10.. Wilders R, Cardiac ion channelopathies and the sudden infant death syndrome: ISRN Cardiology, 2012(2012); 846171, pmid: 23304551
11.. Schwartz PJ, Stramba-Badiale M, Segantini A, Prolongation of the QT interval and the sudden infant death syndrome: N Engl J Med, 1998; 338(24); 1709-14, pmid: 9624190
12.. Lucey JF, Comments on a sudden infant death article in another journal: Pediatrics, 1999; 103(4 pt 1); 812, pmid: 10103306
13.. Guilleminault C, SIDS, near-miss SIDS and cardiac arrhythmia: Ann NY Acad Sci, 1988; 533; 358-67, pmid: 3421634
14.. Sadeh D, Shannon DC, Abboud S, Altered cardiac repolarization in some victims of sudden infant death syndrome: N Engl J Med, 1987; 317(24); 1501-5, pmid: 3683486
15.. Guntheroth WG, Spiers PS, Prolongation of the QT interval and the sudden infant death syndrome: Pediatrics, 1999; 103(4 Pt 1); 813-14, pmid: 10103308
16.. Hoffman JI, Lister G, The Implications of a relationship between prolonged QT interval and the sudden infant death syndrome: Pediatrics, 1999; 103(4 Pt 1); 815-17, pmid: 10103310
17.. Southall DP, Arrowsmith WA, Stebbens V, Alexander JR, QT interval measurements before sudden infant death syndrome: Arch Dis Child, 1986; 61(4); 327-33, pmid: 3707181
18.. Towbin JA, Friedman RA, Prolongation of the QT interval and the sudden infant death syndrome: N Engl J Med, 1998; 338(24); 1760-61, pmid: 9624197
19.. Zupancic JA, Triedman JK, Alexander M, Cost-effectiveness and implications of newborn screening for prolongation of QT interval for the prevention of sudden infant death syndrome: J Pediatr, 2000; 136(4); 481-89, pmid: 10753246
20.. Van Hare GF, Perry J, Berul CI, Triedman JK, Cost effectiveness of neonatal ECG screening for the long QT syndrome: Eur Heart J, 2007; 28(1); 137, pmid: 17158522 author reply 137–39
21.. Maron BJ, Thompson PD, Ackerman MJ, Recommendations and considerations related to preparticipation screening for cardiovascular abnormalities in competitive athletes: 2007 update: A scientific statement from the American Heart Association Council on Nutrition, Physical Activity, and Metabolism: Endorsed by the American College of Cardiology Foundation: Circulation, 2007; 115(12); 1643-455, pmid: 17353433
22.. Skinner JR, Van Hare GF, Routine ECG screening in infancy and early childhood should not be performed: Heart Rhythm, 2014; 11(12); 2322-27, pmid: 25239431
23.. van Langen IM, Wilde AA, Con: Newborn screening to prevent sudden cardiac death?: Heart Rhythm, 2006; 3(11); 1356-59, pmid: 17074645
24.. Walsh SZ, Electrocardiographic intervals during the first week of life: Am Heart J, 1963; 66(1); 36-41, pmid: 14045984
25.. Chang RK, Rodriguez S, Gurvitz MZ, Electrocardiogram screening of infants for long QT syndrome: survey of pediatric cardiologists in North America: J Electrocardiol, 2010; 43(1); 4-7, pmid: 19665725
26.. Yoshinaga M, Kucho Y, Sarantuya J, Genetic characteristics of children and adolescents with long-QT syndrome diagnosed by school-based electrocardiographic screening programs: Circ Arrhythm Electrophysiol, 2014; 7; 107-12, pmid: 24363352
27.. Quaglini S, Rognoni C, Spazzolini C, Cost-effectiveness of neonatal ECG screening for the long QT syndrome: Eur Heart J, 2006; 27(15); 1824-32, pmid: 16840497
28.. Schwartz PJ, Stramba-Badiale M, Crotti L, Prevalence of the congenital long-QT syndrome: Circulation, 2009; 120(18); 1761-67, pmid: 19841298
29.. Gonzalez FM, Veneziano MA, Puggina A, Boccia S, A systematic review on the cost-effectiveness of genetic and electrocardiogram testing for long QT syndrome in infants and young adults: Value Health, 2015; 18(5); 700-8, pmid: 26297099
30.. Berul CI, Perry JC, Contribution of long-QT syndrome genes to sudden infant death syndrome: Is it time to consider newborn electrocardiographic screening?: Circulation, 2007; 115(3); 294-96, pmid: 17242294
31.. Cruz Canete M, Rus Mansilla C, Gomez Lara A, [Usefulness of electrocardiographic screening in a neonatal population]: An Pediatr (Barc), 2011; 74(5); 303-8, pmid: 21342797 [in Spanish]
32.. Vetter VL, The role of ECG screening in the evaluation of risk of sudden cardiac arrest in the young: Pacing Clin Electrophysiol, 2009; 32(Suppl.2); S6-14, pmid: 19602165
33.. Villain E, Denjoy I, Lupoglazoff JM, Low incidence of cardiac events with beta-blocking therapy in children with long QT syndrome: Eur Heart J, 2004; 25(16); 1405-11, pmid: 15321698
34.. Spazzolini C, Mullally J, Moss AJ, Clinical implications for patients with long QT syndrome who experience a cardiac event during infancy: J Am Coll Cardiol, 2009; 54(9); 832-37, pmid: 19695463
In Press
Case report 
Am J Case Rep In Press; DOI: 10.12659/AJCR.949976
Case report 
Am J Case Rep In Press; DOI: 10.12659/AJCR.950290
Case report 
Am J Case Rep In Press; DOI: 10.12659/AJCR.950607
Case report 
Am J Case Rep In Press; DOI: 10.12659/AJCR.950985
Most Viewed Current Articles
07 Dec 2021 : Case report
17,691,734
DOI :10.12659/AJCR.934347
Am J Case Rep 2021; 22:e934347
06 Dec 2021 : Case report 
164,491
DOI :10.12659/AJCR.934406
Am J Case Rep 2021; 22:e934406
21 Jun 2024 : Case report
113,090
DOI :10.12659/AJCR.944371
Am J Case Rep 2024; 25:e944371
07 Mar 2024 : Case report
59,175
DOI :10.12659/AJCR.943133
Am J Case Rep 2024; 25:e943133