Congenital long QT syndrome: Severe Torsades de pointes provoked by epinephrine in a digenic mutation carrier |
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| Affiliation: | 1. Department of Cardiac Sciences, Libin Cardiovascular Institute of Alberta, University of Calgary, Calgary, AB, Canada;2. Cardiology Department, Changi General Hospital, Singapore;1. Division of Pediatric Ophthalmology, King Khaled Eye Specialist Hospital, Riyadh, Saudi Arabia;2. Center for Human Genetics, Bioscientia, Ingelheim, Germany;3. Institute of Human Genetics, University of Cologne, Cologne, Germany;1. Nursing Department, School of Health Sciences, Cyprus University of Technology, 15 Vragadinou Str., 3041 Limassol, Cyprus;2. Department of Health Science, School of Sciences, European University Cyprus, 6, Diogenes Str., Engomi, P.O. Box 22006, 1516 Nicosia, Cyprus;3. Faculty of Nursing, University of Athens, 123 Papadiamantopoulou Str., Goudi, Athens 11527, Greece;4. Cardiology Department, American Medical Center/American Heart Institute, Cyprus;5. Cardiology Department, Larnaca General Hospital, 1 Pandoras, Larnaca, Cyprus;1. Indiana Wesleyan University, Marion, IN, USA;2. VA Loma Linda Healthcare System, Loma Linda, CA, USA |
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| Abstract: | Congenital Long QT Syndrome (LQTS) is a potentially lethal cardiac channelopathy characterized by prolongation of the corrected QT (QTc) interval on the surface electrocardiogram. The hallmark phenotypic features are syncope, seizure or sudden death, however most of the mutation carriers are asymptomatic and their risk for arrhythmias such as Torsade de pointes (TdP) are low. We report a case of Long QT syndrome with a corrected QT of 520 ms. For symptom – arrhythmia correlation a loop recorder was implanted with no documented arrhythmias. Epinephrine testing was performed for clinical risk stratification leading to Torsades de pointes during recovery phase which required defibrillation. Genetic testing discovered two pathogenic heterozygous mutations in two different LQT genes (SCN5A and KCNQ1). We propose a calcium homeostasis mechanism for the interaction of both mutations that exaggerated the phenotype, while each mutation by itself is causing a relatively modest phenotype. |
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