Short QT syndrome
The short QT syndrome (SQTS) is a recently described genetic arrhythmogenic disorder, characterized by abnormally short QT intervals on surface electrocardiogram (ECG) and a high incidence of sudden death (SD) during life, including the first months of life. The inheritance of SQTS is autosomal domi...
| Main Authors: | , , , , |
|---|---|
| Format: | Article |
| Language: | English |
| Published: |
MDPI AG
2011-12-01
|
| Series: | Cardiogenetics |
| Subjects: | |
| Online Access: | http://www.pagepressjournals.org/index.php/cardiogen/article/view/209 |
| id |
doaj-0ebf3f6376c54beda7a166f3bc0e2a31 |
|---|---|
| record_format |
Article |
| spelling |
doaj-0ebf3f6376c54beda7a166f3bc0e2a312021-01-02T07:42:32ZengMDPI AGCardiogenetics2035-82532035-81482011-12-0112e5e510.4081/cardiogenetics.2011.s1.e5Short QT syndromeFiorenzo GaitaCharles AntzelevitchChiara ScroccoDaniela GiachinoCarla GiustettoThe short QT syndrome (SQTS) is a recently described genetic arrhythmogenic disorder, characterized by abnormally short QT intervals on surface electrocardiogram (ECG) and a high incidence of sudden death (SD) during life, including the first months of life. The inheritance of SQTS is autosomal dominant, with genetic heterogeneity. Gain-of-function mutations in 3 genes encoding potassium channels have been associated to the disease: <em>KCNH2</em> encoding IKr (SQT1), <em>KCNQ1</em> encoding IKs (SQT2), and <em>KCNJ2</em> encoding IK1 (SQT3). Loss-of-function mutations in 3 genes encoding the cardiac L-type calcium channel, <em>CACNA1C</em>, <em>CACNB2b</em> and <em>CACNA2D1</em> may underlie a mixed phenotype of Brugada pattern ECG (or non-specific repolarization changes in case of <em>CACNA2D1</em>) and shorter than normal QT intervals. Clinical presentation is often severe, as cardiac arrest represents the first clinical presentation in most subjects. Moreover, often a noticeable family history of cardiac SD is present. Atrial fibrillation may be observed, also in young individuals. At electrophysiological study, short atrial and ventricular refractory periods are found, and atrial and ventricular fibrillation are easily induced by programmed electrical stimulation. The outcome of patients with SQTS becomes relatively safe when they are identified and treated. Currently, the suggested therapeutic strategy is an implantable cardioverter- defibrillator (ICD) in patients with personal history of aborted SD or syncope. In asymptomatic adult patients from highly symptomatic families and in newborn children pharmacological treatment with hydroquinidine, which has been shown to prolong the QT interval and reduce the inducibility of ventricular arrhythmias, may be proposed.http://www.pagepressjournals.org/index.php/cardiogen/article/view/209short QT syndrome, sudden death, hydroquinidine. |
| collection |
DOAJ |
| language |
English |
| format |
Article |
| sources |
DOAJ |
| author |
Fiorenzo Gaita Charles Antzelevitch Chiara Scrocco Daniela Giachino Carla Giustetto |
| spellingShingle |
Fiorenzo Gaita Charles Antzelevitch Chiara Scrocco Daniela Giachino Carla Giustetto Short QT syndrome Cardiogenetics short QT syndrome, sudden death, hydroquinidine. |
| author_facet |
Fiorenzo Gaita Charles Antzelevitch Chiara Scrocco Daniela Giachino Carla Giustetto |
| author_sort |
Fiorenzo Gaita |
| title |
Short QT syndrome |
| title_short |
Short QT syndrome |
| title_full |
Short QT syndrome |
| title_fullStr |
Short QT syndrome |
| title_full_unstemmed |
Short QT syndrome |
| title_sort |
short qt syndrome |
| publisher |
MDPI AG |
| series |
Cardiogenetics |
| issn |
2035-8253 2035-8148 |
| publishDate |
2011-12-01 |
| description |
The short QT syndrome (SQTS) is a recently described genetic arrhythmogenic disorder, characterized by abnormally short QT intervals on surface electrocardiogram (ECG) and a high incidence of sudden death (SD) during life, including the first months of life. The inheritance of SQTS is autosomal dominant, with genetic heterogeneity. Gain-of-function mutations in 3 genes encoding potassium channels have been associated to the disease: <em>KCNH2</em> encoding IKr (SQT1), <em>KCNQ1</em> encoding IKs (SQT2), and <em>KCNJ2</em> encoding IK1 (SQT3). Loss-of-function mutations in 3 genes encoding the cardiac L-type calcium channel, <em>CACNA1C</em>, <em>CACNB2b</em> and <em>CACNA2D1</em> may underlie a mixed phenotype of Brugada pattern ECG (or non-specific repolarization changes in case of <em>CACNA2D1</em>) and shorter than normal QT intervals. Clinical presentation is often severe, as cardiac arrest represents the first clinical presentation in most subjects. Moreover, often a noticeable family history of cardiac SD is present. Atrial fibrillation may be observed, also in young individuals. At electrophysiological study, short atrial and ventricular refractory periods are found, and atrial and ventricular fibrillation are easily induced by programmed electrical stimulation. The outcome of patients with SQTS becomes relatively safe when they are identified and treated. Currently, the suggested therapeutic strategy is an implantable cardioverter- defibrillator (ICD) in patients with personal history of aborted SD or syncope. In asymptomatic adult patients from highly symptomatic families and in newborn children pharmacological treatment with hydroquinidine, which has been shown to prolong the QT interval and reduce the inducibility of ventricular arrhythmias, may be proposed. |
| topic |
short QT syndrome, sudden death, hydroquinidine. |
| url |
http://www.pagepressjournals.org/index.php/cardiogen/article/view/209 |
| work_keys_str_mv |
AT fiorenzogaita shortqtsyndrome AT charlesantzelevitch shortqtsyndrome AT chiarascrocco shortqtsyndrome AT danielagiachino shortqtsyndrome AT carlagiustetto shortqtsyndrome |
| _version_ |
1724357162019323904 |