This study aims to evaluate the electrophysiological properties of the heart conduction system in patients with unexplained polymorphic ventricular tachycardia (VT) and/or ventricular fibrillation (VF), in patients with specific genetic mutations regarding sudden cardiac death or sudden cardiac arrest, in their family members and in a control cohort. The electrophysiological properties will be measured with the relatively new technique ECG-Imaging (ECGI). Also a National Dutch registry for patients with unexplained polymorphic VT and/or VF and their family members will be created. By combining the data from the registry and the results of ECGI, The investigators hope to identity risk markers for patients at higher risk for apparently idiopathic ventricular fibrillation, and use these for an adapted flow chart for the 'general'population of patients at risk for unexplained polymorphic VT and/or VF. The investigators aim to be able to identify patients before the first arrhythmic event, and aim for better treatment strategies in the future.
ECGI combines electrical body-surface mapping with 256 electrodes placed on the thorax with a CT-scan obtaining the anatomy of the heart and torso, hereby able to reconstruct local electrograms, activation and recovery times. In recent research, ECGI provided numerous extra insights into normal cardiac electrophysiology, but also electrophysiological disorders and disease. The results strongly suggest that ECGI can play a pivotal role in further characterizing arrhythmia mechanisms, therefore could do so for polymorphic VT or idiopathic VF leading to diagnosis and treatment improvement. Moreover, ECGI seems to have the potential to detect arrhythmogenic substrate in individuals before their first event, offering the possibility to diagnose and treat patients before sudden cardiac arrest occurs. In the VIGILANCE study: 1. ECGI will be used to noninvasively characterize the epicardial electrophysiological substrate and triggers of: * Patients with unexplained polymorphic VT and VF, * Index patients of family cohorts with a specific genetic mutation related to arrhythmogenesis, at high risk for unexplained polymorphic VT and/or VF. * Family members, * A control cohort. Results will be evaluated for risk stratification. 2. All unexplained polymorphic VT and/or VF patients and their family members will be asked to participate in a National Dutch registry, and these date will be analysed to determine their prognostic value in terms of arrhythmia risk
Study Type
OBSERVATIONAL
Enrollment
500
A body surface potential mapping and a cardiac + low dose CT-scan.
Maastricht Universite Medical Centre
Maastricht, Nederland, Netherlands
Amsterdam University medical Centre, location AMC
Amsterdam, Netherlands
University Medical Centre Utrecht
Utrecht, Netherlands
ECG-Imaging outcome: epicardial potentials
reconstructed epicardial potentials, represented in mV over time(s).
Time frame: 3 years
ECG-Imaging outcome: activation and repolarization maps
Activation and repolarization maps. These are made by measuring acivation and repolarization times from the reconstructed potentials in miliseconds. Then local activation and recovery times are plotted on a CT-derived heart mesh. The entire activation and repolarization of the epicardium of the heart can be visualized this way.
Time frame: 3 years
(Possible) Prognostic risk factors for recurrent ventricular arrhythmias
possible risk factors, found in the registry, given as odds/hazard ratio.
Time frame: 3 years
Recurrence of ventricular arrhythmias
documentation over the period of follow-up, if studysubjects had a recurrence of ventricular arrythmia(s), presented as number of events over a time period.
Time frame: 3 years
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