Body surface potential mapping detects early disease onset in plakophilin-2-pathogenic variant carriers

Author:

Kloosterman Manon1ORCID,Boonstra Machteld J1ORCID,Roudijk Rob W1ORCID,Bourfiss Mimount1ORCID,van der Schaaf Iris1,Velthuis Birgitta K2ORCID,Eijsvogels Thijs M H3ORCID,Kirkels Feddo P1ORCID,van Dam Peter M14ORCID,Loh Peter1ORCID

Affiliation:

1. Department of Cardiology, University Medical Center Utrecht , Utrecht , The Netherlands

2. Department of Radiology, University Medical Center Utrecht , Utrecht , The Netherlands

3. Department of Physiology, Radboud University Medical Center , Nijmegen , The Netherlands

4. ECG-Excellence BV , Nieuwerbrug , The Netherlands

Abstract

Abstract Aims Arrhythmogenic right ventricular cardiomyopathy (ARVC) is a progressive inherited cardiac disease. Early detection of disease and risk stratification remain challenging due to heterogeneous phenotypic expression. The standard configuration of the 12 lead electrocardiogram (ECG) might be insensitive to identify subtle ECG abnormalities. We hypothesized that body surface potential mapping (BSPM) may be more sensitive to detect subtle ECG abnormalities. Methods and results We obtained 67 electrode BSPM in plakophilin-2 (PKP2)-pathogenic variant carriers and control subjects. Subject-specific computed tomography/magnetic resonance imaging based models of the heart/torso and electrode positions were created. Cardiac activation and recovery patterns were visualized with QRS- and STT-isopotential map series on subject-specific geometries to relate QRS-/STT-patterns to cardiac anatomy and electrode positions. To detect early signs of functional/structural heart disease, we also obtained right ventricular (RV) echocardiographic deformation imaging. Body surface potential mapping was obtained in 25 controls and 42 PKP2-pathogenic variant carriers. We identified five distinct abnormal QRS-patterns and four distinct abnormal STT-patterns in the isopotential map series of 31/42 variant carriers. Of these 31 variant carriers, 17 showed no depolarization or repolarization abnormalities in the 12 lead ECG. Of the 19 pre-clinical variant carriers, 12 had normal RV-deformation patterns, while 7/12 showed abnormal QRS- and/or STT-patterns. Conclusion Assessing depolarization and repolarization by BSPM may help in the quest for early detection of disease in variant carriers since abnormal QRS- and/or STT-patterns were found in variant carriers with a normal 12 lead ECG. Because electrical abnormalities were observed in subjects with normal RV-deformation patterns, we hypothesize that electrical abnormalities develop prior to functional/structural abnormalities in ARVC.

Funder

Dutch Heart Foundation

Publisher

Oxford University Press (OUP)

Subject

Physiology (medical),Cardiology and Cardiovascular Medicine

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