Human ventricular activation sequence and the simulation of the electrocardiographic QRS complex and its variability in healthy and intraventricular block conditions

Louie Cardone-Noott; Alfonso Bueno-Orovio; Ana Mincholé; Nejib Zemzemi; Blanca Rodriguez

doi:10.1093/europace/euw346

Human ventricular activation sequence and the simulation of the electrocardiographic QRS complex and its variability in healthy and intraventricular block conditions

Europace. 2016 Dec;18(suppl 4):iv4-iv15. doi: 10.1093/europace/euw346.

Authors

Louie Cardone-Noott¹, Alfonso Bueno-Orovio², Ana Mincholé¹, Nejib Zemzemi^{3

4}, Blanca Rodriguez¹

Affiliations

¹ Department of Computer Science and British Heart Foundation Centre of Research Excellence, University of Oxford, Oxford OX1 3QD, UK.
² Department of Computer Science and British Heart Foundation Centre of Research Excellence, University of Oxford, Oxford OX1 3QD, UK alfonso.bueno@cs.ox.ac.uk.
³ INRIA Bordeaux Sud-Ouest, 200 avenue de la vieille tour, Talence Cedex 33405, France.
⁴ IHU Liryc, Electrophysiology and Heart Modeling Institute, foundation Bordeaux Université, F-33600 Pessac Bordeaux, France.

Abstract

Aims: To investigate how variability in activation sequence and passive conduction properties translates into clinical variability in QRS biomarkers, and gain novel physiological knowledge on the information contained in the human QRS complex.

Methods and results: Multiscale bidomain simulations using a detailed heart-torso human anatomical model are performed to investigate the impact of activation sequence characteristics on clinical QRS biomarkers. Activation sequences are built and validated against experimentally-derived ex vivo and in vivo human activation data. R-peak amplitude exhibits the largest variability in terms of QRS morphology, due to its simultaneous modulation by activation sequence speed, myocardial intracellular and extracellular conductivities, and propagation through the human torso. QRS width, however, is regulated by endocardial activation speed and intracellular myocardial conductivities, whereas QR intervals are only affected by the endocardial activation profile. Variability in the apico-basal location of activation sites on the anterior and posterior left ventricular wall is associated with S-wave progression in limb and precordial leads, respectively, and occasional notched QRS complexes in precordial derivations. Variability in the number of early activation sites successfully reproduces pathological abnormalities of the human conduction system in the QRS complex.

Conclusion: Variability in activation sequence and passive conduction properties captures and explains a large part of the clinical variability observed in the human QRS complex. Our physiological insights allow for a deeper interpretation of human QRS biomarkers in terms of QRS morphology and location of early endocardial activation sites. This might be used to attain a better patient-specific knowledge of activation sequence from routine body-surface electrocardiograms.

Keywords: Activation sequence; Computer modelling and simulation; Electrocardiogram; QRS complex; Variability.

MeSH terms

Action Potentials*
Body Surface Potential Mapping
Case-Control Studies
Electrocardiography*
Female
Heart Block / diagnosis
Heart Block / physiopathology*
Heart Conduction System / physiopathology*
Heart Rate*
Heart Ventricles / physiopathology*
Humans
Male
Models, Anatomic
Models, Cardiovascular*
Patient-Specific Modeling*
Predictive Value of Tests
Reproducibility of Results
Signal Processing, Computer-Assisted
Time Factors
Torso / anatomy & histology
Ventricular Function, Left
Ventricular Function, Right