Transmural and apicobasal gradients in repolarization contribute to T-wave genesis in human surface ECG

Author:

Okada Jun-ichi1,Washio Takumi1,Maehara Akiko2,Momomura Shin-ichi3,Sugiura Seiryo4,Hisada Toshiaki4

Affiliation:

1. Graduate School of Frontier Sciences, University of Tokyo, Chiba, Japan;

2. Columbia University Medical Center/Cardiovascular Research Foundation, New York, New York;

3. Cardiovascular Division, Jichi Medical University Saitama Medical Center, Saitama; and

4. Graduate School of Frontier Sciences, University of Tokyo, Tokyo, Japan

Abstract

The cellular basis of the T-wave morphology of surface ECG remains controversial in clinical cardiology. We examined the effect of action potential duration (APD) distribution on T-wave morphology using a realistic model of the human ventricle and torso. We developed a finite-element model of the ventricle consisting of ∼26 million elements, including the conduction system, each implemented with the ion current model of cardiomyocytes. This model was embedded in a torso model with distinct organ structures to obtain the standard ECG leads. The APD distribution was changed in the transmural direction by locating the M cells in either the endocardial or epicardial region. We also introduced apicobasal gradients by modifying the ion channel parameters. Both the transmural gradient (with M cells on the endocardial side) and the apicobasal gradient produced positive T waves, although a very large gradient was required for the apicobasal gradient. By contrast, T waves obtained with the transmural gradient were highly symmetric and, therefore, did not represent the true physiological state. Only combination of the transmural and the moderate apicobasal gradients produced physiological T waves in surface ECG. Positive T waves in surface ECG mainly originated from the transmural distribution of APD with M cells on the endocardial side, although the apicobasal gradient was also required to attain the physiological waveform.

Publisher

American Physiological Society

Subject

Physiology (medical),Cardiology and Cardiovascular Medicine,Physiology

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