Circulation, Vol 87, 764-772, Copyright © 1993 by American Heart Association
JT Hii, M Traboulsi, LB Mitchell, DG Wyse, HJ Duff and AM Gillis
BACKGROUND. Surviving myocardial cells near the infarct border zone form
the arrhythmogenic substrate for sustained ventricular tachycardia (VT) in
humans. Infarct-related artery (IRA) patency may modulate the
electrophysiological function of this arrhythmogenic substrate and its
response to antiarrhythmic drug therapy. We postulated that effective
antiarrhythmic drug therapy selected during serial electrophysiological
studies in patients with VT after a myocardial infarction would be
identified more frequently when the IRA is patent than when chronically
occluded. METHODS AND RESULTS. Consecutive patients (n = 64) with
documented coronary artery disease and remote myocardial infarction
presenting with spontaneous sustained VT or ventricular fibrillation (VF)
were studied. These patients underwent 4 +/- 2 electropharmacological
studies identifying effective antiarrhythmic drug therapy in 16 (25%)
patients. Drug responders did not differ significantly from nonresponders
in demographic, electrocardiographic, angiographic, or hemodynamic
measurements. A patent IRA was associated with antiarrhythmic drug response
significantly more frequently than was an occluded IRA (45% versus 9%, p =
0.001). Patency of the IRA was the only independent predictor of response
to antiarrhythmic drug therapy in this study population. The sensitivity
and specificity of using a patent IRA to predict successful drug testing
were 81% and 67%, respectively. CONCLUSIONS. The outcome of
electropharmacological studies was predicted by the patency of the IRA. A
patent IRA was associated with a greater probability of finding effective
drug therapy.
ARTICLES
Infarct artery patency predicts outcome of serial electropharmacological studies in patients with malignant ventricular tachyarrhythmias
Department of Medicine, Foothills Medical Centre, Calgary, Alberta, Canada.
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