Circulation, Vol 78, 401-406, Copyright © 1988 by American Heart Association
S Kimura, AL Bassett, JS Cameron, H Huikuri, PL Kozlovskis and RJ Myerburg
Cellular electrophysiological consequences of acute ischemia superimposed
on healed myocardial infarction were studied in isolated, coronary-perfused
cat left ventricles 2-4 months after ligation of multiple distal
tributaries of the left anterior descending and circumflex coronary
arteries. Oxygenated Tyrode's solution was perfused through the left
anterior descending and circumflex coronary arteries, and the preparations
were superfused with Tyrode's solution gassed with 95% N2-5% CO2.
Transmembrane action potentials were recorded from the endocardial cells in
normal and infarcted zones. There were no significant differences in
measured action potential variables and refractory periods between cells in
the normal and infarcted zones before acute ischemia. When coronary
perfusion was discontinued ("ischemia"), resting potential, action
potential amplitude, and action potential duration were reduced, and the
refractory period was shortened progressively in cells of the normal zone.
However, the action potential changes were less prominent, and the
refractory period was unchanged in cells in the infarcted zone. As a
result, there were significant differences in resting membrane potential,
action potential amplitude, action potential duration, and refractory
period between cells in the normal and infarcted zones at 10 minutes of
ischemia. These differences became larger as the ischemic period was
prolonged. Spontaneous rapid ventricular activity was observed during the
last 20- 30 minutes of ischemia in four of eight preparations with healed
myocardial infarction, whereas no spontaneous rapid ventricular activity
was recorded in any of six normal heart preparations. Our data suggest that
superimposition of acute ischemia on healed myocardial infarction produces
electrophysiological inhomogeneities that may enhance arrhythmogenesis.
ARTICLES
Cellular electrophysiological changes during ischemia in isolated, coronary-perfused cat ventricle with healed myocardial infarction
Department of Medicine, University of Miami, School of Medicine, FL 33101.
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