Circulation, Vol 70, 472-478, Copyright © 1984 by American Heart Association
KM Kessler, B Kissane, J Cassidy, KC Pefkaros, P Kozlovskis, C Hamburg and RJ Myerburg
We tested the hypothesis that the changes in free fatty acid and alpha
1-glycoprotein concentrations, which occur during acute myocardial
infarction, exert asynchronous and opposing influences on the serum protein
binding of selected drugs. Free drug fractions of two antiarrhythmic agents
with contrasting binding characteristics, quinidine and procainamide, were
related to free fatty acid and alpha 1- glycoprotein concentrations on days
1 through 5 and 10 in 20 patients with acute myocardial infarction. The
mean free quinidine fraction was elevated on day 1 (9.0 +/- 4.4% vs 6.7 +/-
2.7% in patients with stable heart disease; p less than .05) and fell
progressively to day 10 (4.0 +/- 2.8%; p less than .0002) as free fatty
acid concentration decreased (day 1 = 464 +/- 272 meq/liter; day 10 = 264
+/- 155 meq/liter; p less than .01) and alpha 1-glycoprotein concentration
increased (day 1 = 98 +/- 31 mg/dl; day 10 = 141 +/- 47 mg/dl; p less than
.02). Multiple stepwise regression showed a major influence of changing
alpha 1- glycoprotein concentration on the observed sequential changes in
the free quinidine fraction (p less than .005). In contrast, no serial
changes in procainamide binding were noted. In conclusion, metabolic
changes during the course of acute myocardial infarction sequentially alter
free quinidine fraction and, consequently, may influence pharmacodynamics.
ARTICLES
Dynamic variability of binding of antiarrhythmic drugs during the evolution of acute myocardial infarction