Circulation, Vol 58, 280-283, Copyright © 1978 by American Heart Association
BL Lloyd and TW Smith
Both heterologous IgG and Fab fragments of appropriate affinity and
specificity have been shown capable of reversing advanced cardiac glycoside
toxicity. Fab fragments are more rapidly excreted and theoretically have a
smaller risk of unwanted immunologic effects, but relative rates of
toxicity reversal have not been established. Rates of reversal of advanced
digoxin toxicity by digoxin-specific IgG and Fab fragments were therefore
compared in a dog model of advanced digoxin intoxication. Initial studies
confirmed more rapid distribution of sheep Fab fragments (M.W. 50,000) than
of the parent IgG molecule (M.W. 150,000) after intravenous injection.
Twenty-five pentobarbital- anesthetized dogs were given 0.3 mg/kg digoxin
intravenously, resulting in rapid onset of ventricular tachycardia in all
animals. Eight dogs subsequently given nonspecific IgG or Fab died in
asystole or ventricular fibrillation an average of 55 minutes after digoxin
administration. Ten of 11 dogs given 1.33 moles of binding sites per mole
of digoxin as intact IgG returned to sinus rhythm at a mean time of 85
minutes after antibody infusion. In contrast, six of six dogs given an
equivalent dose of specific Fab fragments returned to sinus rhythm in a
significantly shorter mean time of 36 minutes (P less than 0.01).
Variability of time to arrhythmia reversion was less in Fab- treated dogs.
These data demonstrate a decisive advantage of specific Fab fragments over
intact IgG for potential clinical use in advanced, life-threatening digoxin
intoxication.
ARTICLES
Contrasting rates of reversal of digoxin toxicity by digoxin-specific IgG and Fab fragments