Cardiotoxicity of digitalis glycosides: roles of autonomic pathways, autacoids and ion channels

• Published in: Autonomic & autacoid pharmacology Vol. 25; no. 2; pp. 35 - 52
• Main Authors: Demiryürek, A. T., Demiryürek, S.
• Format: Journal Article
• Language: English
• Published: Oxford, UK Blackwell Science Ltd 01.04.2005
• Subjects: Animals; arrhythmia; Autacoids - physiology; Autonomic Pathways - drug effects; Autonomic Pathways - pathology; cardiac glycosides; Cardiotonic Agents - toxicity; cardiotoxicity; cellular mechanisms; digitalis; Digitalis Glycosides - toxicity; Heart Diseases - chemically induced; Heart Diseases - physiopathology; Humans; Ion Channels - drug effects; Ion Channels - physiology
• ISSN: 1474-8665; 1474-8673
• DOI: 10.1111/j.1474-8673.2004.00334.x

Summary 1 Cardiac glycosides have been used for centuries as therapeutic agents for the treatment of heart diaseases. In patients with heart failure, digoxin and the other glycosides exert their positive inotropic effect by inhibiting Na+–K+‐ATPase, thereby increasing intracellular sodium, which, in turn, inhibits the Na+/Ca2+ exchanger and increases intracellular calcium levels. As the therapeutic index of digitalis is narrow, arrhythmias are common problems in clinical practice. The mechanisms and mediators of these arrhythmias, however, are not completely understood. 2 The involvement of the sympathetic and parasympathetic nervous system in digitalis cardiac toxicity is reviewed. 3 Receptors, channels, exchange systems or other cellular components involved in digitalis‐induced cardiotoxicity are also reviewed. 4 Possible mediators of digitalis‐induced cardiac toxicity are discussed. 5 Management of digitalis toxicity in patients is summarized. 6 The determination of the possible mediators of digitalis‐induced cardiac toxicity will enhance our knowledge and lead to the development of new therapeutic strategies to treat these lethal arrhythmias.