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Most of the estimated 400 000 Canadians who experience heart failure are 65 years of age or older. Heart failure is the most frequent reason for hospital admission for older adults. Admission for heart failure is a marker of disease progression, a cause of poor quality of life and a burden to the health care system. With the increase of the mean age of the population, the prevalence of heart failure and related hospital admissions are projected to double over the next 2–3 decades.
The largest multicentre randomized clinical trial of digoxin use in heart failure, the Digitalis Investigation Group (DIG) trial,1 was conducted in 116 Canadian and 186 US centres during 1991–1993. It demonstrated that use of digoxin, a digitalis glycoside, was associated with a significant 7.9% absolute reduction (34.7% in the placebo group v. 26.8% for patients receiving digoxin) and 28% relative reduction (risk ratio [RR] 0.72, 95% confidence interval [CI] 0.66–0.79) in heart failure–related hospital admissions among patients who were also receiving angiotensin-converting enzyme (ACE) inhibitors and diuretics.1 Differences in the rate of death from all causes (placebo group 35.1%, digoxin group 34.8%) were statistically nonsignificant.1
In 1997, the US Food and Drug Administration approved digoxin for use in heart failure.2 This approval was based primarily on digoxin's effect on the combined end-points of death due to progressive heart failure or hospital admission due to worsening heart failure, in patients with heart failure (RR 0.69, 95% CI 0.63–0.76) and diastolic heart failure (RR 0.72, 95% CI 0.53–0.99) during the first 2 years after group assignment (Table 1).2
The 2006 Canadian Cardiovascular Society practice guidelines on heart failure recommend the use of digoxin (a class I recommendation, based on level A evidence) to relieve symptoms and reduce hospital admissions among patients with heart failure who are in sinus rhythm and whose symptoms persist despite appropriate medical therapy for heart failure.3 Practice guidelines from the American College of Cardiology–American Heart Association (ACC/AHA) in 2005 and the Heart Failure Society of America in 2006 make similar recommendations.4,5 The ACC/AHA recommendation on the use of digoxin was based on level B evidence, since the data supporting it were derived from a single randomized study, the DIG trial.4
Data from large national heart-failure registries and recent trials involving patients with heart failure show a decline in the use of digoxin during recent years.6 Possible reasons for this underuse include a focus on mortality rates and lack of attention to hospital admissions as an outcome in cases of heart failure;1 perceived concerns about the harmful effects of digoxin in women;7 lack of industry promotion and scientific discussions about the role of digoxin in contemporary patients with heart failure who are taking β-blockers and aldosterone antagonists; and lack of clarity about the role of digoxin in those with diastolic heart failure, who compose up to half of all patients with heart failure.
The primary mechanism of action of digoxin in heart failure is the inhibition of the sodium–potassium adenosine triphosphatase (Na–K–ATPase) enzyme. Suppression of this enzyme in myocardial cells increases heart-muscle contractility. It now appears, however, that the benefit of digoxin in heart failure also results partly from the inhibition of this enzyme in noncardiac tissues. Digoxin reduces sympathetic and renin–angiotensin–aldosterone system activities in heart failure by inhibiting Na–K–ATPase in vagal afferent nerve fibres and the renal tubules, respectively.4 The effect of digoxin on neurohormones is believed to be more favourable at low dosages that result in low serum digoxin concentrations.8,9 This view is also supported by evidence that, at low serum concentrations, digoxin may reduce rates of death from heart failure,10,11 and that the effects of digoxin in systolic and diastolic heart failure are comparable (Table 1).1,2,12
The role of serum digoxin concentration in digoxin therapy is now well established; major practice guidelines for heart failure recommend that a concentration below 1.0 ng/mL be achieved for optimum results.3–5 However, serum digoxin concentration was considered neither in the main analysis of the DIG trial, which showed a lack of mortality benefit from digoxin, nor the subgroup analysis that suggested potential harm from digoxin in women.1,7 In the DIG trial, digoxin concentrations of 0.8–2.5 ng/mL in serum were considered therapeutic.13 Chronic digoxin therapy to maintain serum concentrations above 1.0 ng/mL (now considered high and potentially harmful) might have caused the mortality benefit of digoxin in heart failure to be underestimated.1 This is also evident from Kaplan–Meier mortality plots, which showed a reduction in mortality rates in the digoxin group during the first year after group assignment.1 A recent post-hoc analysis11 of the DIG trial demonstrated that digoxin at low serum concentrations may reduce deaths from all causes, as well as hospital admissions due to all causes and due to worsening heart failure (Fig. 1).
Because most people with heart failure are elderly and many are women or have chronic kidney disease, digoxin treatment should begin with low doses (≤ 0.125 mg/d), which is likely to result in low serum concentrations (0.5–0.9 ng/mL). Younger patients with normal renal function who remain symptomatic at this dose may be prescribed 0.25 mg/d or more. Clinically relevant risk factors for high serum digoxin concentrations (≥ 1 ng/mL) include old age, female sex, high levels of serum creatinine, use of non-potassium-sparing diuretics, and digoxin doses of 0.25 mg/d or more. Patients who have more than one of these risk factors should be administered doses of digoxin no greater than 0.0625 mg/d.11 Except in patients with multiple risk factors for high serum concentrations (e.g., an elderly woman with chronic kidney disease), there is no need for routine monitoring of serum digoxin concentrations.11
The evidence for a mortality benefit from low-dose digoxin is derived from post-hoc subgroup analyses. A randomized clinical trial of low-dose digoxin in contemporary patients with heart failure is therefore needed for definitive evidence.
Digoxin can play an important role in the care of contemporary patients with heart failure. It is the drug of choice for the treatment of atrial fibrillation in patients with heart failure. Use of digoxin can effectively reduce occurrences of hospital admission for heart failure, which is considered a marker of disease progression and is associated with poor outcomes.3,6 Women with heart failure should not be deprived of digoxin, because not only is there no known biological basis for a differential effect of digoxin by sex, but several subsequent analyses have confirmed that when serum digoxin concentration is taken into account, the effect of digoxin in women and men does not differ significantly. Many people with heart failure cannot tolerate ACE inhibitors and β-blockers, and many in the developing nations cannot afford these drugs. Digoxin may play an important role in the care of these patients. Patients with heart failure in the DIG trial were not receiving β-blockers or aldosterone antagonists. However, data from spironolactone and carvedilol trials involving patients with heart failure have revealed that digoxin is effective in combination with these drugs.11 Finally, digoxin appears to be safe in the treatment of diastolic heart failure. The effect of digoxin in such patients is similar to that of candesartan, which is the only other drug tested in a randomized clinical trial involving patients with diastolic heart failure (Table 2).12,14
Over 200 years ago, Dr. William Withering predicted the controversy surrounding digitalis and the expected outcome: “After all, in spite of opinion, prejudice or error, time will fix the real value upon this discovery.”15 The cumulative evidence from the DIG trial suggests a need for rehabilitation and wider use of digoxin in patients with heart failure.16 Digoxin in low doses should be used in patients with heart failure with or without atrial fibrillation if they remain symptomatic despite evidence-based pharmacotherapy with neurohormonal antagonists such as an ACE inhibitor or an angiotensin-receptor blocker, a β-blocker approved for heart failure (carvedilol or extended-release metoprolol) and an aldosterone antagonist. Digoxin should also be used in patients with heart failure who cannot tolerate or afford these drugs. The role of intravenous digoxin, given its acute hemodynamic effects in patients with acute heart failure syndromes, remains to be determined.
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Footnotes
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This article has been peer reviewed.
Contributors: Ali Ahmed conceived the study hypothesis and design, accessed the data, conducted the analysis and wrote the first draft of the article. All authors interpreted the data, participated in critical revision of the paper and approved the final version to be published.
Acknowledgements: Ali Ahmed is supported by the National Institutes of Health through grants from the National Institute on Aging (1–K23–AG19211–04) and the National Heart, Lung, and Blood Institute (1–R01–HL085561–01 and P50-HL077100).
Competing interests: None declared for Ali Ahmed. James Young is a paid consultant for Abbott, Acorn, Amgen, AstraZeneca, Artesion Therapeutics, Biomax Canada, Biosite, Boehringer Ingelheim, Cotherix, GlaxoSmithKline, Guidant, Medtronic, Protemix, Savacor, Scios, Sunshine, Transworld Medical Corporation, Vasogen and World Heart, and has accepted research support from 8 of these and from the US National Institutes of Health. Mihai Gheorghiade is a paid consultant for and has accepted speaker fees from GSK, Medtronic, PDL, Sigma Tau and Otsuka.