Australian Prescriber An independent Review Logo
ISSUE 4 AUGUST
Article

Chronic heart failure

  • Ingrid Hopper, Kellie Easton
  • CPD for Pharmacists
  • Podcast

SUMMARY

The clinical diagnosis of heart failure should be confirmed by echocardiogram to determine the underlying mechanism and to measure the left ventricular ejection fraction. Heart failure with reduced ejection fraction and heart failure with preserved ejection fraction have different treatments but are often indistinguishable clinically.

Lifestyle modification and education on self-management are important strategies for all patients. Patients should monitor their symptoms and weight regularly.

Heart failure with reduced ejection fraction should be managed with ACE inhibitors, heart failure specific beta blockers, and aldosterone antagonists. These drugs all reduce mortality.

Angiotensin receptor antagonists should be used if the patient cannot tolerate ACE inhibitors. The combination of sacubitril and valsartan is indicated if patients remain symptomatic despite ACE inhibitors, beta blockers and aldosterone antagonists. Digoxin and diuretics may also have a role in treating persistent symptoms.

In heart failure with preserved ejection fraction no drug has been proven to reduce mortality. Patients should be treated cautiously with diuretics and have aggressive management of risk factors, particularly hypertension.

 

Introduction

Heart failure is present in 1–2% of the Australian population.1 It is predominantly a disease of the elderly,2 present in up to 10% of those aged over 80,3 and this prevalence is rising.4

Heart failure is a syndrome in which the heart cannot provide adequate cardiac output to meet the metabolic requirements of the body and accommodate venous return. The diagnosis is mainly clinical, based on the presence of symptoms including dyspnoea, orthopnoea and fatigue, and signs such as pulmonary and peripheral oedema. 

 

Pathophysiology

Heart failure is the end result of a number of different pathophysiological processes in which there is injury to the heart with loss or impairment of functioning myocardial cells.5 Compensatory neurohormonal mechanisms are activated in order to maintain adequate cardiac function and tissue perfusion. Activation of the sympathetic nervous system increases heart rate and cardiac contractility, while activation of the renin–angiotensin– aldosterone system increases sodium reabsorption and water retention.

Although these responses are initially beneficial, prolonged overstimulation of the sympathetic nervous system and renin–angiotensin–aldosterone system results in maladaptive cardiovascular remodelling.

The release of natriuretic peptides counteracts the vasoconstricting effects of the sympathetic nervous system and renin–angiotensin–aldosterone system.

 

Ejection fraction

Heart failure is often due to myocardial dysfunction and is broadly classified by left ventricular ejection fraction. When the left ventricular ejection fraction is less than 40% it is termed heart failure with reduced ejection fraction. If the ejection fraction is at least 50% the condition is called heart failure with preserved ejection fraction. This accounts for approximately half of all cases of heart failure.6 Although the presentation is clinically indistinguishable from heart failure with reduced ejection fraction, the treatment is different.

Left ventricular ejection fraction in the range 40–49% has recently been termed ‘mid-range’ by the European Society of Cardiology.7 However, given the variation in measuring left ventricular ejection fraction, this is a grey area which requires more research. 

 

Correcting the cause

Underlying causes of heart failure need to be identified and managed. These include cardiovascular causes such as myocardial ischaemia or infarction, uncontrolled hypertension, valvular disease, atrial fibrillation and tachycardia, and pulmonary embolism. There are also systemic causes, such as infection, thyroid dysfunction, anaemia, poorly controlled diabetes, previous chemotherapy or radiotherapy and peripartum cardiomyopathy. Idiopathic or genetic causes include dilated cardiomyopathy, hypertrophic obstructive cardiomyopathy and arrhythmogenic right ventricular cardiomyopathy. Alcohol and substance abuse, for example amphetamines, can also cause heart failure. Acute triggers causing decompensation may include nonadherence to treatment, iatrogenic factors such as inappropriate drugs, and dietary indiscretions.

Comorbid disease may worsen heart failure or complicate its treatment. Over half of patients with heart failure reported five or more chronic conditions in a US community-based study.8 While cardiac diseases including hypertension, hypercholesterolaemia, ischaemic heart disease and myocardial infarction are the more common comorbidities, chronic obstructive pulmonary disorder, diabetes, depression and renal failure are most strongly associated with adverse outcomes. Renal dysfunction with heart failure, termed cardiorenal syndrome, has a particularly poor prognosis.

 

Non-drug interventions 

Ongoing education about self-management is key to caring for patients with heart failure.9 Use of visual aids can support this education.10

A low-salt diet should be recommended, along with smoking cessation, minimal alcohol intake and regular exercise. A cardiac rehabilitation program11 and a multidisciplinary heart failure team (doctors, nurses, pharmacists)12 have been shown to be beneficial.

Early intervention by the GP to address signs and symptoms of heart failure identified by the patient can reduce hospitalisations for heart failure. An exacerbation of heart failure can be heralded by dyspnoea with usual daily activities, reduced exercise tolerance, abdominal bloating and poor appetite.

Patients should know the weight at which their condition was previously stable. They need to monitor their weight regularly so that they and their caregivers are alert to any weight gain which would suggest fluid retention. The patients need to know what to do when their weight rises above set limits, such as contacting their GP. A fluid restriction for volume overload may be required, with a flexible diuretic regimen if appropriate. Resources are available to help in preparing a heart failure action plan.10 

 

Drug therapy for heart failure with reduced ejection fraction

The goal of management of heart failure with reduced ejection fraction is to control symptoms, prevent progression of left ventricular dysfunction, decrease hospitalisation and improve survival. Drugs which block neurohormonal activation are the cornerstone of therapy. They include ACE inhibitors and beta blockers, as well as aldosterone antagonists (Table 1). A new combination of sacubitril and valsartan (a neprilysin inhibitor–angiotensin receptor antagonist) enhances neurohormonal modulation by increasing beneficial natriuretic peptides

Table 1 - Drugs used in heart failure with reduced left ventricular ejection fraction

 

Drug Indications Mechanism Adverse effects Precautions

ACE inhibitors

First-line therapy when LVEF <40%

Reduces sodium reabsorption 


Reduces aldosterone

Hypotension 


Worsening renal function 


Hyperkalaemia
Chronic cough 


Angioedema

Previous angioedema 


Other drugs that increase

 potassium

Angiotensin receptor antagonists (sartans)

If intolerant of ACE inhibitors

Reduces vasoconstriction 


Reduces sodium reabsorption 


Reduces aldosterone

Hypotension 


Worsening renal function 


Hyperkalaemia

Other drugs that increase potassium

Beta blockers

First-line therapy when LVEF <40%

Reduces sympathetic activity 


Has antiarrhythmic effects 


Reverses remodelling

Hypotension 


Bradycardia 


Fatigue 


Bronchospasm 


Impotence 


Worsening heart failure 


Masking hypoglycaemia

2nd and 3rd degree heart block 


Asthma 


Chronic obstructive pulmonary disease – exclude significant reversibility

Aldosterone antagonists

If symptomatic despite ACE inhibitor and beta blocker and LVEF <40%

Is a weak diuretic 


Reduces effects of aldosterone

Hyperkalaemia 


Worsening renal function 


Hypotension 


Gynaecomastia (spironolactone)

Other drugs that increase potassium

Sacubitril with valsartan

Heart failure LVEF <35% 


In place of ACE inhibitor or angiotensin receptor antagonist

Causes vasodilation 


Reduces sympathetic activity 


Enhances diuresis

Angioedema 


Hypotension

Previous angioedema 


A 36-hour ACE inhibitor washout is an absolute requirement before starting

Diuretics

Relief of congestive symptoms

Reduces retention of sodium and water

Renal dysfunction 


Hypokalaemia 


Worsened gout

Other drugs that lower potassium

Ivabradine

Heart rate 77 beats/min or higher despite beta blocker, or intolerant to beta blocker 

Sinus rhythm

Reduces heart rate in sinus rhythm

Visual disturbances (phosphenes) 

Headache 

Bradycardia 

Atrial fibrillation

3rd degree atrioventricular block 

Sinoatrial block

Stop if atrial fibrillation develops

Prolonged QT syndrome

Digoxin

Heart failure in sinus rhythm with symptoms despite ACE inhibitor, beta blocker, aldosterone antagonist, diuretic

Atrial fibrillation

Is a weak positive inotrope 

Reduces heart rate
Increases vagal tone

Bradycardia 

Digoxin toxicity

Narrow therapeutic range requires monitoring 

Interacting drugs 

Impaired renal function

LVEF left ventricular ejection fraction

In order to obtain the maximal symptomatic and mortality benefits from these drugs, they should be up-titrated every 2–4 weeks providing that symptoms, heart rate, blood pressure, serum potassium and renal function remain within acceptable ranges (see Fig.).7 Achievement of target doses can take weeks to months (Table 2). Drugs can be up-titrated together in the absence of symptomatic hypotension, however titrating more cautiously one at a time can distinguish which drug is causing an adverse effect. Adverse effects tend to improve over time. If a dose increase is not tolerated, the dose should be reduced and re-titrated once the patient is clinically stable. When significant adverse effects occur, switching to a different drug within the same class should be tried before permanently discontinuing therapy

Fig. - Approach to the managementof heart failure with reduced ejection fraction 

 

a) New York Heart Association Class II–IV

b) If ACE inhibitor not tolerated or contraindicated, use angiotensin receptor antagonist

c) If aldosterone antagonist not tolerated or contraindicated, use angiotensin receptor antagonist

d) With hospital admission for heart failure in the last six months or with elevated natriuretic peptides

e) With elevated natriuretic peptides

f) In dose equivalent to enalapril 10 mg twice daily

g) With a hospital admission for heart failure in the previous year as per Pharmaceutical Benefits Scheme criteria

h) Cardiac resynchronisation therapy is:

  • recommended if QRS ≥130 msec and left bundle branch block in sinus rhythm
  • considered if QRS ≥130 msec without left bundle branch block in sinus rhythm, or for atrial fibrillation provided a strategy to ensure biventricular capture in place

Source: Adapted from Figure 7.1 of reference 7, with permission

Table 2 - Recommendedtarget doses 

 

 

Daily starting dose

Daily target maintenance dose

ACE inhibitors

Captopril

6.25 mg x3

25–75 mg x2

Enalapril

2.5 mg

10–20 mg x2

Fosinopril

5–10 mg

20–40 mg

Lisinopril

2.5 mg

20–40 mg

Perindopril arginine

2.5 mg

5–10 mg

Perindopril erbumine

2 mg

4–8 mg

Quinapril

5 mg

20–40 mg

Ramipril

2.5 mg

5–10 mg

Angiotensin receptor inhibitors

Candesartan

4–8 mg

32 mg

Valsartan

40 mg x2

160 mg x2

Losartan

50 mg

150 mg

Beta blockers

Bisoprolol

1.25 mg

10 mg

Carvedilol

3.125 mg

25 mg x2

Metoprolol extended release

23.75 mg

190 mg

Nebivolol

1.25 mg

10 mg

Aldosterone antagonists

Eplerenone

25 mg

50 mg

Spironolactone

25 mg

50 mg

Neprilysin inhibitor/angiotensin receptor antagonist

Sacubitril with valsartan

49/51 mg

97/103 mg

ACE inhibitors and angiotensin receptor antagonists

ACE inhibitors are first-line therapy in heart failure with reduced ejection fraction and asymptomatic left-ventricular dysfunction. Their use results in a 3.8% absolute reduction (20% relative) in death, with reductions in myocardial infarction and hospitalisation for heart failure.13 Beneficial effects occur early and continue long term, in all age groups. ACE inhibitors reduce the maladaptive effects of chronic renin– angiotensin–aldosterone system activation, including sodium and water retention, vasoconstriction, and cardiac hypertrophy and fibrosis. Studies of angiotensin receptor antagonists (sartans) have not shown a consistent reduction in mortality.14,15 Sartans are therefore considered as a second choice, indicated only in patients intolerant of ACE inhibitors.

Treatment should begin soon after diagnosis, at the lowest dose. Up-titration is recommended if the blood pressure is 90 mmHg systolic or above, and is limited by symptoms rather than the measured blood pressure. If symptomatic hypotension occurs, other vasodilators should be reduced or stopped first and, provided the patient is not congested, diuretics should be reduced or ceased before reducing the ACE inhibitor dose.

A minor worsening of renal function (up to 30% reduction in estimated glomerular filtration rate (eGFR)) is generally acceptable. A small rise in potassium can be expected, but the ACE inhibitor dose should be halved if the potassium concentration exceeds 5.5 mmol/L. If an ACE inhibitor induces a chronic cough, a change to a sartan may be appropriate after other causes of cough have been excluded such as pulmonary oedema or underlying lung disease.

Beta blockers

Beta blockers are another important first-line therapy for heart failure with reduced ejection fraction. Given with ACE inhibitors, they are associated with a 4.3% absolute reduction (24% relative reduction) in all-cause mortality and comparable reductions in hospital admissions for patients in sinus rhythm.16 Beta blockers reduce myocardial oxygen demand, protect from ischaemia, have antiarrhythmic effects and reduce sudden cardiac death. Only beta blockers that have been shown to be effective in heart failure should be used. These are bisoprolol,17 carvedilol,18,19 extended-release metoprolol succinate,20 and nebivolol if the patient is over 70 years old (as this drug has only been evaluated in the elderly).21

All patients with heart failure with reduced ejection fraction should be given beta blockers. Start soon after an ACE inhibitor, once the patient is clinically stable and euvolaemic. At first the symptoms of heart failure may worsen so the smallest dose should be used. Aim to titrate up to the target dose or as high as tolerated. Heart rate, blood pressure and symptoms of congestion should be reviewed after each up-titration.

Absolute contraindications to beta blockers include second or third degree atrioventricular block. If these occur, a pacemaker or cardiac resynchronisation therapy should be considered to enable continuation of therapy. Asthma is only a relative contraindication. Chronic obstructive pulmonary disease should be assessed with lung function tests before deciding not to give beta blockers. If there is no significant airway reversibility, the patient should be able to tolerate beta blockers. Usually the impact of beta blocker therapy on lung function tests is minimal and without clinical relevance.22

The dose should be reassessed if clinical deterioration occurs or the heart rate is under 50 beats per minute. As with ACE inhibitors, asymptomatic hypotension does not require a change of therapy. If symptomatic, consider reducing other vasodilators first, or the dose of any diuretic if there is no congestion, before deciding to reduce the dose of beta blocker. Bisoprolol and metoprolol have a less vasodilating effect and may be better tolerated if the blood pressure is borderline, however the additional vasodilating effects of carvedilol may offset the early worsening of heart failure.

Aldosterone antagonists

Aldosterone antagonists improve survival across the full spectrum of heart failure with reduced ejection fraction. There is an 11% absolute reduction (30% relative) in mortality in severe heart failure,23 a 7.6% absolute reduction (37% relative) in mortality and cardiovascular hospitalisation in mild heart failure,24 and a 2.3% absolute reduction (15% relative) in death in patients with heart failure after myocardial infarction.25 Aldosterone antagonists block the adverse effects of aldosterone activation, which includes sodium and water reabsorption, and cardiovascular fibrosis. These drugs are markedly underused and should be added to ACE inhibitors and beta blockers in all patients who remain symptomatic.

Serious hyperkalaemia can occur, especially with underlying renal impairment. Serum potassium should be closely monitored, at one week and one, two and three months after starting or increasing the dose, then every three months to 12 months, and then four monthly thereafter. The starting dose can be halved if diabetes or renal impairment is present (Table 2). The dose should be halved if potassium exceeds 5.5 mmol/L, and ceased if it is more than 6.0 mmol/L. Gynaecomastia can occur in men, but is less common with eplerenone than with spironolactone.

Sacubitril with valsartan

Sacubitril with valsartan is a new combination which was shown to be superior to enalapril in a large head-to-head trial, with an absolute reduction of cardiovascular death and heart failure hospitalisation of 4.7% (20% relative reduction).26 Sacubitril is a neprilysin inhibitor. It inhibits the degradation of vasoactive peptides including natriuretic peptides, thereby enhancing their beneficial effects such as vasodilation and diuresis. The combination reduces sympathetic tone, aldosterone and myocardial fibrosis and hypertrophy.

Sacubitril with valsartan can replace an ACE inhibitor or sartan if symptoms persist despite optimal medical therapy.7,27 This combination may become first-choice therapy in the future, given its efficacy. However, currently it should be used when a patient has been stabilised on an ACE inhibitor, beta blocker and aldosterone antagonist.

Previous angioedema (due to any cause) is a contraindication. A 36-hour ACE inhibitor washout period is an absolute requirement to reduce the risk of angioedema. The combination lowers the blood pressure more potently and therefore can cause hypotension. This improves over time, but can be addressed by reducing the dose of other vasodilators or halving the starting dose of sacubitril with valsartan.

Other drugs

Other therapies can be added to the essential drugs for heart failure (beta blockers, ACE inhibitors and aldosterone antagonists). They can also be considered secondary choices if the first-line drugs are not tolerated.

Diuretics

Loop diuretics are used by most patients at some stage for symptomatic control of heart failure. They should be used in addition to ACE inhibitors and beta blockers in patients with heart failure with reduced ejection fraction if there is associated symptomatic congestion. Diuretics can often be reduced as doses of neurohormonal blockers are increased.

A small dose of a thiazide or a potassium-sparing diuretic can be added to furosemide (frusemide) or bumetanide for a short period. This has a synergistic diuretic effect for patients with peripheral oedema resistant to treatment with a loop diuretic. Renal function and potassium need to be closely monitored.

Ivabradine

A raised resting heart rate is a marker of cardiovascular risk.28 Ivabradine reduces heart rate by inhibiting the sinus node, and results in a 5% absolute reduction (18% relative) in the risk of either cardiovascular mortality or heart failure hospitalisations.29 It is used in heart failure with sinus rhythm when the left ventricular ejection fraction is less than 35% as an add-on to an ACE inhibitor, aldosterone antagonist and maximally tolerated beta blocker if the heart rate is at least 77 beats per minute.29 It can be used if the patient cannot tolerate a beta blocker.

Ivabradine can only be used in sinus rhythm. It does not affect blood pressure, intracardiac conduction or myocardial contractility. It may cause visual symptoms, including flashing lights, which are not associated with retinal damage, and which usually resolve spontaneously. Stop ivabradine if atrial fibrillation develops.

Digoxin

Digoxin is useful for symptomatic control of heart failure in sinus rhythm, but only after therapy with an ACE inhibitor, beta blocker, aldosterone antagonist and diuretic has been optimised. It is a weak positive inotrope and increases vagal tone. In atrial fibrillation digoxin slows the heart rate by reducing atrioventricular nodal conduction.30 Digoxin does not improve survival, but can reduce hospitalisations associated with heart failure and improves symptoms.31 It should be used at a low dose in sinus rhythm, aiming for a serum digoxin of 0.5–0.9 nanogram/mL measured at least six hours after oral dosing.32 Digoxin toxicity may result from deteriorating renal function or dehydration, with symptoms most commonly including nausea, vomiting and drowsiness.33 Digoxin may also be useful for rate control in the treatment of atrial fibrillation in heart failure.

Hydralazine plus isosorbide dinitrate

High-dose hydralazine is an arterial vasodilator. Isosorbide dinitrate is predominantly a venodilator. The combination can be used with a beta blocker if the patient is intolerant of ACE inhibitors and sartans. Specialist advice should be sought. 

 

Devices

An implantable cardioverter defibrillator should be considered for primary or secondary prevention of ventricular arrhythmias if left ventricular ejection fraction is 35% or less to reduce the risk of sudden death and all-cause mortality.34 This may be implanted alone, or may be combined with cardiac resynchronisation therapy (or biventricular pacing) if the QRS duration on the ECG is prolonged at 130 milliseconds or above with left bundle branch block morphology. This reduces mortality and heart failure hospitalisations and improves symptoms. 

 

Heart failure with preserved ejection fraction

Compared to those with a reduced ejection fraction, patients with heart failure with preserved ejection fraction are older, more likely to be female and to have hypertension, atrial fibrillation, diabetes or obesity. The mechanism probably relates to a combination of pathophysiological processes including increased myocardial stiffness, abnormal myocardial relaxation and increased arterial stiffness.

No drug has been shown to improve survival,35 however recent data suggest that in a subset of patients with heart failure and preserved ejection fraction, aldosterone antagonists may improve clinical outcomes.36 Sacubitril with valsartan was found to be beneficial in a phase II study.37 The combination is therefore currently under evaluation for heart failure with preserved ejection fraction.

Diuretics should be used judiciously and over-diuresis avoided. Treatment should focus on aggressive control of concurrent conditions particularly hypertension. Atrial fibrillation should be managed according to guidelines, using a rate control strategy and anticoagulation initially, with a trial of rhythm control for persistent symptoms. Myocardial ischaemia, obesity and anaemia should be addressed. Exercise training can improve quality of life. 

 

Withdrawal of treatment

Substantial improvements in symptoms are seen after starting drug therapy and often patients will feel back to normal. Left ventricular ejection fraction can sometimes return to normal or close to the normal range. Drugs that confer a survival benefit, in particular ACE inhibitors and beta blockers, should not be stopped, as this may lead to a recurrence of heart failure.38 Diuretics and digoxin (in sinus rhythm) may be reduced and stopped if the patient remains stable.

When the goals of treatment move to palliation and symptom control, ACE inhibitors, beta blockers and aldosterone antagonists should be continued if possible, as they improve symptoms. Down-titration of doses may be needed if hypotension or issues with renal function and electrolytes occur. Statins and digoxin if not being used for atrial fibrillation can be withdrawn. Deactivation of an implantable cardioverter defibrillator should be considered in a patient entering the palliative phase of their illness, or in a patient making an informed end-of-life decision.39 This decision should be undertaken by the patient, their family, GP and specialist.

 

Drugs to avoid

Many drugs have been shown to exacerbate heart failure.40 Non-steroidal anti-inflammatory drugs (NSAIDs) including COX-2 inhibitors should be avoided as they cause salt and water retention and impair renal function. Non-dihydropyridine calcium channel blockers (verapamil and diltiazem) should be strictly avoided in heart failure with reduced ejection fraction due to their negative inotropic effect. Antiarrhythmic drugs (except beta blockers and amiodarone) and tricyclic antidepressants have pro-arrhythmic potential. Corticosteroids result in salt and water retention. Pioglitazone and some dipeptidyl peptidase 4 (DPP 4) inhibitors may increase the risk of heart failure. Non-potassium sparing diuretics can contribute to digoxin toxicity by causing hypokalaemia, and digoxin concentrations can be increased by amiodarone and spironolactone.

Potential drug–drug interactions occur with various complementary therapies, including St John’s wort, black cohosh and grapefruit juice. These should be avoided.

 

Conclusion

The type of heart failure determines its treatment. Echocardiography should be used to confirm the underlying aetiology. Patient education is key to successful management.

ACE inhibitors and beta blockers are the cornerstone of therapy for heart failure with reduced ejection fraction. Aldosterone antagonists are added if the patient is still symptomatic. These three drugs reduce mortality and morbidity. Digoxin and diuretics may also be useful if symptoms persist. The combination of valsartan with sacubitril is an evolving alternative to ACE inhibitors in heart failure with reduced ejection fraction. Drug doses need to be titrated to maximally tolerated doses to obtain the most benefit on symptoms and survival.

No drugs have been shown to improve survival in patients who have heart failure with preserved ejection fraction. Treatment should focus on related problems such as hypertension.

Conflict of interest: none declared

If you prescribe subscribe
 

References

  1. Sahle BW, Owen AJ, Mutowo MP, Krum H, Reid CM. Prevalence of heart failure in Australia: a systematic review. BMC Cardiovasc Disord 2016;16:32.
  2. Australian Institute of Health and Welfare. Cardiovascular disease, diabetes and chronic kidney disease - Australian facts: prevalence and incidence. Cardiovascular, diabetes and chronic kidney disease series no. 2. Cat. no. CDK 2. Canberra: AIHW; 2014. [cited 2017 Jul 1]
  3. Mosterd A, Hoes AW, de Bruyne MC, Deckers JW, Linker DT, Hofman A, et al. Prevalence of heart failure and left ventricular dysfunction in the general population; The Rotterdam Study. Eur Heart J 1999;20:447-55.
  4. Curtis LH, Whellan DJ, Hammill BG, Hernandez AF, Anstrom KJ, Shea AM, et al. Incidence and prevalence of heart failure in elderly persons, 1994-2003. Arch Intern Med 2008;168:418-24.
  5. Kemp CD, Conte JV. The pathophysiology of heart failure. Cardiovasc Pathol 2012;21:365-71.
  6. Owan TE, Hodge DO, Herges RM, Jacobsen SJ, Roger VL, Redfield MM. Trends in prevalence and outcome of heart failure with preserved ejection fraction. N Engl J Med 2006;355:251-9.
  7. Ponikowski P, Voors AA, Anker SD, Bueno H, Cleland JG, Coats AJ, et al; Authors/Task Force Members; Document Reviewers. 2016 ESC Guidelines for the diagnosis and treatment of acute and chronic heart failure: the Task Force for the diagnosis and treatment of acute and chronic heart failure of the European Society of Cardiology (ESC). Developed with the special contribution of the Heart Failure Association (HFA) of the ESC. Eur J Heart Fail 2016;18:891 975.
  8. Wong CY, Chaudhry SI, Desai MM, Krumholz HM. Trends in comorbidity, disability, and polypharmacy in heart failure. Am J Med 2011;124:136-43.
  9. Boren SA, Wakefield BJ, Gunlock TL, Wakefield DS. Heart failure self-management education: a systematic review of the evidence. Int J Evid-Based Healthc 2009;7:159-68.
  10. Heart Foundation. Living well with chronic heart failure. National Heart Foundation of Australia; 2015. [cited 2017 Jul 1]
  11. Austin J, Williams R, Ross L, Moseley L, Hutchison S. Randomised controlled trial of cardiac rehabilitation in elderly patients with heart failure. Eur J Heart Fail 2005;7:411-7.
  12. McAlister FA, Stewart S, Ferrua S, McMurray JJ. Multidisciplinary strategies for the management of heart failure patients at high risk for admission: a systematic review of randomized trials. J Am Coll Cardiol 2004;44:810-9.
  13. Flather MD, Yusuf S, Kober L, Pfeffer M, Hall A, Murray G, et al. Long-term ACE-inhibitor therapy in patients with heart failure or left-ventricular dysfunction: a systematic overview of data from individual patients. Lancet 2000;355:1575-81.
  14. Young JB, Dunlap ME, Pfeffer MA, Probstfield JL, Cohen Solal A, Dietz R, et al. Mortality and morbidity reduction with candesartan in patients with chronic heart failure and left ventricular systolic dysfunction: results of the CHARM low-left ventricular ejection fraction trials. Circulation 2004;110:2618-26.
  15. Cohn JN, Tognoni G. A randomized trial of the angiotensin-receptor blocker valsartan in chronic heart failure. N Engl J Med 2001;345:1667-75.
  16. Kotecha D, Manzano L, Krum H, Rosano G, Holmes J, Altman DG, et al. Effect of age and sex on efficacy and tolerability of \u03b2 blockers in patients with heart failure with reduced ejection fraction: individual patient data meta analysis. BMJ 2016;353:i1855.
  17. CIBIS Investigators and Committees. The Cardiac Insufficiency Bisoprolol Study II (CIBIS-II): a randomized trial. Lancet 1999;353:9-13.
  18. Packer M, Bristow MR, Cohn JN, Colucci WS, Fowler MB, Gilbert EM, et al. The effect of carvedilol on morbidity and mortality in patients with chronic heart failure. U.S. Carvedilol Heart Failure Study Group. N Engl J Med 1996;334:1349-55.
  19. Packer M, Fowler MB, Roecker EB, Coats AJ, Katus HA, Krum H, et al. Effect of carvedilol on the morbidity of patients with severe chronic heart failure: results of the carvedilol prospective randomized cumulative survival (COPERNICUS) study. Circulation 2002;106:2194-9.
  20. MERIT-HF Study Group. Effect of metoprolol CR/XL in chronic heart failure. Metoprolol CR/XL Randomized Intervention Trial in Congestive Heart Failure (MERIT-HF). Lancet 1999;353:2001-7.
  21. Flather MD, Shibata MC, Coats AJ, Van Veldhuisen DJ, Parkhomenko A, Borbola J, et al. Randomized trial to determine the effect of nebivolol on mortality and cardiovascular hospital admission in elderly patients with heart failure (SENIORS). Eur Heart J 2005;26:215-25.
  22. Hawkins NM, Virani S, Ceconi C. Heart failure and chronic obstructive pulmonary disease: the challenges facing physicians and health services. Eur Heart J 2013;34:2795-807.
  23. Pitt B, Zannad F, Remme WJ, Cody R, Castaigne A, Perez A, et al. The effect of spironolactone on morbidity and mortality in patients with severe heart failure. N Engl J Med 1999;341:709-17.
  24. Zannad F, McMurray JJ, Krum H; EMPHASIS-HF Study Group. Eplerenone in patients with systolic heart failure and mild symptoms. N Engl J Med 2011;364:11-21.
  25. Pitt B, Remme W, Zannad F, Neaton J, Martinez FA, Roniker B, et al. Eplerenone, a selective aldosterone blocker, in patients with left ventricular dysfunction after myocardial infarction. N Engl J Med 2003;348:1309-21.
  26. McMurray JJ, Packer M, Desai AS, Gong J, Lefkowitz MP, Rizkala AR, et al. Angiotensin-neprilysin inhibition versus enalapril in heart failure. N Engl J Med 2014;371:993-1004.
  27. Yancy CW, Jessup M, Bozkurt B, Butler J, Casey DE Jr, Colvin MM, et al. 2016 ACC/AHA/HFSA focused update on new pharmacological therapy for heart failure: an update of the 2013 ACCF/AHA guideline for the management of heart failure: a report of the American College of Cardiology/ American Heart Association Task Force on Clinical Practice Guidelines and the Heart Failure Society of America. J Am Coll Cardiol 2016;68:1476-88.
  28. Cook S, Togni M, Schaub MC, Wenaweser P, Hess OM. High heart rate: a cardiovascular risk factor? Eur Heart J 2006;27:2387-93.
  29. Swedberg K, Komajda M, Bohm M, Borer JS, Ford I, Dubost Brama A, et al. Ivabradine and outcomes in chronic heart failure (SHIFT): a randomised placebo-controlled study. Lancet 2010;376:875-85.
  30. Ambrosy AP, Butler J, Ahmed A, Vaduganathan M, van Veldhuisen DJ, Colucci WS, et al. The use of digoxin in patients with worsening chronic heart failure: reconsidering an old drug to reduce hospital admissions. J Am Coll Cardiol 2014;63:1823-32.
  31. The Digitalis Investigation Group. The effect of digoxin on mortality and morbidity in patients with heart failure. N Engl J Med 1997;336:525-33.
  32. Rathore SS, Curtis JP, Wang Y, Bristow MR, Krumholz HM. Association of serum digoxin concentration and outcomes in patients with heart failure. JAMA 2003;289:871-8.
  33. Pincus M. Management of digoxin toxicity. Aust Prescr 2016;39:18-20.
  34. National Heart Foundation of Australia and the Cardiac Society of Australia and New Zealand (Chronic Heart Failure Guidelines Expert Writing Panel). Guidelines for the prevention, detection and management of chronic heart failure in Australia. Updated October 2011. National Heart Foundation of Australia; 2011. [cited 2017 Jul 1]
  35. Nanayakkara S, Kaye DM. Management of heart failure with preserved ejection fraction: a review. Clin Ther 2015;37:2186-98.
  36. Pfeffer MA, Claggett B, Assmann SF, Boineau R, Anand IS, Clausell N, et al. Regional variation in patients and outcomes in the treatment of preserved cardiac function heart failure with an aldosterone antagonist (TOPCAT) trial. Circulation 2015;131:34-42.
  37. Solomon SD, Zile M, Pieske B, Voors A, Shah A, Kraigher Krainer E, et al. The angiotensin receptor neprilysin inhibitor LCZ696 in heart failure with preserved ejection fraction: a phase 2 double-blind randomised controlled trial. Lancet 2012;380:1387-95.
  38. Hopper I, Samuel R, Hayward C, Tonkin A, Krum H. Can medications be safely withdrawn in patients with stable chronic heart failure? Systematic review and meta-analysis. J Card Fail 2014;20:522-32.
  39. Alhammed NJ, O\u2019Donnell M, O\u2019Donnell D, Mariani JA, Gould PA, McGavigan AD, et al. Cardiac implantable electronic devices and end-of-life care: an Australian perspective. Heart Lung Circ 2016;25:814-9.
  40. Page RL, O\u2019Bryant CL, Cheng D, Dow TJ, Ky B, Stein CM, et al. Drugs that may cause or exacerbate heart failure: a scientific statement from the American Heart Association. Circulation 2016;134:e32-69.

Ingrid Hopper

Clinical pharmacologist and heart failure specialist physician, Alfred Health, Melbourne

Kellie Easton

Heart failure clinical nurse specialist, Alfred Health, Melbourne