2024 ACC Expert Consensus Decision Pathway for Treatment of Heart Failure With Reduced Ejection Fraction PDF

Summary

This document is a 2024 ACC expert consensus decision pathway for the treatment of heart failure with reduced ejection fraction. It details a report from the American College of Cardiology Solution Set Oversight Committee, outlining expert recommendations and consensus-based pathway.

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JOURNAL OF THE AMERICAN COLLEGE OF CARDIOLOGY VOL. 83, NO. 15, 2024
ª 2024 BY THE AMERICAN COLLEGE OF CARDIOLOGY FOUNDATION
PUBLISHED BY ELSEVIER

EXPERT CONSENSUS DECISION PATHWAY

2024 ACC Expert Consensus Decision
Pathway for Treatment of Heart Failure
With Reduced Ejection Fraction
A Report of the American College of Cardiology Solution Set Oversight Committee

Writing Thomas M. Maddox, MD, MSC, FACC, Chair Nasrien E. Ibrahim, MD, MPH, FACC
Committee James L. Januzzi JR, MD, FACC, Vice Chair JoAnn Lindenfeld, MD, FACC
Frederick A. Masoudi, MD, MSPH, MACC
Larry A. Allen, MD, MHS, FACC Shweta R. Motiwala, MD, MPH, FACC
Khadijah Breathett, MD, MS, FACC Estefania Oliveros, MD, MSC, FACC
Sara Brouse, PHARMD, BCCP, BCPS, FACC Mary Norine Walsh, MD, MACC
Javed Butler, MD, MBA, MPH, FACC Alan Wasserman, MD, FACC
Leslie L. Davis, PHD, RN, ANP-BC, FACC Clyde W. Yancy, MD, MSC, MACC
Gregg C. Fonarow, MD, FACC Quentin R. Youmans, MD, MSC

Solution Set Nicole M. Bhave, MD, FACC, Chair Dharam J. Kumbhani, MD, SM, FACC
Oversight Gurusher S. Panjrath, MBBS, FACC
Committee Niti R. Aggarwal, MD, FACC Barbara Wiggins, PHARMD, FACC
Katie Bates, ARNP, DNP David E. Winchester, MD, MS, FACC
Biykem Bozkurt, MD, PHD, FACC Megan Coylewright, MD, MPH, FACC—Ex Officio
John P. Erwin III, MD, FACC

TABLE OF CONTENTS

OVERVIEW....................................... 1445 2.2 Definitions................................... 1446

3. PATHWAY SUMMARY GRAPHIC................... 1447
1. INTRODUCTION................................. 1445
Figure 1. Ten Pivotal Issues About HFrEF........... 1448

2. ASSUMPTIONS AND DEFINITIONS................. 1446
4. DESCRIPTION AND RATIONALE:
2.1. General Clinical Assumptions.................... 1446 ANSWERS TO 10 PIVOTAL ISSUES IN HF........... 1447

This document was approved by the American College of Cardiology Clinical Policy Approval Committee in February 2024.
The American College of Cardiology requests that this document be cited as follows: Maddox TM, Januzzi JL Jr, Allen LA, Breathett K, Brouse S, Butler
J, Davis LL, Fonarow GC, Ibrahim NE, Lindenfeld J, Masoudi FA, Motiwala SR, Oliveros E, Walsh MN, Wasserman A, Yancy CW, Youmans QR. 2024 ACC
expert consensus decision pathway for treatment of heart failure with reduced ejection fraction: a report of the American College of Cardiology Solution
Set Oversight Committee. J Am Coll Cardiol 2024;83(15):1444-1488.
Copies: This document is available on the website of the American College of Cardiology (www.acc.org). For copies of this document, please contact
Elsevier Inc. Reprint Department via fax (212-633-3820) or e-mail ([email protected]).
Permissions: Multiple copies, modification, alteration, enhancement, and/or distribution of this document are not permitted without the express
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copyright/permissions).

ISSN 0735-1097/$36.00 https://doi.org/10.1016/j.jacc.2023.12.024
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APRIL 16, 2024:1444–1488 ACC Expert Consensus Decision Pathway for Treatment of HFrEF

4.1. How to Initiate, Add, or Switch to Evidence- 5. DISCUSSIONS AND IMPLICATIONS OF PATHWAY..... 1477
Based Guideline-Directed Therapy for HFrEF. 1447
4.1.1. Initiating GDMT.................... 1447 REFERENCES................................. 1478
Figure 2. Treatment Algorithm for
Guideline-Directed Medical Therapy...... 1450 APPENDIX 1
Figure 3. GDMT, Including Newer Therapies
in the ECDP for Chronic HF............ 1451 Author Relationships With Industry and
Other Entities (Relevant)....................... 1485
4.1.2. Angiotensin Receptor/Neprilysin
Inhibitor.......................... 1452
APPENDIX 2
4.1.3. Initiation of an ARNI De Novo Without Prior
Exposure to an ACE Inhibitor or ARB... 1455 Peer Reviewer Relationships With Industry and
4.1.4. SGLT Inhibitors.................... 1457 Other Entities (Comprehensive)................. 1487

4.1.5. Ivabradine......................... 1458
APPENDIX 3
4.1.6. Vericiguat......................... 1459
4.1.7. Consensus Pathway Algorithm for Initiation Abbreviations................................ 1488
and Titration of HFrEF Therapies...... 1459
4.1.8. Mitral Regurgitation and the Use of OVERVIEW
Transcatheter Mitral Valve Repair..... 1459
4.1.9. Patients in Whom New Therapies The 2021 Update to the 2017 American College of Cardi-
May Not Be Indicated............... 1460 ology (ACC) Expert Consensus Decision Pathway for
4.2. How to Achieve Optimal Therapy Given Multiple Optimization of Heart Failure Treatment: Answers to 10
Drugs for HF, Including Augmented Clinical Pivotal Issues About Heart Failure With Reduced Ejection
Assessment That May Trigger Additional
Fraction 1 provided a practical, streamlined resource for
Changes in GDMT (eg, Imaging Data,
Biomarkers, and Filling Pressures).......... 1460 clinicians managing patients with heart failure with
reduced ejection fraction (HFrEF). The expert consensus
4.2.1. Target Doses....................... 1460
decision pathway (ECDP) provided guidance on intro-
4.2.2. Barriers to Medication Titration....... 1461
ducing the numerous evidence-based therapies,
4.2.3. Clinical Assessment................. 1462
improving adherence, overcoming treatment barriers,
Figure 4. Testing and Medication Titration
acknowledging contraindications and situations for which
Following Diagnosis of HFrEF.......... 1463
little data exist, affording expensive therapies, treating
4.2.4. When to Order an Echocardiogram.... 1462
special cohorts, and making the transition to palliative
4.2.5. Biomarkers—When to Order care. Rather than focusing on extensive text, the docu-
Natriuretic Peptides................. 1462
ment provided practical tips, tables, and figures to make
4.2.6. Filling Pressure Assessment—When and
clear the steps, tools, and provisos needed to treat the
How to Measure Filling Pressures..... 1464
patient with HFrEF successfully and expeditiously. Many
4.3. When to Refer to an HF Specialist.......... 1464 of the pivotal issues addressed in the ECDP were not the
4.4. How to Optimize Care Coordination......... 1465 substance of clinical trials; rather, they represent the
4.5. How to Improve Adherence................ 1466 challenge of clinical practice.
4.5.1. Medication Nonadherence............ 1466 Since publication of the 2021 ECDP, new data have
4.5.2. General Approaches to developed that necessitate an update to the ECDP,
Improving Adherence............... 1467 including publication of the 2022 AHA/ACC/HFSA Guide-
4.5.3. Systems and Policies to line for the Management of Heart Failure.2 This update
Promote Adherence................. 1468 thus serves as updated guidance to clinicians based on
contemporary knowledge. The treatment of HFrEF can
4.6. What is Needed in Specific Patient Cohorts:
African-American Populations, Older Adults, feel overwhelming, and many opportunities to improve
and Patients Living With Frailty............ 1469 patient outcomes are being missed; hopefully, this ECDP
will streamline care to realize the best possible patient
4.7. How to Manage Patients’ Costs and Access to
HF Medications.......................... 1470 outcomes in HF (heart failure).

4.8. How to Manage the Increasing Complexity of
1. INTRODUCTION
HF Management......................... 1472

4.9. How to Manage Common Comorbidities..... 1475 The prevalence of HF is escalating rapidly, with a pro-
4.10. How to Integrate Palliative Care and Transition jected increase of 34% in upcoming decades.3,4 Com-
to Hospice Care.......................... 1476 pounding this, HF is a syndrome that consumes
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substantial health care resources, inflicts considerable with left ventricular ejection fractions (LVEFs) higher
morbidity and mortality, and adversely affects quality of than 40%, this document focuses primarily on the
life. Important breakthroughs have redefined opportu- management of patients with chronic HFrEF with
nities to change the natural history of HF with a broad LVEF #40% in the ambulatory setting and without
range of medical therapies, devices, and care strategies. symptoms or signs of clinical instability. For a patient
The purpose of this document is to update the 2021 presenting with symptoms of orthopnea or uncom-
ECDP with further data from recent studies and to provide fortable peripheral edema, the initial therapy would
succinct, practical guidance for managing patients with include diuretic agent therapy with early follow-up to
HFrEF. The format of the 10 Pivotal Issues in the ensure progress toward decongestion; following that,
prior versions of this ECDP was preserved, and their the steps outlined in this document would apply. For
associated treatment algorithms and tables have been more information on care of worsening HF/congestion,
updated to accommodate the evolving evidence. The the reader is directed to the ACC ECDP on Risk
Preface and Methods sections are accessible online in the Assessment, Management, and Clinical Trajectory of
Supplemental Appendix. Patients Hospitalized with HF. 6
3. The expert consensus Writing Committee endorses the
Ten Pivotal Issues in HFrEF evidence-based approaches to HF therapy and man-
1. How to initiate, add, or switch therapies with agement enumerated in the 2022 AHA/ACC/HFSA HF
consideration of newer evidence-based guideline- guideline.2
directed treatments for HFrEF. 4. These algorithms assume the clinician will seek input
2. How to achieve optimal therapy given multiple drugs as needed from a pharmacist, a cardiologist, an HF
for HF, including augmented clinical assessment (eg, specialist, and/or a disease management program, and/
imaging data, biomarkers, and filling pressures) that or other relevant specialists (eg, endocrinologists or
may trigger modifications in guideline-directed nephrologists) to guide clinical management.
therapy. 5. In all cases, patient preferences and values, in addition
3. When to refer to an HF specialist. to evidence-based clinical judgment, should guide
4. How to enhance care coordination. clinical decision-making.
5. How to improve medication adherence. 6. At any point in time, these suggestions and algorithms
6. How to tailor treatment in specific patient cohorts: may be superseded by new data.
African-American patients, older adults, and patients
with frailty. 2.2. Definitions
7. How to manage patients’ costs and increase access to AHA/ACC/HFSA Stages of HF:
HF medications.
8. How to manage the increasing complexity of HF. n Stage A: At risk for HF but without symptoms, struc-
9. How to manage common comorbidities. tural heart disease, or cardiac biomarkers of stretch or
10. How to integrate palliative care and the transition to injury (eg, patients with hypertension, atherosclerotic
hospice care. cardiovascular disease, diabetes, metabolic syndrome
and obesity, exposure to cardiotoxic agents, genetic
variant for cardiomyopathy, or positive family history
2. ASSUMPTIONS AND DEFINITIONS of cardiomyopathy).
n Stage B: Structural heart disease but no prior or current
To limit inconsistencies in interpretation, specific as- signs or symptoms of HF. Structural heart disease may
sumptions (eg, treatment effects in varied populations) include reduced left or right ventricular function, left
were considered by the writing group in development of ventricular (LV) hypertrophy, chamber enlargement,
the ECDP. References are supplied when applicable or wall motion abnormalities, or valvular heart disease.
appropriate. Additionally, evidence for increased filling pressures by
invasive hemodynamic measurements or imaging as
2.1. General Clinical Assumptions well as elevated concentrations of B-type natriuretic
1. Although many topics are generalizable to all patients peptide (BNP)/N-terminal pro–B-type natriuretic pep-
with HF, the focus of this effort is on patients with tide (NT-proBNP) or high-sensitivity cardiac troponins.
HFrEF. The reader is directed to the 2023 ACC ECDP on n Stage C: Structural heart disease with prior or current
Management of HFpEF for more focused details on symptoms of HF.
care for this population. 5 n Stage D: Marked HF symptoms that interfere with daily
2. Although some of the recommendations may be rele- life, with recurrent hospitalizations despite attempts to
vant to patients hospitalized with acute HF or in those optimize GDMT.
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GDMT: Guideline-directed medical therapy, repre- of the “4 pillars” of GDMT to maximize the early benefits
senting treatment options supported for use by clinical of improvement in patient-reported outcomes, reduction
practice guidelines. in HF hospitalizations, reduction in mortality, and
HFrEF: Clinical HF and LVEF #40%. improved adherence to GDMT.8-14 When using the thera-
New York Heart Association (NYHA) functional peutic standard of a 4-drug regimen (ARNI, beta-blocker,
classification: mineralocorticoid antagonist, SGLT inhibitor), there is an
aggregate treatment effect that includes increasing years
n Class I: No limitation of physical activity. Ordinary
of survival and years free from cardiovascular (CV) death
physical activity does not cause symptoms of HF.
or HF hospitalizations. 15 As an example, 4-class medica-
n Class II: Slight limitation of physical activity. Comfort-
tion initiation reduced the hazard of CV death or hospital
able at rest, but ordinary physical activity results in
admission for HF significantly (HR: 0.38; 95% CI: 0.3-0.47)
symptoms of HF.
compared with therapy with just an ACE inhibitor/ARB
n Class III: Marked limitation of physical activity.
plus a beta-blocker.15-18
Comfortable at rest, but less than ordinary activity
Another important development since the publication
causes symptoms of HF.
of the 2021 ECDP is the growing recognition of the safety
n Class IV: Unable to perform any physical activity
and urgency of initiating therapies rapidly. As an
without symptoms of HF, or symptoms of HF at rest.
example, the STRONG-HF (Safety, Tolerability, and Effi-
Optimal therapy: GDMT provided at either the target or cacy of Rapid Optimization, Helped by NT-proBNP
the highest-tolerated dose for a given patient. Testing, of Heart Failure Therapies) trial showed that
Target doses: Doses targeted in clinical trials. among patients admitted to the hospital with acute HF,
high-intensity management that included rapid up-
3. PATHWAY SUMMARY GRAPHIC titration of GDMT and close follow-up, with a goal of
reaching target doses within 6 weeks of discharge after
Figure 1 is an update of the 2017 ACC ECDP Summary hospitalization, was safe, well-tolerated, and associated
Graphic outlining the 10 pivotal issues about HFrEF. with a reduced risk of 180-day all-cause death or HF
readmission compared with usual care. 18,19
4. DESCRIPTION AND RATIONALE: ANSWERS Finally, the VICTORIA (Vericiguat Global Study in Pa-
TO 10 PIVOTAL ISSUES IN HF tients With Heart Failure and Reduced Ejection Fraction)
trial showed that in higher-risk patients with HFrEF
4.1. How to Initiate, Add, or Switch to Evidence-Based already on GDMT with worsening symptoms, the oral
Guideline-Directed Therapy for HFrEF soluble guanylyl cyclase stimulator vericiguat was supe-
Although loop diuretic agents are an important part of the rior to placebo in reducing the risk of HF hospitalization
treatment of congestion in the individual with HFrEF, and/or CV death.20 Subsequently, vericiguat was given a
once approaching or achieving euvolemia, it is critical to Class 2b recommendation in the updated 2022 AHA/ACC/
add and optimize therapies proven to reduce morbidity HFSA HF guideline.2 In light of these developments, an
and mortality. Established pharmacological therapies for update on when and how to add, switch, and titrate all
chronic HFrEF include renin-angiotensin inhibitors such HFrEF therapies to maximally tolerated and, ideally,
as angiotensin II receptor/neprilysin inhibitors (ARNIs), target doses (Figure 1, Table 1) was deemed important.
angiotensin-converting enzyme (ACE) inhibitors, and HF is a complex clinical syndrome typically associated
angiotensin receptor blockers (ARBs), along with with multiple comorbidities; most patients are on multi-
evidence-based beta-blockers, sodium-glucose cotrans- ple medications. No clinical trials have specifically eval-
porter (SGLT) inhibitors, mineralocorticoid antagonists, uated the potential for greater benefit or excessive risk of
loop diuretic agents, hydralazine/isosorbide dinitrate indicated therapies among patients with multimorbidity.
(HYD/ISDN), ivabradine, and vericiguat. With the excep- To assess tolerability of medications and best assess the
tion of loop diuretic agents, all of these therapies have trajectory of HF, it is often necessary for patients to have
been shown in randomized controlled trials to improve more frequent follow-ups, especially after initiation or
symptoms, reduce hospitalizations, and/or prolong sur- titration of therapy. These follow-ups may be in-person or
vival. 2,7 In contrast, use of digoxin as a treatment for virtual on a case-by-case basis and depending on patient
HFrEF lacks contemporary data; most of its use in modern stability and adjustment(s) made.
HFrEF management focuses on its role as a rate control
agent for atrial fibrillation (AF) in those with low blood 4.1.1. Initiating GDMT
pressure. Recommendations for starting GDMT in a patient with a
Since the publication of the 2021 ECDP, more data have new diagnosis of symptomatic HFrEF are detailed in
emerged to support early and rapid initiation and titration Figure 2.
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F I G U R E 1 Ten Pivotal Issues About HFrEF

CV ¼ cardiovascular; GDMT, guideline-directed medical treatment; HF ¼ heart failure; HFrEF ¼ heart failure with reduced ejection fraction.

In a patient with new-onset Stage C HFrEF, a com- and titration of GDMT should be early and as rapid as
mon question is which medication class to initiate first, possible with a goal to use the 4 key medication classes
and a common second question is how rapidly to add in each patient.
additional agents and titrate medication doses. There is For the person with de novo HFrEF, therapies should
no optimal order of initiation and/or titration, so the be initiated with a goal of reaching target or maximally
Writing Committee recommends that clinicians will tolerated doses of the 4 key medication classes as soon
need to approach each patient in an individual as possible, and ideally no longer than 3 months. In
fashion to decide on which agents to titrate and when many individuals, some GDMT may already be in place,
to do so. The Writing Committee also recommends that and the Writing Committee recommends initiation and
regardless of the sequencing of agents, careful initiation titration of missing key therapies as rapidly as possible,
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Starting and Target Doses of GDMT for HF (Choice and timing of each therapy and who should have them added are
TABLE 1
discussed in the text)*

Starting Dose Target Dose

Beta-blockers

Bisoprolol 1.25 mg once daily 10 mg once daily

Carvedilol 3.125 mg twice daily 25 mg twice daily for weight