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Transcript
European Heart Journal (2011) 32, 2507–2515
doi:10.1093/eurheartj/ehr311
ESC CLINICAL TRIAL UPDATE
Effects of selective heart rate reduction
with ivabradine on left ventricular remodelling
and function: results from the SHIFT
echocardiography substudy
1
Montreal Heart Institute, Université de Montréal, 5000 Belanger Street, Montreal, Quebec, Canada H1T 1C8; 2Department of Cardiology, University Pierre et Marie Curie Paris VI,
La Pitié-Salpétrière Hospital, Paris, France; 3Universitätskliniken des Saarlandes, Klinik für Innere Medizin III, Homburg/Saar, Germany; 4Division of Cardiovascular Medicine and the
Howard Gilman Institute for Heart Valve Disease, State University of New York Downstate Medical Center, Brooklyn and New York, NY, USA; 5Robertson Centre for Biostatistics,
University of Glasgow, Glasgow, UK; 6Maria Cecilia Hospital—GVM Care and Research, Ettore Sansavini Health Science Foundation, Cotignola, Italy; and 7Department of Emergency
and Cardiovascular Medicine, Sahlgrenska Academy, University of Gothenburg, Gothenburg, Sweden
Received 22 June 2011; revised 29 July 2011; accepted 3 August 2011; online publish-ahead-of-print 29 August 2011
See page 2481 for the commentary on this article (doi:10.1093/eurheartj/ehr317)
Aims
The SHIFT echocardiographic substudy evaluated the effects of ivabradine on left ventricular (LV) remodelling in
heart failure (HF).
.....................................................................................................................................................................................
Methods
Eligible patients had chronic HF and systolic dysfunction [LV ejection fraction (LVEF) ≤35%], were in sinus rhythm,
and results
and had resting heart rate ≥70 bpm. Patients were randomly allocated to ivabradine or placebo, superimposed
on background therapy for HF. Complete echocardiographic data at baseline and 8 months were available for
411 patients (ivabradine 208, placebo 203). Treatment with ivabradine reduced LVESVI (primary substudy endpoint)
vs. placebo [27.0 + 16.3 vs. 20.9 + 17.1 mL/m2; difference (SE), 25.8 (1.6), 95% CI 28.8 to 22.7, P , 0.001]. The
reduction in LVESVI was independent of beta-blocker use, HF aetiology, and baseline LVEF. Ivabradine also improved
LV end-diastolic volume index (27.9 + 18.9 vs. 21.8 + 19.0 mL/m2, P ¼ 0.002) and LVEF (+2.4 + 7.7 vs. 20.1
+ 8.0%, P , 0.001). The incidence of the SHIFT primary composite outcome (cardiovascular mortality or hospitalization for worsening HF) was higher in patients with LVESVI above the median (59 mL/m2) at baseline (HR 1.62, 95%
CI 1.03– 2.56, P ¼ 0.04). Patients with the largest relative reductions in LVESVI had the lowest event rates.
.....................................................................................................................................................................................
Conclusion
Ivabradine reverses cardiac remodelling in patients with HF and LV systolic dysfunction.
----------------------------------------------------------------------------------------------------------------------------------------------------------Keywords
Heart failure † Heart rate † Ventricular remodelling † Systolic dysfunction † Ivabradine
Introduction
Cardiac remodelling is central to the pathophysiology of heart
failure (HF)1 and is an established prognostic factor in patients
with HF. Left ventricular (LV) enlargement has been shown to
be associated with an increased risk for adverse cardiac events,2
while reduced LV ejection fraction (LVEF) is a powerful predictor
of cardiovascular outcomes and all-cause mortality.3 The therapeutic
effects of beta-blockade, angiotensin-converting enzyme (ACE) inhibition, and cardiac resynchronization therapy have been linked to
* Corresponding author. Tel: +1 514 376 3330 ext. 3612, Fax: +1 514 593 2500, Email: [email protected]
Published on behalf of the European Society of Cardiology. All rights reserved. & The Author 2011. For permissions please email: [email protected].
The online version of this article has been published under an open access model. Users are entitled to use, reproduce, disseminate, or display the open access version of this article
for non-commercial purposes provided that the original authorship is properly and fully attributed; the Journal, Learned Society and Oxford University Press are attributed as the
original place of publication with correct citation details given; if an article is subsequently reproduced or disseminated not in its entirety but only in part or as a derivative work this
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Jean-Claude Tardif 1*, Eileen O’Meara 1, Michel Komajda 2, Michael Böhm 3,
Jeffrey S. Borer 4, Ian Ford 5, Luigi Tavazzi 6, and Karl Swedberg 7, on behalf of the
SHIFT Investigators
2508
Methods
Study design and patients
The design of the SHIFT study has been described in detail in previous
publications.6,7 Briefly, this randomized, double-blind, placebocontrolled, parallel-group, international multicentre clinical trial evaluated 6505 male or female patients with moderate-to-severe chronic
HF and documented LV systolic dysfunction (LVEF ≤35%). Eligible
patients were in sinus rhythm and had resting heart rate of ≥70
beats per minute (bpm) on 12-lead electrocardiography; they had
been clinically stable for ≥4 weeks, and had been admitted to hospital
for worsening HF within the previous 12 months. All participants were
receiving background therapy for HF, including a beta-blocker. Other
inclusion and exclusion criteria are detailed elsewhere.6,7 After a
2-week run-in period, patients were randomly allocated to receive
ivabradine 5 mg bid or placebo. Randomization was stratified according
to beta-blocker intake at randomization and country. At subsequent
visits at 14 days, 28 days, and every 4 months thereafter (or at any
other time if necessary), the dosage of blinded study medication
could be adjusted upward (7.5 mg bid) or downward (2.5 mg bid)
depending on resting heart rate and tolerability.
The SHIFT echocardiography substudy was performed in 89 centres
in 21 countries participating in the main SHIFT study. To avoid selection bias, all the patients in each participating centre were invited to
enter the substudy, and those included signed a specific informed
consent form in addition to the documents related to the main
study. The locally appointed Ethics Committees have approved the
research protocol. The substudy was carried out in accordance with
the Declaration of Helsinki, 1964, and its text revisions. The SHIFT
trial is registered, number ISRCTN70429960.
The primary endpoint of the SHIFT echocardiography substudy was
the change in the LV end-systolic volume index (LVESVI) from baseline
to 8 months. Secondary endpoints were changes in LV end-diastolic
volume index (LVEDVI), non-indexed LV end-systolic and end-diastolic
volumes (LVESV and LVEDV), and LVEF during the same interval.
Tertiary endpoints included left atrial end-systolic volume index, grade
of diastolic dysfunction (assessed by Doppler imaging), grade of mitral
regurgitation, right ventricular (RV) myocardial performance index,
and RV s wave peak velocity (assessed by Doppler imaging). The
8-month duration of the substudy was selected because it was
considered long enough to allow detection of a benefit on LV
remodelling on the basis of the observed effects of ACE inhibitors and
beta-blockers1 while minimizing loss of patients to follow-up because
of death in this HF population.
Echocardiographic imaging and analyses
Echocardiography was performed at baseline (in the 2 weeks between
selection and inclusion) and within 1 month of the 8-month visit. The
two recordings were to be made by the same technician using
the same technique and the same equipment. Transthoracic echocardiography was performed with a phased-array imaging system equipped
with a transducer with second harmonics capability. Images were
obtained in the parasternal long- and short-axis and apical views, with
the subject lying in the left lateral position. Tissue Doppler imaging was
performed in the centres where technically feasible. All images were
stored digitally on CD-ROM. All participating sites received a detailed
imaging manual before initiation of the substudy, needed to be certified
by the core laboratory, and were regularly monitored for and informed
of quality of imaging recordings throughout the study.
The echocardiograms were read centrally according to predefined procedures in the core laboratory at the Montreal Heart Institute (Canada) by
technicians supervised by two cardiologists, all of them blinded to treatment and examination sequence (baseline vs. follow-up). Both recordings
from the same patient were assessed during two separate imaging analysis
sessions by the same technician and validated by the same cardiologist,
without knowledge of the results of the other imaging exam (i.e. results
of the first recording analysis were not known to the core laboratory
team when the second recording from the same patient was analysed).
All measurements were made according to the recommendations of the
American Society of Echocardiography (ASE) and the European Association of Echocardiography.8 Each assessment was analysed for at least
three consecutive cycles (or at least five in case of atrial fibrillation), avoiding post-ectopic beats. Atrial fibrillation was an exclusion criterion in the
SHIFT study. Two patients in the ivabradine group had atrial fibrillation
at the time of the 8-month echocardiogram; four patients (two ivabradine,
two placebo) sustained atrial fibrillation during the substudy (M0 to M8).
Primary and secondary criteria were assessed on two-dimensional apical
four- and two-chamber views, using biplane views when they were
analysable at both time points; if biplane apical views were not available
at baseline and follow-up, the analysis was conducted using the apical fourchamber view. Patients who only had analysable images from the apical
two-chamber view were excluded from the substudy. Each recording
was graded for the quality of LV endocardial border resolution: Grade
1, acceptable four- and two-chamber views; Grade 2, acceptable fouror two-chamber view; Grade 3, poor quality four- and two-chamber
views. Grade 3 recordings were excluded from the analysis of LV
volumes. Grade 3 was assigned to recordings with insufficient resolution
of LV endocardial border in 4 or more of the 17 ventricular segments
(using the ASE 17-segment model). Inter-reader and intra-reader variability was evaluated at the echocardiography core laboratory using 60
recordings analysed twice by each technician. Intra-class correlation
coefficients (ICCs) were found to be satisfactory for all readers (ranges
for LVESVI: intra-reader ICC, 0.96–0.99; inter-reader ICC, 0.95–0.98).
Left ventricular diastolic function was classified as normal, impaired LV
relaxation, pseudonormal, or restrictive based on standard criteria.
Statistical analysis
The sample size was estimated to demonstrate the superiority of
ivabradine over placebo on the change from baseline to 8 months in
LVESVI (primary substudy endpoint), using a two-sided Student’s
t-test for independent samples at a 5% type I error rate. Considering
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their beneficial effects on cardiac remodelling.1,4 A recent analysis
compared 30 clinical event trials and 88 remodelling trials with the
same drug or device therapy and reported that the odds ratio associated with therapy for long-term mortality correlate with the shorter
term effect of the therapy on LVEF, end-systolic volume, and enddiastolic volume.5 It is therefore relevant to evaluate the impact of
novel HF therapies on cardiac remodelling.
The heart rate lowering effect of ivabradine, a specific inhibitor of
the If current in the sinoatrial node, has been found to be beneficial in
patients with HF. The results of the Systolic Heart failure treatment
with the If inhibitor ivabradine Trial (SHIFT) showed that treatment
with ivabradine superimposed on background therapy for HF was
associated with an 18% reduction in risk for the primary composite
endpoint of cardiovascular death or hospitalization for worsening HF
(P , 0.0001).6 In this article, we present the results of the prespecified echocardiographic substudy of the SHIFT trial, aiming to evaluate the effects of ivabradine vs. placebo on LV remodelling and
function in HF.
J.-C. Tardif et al.
2509
Effects of ivabradine on left ventricular remodelling
Figure 1 Trial profile. FAS, full analysis set.
proportional hazards models adjusted for the echocardiography
endpoint as a dichotomous variable (below and above the median
value) and for other relevant factors at baseline [age, New York
Heart Association (NYHA) class, heart rate, ischaemic aetiology, systolic blood pressure, estimated glomerular filtration rate, and betablocker intake] were used to estimate hazard ratio comparing
classes of baseline echocardiography endpoints, with associated
95% CIs and P-values. Time-to-event curves were presented by
class of baseline LVESVI and estimated using the Kaplan–Meier
method. The number and percentage of SHIFT primary composite
endpoints subsequent to 8 months was calculated in each group
divided by tertile of relative change in LVESVI from baseline to 8
months, for ivabradine and placebo groups separately. The correlation between changes in LVEF and heart rate was tested using
the linear regression model including the two treatment groups.
The analyses on primary and secondary endpoints of the substudy
were all prespecified (LVESVI, LVEDVI, LVESV, LVEDV, and LVEF), as
was the case for tertiary echocardiographic endpoints (e.g. mitral
regurgitation). The exploratory analyses linking echocardiographic parameters to outcomes or heart rate were performed on a post hoc basis.
SAS (version 9.1) was used for all analyses.
Role of the funding source
The sponsor was responsible for data management and final data
analyses. The independent centre for statistics Keyrus Biopharma
(Nantes, France) verified all analyses. The cardiologists in charge of
the core laboratory and the SHIFT executive committee were responsible for the study design, the interpretation of the results, the development and writing of the report, and the decision to submit for
publication and had full access to all data. Members of the medical
and scientific departments of the sponsor supported the work of
the executive committee, but did not make any scientific or research
decisions independent of this committee.
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a standard deviation of 25 mL/m2, it was estimated that 414 patients
would be necessary to detect at least 8 mL/m2 difference between
treatment groups with 90% power. The sample size was adjusted to
520 patients since it was anticipated that the change from baseline in
LVESVI would not be assessable for approximately 20% of patients,
on the basis of the estimated rate of mortality and the projected
proportion of non-assessable echocardiographic recordings.
Baseline characteristics were presented by treatment group on all
patients randomized in the main study and participating in the echocardiography substudy, with means + SD for continuous variables, and
numbers and percentages for categorical variables. Changes in
primary and secondary endpoints were compared between treatment groups on patients included in the substudy who had taken at
least one dose of study drug and with an evaluation of the primary
endpoint considered reliable, using a covariance analysis adjusted
for beta-blocker intake at randomization, country, and baseline
value. The treatment effect was estimated using adjusted least
square means from this model, with associated two-sided 95%
confidence intervals (CI) and P-values (significance level set at
5%). A sensitivity analysis with imputation for missing values of
LVESVI (imputing conservatively no change in the ivabradine arm
and a mean change from baseline of 210 mL/m2 in the placebo
arm) indicated that the results are not unduly influenced by
missing data. Changes in LVESVI and LVEF from baseline to 8
months were divided into three classes (improvement, no change,
and worsening) according to clinical thresholds (15% for LVESVI
and 5% for LVEF, respectively). The percentages of patients with
an improvement were compared between treatment groups using
a x2 test. The relationship between baseline echocardiography criteria and the SHIFT primary composite endpoint (defined as first
event among hospitalization for worsening HF or cardiovascular
death) as well as its components was investigated in patients
included in the substudy and allocated to the placebo group. Cox
2510
J.-C. Tardif et al.
Table 1 Baseline characteristics of the substudy population (included set) vs. the population of the main SHIFT study6
(randomized set)
SHIFT echocardiography substudy
................................................................................
Ivabradine (n 5 304)
Placebo (n 5 307)
Main study (n 5 6505)
All (n 5 611)
...............................................................................................................................................................................
Demographic parameters
Age (years)
Sex (male)
Caucasian
Current smoker
BMI (kg/m2)
60.4 + 10.9
244 (80%)
59.1 + 11.1
252 (82%)
59.7 + 11.0
496 (81%)
60.4 + 11.4
4970 (76%)
276 (91%)
281 (92%)
557 (91%)
5771 (89%)
48 (16%)
48 (16%)
96 (16%)
1118 (17%)
27.7 + 4.5
27.7 + 4.9
27.7 + 4.7
28.0 + 5.1
78.4 + 9.0
78.8 + 9.2
78.6 + 9.1
79.9 + 9.6
137 (45%)
120.5 + 15.9
129 (42%)
119.1 + 15.4
266 (44%)
119.8 + 15.6
3357 (52%)
121.7 + 16.0
...............................................................................................................................................................................
Cardiac parameters
Heart rate (bpm)
Heart rate ≥77 bpm
Sitting SBP (mm Hg)
75.2 + 9.3
75.4 + 9.0
75.3 + 9.1
75.7 + 9.5
eGFR (MDRD formula) (mL/min/1.73 m2)
73.7 + 20.6
75.8 + 25.3
74.7 + 23.1
74.7 + 23.0
NYHA class
Class II
146 (48%)
140 (46%)
286 (47%)
3169 (49%)
Class III
156 (51%)
164 (53%)
320 (52%)
3223 (50%)
Class IV
2 (0.7%)
3 (1.0%)
5 (0.8%)
111 (1.7%)
...............................................................................................................................................................................
...............................................................................................................................................................................
Medical history
Duration of heart failure (years)
3.5 + 4.0
3.5 + 4.5
3.5 + 4.3
3.5 + 4.2
...............................................................................................................................................................................
Primary cause of heart failure
Ischaemic
205 (67%)
200 (65%)
405 (66%)
4418 (68%)
Non-ischaemic
Myocardial infarction
99 (33%)
180 (59%)
107 (35%)
178 (58%)
206 (34%)
358 (59%)
2087 (32%)
3666 (56%)
Hypertension
179 (59%)
175 (57%)
354 (58%)
4314 (66%)
Diabetes
Previous stroke
96 (32%)
25 (8%)
98 (32%)
28 (9%)
194 (32%)
53 (9%)
1979 (30%)
522 (8%)
History atrial fibrillation and/or atrial flutter
18 (6%)
20 (7%)
38 (6%)
522 (8%)
Left bundle branch block
45 (15%)
40 (13%)
85 (14%)
865 (13%)
b-blocker
281 (92%)
281 (92%)
562 (92%)
5820 (90%)
ACE inhibitor
243 (80%)
255 (83%)
498 (82%)
5116 (79%)
ARB
Diuretic (excluding antialdosterone)
51 (17%)
264 (87%)
36 (12%)
266 (87%)
87 (14%)
530 (87%)
927 (14%)
5414 (83%)
Aldosterone antagonist
224 (74%)
218 (71%)
442 (72%)
3922 (60%)
83 (27%)
99 (32%)
182 (30%)
1416 (22%)
10 (3%)
13 (4%)
23 (4%)
244 (4%)
9 (3%)
11 (4%)
20 (3%)
207 (3%)
...............................................................................................................................................................................
Treatment at randomization
Digitalis
...............................................................................................................................................................................
Devices
At least one device
ICD
Data are numbers of patients (%) or means + SD.
BMI, body mass index; bpm, beats per minute; SBP, systolic blood pressure; DBP, diastolic blood pressure; eGFR, estimated glomerular filtration rate; NYHA, New York Heart
Association; ACE, angiotensin-converting enzyme; ARB, angiotensin II receptor blocker; ICD, implantable cardioverter defibrillator; MDRD, Modification of Diet in Renal Disease
Study equation.
Results
A total of 613 patients were screened for the substudy and 611
were included (304 ivabradine, 307 placebo, Figure 1). A total of
200 patients were excluded leaving 411 patients (67% of the
included set, 208 ivabradine and 203 placebo) for analysis. The
main reasons for exclusion were poor quality of two- or fourchamber views (104 patients with insufficient resolution of LV
endocardial border, precluding reliable measurement of LV
volumes), no baseline and/or 8-month recording received at the
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Sitting DBP (mm Hg)
2511
Effects of ivabradine on left ventricular remodelling
Table 2 Types and doses of beta-blockers at baseline in the substudy population (included set) vs. the population of the
main SHIFT study6 (randomized set)
SHIFT echocardiography substudy
..................................................................................
Ivabradine (n 5 304)
Placebo (n 5 307)
Main study (n 5 6505)
All (n 5 611)
...............................................................................................................................................................................
b-blockers
281 (92%)
281 (91.5%)
562 (92%)
5820 (90%)
160 (57%)
46 (16%)
149 (53%)
60 (21%)
309 (55%)
106 (19%)
2604 (45%)
1486 (26%)
Metoprolol succinate
48 (17%)
45 (16%)
93 (17%)
815 (14%)
Metoprolol tartrate
16 (6%)
19 (7%)
35 (6%)
618 (11%)
18 (3%)
2 (0.4%)
198 (3%)
107 (1.8%)
Carvedilol
Bisoprolol
Nebivolol
Other
9 (3%)
2 (0.7%)
9 (3%)
–
...............................................................................................................................................................................
Mean daily dosage of b-blocker (mg)
23.5 + 17.1
5.7 + 3.2
23.5 + 16.5
5.9 + 3.2
25.0 + 17.8
6.2 + 3.3
Metoprolol succinate
131.3 + 80.2
131.9 + 73.3
131.6 + 76.5
89.9 + 60.0
72.7 + 46.2
6.4 + 2.8
115.8 + 50.8
4.3 + 2.6
96.1 + 52.8
5.4 + 2.8
69.1 + 47.4
5.9 + 2.9
Metoprolol tartrate
Nebivolol
...............................................................................................................................................................................
Patients at target dose of b-blocker
Patients at ≥50% target dose of b-blocker
76 (27%)
87 (31%)
163 (29%)
1488 (26%)
159 (57%)
154 (55%)
313 (56%)
3181 (56%)
Data are numbers of patients (%) or means + SD.
Table 3
Echocardiographic parameters at baseline, 8 months, and their changes in the substudy
Variable
Ivabradine
Placebo
Treatment effect
..................................................... .................................................... .........................................
n
Baseline
8 months
Change
n
Baseline
8 months
Change
E (SE), 95% CI
P-value
...............................................................................................................................................................................
Primary endpoint
LVESVI (mL/m2)
208
65.2 + 29.1
58.2 + 28.3
27.0 + 16.3
203
63.6 + 30.1
62.8 + 28.7
LVESV (mL)
208
123.8 + 55.6
110.8 + 54.6
LVEDVI (mL/m2)
204
93.9 + 32.8
85.9 + 30.9
LVEDV (mL)
204
178.4 + 63.4
163.7 + 60.6
LVEF (%)
204
32.3 + 9.1
34.7 + 10.2
20.9 + 17.1
25.8 (1.6), 28.8 to 22.7
,0.001
213.0 + 31.6
203
122.2 + 59.8
27.9 + 18.9
199
90.8 + 33.1
120.9 + 56.4
21.3 + 32.8
211.2 (3.0), 217.1 to 25.4
,0.001
89.0 + 31.6
21.8 + 19.0
25.5 (1.8), 28.9 to 22.0
214.7 + 36.4
199
0.002
174.7 + 67.6
171.7 + 63.8
22.9 + 36.8
210.9 (3.4), 217.6 to 24.2
199
31.6 + 9.3
31.5 + 10.0
20.1 + 8.0
...............................................................................................................................................................................
Secondary endpoints
2.4 + 7.7
2.7 (0.8),
1.3 to 4.2
0.001
,0.001
Data are numbers of patients (%) or means + SD. Parametric approach with adjustment for country, beta-blocker intake at randomization, and baseline value. E (SE), estimate
(standard error of treatment effect); CI, confidence interval.
LVESV, left ventricular end-systolic volume; LVESVI, left ventricular end-systolic volume index; LVEDV, left ventricular end-diastolic volume; LVEDVI, left ventricular end-diastolic
volume index; LVEF, left ventricular ejection fraction.
core laboratory (34 patients), and no matching apical biplane or
apical four-chamber views (nine patients). Other reasons for
exclusion were death (36 patients) and consent withdrawal
(17 patients).
The characteristics of the substudy population at baseline are
presented in Table 1, and compared with those of the main
study population.6 The mean age of the population was 59.7
years. The majority of patients were men (81%) and Caucasians
(91%). Mean resting heart rate at baseline was 78.6 + 9.1 bpm
and 66% had HF of ischaemic aetiology. The population was
evenly distributed between NYHA classes II and III. Most of
the patients were receiving a beta-blocker (92%) and a renin –
angiotensin–aldosterone system (RAAS) antagonist (94%). The
main beta-blockers used were carvedilol, bisoprolol, and metoprolol succinate (Table 2), with 29% of the population at guidelinesbased target dose of beta-blocker and 56% receiving ≥50% of
the target dose. The characteristics of the substudy population
were similar to those of the population in the main study,
except for a lower rate of history of hypertension in the substudy
(59 vs. 66%) and a higher rate of use of aldosterone antagonists
(72 vs. 60%). There were no clinically relevant differences
between the treatment groups in the substudy, between the
SHIFT patients included in the substudy and SHIFT patients not
included in the substudy (see online Supplementary material), or
between patients randomized in the study and the full analysis
set for the substudy.
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23.5 + 16.0
6.2 + 3.2
Carvedilol
Bisoprolol
2512
J.-C. Tardif et al.
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Figure 2 (A) Relative change in left ventricular end-systolic volume index (LVESVI) and (B) absolute change in left ventricular ejection fraction
(LVEF) from baseline to 8 months. The grey and white bars represent percentages of patients reaching echocardiographic criteria for the ivabradine and placebo groups, respectively.
Median treatment duration during the substudy was 8.1 months
(IQR, 7.8 –8.3) and median follow-up after the 8-month echocardiogram was 16.1 months (IQR, 13–19.9). Mean dosage of
ivabradine during the substudy was 6.0 + 1.6 mg bid. Heart rate
was reduced by 14.7 + 11.4 bpm in the ivabradine group to
63.5 + 9.5 bpm at 8 months vs. by 5.8 + 10.8 bpm to 72.2 +
12.4 bpm with placebo.
Mean baseline LVESVI was similar in the ivabradine and placebo
groups (65.2 + 29.1 and 63.6 + 30.1 mL/m2, respectively). Treatment with ivabradine for 8 months was associated with a significant
reduction in LVESVI vs. placebo [27.0 + 16.3 vs. 20.9 + 17.1 mL/m2,
estimate (SE) 25.8 (1.6), 95% CI 28.8 to 22.7, P , 0.001,
Table 3]. More patients in the ivabradine group had a 15% or
more decrease in LVESVI than in the placebo group (38 vs. 25%,
respectively, P ¼ 0.005) (Figure 2). The ivabradine-associated
improvement in LVESVI was consistent in all the prespecified subgroups: ischaemic vs. non-ischaemic HF (estimate of treatmentplacebo difference 25.51 vs. 27.61), with or without half target
beta-blocker dose at randomization (24.39 vs. 27.89), and
baseline LVEF above and below 32% (26.08 vs. 25.77).
2513
Effects of ivabradine on left ventricular remodelling
The mean values of the secondary efficacy criteria were similar at
baseline in the ivabradine and placebo groups (Table 3). Significant
treatment effects were found at 8 months for ivabradine vs.
placebo on LVEDVI (P ¼ 0.002), LVESV (P , 0.001), LVEDV
(P ¼ 0.001), and LVEF (P , 0.001) (Table 3). Left ventricular ejection
fraction was increased by 2.4 + 7.7% in the ivabradine group but was
unchanged in the placebo group (20.1 + 8.0%). More than a third
(36%) of the patients in the ivabradine group had ≥5% increase
in LVEF vs. less than a quarter (23%) of the placebo group
(P ¼ 0.003) (Figure 2). Tertiary endpoints were measured in
limited numbers of patients. There were no significant changes in
left-atrial end-systolic volume index or RV myocardial performance
index in either group, while RV s wave peak velocity increased over
8 months with ivabradine and decreased with placebo (data not
shown). There were 351 patients who had an evaluation of mitral
regurgitation at baseline and 8 months. Of these, mitral regurgitation
improved by at least one grade in 18 patients (18/176, 10%) in the
ivabradine group vs. 14 patients (14/175, 8%) in the placebo group
(P ¼ 0.47). More patients improved by at least one grade of LV diastolic function from baseline to 8 months with ivabradine [26 patients
out of 120 fully documented patients (22%)] than with placebo
[11 patients out of 106 (10%), P ¼ 0.02].
To explore the impact of baseline values of echocardiographic
parameters reflecting LV systolic function, we divided the
placebo group by median baseline LVESVI (59 mL/m2) and found
that the incidence of the primary composite endpoint of hospitalization for worsening HF or cardiovascular mortality was significantly greater in the patients with higher values (HR 1.62, 95%
CI 1.03–2.56, P ¼ 0.04, Figure 3). The increase in risk appeared
to be driven by both hospitalizations for worsening HF (HR
1.80, 95% CI 1.06–3.07, P ¼ 0.03) and cardiovascular deaths (HR
1.56, 95% CI 0.78–3.10, P ¼ 0.21, Table 4). Similar changes in
risk were observed when the placebo group was split by median
baseline LVEDVI (85 mL/m2), or for median baseline LVEF (31%),
though the differences were not statistically significant for LVEF
(Table 4).
In the SHIFT echocardiography substudy population, there were
102 primary composite endpoint events (81 hospitalizations for
worsening HF and 21 cardiovascular deaths), 63 of which occurred
after 8 months. This relatively low number of events provided little
power to detect an effect of treatment on outcomes according to
echocardiographic parameters. To obtain some measure of the
effect, we divided the ivabradine group and the placebo group
by tertiles of change in LVESVI and determined the incidence of
primary composite endpoint after 8 months for each third.
Despite few events in this exploratory analysis, patients in the
lowest third, i.e. those with the greatest relative reductions in
LVESVI, had numerically lower event rates than those with
smaller relative reductions or relative increases (data not shown).
The relationships between changes in heart rate and both changes
in LV volumes and LVEF were explored. There was an inverse
relation between the change in heart rate and the change in LVEF
(r ¼ 20.17, P ¼ 0.0006); expressed differently, larger decreases in
heart rate were associated with greater increases in LVEF. In contrast, there was no significant relationship between changes in
heart rate and changes in LV volumes for all patients. However,
when split by baseline median heart rate, those patients who were
above the median of 77 bpm had larger LV volumes (LVESVI: 68.1
+ 29.3 vs. 61.8 + 30.3 mL/m2, P ¼ 0.019) and lower LVEF (29.4
+ 9.0 vs. 33.1 + 8.8%, P , 0.001) at baseline.
Discussion
Our results indicate a reversal of cardiac remodelling with ivabradine, with significant reductions in LV volumes and an increase in
LVEF over 8 months of treatment. These changes were consistent
in the prespecified subgroups, irrespective of baseline LVEF,
beta-blocker intake, and aetiology of HF. Moreover, these results
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Figure 3 Kaplan –Meier cumulative event curves for the SHIFT primary composite endpoint of cardiovascular death or hospitalization for
worsening heart failure in the placebo group split by median left ventricular end-systolic volume index (LVESVI) ≥59 vs. ,59 mL/m2.
2514
J.-C. Tardif et al.
Table 4 Relationship between echocardiography
parameters at baseline and the SHIFT primary
composite endpoint and its components in the placebo
group of the substudy (included set echo)
Number of
events
HR (95% CI)
P-value
................................................................................
LVESVI (n ¼ 263)
SHIFT primary composite endpoint
≥59 mL/m2
,59 mL/m2
56
35
1.62 (1.03– 2.56) 0.04
Hospitalization for worsening heart failure
≥59 mL/m2
,59 mL/m2
1.80 (1.06– 3.07) 0.03
28
15
1.56 (0.78– 3.10) 0.21
Cardiovascular deatha
≥59 mL/m2
,59 mL/m2
................................................................................
LVEDVI (n ¼ 257)
SHIFT primary composite endpoint
≥85 mL/m2
,85 mL/m2
56
34
1.75 (1.11– 2.75) 0.02
Hospitalization for worsening heart failure
≥85 mL/m2
,85 mL/m2
44
24
1.96 (1.15– 3.34) 0.01
28
15
1.65 (0.84– 3.23) 0.14
Cardiovascular death
≥85 mL/m2
,85 mL/m2
................................................................................
LVEF (n ¼ 257)
SHIFT primary composite endpoint
,31%
50
≥31%
1.21 (0.78– 1.88) 0.40
40
Hospitalization for worsening heart failure
,31%
39
1.28 (0.77– 2.13) 0.34
≥31%
Cardiovascular death
,31%
≥31%
29
26
1.29 (0.67– 2.51) 0.45
17
LVESVI, left ventricular end-systolic volume index; LVEDVI, left ventricular
end-diastolic volume index; LVEF, left ventricular ejection fraction; HR, hazard
ratio; CI, confidence interval.
a
There were 43 cardiovascular deaths in the placebo group over the entire
duration of the main SHIFT study (Table 4), compared with 36 deaths in the two
study arms combined during the 8 months of follow-up of the echocardiography
substudy (Figure 1).
occurred despite treatment with beta-blockers and RAAS
antagonists, each used in more than 90% of patients.
Our results have important clinical implications since cardiac
remodelling is a central feature of the progression of HF. We
explored the association between the risk of clinical cardiovascular
adverse outcomes and echocardiographic parameters in a series
of complementary analyses. Left ventricular end-systolic volume
index ≥59 mL/m2 at baseline was associated with a 62% increase
in relative risk for the SHIFT primary composite endpoint of
cardiovascular death or hospitalization for worsening HF vs.
Limitations
The reduction in morbidity and mortality with RAAS antagonists
and beta-blockade in HF is associated with improvement in LV
function.16 – 20 Our analysis was not designed to clarify the timecourse of treatment effects and could not evaluate the acute
effect of ivabradine. In the absence of acute measurements, the
degree to which volumetric changes are influenced by heart rate
itself cannot be determined. Our finding of improved LV function
with ivabradine shows that further improvement in reverse cardiac
remodelling and slowing of disease progression can be achieved, in
addition to that obtained with background therapy for HF. Patients
needed to be treated with a beta-blocker to be eligible for this
study, and the SHIFT trial sought to exclude patients who were
not receiving guidelines-driven beta-blocker dosing. Given the
Downloaded from http://eurheartj.oxfordjournals.org/ by guest on June 29, 2016
44
25
patients with LVESVI ,59 mL/m2. Using the median to divide
these data may have diluted the relation to the SHIFT primary
composite endpoint observed at higher LV volumes. In addition,
the patients with the largest treatment-related reductions in
LVESVI at follow-up had a numerically lower rate of the SHIFT
primary composite endpoint than patients with smaller reductions
in LVESVI. This exploratory analysis suggests that there is a link
between treatment-related improvement in LV function and prognosis in HF patients, and is consistent with the observation that
short-term effects of drugs or devices are associated with longterm effects on mortality.5
The study provides further support for the role of heart rate
reduction with ivabradine to improve cardiac remodelling. Compared with those with lower heart rates, patients with a heart
rate ≥77 bpm at baseline had larger LVESVI and lower LVEF at
baseline. Furthermore, there was a statistically significant albeit
weak inverse relationship between the change in heart rate and
the change in LVEF, which means that larger decreases in heart
rate during follow-up were associated with greater increases in
LVEF. A positive effect of ivabradine on LV remodelling was also
demonstrated in the echocardiographic substudy of the BEAUTIFUL (morBidity-mortality EvAlUaTion of the If inhibitor ivabradine
in patients with coronary disease and left ventricULar dysfunction)
trial, in a different population of patients with stable coronary
artery disease and LV systolic dysfunction.9 Results in experimental
studies are consistent with the effects of ivabradine on cardiac
remodelling that we observed. In a rat model of chronic mild
HF, ivabradine preserved cardiac output and improved LV function
and geometry.10 These changes were linked to modifications in the
extracellular matrix and in cardiac myocyte function. Ivabradine
also has had beneficial effects on the global cardiac remodelling
process involved in HF, including optimization of energy consumption, reverse electrophysiological and structural cardiac remodelling.11 Similar effects with ivabradine have been found by other
workers in a rat model of chronic severe HF, including reductions
in fibrosis, local RAAS stimulation, and sympathetic drive, as well as
improvement in endothelial function.12 – 14 Experiments in a canine
model also indicated a positive impact on sarcoplasmic reticulum
calcium overload.15 Together, these experimental results support
a beneficial role of ivabradine on LV remodelling and function
that may contribute to the reduction in cardiac morbidity and mortality found in patients with HF.
Effects of ivabradine on left ventricular remodelling
beta-blocker dosage observed in SHIFT (which was similar to
other recently published data21) and the effect on LV ejection fraction of higher doses,22 further investigation would be required to
shed light on the comparison between ivabradine and more aggressive beta-blockade (when tolerated). Our data were recorded in
patients with heart rates ≥70 bpm and in sinus rhythm and predominantly in men, which may limit the generalization of our results
to all patients with HF. Another limitation of our study is that
about a third of patients were excluded from the analysis, usually
for reasons related to the quality or collection of the echocardiographic recordings.
Conclusions
Supplementary material
Supplementary material is available at European Heart Journal
online.
Funding
This work was supported by Servier, France. Funding to pay the Open
Access publication charges for this article was provided by Servier.
Conflict of interest: All authors have received fees, research grants,
or both from Servier.
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Heart rate reduction with ivabradine reverses LV remodelling in
patients with HF and LV systolic dysfunction. Treatment with ivabradine is associated with marked reductions in LV volumes and a
significant improvement in LVEF, therefore suggesting that it is
modifying disease progression in patients with HF.
2515