Empaglifozin improved CV outcomes in patients with HFrEF

Empagliflozin improved CV
outcomes in patients with HFrEF
Empagliflozin significantly improved clinical outcomes
vs placebo in patients with HFrEF with or without
T2D in the EMPEROR-Reduced study1
Primary endpoint
Secondary endpoints
30% RRR
25% RRR
Reduced risk
of first and
recurrent HHF
5.2% ARR, NNT=19
Reduced risk of CV death or HHF
Empagliflozin
Cumulative incidence (%)
35
30
Placebo
Significantly
slowed decline
in eGFR slope
Empagliflozin vs placebo
−2.28
−0.55
25
20
HR: 0.75
15
(95% CI: 0.65, 0.86)
p<0.001
10
5
0
0
90
180
270
360
450
540
630
720
810
Days since randomization
No. at risk
Placebo
1867
1715
1612
1345
1108
854
611
410
224
109
Empa
1863
1763
1677
1424
1172
909
645
423
231
101
HR: 0.70 (95% CI: 0.58, 0.85)
p<0.001
mL/min/1.73 m2/year
p<0.001
View more
safety data
Overall safety data
Similar rates of AEs and serious AEs in the empagliflozin and placebo treatment arms
76.2%
Any AEs
41.4%
Any serious AEs
78.5%
48.1%
No clinically meaningful increases in hypovolaemia,
1,2
symptomatic hypotension, hyperkalaemia or UTIs
Click-to-view inclusion
criteria and study design
Access full EMPEROR-Reduced paper here
https://pubmed.ncbi.nlm.nih.gov/33197559/
In addition, empagliflozin reduced the
risk of inpatient and outpatient worsening
HF events* vs placebo3
Exploratory outcomes
Empagliflozin reduced the severity of HF hospitalizations
and the utilization of interventions, vs placebo
Time to first
Inpatient
Outpatient
25% RRR
35% RRR
34% RRR
33% RRR
HHF requiring IV
vasopressor or positive
inotropic drugs or
mechanical or
surgical intervention
HHF that required
intensive care
emergency or urgent
care visit for worsening
HF requiring IV therapy
study visit requiring
intensification
of diuretics
HR: 0.65 (95% CI: 0.50, 0.85)
p=0.002
HR: 0.66 (95% CI: 0.53, 0.83)
p=0.0004
HR: 0.67 (95% CI: 0.58, 0.78)
p<0.0001
HR: 0.75 (95% CI: 0.57, 0.98)
p=0.03
12
DAYS
Empagliflozin reduced the risk of a worsening
HF event* with statistical significance
reached at 12 days after randomization
Improvements were seen across both
inpatient and outpatient outcomes
Access full clinical stability paper here
https://pubmed.ncbi.nlm.nih.gov/33081531/
Patients treated with empagliflozin vs placebo showed benefits
in terms of quality of life and NYHA functional class3,4
20–40%
less likely
to experience
20–40%
more likely
to experience
Patients
treated with
empagliflozin
vs placebo
worsening
NYHA class3
improvement
in NYHA class3
Shifts in NYHA class were apparent at every scheduled
assessment throughout the first year of follow-up
Empagliflozin provided a significant early
and sustained improvement in patients'
quality of life based on KCCQ scores4
Conclusion
Empagliflozin reduced the risk and total number of inpatient and outpatient
worsening HF events as well as improved quality of life and NYHA functional class,
vs placebo. Benefits were seen early and were sustained during follow-up.
All hazard ratios (95% CI) are for empagliflozin vs placebo.
*Worsening HF event defined as death, hospitalization for HF or an emergent or urgent HF visit requiring
intravenous treatment.
AE, adverse event; ARR, absolute risk reduction; CI, confidence interval; CV, cardiovascular; EF, ejection fraction; eGFR, estimated
glomerular filtration rate; Empa, empagliflozin; GTI, genital tract infection; HF, heart failure; HFrEF, heart failure with reduced ejection
fraction; HHF, hospitalization for heart failure; HR, hazard ratio; IV, intravenous; KCCQ, Kansas City Cardiomyopathy Questionnaire; LVEF,
left ventricular ejection fraction; NNT, number needed to treat; NT-proBNP, N-terminal prohormone of brain natriuretic peptide; NYHA, New
York Heart Association; OD, once daily; RRR, relative risk reduction; SOC, standard of care; T2D, Type 2 diabetes; UTI, urinary tract infection.
This document provides a summary of key efficacy outcomes and related subanalyses from the EMPEROR-Reduced trial
and is not intended to be a comprehensive reproduction. For full information, please refer to the original publications.
1. Packer M et al. N Engl J Med. 2020;383:1413; 2. Anker SD et al. Circulation 2021;143:337; 3. Packer M et al. Circulation
2021;143:326; 4. Butler J et al. Eur Heart J. 2021;42:1203.
SC-CRP-08448
June 2021
Empagliflozin improved CV
outcomes inPrimary
patients
with
HFrEF
endpoint
Empagliflozin significantly improved clinical outcomes
vs placebo in patients with HFrEF with or without
T2D in the EMPEROR-Reduced study1
25% RRR
5.2% ARR, NNT=19
Secondary endpoints
Reduced
risk
of
CV
death
or
HHF
Significantly
30%
RRR
25% RRR
Cumulative incidence (%)
Cumulative incidence (%)
Primary endpoint
30Empagliflozin
35
30
slowed decline
Reduced risk
of first and
Placebo
recurrent HHF
5.2% ARR, NNT=19
35
Reduced
risk of CVEmpagliflozin
death or HHF
in eGFR slope
Empagliflozin vs placebo
Placebo
20
HR: 0.75
20
15
10
(95% CI: 0.65, 0.86)
p<0.001
15
5
HR: 0.75
(95% CI: 0.65, 0.86)
p<0.001
0
0
No. at risk
90
10
180
270
360
450
540
630
720
810
Days since randomization
Placebo
1867
1715
1612
1345
1108
854
611
410
224
109
Empa
1863
1763
1677
1424
1172
909
645
423
231
101
5
−2.28
−0.55
25
25
HR: 0.70 (95% CI: 0.58, 0.85)
p<0.001
0
0
90
180
270
360
450
mL/min/1.73 m2/year
p<0.001
540
630
720
Days since randomization
No. at risk
1715
Overall safety data
1612 1345 1108 854
611
810
View more
safety data
Placebo
1867
410
224
Empa
Similar
1863of AEs
1763
1677 AEs
1424
909 and
645placebo
423 treatment
231 arms
101
rates
and serious
in the1172
empagliflozin
76.2%
109
41.4%
Any empagliflozin;
serious AEs
Any AEs
ARR, absolute
risk reduction; CI, confidence interval; CV, cardiovascular; Empa,
HHF, hospitalization for heart failure;
78.5%risk reduction. Packer M et al. N Engl J Med. 2020;383:1413.48.1%
HR, hazard ratio; NNT, number needed to treat; RRR, relative
No clinically meaningful increases in hypovolaemia,
1,2
symptomatic hypotension, hyperkalaemia or UTIs
Click-to-view inclusion
criteria and study design
Access full EMPEROR-Reduced paper here
https://pubmed.ncbi.nlm.nih.gov/33197559/
Close
Inclusion criteria
No clinically meaningful increases
in hypovolaemia,
In addition,
empagliflozin
symptomatic
hypotension,
hyperkalaemiareduced
or UTIs1,2
the
risk of inpatient and outpatient worsening
10.6% 3
HF events* vs placebo
Volume
depletion
5.7%
Symptomatic
hypotension
5.5% reduced the severity of HF hospitalizations
Empagliflozin
and the utilization of interventions, vs placebo
Empagliflozin (n=1863)
5.9%
Hyperkalaemia
events
Placebo (n=1863)
6.8%
Time to first
Inpatient
4.9%
Urinary tract
infection (UTI)
Genital tract
infection (GTI)
9.9%
Exploratory outcomes
Outpatient
Complicated 1.0%
UTIs 0.8%
4.5%
1.7%
0.6%
25% RRR
0.3%
Complicated
GTIs
35% RRR
34% RRR
0.3%
33% RRR
HHF requiring IV
HHF that required
or urgent
study visit requiring
No severe hypoglycaemia*
inemergency
patients without
diabetes
vasopressor or positive
intensive care
care visit for worsening
2intensification
and
no
cases
of
ketoacidosis/diabetic
ketoacidosis
HR: 0.65 (95% CI: 0.50, 0.85)
inotropic drugs or
HF requiring IV therapy
of diuretics
p=0.002
HR: 0.66 (95% CI: 0.53, 0.83)
HR: 0.67 (95% CI: 0.58, 0.78)
mechanical or
p=0.0004
p<0.0001
surgical intervention
HR:
0.75 (95%
CI: 0.57, 0.98) episode requiring assistance.
*Defined
as a hypoglycaemic
p=0.03
1. Packer M et al. N Engl J Med. 2020;383:1413; 2. Anker SD et al. Circulation 2021;143:337.
12
DAYS
Close
Empagliflozin reduced the risk of a worsening
HF event* with statistical significance
criteriarandomization
reached at 12Inclusion
days after
Improvements were seen across both
• Ageand
≥18 years
inpatient
outpatient outcomes
• Chronic HFrEF, NYHA II–IV
• LVEF ≤40%
• Receiving standard of care (SOC)
Access full clinical stability paper here
https://pubmed.ncbi.nlm.nih.gov/33081531/
No hospitalization required
Ejection fraction (EF)
≥36% to ≤40%
≤40%
≥31% to ≤35%
≤30%
Patients treated with empagliflozin vs placebo showed benefits
in terms of quality of life and NYHA functional class3,4
and
hospitalization
for HF within
12 months
20–40%
Without atrial fibrillation
more
likely
With atrial fibrillation
improvement
less likely
to experience
worsening
Patients
treated with
empagliflozin
vs placebo
NT-proBNP
to experience
20–40%
≥600 ≥1200
pg/mL
pg/mL
≥2500 ≥5000
pg/mL
pg/mL
NYHA class3
≥1000 ≥2000
pg/mL
pg/mL
≥600 ≥1200
pg/mL
pg/mL
in NYHA class3
Study design
Shifts in NYHA class were apparent at every scheduled
assessment throughout the first year of follow-up
Empagliflozin 10 mg OD + SOC
EMPEROR-Reduced
LVEF ≤40%
Placebo OD + SOC
3730 patients
Median follow-up =16 months
(event-driven)
Empagliflozin provided a significant early
HFrEF, heart failure with reduced ejection fraction; and
LVEF, leftsustained
ventricular ejection
fraction; NT-proBNP, N-terminal
prohormone of brain
improvement
in patients'
natriuretic peptide; NYHA, New York Heart Association; OD, once daily; SOC, standard of care. Packer M et al. N Engl
J Med. 2020;383:1413.
quality of life based on KCCQ scores4
Conclusion
Empagliflozin reduced the risk and total number of inpatient and outpatient
worsening HF events as well as improved quality of life and NYHA functional class,
vs placebo. Benefits were seen early and were sustained during follow-up.
All hazard ratios (95% CI) are for empagliflozin vs placebo.
*Worsening HF event defined as death, hospitalization for HF or an emergent or urgent HF visit requiring
intravenous treatment.
AE, adverse event; ARR, absolute risk reduction; CI, confidence interval; CV, cardiovascular; EF, ejection fraction; eGFR, estimated
glomerular filtration rate; Empa, empagliflozin; GTI, genital tract infection; HF, heart failure; HFrEF, heart failure with reduced ejection
fraction; HHF, hospitalization for heart failure; HR, hazard ratio; IV, intravenous; KCCQ, Kansas City Cardiomyopathy Questionnaire; LVEF,
left ventricular ejection fraction; NNT, number needed to treat; NT-proBNP, N-terminal prohormone of brain natriuretic peptide; NYHA, New
York Heart Association; OD, once daily; RRR, relative risk reduction; SOC, standard of care; T2D, Type 2 diabetes; UTI, urinary tract infection.
This document provides a summary of key efficacy outcomes and related subanalyses from the EMPEROR-Reduced trial
and is not intended to be a comprehensive reproduction. For full information, please refer to the original publications.
1. Packer M et al. N Engl J Med. 2020;383:1413; 2. Anker SD et al. Circulation 2021;143:337; 3. Packer M et al. Circulation
2021;143:326; 4. Butler J et al. Eur Heart J. 2021;42:1203.
SC-CRP-08448
June 2021