Newer Diabetes Drugs: Results From The EMPA-REG and LEADER Trials - - PowerPoint PPT Presentation
Cardiovascular Outcomes With Newer Diabetes Drugs: Results From The EMPA-REG and LEADER Trials Rajiv Roy, MD Endocrinology Sharp Rees-Stealy Medical Group Background Between 1990 and 2010: Incidence of acute MI dropped by approximately
Rajiv Roy, MD Endocrinology Sharp Rees-Stealy Medical Group
Between 1990 and 2010:
In the diabetic population:
Despite improvements in care, diabetics still have a 1.5X higher incidence
Demonstrated that LIRAGLUTIDE (LIRA) in addition to standard of care reduced risk of combined endpoint of CV death, non fatal MI and non fatal stroke vs placebo in adults with type 2 DM and high CV risk More recently, LIRA has received a new indication to reduce the risk of major cardiovascular events, MI, stroke and CV death in adults with type 2 DM and established CV disease
coronary revascularization, and hospitalization for unstable angina or HF
Cardiovascular outcomes: PRIMARY: HR 0.87 (95% CI 0.78 TO 0.97); P = 0.01 FOR SUPERIORITY (608 vs 694 pts) DEATH FROM CV CAUSES: HR 0.78 (95% CI, 0.66-0.93); P = 0.007 (219 vs 278 pts)
NO STATISTICALLY SIGNIFICANT DIFFERENCE IN NONFATAL MI OR NONFATAL STROKE
DEATH FROM ANY CAUSE: HR 0.85; P = 0.02 (381 vs 447 pts) HOSPITALIZATION FOR CHF: HR: 0.87; P = 0.14 (NOT STATISTICALLY SIGNIFICANT) (218 vs 248 pts)
Marso SP et al. NEJM 2016;375:1834-1844
SUSTAIN-6 TRIAL RESULTS
Holman RR et. Al, NEJM 2017;377:1228-1239
EXSCEL TRIAL RESULTS
Demonstrated that EMPAGLIFLOZIN (EMPA), in addition to standard of care, reduced 3 point MACE of cardiovascular death, non fatal MI and non fatal stroke versus placebo in a high risk population of type 2 diabetic adults with established CV disease Risk of CV death was significantly reduced versus placebo
14% reduction in 3 point composite endpoint (MACE): HR 0.86; p=0.04 superiority 38% reduction in cardiovascular death: HR 0.62; p < 0.001 32% reduction in all cause mortality: HR 0.68; p < 0.001 35% reduction in CHF hospitalization: HR 0.65; p = 0.002 Zinman B et al, NEJM 2015; 373:2117-2128
Composite endpoint (3 point MACE) occurred in 10.5% EMPA patients vs 12.1% PBO 1.6% absolute risk reduction, 14% relative risk reduction
CV Death occurred in 3.7% of EMPA group vs 5.9% PBO group EMPA treated patients had a 2.2 % absolute risk reduction, 38% relative risk reduction versus placebo (p < 0.001) Non fatal MI and non fatal stroke: No significant difference between EMPA and PBO groups. Difference in CV death drove 3 point MACE
Zinman B et al, NEJM 2015; 373:2117-2128
Death from any cause occurred in 5.7% in EMPA group vs 8.3% in PBO group ACM: 2.6% absolute risk reduction and 32% relative risk reduction in EMPA treated patients versus placebo (p<0.001)
Heart failure hospitalization occurred in 2.7% EMPA patients vs 4.1% PBO Absolute risk reduction in EMPA group: 1.4%; Relative risk reduction 35% (p=0.002)
R), there was a statistically significant reduction in 3 point MACE but no statistically significant reduction in all cause mortality or CV death (26.9 vs 31.5 participants per 1000 pt years; HR 0.86)
treated patients vs PBO (6.3 vs 3.4 participants per 1000 patient yrs; HR 1.97). Not seen in previous canagliflozin trials. Mechanism unknown
patients were on CANA (53%) or DAPA(42%) or EMPA(5%) showed a 39% reduction in CHF admission, 51% reduction in death, and 46% reduction in composite of heart failure or death. Only 13% had CVD at baseline.
CANVAS AND CANVAS-R RESULTS Neal B et. Al, NEJM 2017;377:644-657
CANVAS AND CANVAS-R RESULTS
Neal B et. Al, NEJM 2017;377:644-657
Neal B et. Al, NEJM 2017;377:644-657
CANVAS AND CANVAS-R RESULTS
Neal B et. Al, NEJM 2017;377:644-657
CANVAS AND CANVAS-R RESULTS
Neal B et. Al, NEJM 2017;377:644-657
CANVAS AND CANVAS-R RESULTS