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Heartbeat – ESC 2004
ESC 2004
ESC 2004: Learning as a journey
Valentin Fuster MDDirector, Cardiovascular InstituteMount Sinai Medical CenterNew York, NY
Christopher Cannon MDStaff cardiologistBrigham and Women’s HospitalBoston, MA
James Ferguson MDAssociate Director, CardiologySt Luke's Episcopal Hospital and Texas Heart InstituteHouston, TX
Michael Weber MDProfessor of MedicineSUNY Downstate College of MedicineBrooklyn, NY
Heartbeat – ESC 2004
ESC 2004
PROVE-IT TIMI-22Pravastatin or atorvastatin evaluation
and infection therapy
A to ZAggrastat to Zocor
RIO-EUROPE
Rimonabant in Obesity - Europe
Topics
Heartbeat – ESC 2004
ESC 2004
Pravastatin or Atorvastatin Evaluation and Infection
Therapy
PROVE-IT TIMI-22
Heartbeat – ESC 2004
ESC 2004
PROVE-IT: Background
• Previous studies have shown that patients with high titers of Chlamydia pneumoniae at greater risk of MI
• PROVE-IT TIMI-22 and ACES presented at ESC 2004
Heartbeat – ESC 2004
ESC 2004
PROVE-IT: Design
Long-term study of antibiotic therapy against Chlamydia pneumoniae on the occurrence of cardiovascular events in patients with coronary heart disease
• 4162 patients with ACS (<10 days)
• Pravastatin (40 mg daily) vs atorvastatin (80 mg daily)
• Patients were randomized a second time to receive treatment with either gatifloxacin 400 mg/day for a full course of 10 days per month followed by 20 days without treatment or placebo
• Repeated each month for two years
Heartbeat – ESC 2004
ESC 2004
PROVE IT-TIMI 22: CVD events by treatment group
Cannon C. ESC Congress 2004; August 28-September 1, 2004; Munich, Germany
End point
Gatifloxacin Placebo Hazard risk reduction (95% CI)
P
CV events (%)
23.7 25.1 5 (16, -8) 0.41
Primary endpoint a composite of all-cause mortality, MI, unstable angina requiring hospitalization, revascularization, and stroke
Heartbeat – ESC 2004
ESC 2004
PROVE-IT: Great hope
“I think it’s a solid ‘no’ that this doesn’t work.”
Cannon
Heartbeat – ESC 2004
ESC 2004
PROVE-IT: No benefit
“We’ve been at this antibiotic question a couple of times.”
• Can these results be extended to patients who have less atherosclerotic burden?
•For patients with established coronary disease, three “resounding studies” suggest no benefit
Ferguson
Heartbeat – ESC 2004
ESC 2004
ACES: Design
Study compared treatment with azithromycin 600 mg once a week for a year with placebo in 4012 patients with established coronary disease
• Patients were then followed for four years for the occurrence of primary end point events, any one of CHD death, nonfatal MI, coronary revascularization, or hospitalization for unstable angina
RESULTS
• Primary end point was almost identical between the groups: 22.4% with placebo and 22.3% with azithromycin)
Heartbeat – ESC 2004
ESC 2004
Antibiotics in CHD
“We’ve come to learn that things like hs-CRP can be produced by non-infectious causes.”
• Inflammatory markers do not necessarily reflect an infectious etiology
• Still possible that C pneumoniae and other organisms having an earlier etiologic role
Weber
Heartbeat – ESC 2004
ESC 2004
PROVE-IT: 30 days
Difficult to translate into a primary prevention trial
• Two other leading infectious organisms are viruses
• Antiviral therapies still limited
Cannon
Heartbeat – ESC 2004
ESC 2004
PROVE-IT: Final thoughts
“From the standpoint of using it in people with established coronary disease, I think we have the answer.”
- Ferguson
“It may be that we’ve identified that the process was over at the stage when patients were 60 years old with established disease and the infectious activity had been decades before.”
- Cannon
Heartbeat – ESC 2004
ESC 2004
Aggrastat to Zocor
A to Z
Heartbeat – ESC 2004
ESC 2004
PROVE-IT: Design
Intensive and moderate lipid lowering with statin therapy after acute coronary syndrome (ACS) (N Engl J Med 2004; 350: published March 8th)
• 4162 patients with ACS (<10 days)
• Pravastatin (40 mg daily) vs atorvastatin (80 mg daily)
• Primary end point: a composite of all-cause mortality, MI, unstable angina requiring hospitalization, revascularization, and stroke
• Two-year follow-up
Heartbeat – ESC 2004
ESC 2004
End point Pravastatin 40 mg (n=1973)
Atorvastatin 80 mg (n=2003)
P
Primary composite end point
26.3 22.4 0.005
PROVE-IT: Results
N Engl J Med 2004; 350
16% reduction in risk favoring atorvastatin
Heartbeat – ESC 2004
ESC 2004
PROVE-IT: 30 days
Curves begin to diverge at 30 days
•Curves similar in terms of the overall time course
•Greater reductions in LDL and CRP levels with atorvastatin 80 mg
Heartbeat – ESC 2004
ESC 2004
PROVE-IT: Understanding CRP
Evolving understanding of lipid-lowering treatment
•LDL cholesterol as a major target to prevent major cardiovascular events and death
• Increasing focus on reducing CRP as a component of intensive statin therapy
Cannon
Heartbeat – ESC 2004
ESC 2004
A to Z: Design
Z phase of the A to Z trial evaluating aggressive versus conservative statin therapy in 4497 ACS patients
TREATMENT
Early intensive treatment: Simvastatin 40 mg for one month followed by simvastatin 80 mg for the remainder of the trial
Conservative treatment: Placebo for four months followed by simvastatin 20 mg for the remainder of the trial
Primary end point a composite of all-cause mortality, MI, unstable angina requiring hospitalization, revascularization, and stroke
Heartbeat – ESC 2004
ESC 2004
A to Z: Changes in LDL cholesterol
Group Baseline LDL cholesterol (mg/dL)
4 months (mg/dL)
24 months (mg/dL)
Placebo/simvastatin 20 mg
111 124 81
Simvastatin 40 mg/simvastatin 80 mg
112 62 66
De Lemos J et al. JAMA 2004
Heartbeat – ESC 2004
ESC 2004
A to Z: Primary composite end point
De Lemos J et al. JAMA 2004
End point Placebo/simvastatin 20 mg (%)
Simvastatin 40 mg/simvastatin 80 mg (%)
P
Primary composite end point of cardiovascular death, MI, readmission for ACS, or stroke
16.7 14.4 0.14
Heartbeat – ESC 2004
ESC 2004
A to Z: Results
“Now come the surprises.”
• Why do the curves not separate early, when one group was treated with placebo and the other simvastatin 40 mg?
• Curves begin to separate between months 4 and 24 – What is going on here?
Heartbeat – ESC 2004
ESC 2004
A to Z: What’s going on here?
Easier to deal with what happens later in the study
• Not enough difference in LDL levels to reflect significant differences between the two treatment strategies at 24 months
• Effects of different statins beyond lipid lowering
Weber
Heartbeat – ESC 2004
ESC 2004
A to Z: What’s going on here?
“I have no problem with A to Z overall, but that first four months is troubling.”
• Is there something unique about atorvastatin that could explain the discrepancy between PROVE-IT and A to Z?
Weber
Heartbeat – ESC 2004
ESC 2004
A to Z: Different patients
“Is it the drug? Is it the population? Or is it the study design?”
DIFFERENCES
• Patients in PROVE-IT recruited within 10 days, with many ‘out’ from acute episode versus those in A to Z who were in the midst of ACS
• A to Z underpowered
Ferguson
Heartbeat – ESC 2004
ESC 2004
A to Z: No support for early use
A to Z does not support early administration of statins in ACS patients
“I’m a little bit mystified as to how some people have taken this as an endorsement of early administration of statins. It doesn’t support it. PROVE-IT TIMI-22 does, but A to Z goes in exactly the opposite direction.”
Ferguson
Heartbeat – ESC 2004
ESC 2004
A to Z: Two hypotheses
WHY THE DISCREPANCY WITH PROVE-IT?
• Final between-group reduction in CRP was 16.7%, whereas as in PROVE-IT, the difference between treated groups was 38%
• Different patient population
• Different dose
Fuster
Heartbeat – ESC 2004
ESC 2004
PROVE-IT: Role of CRP
CRP does provide a hint as to why no benefit observed at four months
• But, CRP issue clouded as A to Z patients stabilized with aggressive medical therapy, possibly resulting in more patients entering the trial with an ongoing thrombotic process
• PROVE-IT patients more stable
Cannon
Heartbeat – ESC 2004
ESC 2004
A to Z: Safety profile
Side effect Placebo/simvastatin 20 mg (%)
Simvastatin 40 mgsimvastatin 80 mg (%)
Discontinued study for AST or ALT >3X upper limit of normal
0.4 0.9
Discontinued study drug for muscle-related adverse event
1.5 1.8
Myopathy (creatine kinase >3X upper limit of normal)
0.04 0.4 (n=9;all on simvastatin 80 mg)
Rhabdomyolysis (CK>10 000 units/L)
-- 3 of 9 myopathy cases
De Lemos J et al. JAMA 2004
Heartbeat – ESC 2004
ESC 2004
A to Z: Safety profile
“It is a useful reminder to all of us that we do have to keep safety on the radar screen. We can’t put this in the drinking water.”
• Careful in using simvastatin 80 mg, whereas 40 mg dose looks fine
- Cannon
Heartbeat – ESC 2004
ESC 2004
A to Z: Case study
In a patient with unstable angina, are you concerned about lipid levels during the acute phase?
Are you using a statin during the acute phase?
If yes, what statin will you use, and what dose?
Fuster
Heartbeat – ESC 2004
ESC 2004
A to Z: Three questions
I care about the lipid levels, but I’m not going to treat elevated lipid levels in the acute phase
• Data still soft on benefit during the acute phase of treatment
• Once stable, I would start with high-dose atorvastatin
Ferguson
Heartbeat – ESC 2004
ESC 2004
A to Z: Three questions
“We’ve learned that there doesn’t seem to be any benefit from super-early treatment of high lipid levels.”
•Once stable, then start statin therapy
•Based on evidence, I would start with high-dose atorvastatin
Weber
Heartbeat – ESC 2004
ESC 2004
A to Z: Three questions
Start statin, on admission, across the board
• In ACS patients, start statin therapy aggressively and early
• Aim to lower LDL levels to 60 or 70 mg/dL as shown in PROVE-IT
• Atorvastatin 80 mg, but more cautious with simvastatin 80 mg
Cannon
Heartbeat – ESC 2004
ESC 2004
A to Z: Switching statins
In a patient with unstable angina who is currently taking simvastatin 40 mg, would you switch to atorvastatin?
Fuster
Heartbeat – ESC 2004
ESC 2004
A to Z: Switching statins
“On the one hand you say this guy’s already been on simvastatin and its let him down.”
•Not good enough for this patient
•Absolute event rate in A to Z still quite low
Weber
Heartbeat – ESC 2004
ESC 2004
A to Z: Switching statins
I would not reflexively switch from product X to product Y
• Depends on the LDL number and if patient is at goal
Ferguson
Heartbeat – ESC 2004
ESC 2004
Rimonabant in Obesity – Europe
RIO-Europe
Heartbeat – ESC 2004
ESC 2004
RIO-Europe: Rational
• Obesity a world wide epidemic
• The so-called “pleasure center” may generate appetite and tobacco addiction
• A new drug, rimonabant, blocks the CB1 receptor
• The question is, can taking this drug decrease appetite and help stop smoking at the same time?
Heartbeat – ESC 2004
ESC 2004
RIO-Europe: Design and Results
• 1500 overweight patients
• Randomized to rimonabant 20 mg, rimonabant 5 mg, or placebo
• One year follow-up
• Patients in the 20 mg dose lost 6.6 kg, those on the 5 mg dose lost 3.4 kg, and those on placebo lost 1.8 kg
• In patients on the 20 mg dose: HDL increased by 27%, triglycerides decreased by 10%, and proportion of patients with metabolic syndrome decreased by 50%
Heartbeat – ESC 2004
ESC 2004
RIO-Europe: Results
“It seems to me that we are dealing with something quite striking.”
Fuster
Heartbeat – ESC 2004
ESC 2004
RIO-Europe
“I am excited about this, I think that this is absolutely fascinating…[but] you gotta worry a little bit about a drug that’s a pleasure-center blocker.”
• Significant clinical applications
• No quick fix, no magic pill
Ferguson
Heartbeat – ESC 2004
ESC 2004
RIO-Europe
• HDL and triglycerides linked to insulin sensitivity
• In early phase of weight loss: a sharp improvement in insulin sensitivity
• HDL: One of the most difficult things to manipulate – anything that can increase HDL is exciting
“I am a bit concerned . . . What happens when you stop this drug?”
- Weber
Heartbeat – ESC 2004
ESC 2004
RIO-Europe
• Smoking cessation aid is desperately needed
• Reduction in CRP also promising
“It’s a fascinating, multifactorial agent.”
- Cannon
Heartbeat – ESC 2004
ESC 2004
RIO-Europe
• Mood changes mild and transient
• So far, 3000 people in different trials
• Trials include:
RIO-Europe, RIO Lipids, RIO North America, RIO-Diabetes, STRATUS-US (tobacco cessation)
Fuster
Heartbeat – ESC 2004
ESC 2004
Final thoughts
PROVE-IT: Antibiotic study “negative” but extremely definitive - We can go to the bank with that information
A to Z: “A bit troubling” – is there really a difference between the statins?
RIO-EUROPE: Rimonabant “very promising”
Weber
Heartbeat – ESC 2004
ESC 2004
Final thoughts
PROVE-IT: Antibiotics didn’t work - we need to focus on real things like diet, exercise, weight reduction, controlling lipids, antiplatelet therapy, and ACE inhibitors
A to Z: Early effects may be linked to anti-inflammatory effects of statins
RIO-EUROPE: going beyond LDL to control all other CV risk factors is the wave of the future
Cannon
Heartbeat – ESC 2004
ESC 2004
Final thoughts
“Each one of these trials is a doorway.”
• The antibiotic trial basically closed the door
• A to Z trial opened a door and showed us a lot more doors
• Rimonabant a whole new doorway
Ferguson
Heartbeat – ESC 2004
ESC 2004
Final thoughts
“I’m most excited about A to Z . . . I’m most excited when I’m wrong. The situation is a little more complicated than we thought.”
Ferguson