Coronary Artery Disease Clinical Trial
Official title:
A Randomized Comparison of a Sirolimus-eluting Stent With Biodegradable Polymer Versus an Everolimus-eluting Stent With a Durable Polymer for Percutaneous Coronary Revascularization
Coronary artery stents have improved the safety and efficacy of percutaneous coronary
intervention for coronary artery disease. Drug-eluting stents have been shown to decrease
neointimal hyperplasia and to reduce the rate of restenosis and target-lesion
revascularization as compared to bare-metal stents. Drug-eluting stents consist of a metallic
platform and a therapeutic substance that is usually released from a polymer matrix. A
previous study utilizing a bioresorbable polymer has demonstrated a favorable safety and
efficacy profile in a large-scale clinical trial as compared to a first-generation
druf-eluting stent (LEADERS trial).
The objective of the study is to compare the safety and efficacy of a sirolimus-eluting stent
with a biodegradable polymer with an everolimus-eluting stent with a durable polymer in a
prospective multicenter randomized controlled non-inferiority trial in patients undergoing
percutaneous coronary intervention in routine clinical practice.
Background
Coronary artery stents have improved the safety and efficacy of percutaneous coronary
interventions compared with balloon angioplasty alone (New Engl J Med 1994; 331:489-495).
Notwithstanding, restenosis is still encountered in 20 to 30% of lesions after implantation
of bare metal stents (JAMA 2000; 284:1828-36) and may require repeat revascularization
procedures with a negative impact on quality of life and health care expenditures.
Drug-eluting stents with local, controlled release of therapeutic agents have addressed this
problem successfully (Circulation 2003; 107:3003-7). Current drug-eluting stents consist of a
metallic stent platform and a therapeutic agent, which is either directly immobilized on the
stent surface or released from a polymer matrix. Polymers currently utilized for drug-eluting
stents are either biodegradable or non-biodegradable. While biodegradable polymers are
released together with the drug and dissolve after a certain period of time,
non-biodegradable polymers reside permanently on the stent surface.
First-generation drug-eluting stents utilized sirolimus and paclitaxel for prevention of
restenosis. Both drugs are highly lipophilic and show rapid and strong uptake in arterial
wall tissue. In addition, Sirolimus (Circulation 2001; 104:852-5) and paclitaxel (Circulation
1997; 96:636-45) have been shown to reduce smooth muscle cell proliferation and neointimal
hyperplasia, the principal cause of restenosis after coronary stenting in experimental
models. A polymer-encapsulated stent releasing Sirolimus has been compared with the
respective bare metal stent in several randomized clinical trials, demonstrating a consistent
reduction in angiographic and clinical restenosis (N Engl J Med 2002; 346:1773-80).
Similarly, a polymer-based, paclitaxel-eluting stent consistently reduced restenosis and the
need for repeated revascularization procedures compared with the respective bare metal stent
(N Engl J Med 2004; 350:221-31). A meta-analysis of drug-eluting stent trials confirmed the
reduction in restenosis and repeat revascularization procedures for polymer-based,
drug-eluting stents (Lancet 2004; 364:583-91). Moreover, the rates of death and myocardial
infarction were comparable to those with bare metal stents, attesting to the safety of these
devices, which have been approved by the US Food and Drug Administration.
Newer generation drug-eluting stents with durable polymer coating utilize Limus analogues
such as everolimus, zotarolimus or novolimus. Everolimus-eluting stents have been compared to
first-generation drug-eluting stents in several randomized clinical trials. A pooled analysis
of the four largest randomized trials to date comparing everolimus-eluting stents with
paclitaxel-eluting stents demonstrated a lower rate of MACE (4.4% versus 7.6%), myocardial
infarction (2.1% vs. 4.0%, p<0.001), ischemic TLR (2.3% vs. 4.7%, p<0.001), and definite
stent thrombosis (0.4% vs. 1.2%, p<0.001) in favor of EES, whereas there was no difference
with regard to overall and cardiac mortality (Stone GW. The XIENCE V - PROMUS
Everolimus-Eluting Stent: New Insights from the SPIRIT/COMPARE Meta-analysis and other
randomized trials. Presentation at Transcatheter Cardiovascular Therapeutics, September 22nd
2010). At the same time several trials comparing everolimus-eluting stents with
sirolimus-eluting stents reported favorable performance of everolimus-eluting stents. In a
randomized trial enrolling 2'774 patients everolimus-eluting stents were non-inferior
compared with sirolimus-eluting stents at nine months with regard to MACE (4.9% vs. 5.2%, HR
0.94, 0.67-1.31) and TLR (1.4% vs. 1.7%, HR 0.87, 0.48-1.58) (N Engl J Med
2010;362(28):1663-74). Likewise, event rates at two years were similar for everolimus-eluting
stents and sirolimus-eluting stents (3.7% versus 4.3%, p=0.85) in a randomized controlled
trial comparing EES, SES, and BMS in large vessels (stent diameter >3.0 mm), whereas TVR was
lower with both EES (3.7%) and SES (4.3%) as compared with bare-metal stents (10.3%, P=0.005
vs SES, P=0.002 vs EES) (N Engl J Med 2010;363(24):2310-9). A propensity-score matched
comparison of EES and SES reported lower event rates of myocardial infarction (3.3% versus
5.0%, HR 0.62, 95% CI 0.42-0.92, P=0.017) in part due to a lower risk of stent thrombosis
(definite or probable 2.5% versus 4.0%, HR 0.64, 95% CI 0.41-0.98, P=0.041), as well as a
lower rate of target vessel revascularization (7.0% versus 9.6%, HR 0.75, 95% CI 0.57-0.99,
P=0.039) for EES at three years while mortality was similar (Windecker S. Long-term
comparison of Everolimus-eluting and Sirolimus-eluting Stents for coronary revascularization
1 (LESSON1) study. Presentation at the European Society of Cardiology meeting, Stockholm,
Sweden, 31st August 2010. 2010).
A previous study utilizing a bioresorbable polymer has demonstrated a favorable safety and
efficacy profile in a large-scale clinical trial as compared to a first-generation
drug-eluting stent. Among 1,707 patients randomized to either a biolimus-eluting stent with a
bioresorbable polymer or a sirolimus-eluting stent with a durable polymer no significant
differences with regard to the primary endpoint of cardiac death, myocardial infarction or
target-vessel revascularization were observed (9.2% versus 10.5%, HR 0.88, 95% CI 0.64-1.19;:
p=0.39)(Lancet 2008;372:1163-73.)
Objective
The objective of the study is to compare the safety and efficacy of a sirolimus-eluting stent
with a biodegradable polymer with an everolimus-eluting stent with a durable polymer in a
prospective multicenter randomized controlled non-inferiority trial in patients undergoing
percutaneous coronary intervention in routine clinical practice.
Methods
Design: Prospective, multi-center, randomized, non-inferiority trial. Patients will be
randomized in a single-blind fashion (1:1 randomization) to either the Orsiro® Stent system
(Sirolimus-eluting stent with a biodegradable polymer) with the Xience PRIME® stent system
(Everolimus-eluting stent with a durable polymer).
Primary endpoint: Target lesion failure (TLF), defined as the composite of cardiac death,
target vessel myocardial infarction (MI), and clinically driven target-lesion
revascularization (TLR).
Inclusion Criteria: "Real world, all comer" patients with symptomatic coronary artery disease
including patients with chronic stable angina, silent ischemia, and acute coronary syndromes
including NSTE-ACS and STE-ACS, and presence of one or more coronary artery stenoses >50% in
a native coronary artery or a saphenous bypass graft which can be treated with a stent
ranging in diameter from 2.25 to 4.0 mm and can be covered with one or multiple stents.
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