Myocardial Infarction Clinical Trial
Official title:
Comparison of the Efficacy of Everolimus-Eluting Versus Zotarolimus-Eluting Stent for Coronary Lesions in Acute Myocardial Infarction
Most of the previous data regarding the efficacy of the everolimus-eluting stent (EES) was derived from studies comparing EES with bare metal stent (BMS) or EES with paclitaxel-eluting (PES). Although sirolimus-eluting stents (SES) have been shown to be the most efficacious drug regarding inhibition of neointima and late loss, there have been no previous head to head comparisons between EES and zotarolimus-eluting stent (ZES). Both everolimus and sirolimus are macrocyclic lactones that target the mTOR (mammalian target of rapamycin) to reduce vascular smooth muscle proliferation after vessel injury and therefore in principle may show similar results after stenting in humans. Data pooled from the EES arm that received follow up angiography in the SPIRIT III trial and the SES arm in the SIRIUS trial show similar rates of binary restenosis and late loss. However, the stent and polymer platform is not the same between the EES and ZES and it is reported that the EES system has the thinnest stent + polymer thickness (88.6um) of all of the previously KFDA-approved drug-eluting stent (DES). In addition, there are no data available on the efficacy of the EES and ZES in "real world" lesions other than the selected lesions studied in the previous trials, such as acute myocardial infarction.
Previous randomized trials have shown the efficacy of a slow-release polymeric
sirolimus-eluting stent (CYPHER, Cordis, Warren, NJ, USA), paclitaxel-eluting stent (TAXUS,
Boston Scientific, Natick, MA, USA), and zotarolimus-eluting stent (Endeavor, Medtronic,
Minneapolis, MN, USA) over bare metal stents in reducing neointimal hyperplasia, late
luminal loss, and angiographic restenosis leading to decreased target lesion
revascularization. The everolimus-eluting stent (XIENCE V, Abott Vascular, Santa Clara, CA,
USA, PROMUS, Boston Scientific, Natick, MA, USA) is a newly developed drug eluting stent
using the MULTILINK VISION® stent platform combined with the drug everolimus contained in a
polymer coating.
In the first-in-man SPIRIT First clinical trial, XIENCE V showed a significant benefit over
the bare metal VISION stent. Compared with late loss of 0.85 ± 0.36mm in the VISION arm,
XIENCE V reduced late loss by 88% (0.10 ± 0.23mm). Also the clinical safety of XIENCE V was
confirmed with a 6-month MACE rate of 7.7%. In the SPIRIT II clinical trial, which compared
the efficacy and safety of the XIENCE V stent versus the TAXUS PECSS stent, the primary
endpoint was met showing a non-inferiority of the XIENCE V compared with the TAXUS regarding
in-stent late loss at 180 days. Actually, XIENCE V was superior to TAXUS and reduced
in-stent late loss by 72% from a mean of 0.36 mm to 0.11 mm. In addition, analysis of other
key clinical endpoints showed a lower rate of ischemia driven MACE (2.7% vs. 6.5% for XIENCE
V vs. TAXUS) and protocol-defined stent thrombosis (0.5% vs. 1.3% for XIENCE V vs. TAXUS).
The lower rate of ischemia driven MACE at 180 days was sustained through 1 year and there
were no new instances of late stent thrombosis in either group up to 1 year.
The SPIRIT III RCT was a prospective, 2:1 randomized, active-controlled, single blinded,
parallel, multi-center clinical evaluation of the XIENCE V Everolimus Eluting Coronary Stent
System (XIENCE V EECSS) compared to TAXUS Paclitaxel Eluting Coronary Stent System (TAXUS
PECSS) in the treatment of up to two de novo lesions. This pivotal clinical trial was
designed to demonstrate the non-inferiority of the XIENCE V EECSS to the TAXUS PECSS.
Patients were randomized 2:1 to XIENCE V or TAXUS and the primary endpoint was in-segment
late loss at 240 days. The results showed a mean in-segment late loss of 0.14mm for XIENCE V
and 0.28 mm for TAXUS (p<0.001 for non-inferiority, p=0.0037 for superiority). The secondary
endpoint, which was ischemia-driven target vessel failure (TVF), was 7.6% for XIENCE V and
9.7% for TAXUS, confirming the non-inferiority of XIENCE V. Furthermore, the rate of
definite and probable stent thrombosis was 1.1% and 0.6% for XIENCE V and TAXUS,
respectively.
With a recent approval of new DES, zotarolimus-eluting stent (Endeavor, Medtronic,
Minneapolis, MN), other comparison studies have been conducted to compare Endeavor
zotarolimus-eluting stent with the sirolimus-eluting stent and paclitaxel-eluting stent.
zotarolimus and sirolimus share some common structural and biological properties. In vitro
data suggest that sirolimus and tetrazole containing rapamycin analogs have similar
inhibitory effects in a mixed lymphocyte reaction assay. The ENDEAVOR clinical trials are
currently in progress to evaluate a phosphoryl choline (PC)-coated zotarolimus-eluting
stent(ZES) for the prevention of restenosis. The Endeavor zotarolimus-eluting stent utilizes
a cobalt alloy balloon-expandable stent (Driver; Medtronic) with a geometry similar to the
stainless steel stent used in this preliminary study (S7; Medtronic). The Endeavor ZES also
employees a PC strut surface coating as the drug delivery reservoir with a dose of 10 g/mm
of ABT-578. The Endeavor (ZES), however, differs from the stent used in this experimental
study by the addition of a drug-free PC topcoat to serve as a diffusion barrier to retard
drug release from the polymer reservoir. Angiographic analysis at 4 months in the
100-patient focal de novo lesion ENDEAVOR I feasibility study demonstrated a mean in-stent
percent diameter stenosis of approximately 14% and a late lumen loss of 0.3 mm with a low
frequency of target lesion revascularization (1%). The clinical outcomes from the ENDEAVOR
II (1,500 patients randomized to ABT-578 or bare metal stent) and the ENDEAVOR III (436
patients randomized 3:1 to ABT-578 or Cypher) trials as well as other ongoing studies showed
efficacy of the PC-coated ABT-578-eluting stent. In ENDEAVOR III study, the Endeavor stent
had larger late loss and higher binary restenosis in both the analysis segment and stented
segment.
Most of the previous data regarding the efficacy of the EES was derived from studies
comparing EES with BMS or EES with PES. Although sirolimus eluting stents (SES) have been
shown to be the most efficacious drug eluting stent regarding inhibition of neointima and
late loss, there have been no previous head to head comparisons between EES and ZES. Both
everolimus and sirolimus are macrocyclic lactones that target the mTOR (mammalian target of
rapamycin) to reduce vascular smooth muscle proliferation after vessel injury and therefore
in principle may show similar results after stenting in humans. Data pooled from the EES arm
that received follow up angiography in the SPIRIT III trial and the SES arm in the SIRIUS
trial show similar rates of binary restenosis and late loss. However, the stent and polymer
platform is not the same between the EES and ZES and it is reported that the EES system has
the thinnest stent + polymer thickness (88.6um) of all of the previously KFDA-approved DES.
In addition, there are no data available on the efficacy of the EES and ZES in "real world"
lesions other than the selected lesions studied in the previous trials, such as acute
myocardial infarction.
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Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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