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| Sponsor: | Translumina GmbH |
|---|---|
| Information provided by: | Translumina GmbH |
| ClinicalTrials.gov Identifier: | NCT00152308 |
Purpose
The purpose of the study is to evaluate the effectively of coating of coronary stents with two different doses of rapamycin for the prevention of coronary vessel re-blockage
| Condition | Intervention | Phase |
|---|---|---|
|
Coronary Disease |
Device: 2% rapamycin-eluting YUKONdes PEARL-stent Device: 1% rapamycin-eluting YUKONdes PEARL-stent Device: YUKONdes PEARL-stent coated with placebo (ethanol) |
Phase IV |
| Study Type: | Interventional |
| Study Design: | Treatment, Randomized, Double-Blind, Placebo Control, Parallel Assignment, Efficacy Study |
| Official Title: | A Prospective, Placebo-Controlled, Double-Blind, Randomized Study Evaluating the Efficacy of Non-Polymer-Based Coating With Two Different Rapamycin-Dosages for the Prevention of Restenosis After Percutaneous Coronary Interventions |
| Estimated Enrollment: | 333 |
| Study Start Date: | December 2004 |
| Estimated Study Completion Date: | February 2007 |
In-stent restenosis remains the major problem limiting the efficacy of coronary stenting. Either sirolimus or paclitaxel drug-eluting stents have been demonstrated to decrease neointima proliferation resulting in a remarkable reduction of restenosis rate. However, despite the outstanding results achieved with this novel approach to restenosis, some caveats still remain. Although sirolimus markedly decreased the restenosis rate among diabetic patients in SIRIUS trial, the benefit of treatment was modest in those diabetics treated with insulin as well as with lesions longer than 15 mm located in vessels smaller than 2.5 mm. Additionally, in a recent study it was reported that the restenosis rate in high-risk lesions such as coronary bifurcations still remains a problem Data from patient populations other than those enrolled in randomized trials suggest even more caution in the evaluation of the impact of DES on restenosis in the “real world”, where the operator must deal with in-stent restenosis, bifurcation lesions, chronic total occlusions, small vessels, and long lesions. The identification of some of the traditional risk factors for restenosis as important predictors for in-DES restenosis could be explained as an insufficient inhibition of tissue reaction and neointimal growth by the antiproliferative action of the specific drug or dose used. This leads to the inference that an individualized approach should be adopted by tailoring the choice and the dosing of eluting drug(s) according to the specific lesion or patient characteristics. On the other hand, although drug-eluting stents are currently considered as the most effective way to reduce in-stent restenosis, their widespread use is hampered by the high costs. Therefore, it is important to develop new methods and techniques that would result in a more effective prevention of in-stent restenosis while being available for a larger number of patients. These considerations as well as the proven efficacy of rapamycin in lowering the rate of coronary restenosis, support the rationality of the concept of on-site coating of stents in the catheterization laboratory with individualized doses of rapamycin after the clinical and the angiographic profiles of the patient scheduled to coronary stenting have been determined
Eligibility| Ages Eligible for Study: | 18 Years to 85 Years |
| Genders Eligible for Study: | Both |
| Accepts Healthy Volunteers: | No |
Inclusion Criteria:
Age 18-85 years; Symptoms (stable or unstable angina) or signs of myocardial ischemia; Single de novo diagnosed lesion in a native coronary artery (50-99% DS); Lesion length 8 – 25 mm; Vessel diameter 2.25-3.75 mm; Written informed consent
Exclusion Criteria:
Left main target lesion unprotected by a graft; Ostial and bifurcation target lesion; Severely calcified lesions; Thrombus in target lesion; Tortuosity or angulation of target vessel or lesion; Treatment of nontarget lesions in the same or a different coronary vessel during the index procedure; Contraindications to the study medications; Acute myocardial infarction (< 48 h); Left ventricular ejection fraction < 25%; Participation in another trial; Pregnancy or lack of protection against pregnancy during the study Coexisting conditions limiting the life expectancy to less 24 months or that could affect the compliance of patients with protocol; Serum creatinin >2.0mg/dL; Hemorrhagic diathesis; Leukocyte count <3500/ml^3 Platelet count <100.000/ml^3
Contacts and Locations| Contact: Gisela Schoemig | +49 89 2102 8920 | Gisela.Schoemig@translumina.de |
| Austria | |
| Allgemeines Krankenhaus Wien | Recruiting |
| Vienna, Austria, 1090 | |
| Contact: Dietmar Glogar, MD helmut-dietmar.glogar@univie.ac.at | |
| Principal Investigator: Dietmar Glogar, MD | |
| Wilhelminenspital der Stadt Wien | Recruiting |
| Vienna, Austria, 1160 | |
| Contact: Kurt Huber, MD +43 1 49150 0 kurt.huber@meduniwien.ac.at | |
| Principal Investigator: Kurt Huber, MD | |
| St. Johanns Spital | Recruiting |
| Salzburg, Austria, 5020 | |
| Contact: Mathias Heigert, MD M.heigert@salk.at | |
| Principal Investigator: Mathias Heigert, MD | |
| Donauspital der Stadt Wien | Recruiting |
| Vienna, Austria, 1020 | |
| Contact: Georg Norman, MD +43 1 28802 | |
| Principal Investigator: Georg Norman, MD | |
| Germany | |
| Deutsches Herzzentrum Muenchen | Recruiting |
| Munich, Germany, 80636 | |
| Contact: Adnan Kastrati, MD +49 89 1218 4577 kastrati@dhm.mhn.de | |
| Principal Investigator: Adnan Kastrati, MD | |
| First Medizinische Klinik rechts der Isar | Recruiting |
| Munich, Germany, 81675 | |
| Contact: Josef , Dirschinger +49 89 4140 2947 dirschinger@med1.med.tu-muenchen.de | |
| Principal Investigator: Josef Dirschinger, MD | |
| Kardiologische Praxis und Praxisklinik | Recruiting |
| Munich, Germany, 81379 | |
| Contact: Sigmund Silber, MD +49 89 742 15130 sigmund@silber.com | |
| Principal Investigator: Sigmund Silber, MD | |
| Israel | |
| Hadassah University Hospital | Recruiting |
| Jerusalem, Israel, 91120 | |
| Contact: Chaim Lotan, MD Lotan@hadassah.org.il | |
| Principal Investigator: Chaim Lotan, MD | |
| Assaf Harofeh Medical Center | Recruiting |
| Zrifin, Israel, 70300 | |
| Contact: Ricardo Krakover, MD +972 08 9779738 | |
| Principal Investigator: Ricardo Krakover, MD | |
| Sourasky Medical Center | Recruiting |
| Tel Aviv, Israel, 64239 | |
| Contact: Hylton Miller, MD himiller@tasmc.health.gov.il | |
| Principal Investigator: Hylton Miller, MD | |
| Study Chair: | Albert Schomig, MD | Deutsches Herzzentrum Muenchen |
| Principal Investigator: | Adnan Kastrati, MD | Deutsches Herzzentrum Muenchen |
| Study Director: | Kurt Huber, MD | Wilhelminenspital der Stadt Wien |
More Information
| Study ID Numbers: | GE IDE No. S01903 |
| Study First Received: | September 8, 2005 |
| Last Updated: | September 8, 2005 |
| ClinicalTrials.gov Identifier: | NCT00152308 History of Changes |
| Health Authority: | Germany: Federal Institute for Drugs and Medical Devices |
|
Arterial Occlusive Diseases Sirolimus Anti-Infective Agents Heart Diseases Immunologic Factors Antineoplastic Agents Myocardial Ischemia Physiological Effects of Drugs Vascular Diseases Arteriosclerosis |
Antibiotics, Antineoplastic Immunosuppressive Agents Pharmacologic Actions Coronary Disease Anti-Bacterial Agents Antifungal Agents Therapeutic Uses Cardiovascular Diseases Coronary Artery Disease |
