Adverse Effect of Antithrombotic Drugs Clinical Trial
Official title:
Effects of Combinated Administration of Lysine Acetylsalicylate Versus Prasugrel and Aspirin on Platelet Aggregation in Healthy Volunteers
This is a phase I clinical trial in healthy volunteers comparing the effect of lysine acetylsalicylate or aspirin on platelet function.
1. SUMMARY 1.1. Type of trial Phase I clinical trial in healthy volunteers and marketed
drugs 1.2. Identification of the promoter (correspondence to) Dr. David Vivas Balcones
Cardiology Department Hospital Clínico San Carlos C/Prof Martín Lagos SN 28040 Madrid Phone:
+34 91 330 31 49 Fax: +34 913303142 Email: dvivas@secardiologia.es 1.3. Clinical trial title
Effect of combined administration of prasugrel and lysine acetylsalicylate intravenously
versus prasugrel and aspirin on platelet aggregation in healthy volunteers (ECCLIPSE trial).
1.4. Protocol code Nº EudraCT: 2012-001702-20 Code: 2012-ECCLIPSE-01 Version: V3 Date:
13/04/2012
1.5. Project principal investigator Dr. David Vivas Balcones Cardiology Department Hospital
Clínico San Carlos C/Prof Martín Lagos SN 28040 Madrid Phone: +34 91 330 31 49 Fax: +34
913303142 Email: dvivas@secardiologia.es 1.6. Centers Investigators
San Carlos University Hospital (Madrid). Within the following services and researchers are
involved:
Cardiology Department Hospital Clínico San Carlos C/Prof Martín Lagos SN 28040 Madrid
Teléfono: +34 91 330 31 49 Fax: +34 913303142 Project principal investigator and Promoter:
Dr. David Vivas Balcones Co-Investigators: Dr. Agustín Martín, Dr. Isidre Vilacosta, Dr.
Iván Núñez-Gil y Dr. Carlos Macaya
Platelet function laboratory Cardiology Department Hospital Clínico San Carlos C/Prof Martín
Lagos SN 28040 Madrid Phone: +34 913307260 Fax: +34 913303142 Co-Investigators: Dr. Antonio
Fernández-Ortiz, Esther Bernardo y María Aranzazu Ortega Pozzi
Clinical Trials Unit (CEIC) Biomedical Research Foundation Hospital Clínico San Carlos C/
Prof. Martín Lagos S/N 28040 Madrid Phone: + 34 913303793 Fax: +34 913303515
Co-Investigator: Dra. Saioa Alonso
Clinical Research Ethics Committee The Clinical Research Ethics Committee (CEIC) charged
with assessing the project will be the CEIC of the San Carlos University Hospital.
1.7. Responsible for Monitoring: MEDITRIALS 1.8. Experimental and control drug •
Experimental group: Loading dose (LD) of intravenous lysine acetylsalicylate 450 mg and
prasugrel 60 mg orally.
• Control group: Loading dose (LD) of aspirin 300 mg orally and prasugrel 60 mg orally.
Being a crossover study, subjects will receive both treatment arms in the two treatment
periods with a gap of 15 days (washout period) between the two administrations.
1.9. Study endpoints Primary endpoint To compare the inhibition of platelet aggregation
(IPA) at 30 minutes after administration of prasugrel loading dose in association with
intravenous lysine acetylsalicylate versus prasugrel plus aspirin.
Secundary endpoints To compare the inhibition of platelet aggregation (IPA) at 0 (baseline),
1, 4 and 24 hours after the administration of both treatment groups.
To compare the inhibition of platelet reactivity (IPR) throughout the time period in both
treatment groups.
To evaluate the safety of the treatment administered.
1.10. Study design The ECCLIPSE study is a phase I, randomized, single center, open,
two-period crossover trial in each of which subjects receive a single dose of certain drugs
in each treatment group.
1.11. Pathology study None. 1.12. Population and sample size The study population will be
healthy volunteers (total 30 subjects). This is a pharmacodynamic study, with subsequent
extrapolation of findings to patients with acute coronary syndrome 1.13. Duration of
treatment In each period of treatment, subjects will received a single dose of drugs
determined in each treatment arm and the analysis of the parameters under study will be
processed over the next 24 hours. After the two weeks washout period, subjects will receive
the other study drug regimen in a single dose and it will take place the analysis within 24
hours of the parameters studied.
1.14. Primary variable Inhibition of platelet aggregation measured by light transmission
aggregometry at 30 minutes.
;
Allocation: Randomized, Endpoint Classification: Pharmacodynamics Study, Intervention Model: Crossover Assignment, Masking: Open Label, Primary Purpose: Treatment