Arzneimittelforschung 2008; 58(8): 376-384
DOI: 10.1055/s-0031-1296524
Anticoagulants · Antithrombotics · Antivaricosis Drugs · Blood Flow Stimulants
Editio Cantor Verlag Aulendorf (Germany)

Effects of D-003, a Mixture of Sugarcane Wax Acids, on Platelet Aggregation in Hypercholesterolemic Patients

A dose-titration, randomised, placebo-controlled trial
María De Lourdes Arruzazabala
1   National Center for Scientific Research, Havana City, Cuba
,
Vivian Molina
1   National Center for Scientific Research, Havana City, Cuba
,
Ernesto Lόpez
2   Medical Surgical Research Centre, Havana City, Cuba
,
Gladys Castaño
2   Medical Surgical Research Centre, Havana City, Cuba
,
Lilia Fernández
1   National Center for Scientific Research, Havana City, Cuba
,
Daisy Carbajal
1   National Center for Scientific Research, Havana City, Cuba
,
Rosa Mas
1   National Center for Scientific Research, Havana City, Cuba
,
José I. Ferrer
1   National Center for Scientific Research, Havana City, Cuba
,
Sarahi Mendoza
1   National Center for Scientific Research, Havana City, Cuba
,
Yoandri Ramírez
2   Medical Surgical Research Centre, Havana City, Cuba
› Author Affiliations
Further Information

Publication History

Publication Date:
15 December 2011 (online)

Abstract

Increased platelet aggregation contributes to vascular risk. D-003, a mixture of high molecular weight sugarcane wax acids, has shown antiplatelet effects in experimental models and healthy volunteers. This randomised, double-blinded, placebo-controlled study investigated the effects of titrated doses of D-003 (5-20 mg/d) on platelet aggregation in hypercholesterolemic patients. After a 4-week baseline phase, 56 patients were randomised to D-003 5 mg/d or placebo. The doses were doubled every 15 days if arachidonic acid (AA)-induced platelet aggregation was not inhibited at least by 15%.AA (0.75 and 1.5 mmol/L) and collagen (1 µg/mL)-induced platelet aggregation, laboratory and physical safety indicators were assessed at baseline and every 15 days thereafter, when adverse events (AE) were also reported. No significant change of platelet aggregation was found in the placebo group. After 15, 30 and 45 on therapy, D-003 reduced platelet aggregation induced with both AA 0.75 mmol/L (18.1%, 19.0% and 30.3%, respectively) and AA 1.5 mmol/L (17.0%, 16.3% and 22.5%, respectively), and also collagen-induced platelet aggregation (26.6%, 20.8% and 29.4%) (p < 0.01 at days 15 and 30 versus placebo, p < 0.0001 at study completion). The mean inhibition of platelet aggregation with D-003 at day 15, at which all patients had received the lowest dose, was over 15%. Nineteen out of 28 D-003 randomised patients (67.9%) required dose titration to achieve such goal. At trial completion, the mean estimated dose was 11.6 mg/d. D-003 lowered low-density lipoprotein (22.0%), total cholesterol (14.7%) and raised high-density lipoprotein-cholesterol (10.9%) (p < 0.0001 versus placebo). Six patients (2 placebo, 4 D-003) withdrew from the trial, none due to AE. D-003 did not modify the safety indicators with respect to placebo. Four patients (2 placebo, 2 D-003-treated) reported AE: pruritus and increased blood pressure (2 placebo) and rash and polyphagia (2 D-003). In conclusion, D-003 (5-20 mg/d) given as doses titrated every 15 days (5-20 mg/d) inhibited AA- and collagen-induced platelet aggregation in hypercholesterolemic patients and was well tolerated.

 
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