Neubauer Horst, Krüger Jan Christopher, Lask Sebastian, Endres Heinz G, Pepinghege Fenena, Engelhardt Andreas, Bulut Daniel, Mügge Andreas
Cardiovascular Center, St. Josef Hospital, Ruhr University Bochum, Gudrunstrasse 56, 44791, Bochum, Germany.
Clin Res Cardiol. 2009 Sep;98(9):533-40. doi: 10.1007/s00392-009-0033-1. Epub 2009 Jun 6.
Clopidogrel hydrogensulfate is a thienopyridine acting as an important antiplatelet agent alone or in combination with acetyl salicylic acid to prevent cardiovascular complications. A different clopidogrel salt, clopidogrel besylate, was approved in Germany as a "new drug" in May 2008. Only one study with 46 healthy men compared the plasma concentrations of both clopidogrel formulas. In our crossover study we measured the antiplatelet effect of clopidogrel hydrogensulfate (CHS, clopidogrel bisulfate) and clopidogrel besylate (CB) using two techniques, whole blood impedance aggregometry and flow cytometry in healthy subjects.
Twenty-one healthy volunteers (14 male, 7 female, mean age 36.3 years) were treated either with CHS or CB (300 mg loading, followed by 75 mg/day) and after a wash-out period of at least 21 days, the participants were switched to the other clopidogrel salt in a crossover design. Blood samples were drawn before and 2, 4 and 48 h after the initial dose was taken. Flow cytometry measurements of CD62P (P-selectin) expression were done at baseline and 48 h thereafter with three different ADP concentrations (5, 15, 50 micromol/L ADP). Whole blood impedance aggregometry testing (Chrono-log Model 590) was performed at baseline and after 2, 4 and 48 h with two ADP concentrations (5 and 20 micromol/L ADP).
Using flow cytometry, the mean inhibitory effect of clopidogrel on the CD62P expression was similar and no significant differences were noted in subjects treated with either of the clopidogrel formulas for hydrogensulfate or besylate salt (5 micromol/L ADP: 8.12 +/- 5.53 CHS vs. 6.48 +/- 5.01 CB; 15 micromol/L ADP: 9.33 +/- 6.44 CHS vs. 8.99 +/- 8.27 CB; 50 micromol/L ADP: 11.17 +/- 6.81 CHS vs. 9.52 +/- 6.17 CB). It is important to note that clopidogrel CB shows similar and conspicuously high interindividual variability as was reported earlier on CHS. We observed both possibilities, subjects responding less to the hydrogensulfate salt, but better to the besylate salt, and vice versa. Using aggregometry, both salt formulas achieved similar inhibitory effects regarding initial platelet function (2 h/5 micromol/L ADP: CHS 4.5 +/- 3.66 Omega; CB 3.89 +/- 3.81 Omega and 4 h/5 micromol/L ADP: CHS 5.78 +/- 3.51 Omega; CB 4.89 +/- 4.03 Omega) as well as during the maintenance phase (48 h/5 micromol/L ADP: CHS 2.86 +/- 2.92 Omega; CB 3.43 +/- 3.06 Omega). Once again the aggregometry results for CB showed a similarly high interindividual variability as also holds true for CHS. Some subjects had a better antiplatelet effect with clopidogrel besylate and vice versa with clopidogrel hydrogensulfate.
The crossover study using whole blood aggregometry and flow cytometry shows no overall significant difference in the antiplatelet effect of clopidogrel hydrogensulfate as compared to clopidogrel besylate. However, it is important to note that besides high interindividual there is also high intraindividual variability between the two different clopidogrel formulas. We observed both: subjects responding less to besylate salt, but better to hydrogensulfate salt, and vice versa.
硫酸氢氯吡格雷是一种噻吩并吡啶类药物,单独使用或与乙酰水杨酸联合使用时,是一种重要的抗血小板药物,可预防心血管并发症。另一种氯吡格雷盐,即氯吡格雷苯磺酸盐,于2008年5月在德国作为“新药”获批。仅有一项针对46名健康男性的研究比较了两种氯吡格雷制剂的血浆浓度。在我们的交叉研究中,我们使用全血阻抗聚集测定法和流式细胞术这两种技术,在健康受试者中测量了硫酸氢氯吡格雷(CHS,氯吡格雷硫酸氢盐)和氯吡格雷苯磺酸盐(CB)的抗血小板作用。
21名健康志愿者(14名男性,7名女性,平均年龄36.3岁)接受CHS或CB治疗(300mg负荷剂量,随后75mg/天),在至少21天的洗脱期后,参与者按照交叉设计换用另一种氯吡格雷盐。在服用初始剂量前以及服用后2、4和48小时采集血样。在基线以及之后48小时,使用三种不同的ADP浓度(5、15、50μmol/L ADP)进行CD62P(P-选择素)表达的流式细胞术测量。使用两种ADP浓度(5和20μmol/L ADP),在基线以及2、4和48小时后进行全血阻抗聚集测定(Chrono-log Model 590)。
使用流式细胞术,氯吡格雷对CD62P表达的平均抑制作用相似,在用硫酸氢盐或苯磺酸盐形式的氯吡格雷治疗的受试者中未观察到显著差异(5μmol/L ADP:CHS为8.12±5.53,CB为6.48±5.01;15μmol/L ADP:CHS为9.33±6.44,CB为8.99±8.
