Lilly Research Laboratories, Eli Lilly and Company, Lilly Corporate Center, Indianapolis, Indiana 46285, USA.
Clin Ther. 2010 Feb;32(2):365-79. doi: 10.1016/j.clinthera.2010.02.015.
Prasugrel is an oral antiplatelet agent approved for the reduction of atherothrombotic cardiovascular events in patients presenting with acute coronary syndrome and undergoing percutaneous coronary intervention. Although the approved loading dose is 60 mg, earlier studies of prasugrel suggested that active-metabolite exposure and pharmacodynamic response may be higher in Asian subjects than in white subjects.
This study compared the pharmacodynamic response to a single 30-mg dose of prasugrel in healthy Chinese and white subjects and the response to a single 30-mg dose of prasugrel and a single 300-mg dose of clopidogrel in healthy Chinese subjects. The pharmacokinetics and tolerability of both drugs were also assessed.
This was an open-label, single-dose study conducted in Singapore. Chinese subjects were randomly allocated to receive prasugrel 30 mg or clopidogrel 300 mg; after a 14-day washout period, they received the alternative drug. White subjects received only prasugrel 30 mg. Blood samples for pharmaco-dynamic assessments were collected before dosing and at 0.5, 1, 2, 4, and 24 hours after dosing. Three methods were used to measure inhibition of platelet aggregation (IPA)-traditional light transmission aggregometry (LTA), the Verify Now P2Y12 (VN-P2Y12) assay, and a vasodilator-stimulated phosphoprotein (VASP) phosphorylation flow cytometry assay-and their results were compared. Blood samples for pharmacokinetic assessments were collected at 0.25, 0.5, 1, 1.5, 2, 4, 8, 12, and 24 hours after dosing. Concentrations of the active metabolite of prasugrel were measured using a validated LC-MS/MS method.
The study enrolled 18 Chinese subjects and 14 white subjects. Chinese subjects had a mean (SD) age of 31 (10) years and a mean body weight of 65.2 (8.9) kg; 83% were male. The corresponding values for white subjects were 30 (10) years, 77.2 (12.4) kg, and 86%. Thirty of the 32 enrolled subjects completed the study. Two Chinese men were withdrawn from the study, one due to a low platelet-rich plasma count after receipt of prasugrel 30 mg and the other due to mild, intermittent rectal bleeding after bowel movements that began approximately 2 days after receipt of clopidogrel 300 mg. The mean IPA with prasugrel was significantly higher in Chinese than in white subjects at 0.5, 1, and 2 hours after dosing (P < 0.05), but not at 4 or 24 hours. In Chinese subjects, mean maximal IPA (87%) occurred 1 hour after prasugrel dosing; in white subjects, mean maximal IPA (78%) occurred 2 hours after prasugrel dosing. In Chinese subjects, the mean IPA was significantly higher at all time points after administration of prasugrel 30 mg than after administration of clopidogrel 300 mg (P <0.001). After administration of Clopidogrel 300 mg in Chinese subjects, mean maximal IPA (58%) occurred at 4 hours. The VN-P2Y12 and VASP phosphorylation assays yielded results comparable to those obtained by LTA. Mean exposure to prasugrel's active metabolite was higher in Chinese than in white subjects (geometric least squares mean ratio for AUC(0-t) = 1.47 (90% CI, 1.24-1.73). Both drugs were well tolerated.
In this study, platelet inhibition was significantly higher in Chinese than in white subjects up to 2 hours after a single 30-mg dose of prasugrel. Platelet inhibition was significantly higher in Chinese subjects at all time points after a 30-mg dose of prasugrel than after a 300-mg dose of clopidogrel. Both treatments were generally well tolerated.
普拉格雷是一种口服抗血小板药物,适用于急性冠脉综合征并接受经皮冠状动脉介入治疗的患者,以减少动脉粥样硬化血栓心血管事件。尽管批准的负荷剂量为 60mg,但普拉格雷的早期研究表明,与白人受试者相比,亚洲受试者的活性代谢物暴露和药效反应可能更高。
本研究比较了健康的中国和白人受试者单次服用 30mg 普拉格雷的药效反应,以及健康的中国受试者单次服用 30mg 普拉格雷和单次服用 300mg 氯吡格雷的药效反应。还评估了这两种药物的药代动力学和耐受性。
这是一项在新加坡进行的开放标签、单次剂量研究。中国受试者随机分配接受普拉格雷 30mg 或氯吡格雷 300mg;在 14 天洗脱期后,他们接受了另一种药物。白人受试者仅接受普拉格雷 30mg。在给药前和给药后 0.5、1、2、4 和 24 小时采集血样进行药效学评估。使用三种方法测量血小板聚集抑制(IPA)-传统光传输聚集测定法(LTA)、VerifyNow P2Y12(VN-P2Y12)测定法和血管扩张刺激磷酸蛋白(VASP)磷酸化流式细胞术测定法-并比较其结果。在给药后 0.25、0.5、1、1.5、2、4、8、12 和 24 小时采集血样进行药代动力学评估。使用经过验证的 LC-MS/MS 方法测量普拉格雷活性代谢物的浓度。
该研究纳入了 18 名中国受试者和 14 名白人受试者。中国受试者的平均(SD)年龄为 31(10)岁,平均体重为 65.2(8.9)kg;83%为男性。白人受试者的相应值为 30(10)岁、77.2(12.4)kg 和 86%。32 名入组受试者中,有 30 名完成了研究。两名中国男性因接受普拉格雷 30mg 后血小板富血浆计数低和接受氯吡格雷 300mg 后约 2 天开始出现间歇性轻微直肠出血而退出研究。给药后 0.5、1 和 2 小时,中国受试者的 IPA 平均值明显高于白人受试者(P <0.05),但在 4 小时和 24 小时时则不然。在中国受试者中,最大 IPA(87%)平均在普拉格雷给药后 1 小时出现;在白人受试者中,最大 IPA(78%)平均在普拉格雷给药后 2 小时出现。在中国受试者中,与服用氯吡格雷 300mg 相比,服用普拉格雷 30mg 后所有时间点的 IPA 平均值均明显更高(P <0.001)。在中国受试者中,服用氯吡格雷 300mg 后,最大 IPA(58%)平均在 4 小时出现。VN-P2Y12 和 VASP 磷酸化测定法的结果与 LTA 测定法的结果相当。中国受试者中普拉格雷活性代谢物的暴露量明显高于白人受试者(AUC(0-t)的几何最小平方均值比为 1.47(90%CI,1.24-1.73)。两种药物均具有良好的耐受性。
在这项研究中,与白人受试者相比,中国受试者在单次服用 30mg 普拉格雷后 2 小时内的血小板抑制作用明显更高。与服用氯吡格雷 300mg 相比,中国受试者在服用 30mg 普拉格雷后的所有时间点的血小板抑制作用均明显更高。两种治疗方法通常都具有良好的耐受性。
