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基于血小板聚集试验,采用群体药效学建模与模拟预测S-吲哚布芬和R-吲哚布芬对人体的抗血小板作用。

Prediction of the human antiplatelet effect of S- and R-indobufen using population pharmacodynamic modeling and simulation based on platelet aggregation test.

作者信息

Noh Yook-Hwan, Han Sungpil, Choe Sangmin, Jung Jin-Ah, Jung Jin-Ah, Hwang Ae-Kyung, Lim Hyeong-Seok

机构信息

Department of Clinical Pharmacology and Therapeutics, University of Ulsan College of Medicine, Asan Medical Center, Seoul 05505, Korea.

Pharmacokinetic and Pharmacogenetic Laboratory, Clinical Research Center, Asan Medical Center, Seoul 05505, Republic of Korea.

出版信息

Transl Clin Pharmacol. 2018 Dec;26(4):160-165. doi: 10.12793/tcp.2018.26.4.160. Epub 2018 Dec 19.

Abstract

Indobufen (Ibustrin®), a reversible inhibitor of platelet aggregation, exists in two enantiomeric forms in 1:1 ratio. Here, we characterized the anti-platelet effect of S- and R-indobufen using response surface modeling using NONMEM® and predicted the therapeutic doses exerting the maximal efficacy of each enantioselective S- and R-indobufen formulation. S- and R-indobufen were added individually or together to 24 plasma samples from drug-naïve healthy subjects, generating 892 samples containing randomly selected concentrations of the drugs of 0-128 mg/L. Collagen-induced platelet aggregation in platelet-rich plasma was determined using a Chrono-log Lumi-Aggregometer. Inhibitory sigmoid I model adequately described the anti-platelet effect. The S-form was more potent, whereas the R-form showed less inter-individual variation. No significant interaction was observed between the two enantiomers. The anti-platelet effect of multiple treatments with 200 mg indobufen twice daily doses was predicted in the simulation study, and the effect of S- or R-indobufen alone at various doses was predicted to define optimal dosing regimen for each enantiomer. Simulation study predicted that 200 mg twice daily administration of S-indobufen alone will produce more treatment effect than S-and R-mixture formulation. S-indobufen produced treatment effect at lower concentration than R-indobufen. However, inter-individual variation of the pharmacodynamic response was smaller in R-indobufen. The present study suggests the optimal doses of R-and S-enantioselective indobufen formulations in terms of treatment efficacy for patients with thromboembolic problems. The proposed methodology in this study can be applied to the develop novel enantio-selective drugs more efficiently.

摘要

吲哚布芬(易抗凝®)是一种血小板聚集的可逆抑制剂,以1:1的比例存在于两种对映体形式中。在此,我们使用NONMEM®通过响应面建模来表征S-和R-吲哚布芬的抗血小板作用,并预测了发挥每种对映选择性S-和R-吲哚布芬制剂最大疗效的治疗剂量。将S-和R-吲哚布芬单独或一起添加到24份来自未用过药的健康受试者的血浆样本中,生成892份含有随机选择的0 - 128 mg/L药物浓度的样本。使用Chrono-log Lumi-Aggregometer测定富含血小板血浆中胶原诱导的血小板聚集。抑制性S形I模型充分描述了抗血小板作用。S型更有效,而R型个体间差异较小。两种对映体之间未观察到显著相互作用。在模拟研究中预测了每日两次200 mg吲哚布芬多次治疗的抗血小板作用,并预测了不同剂量的S-或R-吲哚布芬单独使用的作用,以确定每种对映体的最佳给药方案。模拟研究预测,单独每日两次给予200 mg S-吲哚布芬将比S-和R-混合制剂产生更大的治疗效果。S-吲哚布芬在比R-吲哚布芬更低的浓度下产生治疗效果。然而,R-吲哚布芬药效学反应的个体间差异较小。本研究提出了针对血栓栓塞问题患者的R-和S-对映选择性吲哚布芬制剂在治疗效果方面的最佳剂量。本研究中提出的方法可更有效地应用于开发新型对映选择性药物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bd52/6989252/b6a2cadd615f/tcp-26-160-g001.jpg

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