在癌症患者中的研究性 Aurora A 激酶抑制剂alisertib 的全球人群药代动力学：在亚洲降低剂量的原理。

Global population pharmacokinetics of the investigational Aurora A kinase inhibitor alisertib in cancer patients: rationale for lower dosage in Asia.

机构信息

Millennium Pharmaceuticals, Inc., a wholly owned subsidiary of Takeda Pharmaceutical Company Limited, Cambridge, MA, USA.

Projections Research Inc., Phoenixville, PA, USA.

出版信息

Br J Clin Pharmacol. 2018 Jan;84(1):35-51. doi: 10.1111/bcp.13430. Epub 2017 Nov 24.

AIMS

This population pharmacokinetic analysis was conducted to describe quantitatively the regional differences and sources of interpatient variability on the apparent oral clearance of alisertib.

METHODS

A population pharmacokinetic analysis was performed on data from 671 cancer patients in Western countries and in Japan/East Asia to whom alisertib 5-150 mg once or twice daily (b.i.d.) was administered in multiple dosing schedules. The final model was used to simulate alisertib pharmacokinetics in patients in the West and East Asian regions in the single-agent schedule of 7 days of dosing in a 21-day cycle. Exposure-safety relationships for mechanism-related antiproliferative toxicities (neutropenia, mucositis and diarrhoea) were estimated by logistic regression.

RESULTS

Alisertib pharmacokinetics were described by a two-compartment model with four-transit compartment absorption and linear elimination. The final model included a covariate effect of region on relative bioavailability, with patients in the East Asian region estimated to have a 52% higher bioavailability compared with Western patients. Population simulated exposure at 30 mg b.i.d. in patients in Asia was similar to that at 50 mg b.i.d. in Western patients [geometric mean (coefficient of variation) steady state area under the concentration-time curve over the dosing interval (AUC ): 21.4 μM.h (52.3%) and 24.1 μM.h (53.6%), respectively]. Exposure-AE relationships could be described for neutropenia, stomatitis and diarrhoea, supporting the lower dosage of alisertib in Asia for global clinical development.

CONCLUSIONS

Model-based simulations support the achievement of similar alisertib exposures in patients in Asia who are administered a 40% lower dose compared with the Western population, thereby providing a quantitative clinical pharmacology bridging and regional dosing rationale for global drug development.

目的

本群体药代动力学分析旨在定量描述阿利斯替尼口服清除率的个体间差异和区域性差异的来源。

方法

对来自西方国家和日本/东亚的 671 例癌症患者的数据进行群体药代动力学分析，这些患者接受了多种剂量方案的阿利斯替尼 5-150mg 每日一次或两次（bid）给药。最终模型用于模拟在单药方案中，7 天给药，21 天为一个周期时，在西方国家和东亚地区患者中的阿利斯替尼药代动力学。通过逻辑回归估计与机制相关的抗增殖毒性（中性粒细胞减少症、黏膜炎和腹泻）的暴露-安全性关系。

结果

阿利斯替尼药代动力学采用两室模型加四个转运室吸收和线性消除描述。最终模型包括一个区域性对相对生物利用度的协变量效应，东亚地区的患者估计比西方患者的生物利用度高 52%。在亚洲患者中，以 30mg bid 给药时，群体模拟的暴露量与西方患者以 50mg bid 给药时相似[稳态时浓度-时间曲线下面积（AUC）的几何平均值（变异系数）：21.4μM.h（52.3%）和 24.1μM.h（53.6%）]。可以描述暴露-不良反应（AE）关系，包括中性粒细胞减少症、口腔炎和腹泻，支持在亚洲地区使用较低剂量的阿利斯替尼进行全球临床开发。