Population pharmacokinetics of TLD-1, a novel liposomal doxorubicin, in a phase I trial.

IF 2.7 4区医学 Q3 ONCOLOGY Cancer Chemotherapy and Pharmacology Pub Date : 2024-09-01 Epub Date: 2024-06-15 DOI:10.1007/s00280-024-04679-z

Anna M Mc Laughlin, Dagmar Hess, Robin Michelet, Ilaria Colombo, Simon Haefliger, Sara Bastian, Manuela Rabaglio, Michael Schwitter, Stefanie Fischer, Katrin Eckhardt, Stefanie Hayoz, Christoph Kopp, Marian Klose, Cristiana Sessa, Anastasios Stathis, Stefan Halbherr, Wilhelm Huisinga, Markus Joerger, Charlotte Kloft

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Abstract

Study objectives: TLD-1 is a novel pegylated liposomal doxorubicin (PLD) formulation aiming to optimise the PLD efficacy-toxicity ratio. We aimed to characterise TLD-1's population pharmacokinetics using non-compartmental analysis and nonlinear mixed-effects modelling.

Methods: The PK of TLD-1 was analysed by performing a non-compartmental analysis of longitudinal doxorubicin plasma concentration measurements obtained from a clinical trial in 30 patients with advanced solid tumours across a 4.5-fold dose range. Furthermore, a joint parent-metabolite PK model of doxorubicin_entrapped, doxorubicin_free, and metabolite doxorubicinol was developed. Interindividual and interoccasion variability around the typical PK parameters and potential covariates to explain parts of this variability were explored.

Results: Medians $\pm$ standard deviations of dose-normalised doxorubicin_{entrapped+free} C_max and AUC_0-∞ were 0.342 $\pm$ 0.134 mg/L and 40.1 $\pm$ 18.9 mg·h/L, respectively. The median half-life (95 h) was 23.5 h longer than the half-life of currently marketed PLD. The novel joint parent-metabolite model comprised a one-compartment model with linear release (doxorubicin_entrapped), a two-compartment model with linear elimination (doxorubicin_free), and a one-compartment model with linear elimination for doxorubicinol. Body surface area on the volumes of distribution for free doxorubicin was the only significant covariate.

Conclusion: The population PK of TLD-1, including its release and main metabolite, were successfully characterised using non-compartmental and compartmental analyses. Based on its long half-life, TLD-1 presents a promising candidate for further clinical development. The PK characteristics form the basis to investigate TLD-1 exposure-response (i.e., clinical efficacy) and exposure-toxicity relationships in the future. Once such relationships have been established, the developed population PK model can be further used in model-informed precision dosing strategies.

Clinical trial registration: ClinicalTrials.gov-NCT03387917-January 2, 2018.

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新型多柔比星脂质体 TLD-1 在 I 期试验中的群体药代动力学。

研究目标TLD-1是一种新型聚乙二醇多柔比星脂质体（PLD）制剂，旨在优化PLD的效毒比。我们旨在利用非室分析和非线性混合效应模型来描述 TLD-1 的群体药代动力学特征：方法：通过对30名晚期实体瘤患者在4.5倍剂量范围内的临床试验中获得的纵向多柔比星血浆浓度测量值进行非室分析，分析了TLD-1的PK。此外，还建立了多柔比星、不含多柔比星和代谢物多柔比星醇的母体-代谢物联合 PK 模型。探讨了典型 PK 参数的个体间和事件间变异性，以及解释部分变异性的潜在协变量：结果：剂量归一化后的多柔比星Cmax和AUC0-∞的中位数±标准偏差分别为0.342±0.134 mg/L和40.1±18.9 mg-h/L。中位半衰期（95 小时）比目前市场上销售的 PLD 的半衰期长 23.5 小时。新型母体-代谢物联合模型包括线性释放的一室模型（多柔比星包裹）、线性消除的二室模型（不含多柔比星）以及多柔比星醇线性消除的一室模型。体表面积是影响游离多柔比星分布容积的唯一重要协变量：结论：使用非室分析和室分析成功地描述了TLD-1的群体PK，包括其释放和主要代谢物。TLD-1的半衰期较长，有望进一步用于临床开发。这些 PK 特性为今后研究 TLD-1 的暴露-反应（即临床疗效）和暴露-毒性关系奠定了基础。一旦建立了这种关系，所开发的群体 PK 模型就可以进一步用于以模型为依据的精准给药策略：临床试验注册：ClinicalTrials.gov-NCT03387917-2018年1月2日。

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来源期刊

Cancer Chemotherapy and Pharmacology 医学-药学

CiteScore

6.10

自引率

3.30%

发文量

116

审稿时长

2.5 months

期刊介绍： Addressing a wide range of pharmacologic and oncologic concerns on both experimental and clinical levels, Cancer Chemotherapy and Pharmacology is an eminent journal in the field. The primary focus in this rapid publication medium is on new anticancer agents, their experimental screening, preclinical toxicology and pharmacology, single and combined drug administration modalities, and clinical phase I, II and III trials. It is essential reading for pharmacologists and oncologists giving results recorded in the following areas: clinical toxicology, pharmacokinetics, pharmacodynamics, drug interactions, and indications for chemotherapy in cancer treatment strategy.