了解药物暴露和毛滴虫治愈率:坦桑尼亚和科特迪瓦阿苯达唑-伊维菌素联合用药的药物计量学方法。

IF 2.2 4区 医学 Q3 PHARMACOLOGY & PHARMACY Drugs in Research & Development Pub Date : 2024-06-01 Epub Date: 2024-07-22 DOI:10.1007/s40268-024-00476-4
Veshni Pillay-Fuentes Lorente, Jacinta N Nwogu-Attah, Britta Steffens, Dominic Bräm, Viviane Sprecher, Daniela Hofmann, Michael Buettcher, Goonaseelan Pillai, Samer Mouksassi, Jean Coulibaly, Marc Pfister, Jennifer Keiser
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引用次数: 0

摘要

背景和目的:由人类鞭虫毛滴虫引起的毛滴虫病是一个重大的公共卫生问题。阿苯达唑-伊维菌素联合用药是目前最有效的治疗方法。在坦桑尼亚和科特迪瓦进行的研究揭示了阿苯达唑-伊维菌素联合疗法在这两个国家的疗效差异。研究采用药物计量学方法评估联合用药情况,并研究人群对阿苯达唑两种主要代谢物药物动力学的影响。此外,还进行了一项探索性暴露-疗效分析,以研究暴露量与虫卵减少率之间的关系:药代动力学分析包括坦桑尼亚和科特迪瓦青少年(12-19 岁)的研究数据。参与者单次服用阿苯达唑 400 毫克,或与伊维菌素 200 微克/千克联合使用。研究人员进行了一项药效学分析,以探讨研究人群和合用伊维菌素对阿苯达唑代谢物表观清除率的潜在影响。使用 MonolixSuite 2023R1 进行了非线性混合效应建模。在探索-暴露反应分析中使用了通过模拟单个模型参数得出的药代动力学暴露量:结果:阿苯达唑亚砜的药代动力学曲线由两室模型和阿苯达唑砜的一室模型进行了最佳描述,阿苯达唑砜有一个转运室和线性消除室。虽然没有发现联合用药效应,但坦桑尼亚研究人群的阿苯达唑亚砜(阿苯达唑砜)表观清除率比科特迪瓦研究人群高 75%(46%)。暴露-疗效反应分析表明,峰值浓度和高于暴露阈值的时间与虫卵减少率有关:结论:研究人群而非联合用药的伊维菌素对阿苯达唑亚砜和阿苯达唑砜的表观清除率有影响。药物代谢酶的多态性以及宿主与寄生虫之间的相互作用可能是造成这一结果的原因。药物接触的差异并不能解释坦桑尼亚和科特迪瓦不同的药效反应。峰值浓度和超过阈值的时间是与虫卵减少率相关的暴露测量指标。有必要开展进一步研究,评估非洲各地区的遗传和抗药性模式。
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Understanding Drug Exposure and Trichuris trichiura Cure Rates: A Pharmacometric Approach for Albendazole-Ivermectin Co-medication in Tanzania and Côte d'Ivoire.

Background and objective: Trichuriasis caused by the human whipworm Trichuris trichiura poses a significant public health concern. Albendazole-ivermectin co-medication is currently the most effective treatment. Studies conducted in Tanzania and Côte d'Ivoire unveiled differences in efficacy for albendazole-ivermectin combination therapy in both countries. A pharmacometrics approach was used to assess co-medication and study population effects on the pharmacokinetics of the two main metabolites of albendazole. An exploratory exposure-efficacy analysis was also carried out to investigate relationships between exposure measures and the egg reduction rate.

Methods: Pharmacokinetic data from studies in Tanzania and Côte d'Ivoire in adolescents (aged 12-19 years) were included in the pharmacometric analysis. Participants received a single dose of either albendazole 400 mg alone or in combination with ivermectin 200 µg/kg. A pharmacometric analysis was performed to investigate the potential effects of the study population and co-administered ivermectin on the apparent clearance of the metabolites of albendazole. Non-linear mixed-effects modeling was conducted with MonolixSuite 2023R1. The pharmacokinetic exposure measures derived from simulations with individual model parameters were used in the exploratory-exposure response analysis.

Results: Pharmacokinetic profiles were best described by a two-compartment model for albendazole sulfoxide and a one-compartment model for albendazole sulfone, with a transit compartment and linear elimination. While no co-medication effect was found, apparent clearance of albendazole sulfoxide (albendazole sulfone) in the Tanzanian study population was 75% (46%) higher than that in the Côte d'Ivoire study population. Exposure-efficacy response analyses indicated that peak concentration and the time-above-exposure threshold were associated with the egg reduction rate.

Conclusions: Study population but not co-administered ivermectin showed an effect on apparent clearance of albendazole sulfoxide and albendazole sulfone. Polymorphisms in drug-metabolizing enzymes and host-parasite interaction may explain this result. Difference in drug exposure did not explain the disparate efficacy responses in Tanzania and Côte d'Ivoire. Peak concentration and time-above-threshold were exposure measures associated with the egg reduction rate. Further studies evaluating genetic and resistance patterns in various regions in Africa are warranted.

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来源期刊
Drugs in Research & Development
Drugs in Research & Development Pharmacology, Toxicology and Pharmaceutics-Pharmacology
CiteScore
5.10
自引率
0.00%
发文量
31
审稿时长
8 weeks
期刊介绍: Drugs in R&D is an international, peer reviewed, open access, online only journal, and provides timely information from all phases of drug research and development that will inform clinical practice. Healthcare decision makers are thus provided with knowledge about the developing place of a drug in therapy. The Journal includes: Clinical research on new and established drugs; Preclinical research of direct relevance to clinical drug development; Short communications and case study reports that meet the above criteria will also be considered; Reviews may also be considered.
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