成人、青少年和儿童恶性疟原虫疟疾患者使用加纳吡酰胺加利美蒽林固体分散制剂治疗时加纳吡酰胺和利美蒽林的药代动力学:多国 2 期研究数据分析》。

IF 2.9 4区 医学
Ramachandra Sangana, Bernhards Ogutu, Adoke Yeka, Sylvia Kusemererwa, Halidou Tinto, Andre Offianan Toure, Afizi Kibuuka, Moussa Lingani, Carlos Lourenço, Ghyslain Mombo-Ngoma, Videlis Nduba, Tiacoh Landry N'Guessan, Guétawendé Job Wilfried Nassa, Mary Nyantaro, Lucas Otieno Tina, Anup Anvikar, Abhinav Sinha, Grace Kaguthi, Bakary Fofana, Martin Peter Grobusch, Myriam El Gaaloul, Anne Claire Marrast, Rashidkhan Pathan, Havana Chikoto, Katalin Csermak, Celine Risterucci, Guoqin Su, Cornelis Winnips, Jie Zhang, Julia Zack
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引用次数: 0

摘要

在2017年8月至2021年6月期间进行的一项多国、前瞻性、随机、主动对照II期研究中,新型抗疟药物甘那吡啶联合鲁班群固体分散制剂(LUM-SDF)在治疗成人、青少年和儿童的无并发症恶性疟原虫疟疾中疗效显著且耐受性良好(EudraCT 2020-003284-25,Clinicaltrials.gov NCT03167242)。本文报告了该研究的药代动力学数据。试验包括三个部分:在 A 部分中,成人/青少年患者接受六种甘那吡啶-LUM-SDF 治疗方案之一或蒿甲醚-本芴醇;在 B 部分中,成人/青少年患者接受三种剂量治疗方案之一或蒿甲醚-本芴醇;在 C 部分中,成人/青少年患者接受两种剂量治疗方案之一或蒿甲醚-本芴醇;在 D 部分中,成人/青少年患者接受两种剂量治疗方案之一或蒿甲醚-本芴醇;在 E 部分中,成人/青少年患者接受两种剂量治疗方案之一或蒿甲醚-本芴醇;在 F 部分中,成人/青少年患者接受两种剂量治疗方案之一或蒿甲醚-本芴醇;在B部分中,对A部分中确定的三种剂量方案和蒿甲醚-本芴醇在2至婴幼儿中的疗效进行了评估,在可能的情况下采用非室分析法报告AUClast、AUC0-t、Cmax和tmax。在 PK 试验阶段,合用甘纳普拉啶或卢曼蒽林时,甘纳普拉啶或卢曼蒽林的暴露量没有明显增加。在 A 部分和 B 部分中,甘那匹胺的暴露量随剂量的增加而增加,但鲁曼群胺的暴露量在数量上与剂量不成比例。与蒿甲醚-卢曼芬特林相比,甘那匹胺-LUM-SDF的卢曼芬特林暴露量更高,但也存在较大的变异性。不同年龄组和体重组的甘那吡啶和卢班亭暴露量(Cmax和AUC0-24 h)相当。在空腹条件下,采用400毫克加纳普拉啶加960毫克卢曼芬汀的剂量方案,每天一次,连续3天,可达到疗效所需的药物暴露量。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Pharmacokinetics of Ganaplacide and Lumefantrine in Adults, Adolescents, and Children with Plasmodium falciparum Malaria Treated with Ganaplacide Plus Lumefantrine Solid Dispersion Formulation: Analysis of Data from a Multinational Phase 2 Study.

The novel antimalarial ganaplacide combined with lumefantrine solid dispersion formulation (LUM-SDF) was effective and well tolerated in the treatment of uncomplicated falciparum malaria in adults, adolescents, and children in a multinational, prospective, randomized, active-controlled Phase II study conducted between August 2017 and June 2021 (EudraCT 2020-003284-25, Clinicaltrials.gov NCT03167242). Pharmacokinetic data from that study are reported here. The trial comprised three parts: a run-in part in 12 adult/adolescent patients treated with a single dose of ganaplacide 200 mg plus LUM-SDF 960 mg assessed potential pharmacokinetic (PK) interactions between ganaplacide and lumefantrine; in Part A, adult/adolescent patients received one of the six ganaplacide-LUM-SDF regimens or artemether-lumefantrine; and in Part B, three dose regimens identified in Part A, and artemether-lumefantrine, were assessed in children aged 2 to <12 years, with body weight ≥10 kg. A rich blood sampling schedule was used for all 12 patients in the PK run-in part and a subset of patients (N = 32) in Part A, with sparse sampling for remaining patients in Parts A (N = 275) and B (N = 159). Drug concentrations were determined by a validated protein precipitation and reverse phase liquid chromatography with tandem mass spectrometry detection method. Parameters including AUCinf, AUClast, AUC0-t, Cmax, and tmax were reported where possible, using non-compartmental analysis. In the PK run-in part, there was no notable increase in ganaplacide or lumefantrine exposure when co-administered. In Parts A and B, ganaplacide exposures increased with dose, but lumefantrine exposure was numerically under dose-proportional. Lumefantrine exposure was higher with ganaplacide-LUM-SDF than with artemether-lumefantrine, although high variability was observed. Ganaplacide and lumefantrine exposures (Cmax and AUC0-24 h) were comparable across age and body weight groups. Drug exposures needed for efficacy were achieved using the dose regimen 400 mg ganaplacide plus lumefantrine 960 mg once daily for 3 days under fasted conditions.

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来源期刊
Journal of Clinical Pharmacology
Journal of Clinical Pharmacology PHARMACOLOGY & PHARMACY-
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3.40%
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期刊介绍: The Journal of Clinical Pharmacology (JCP) is a Human Pharmacology journal designed to provide physicians, pharmacists, research scientists, regulatory scientists, drug developers and academic colleagues a forum to present research in all aspects of Clinical Pharmacology. This includes original research in pharmacokinetics, pharmacogenetics/pharmacogenomics, pharmacometrics, physiologic based pharmacokinetic modeling, drug interactions, therapeutic drug monitoring, regulatory sciences (including unique methods of data analysis), special population studies, drug development, pharmacovigilance, womens’ health, pediatric pharmacology, and pharmacodynamics. Additionally, JCP publishes review articles, commentaries and educational manuscripts. The Journal also serves as an instrument to disseminate Public Policy statements from the American College of Clinical Pharmacology.
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