Incompatibility of antimalarial drugs: challenges in formulating combination products for malaria.

IF 6.5 2区 医学 Q1 PHARMACOLOGY & PHARMACY Drug Delivery Pub Date : 2024-12-01 Epub Date: 2024-01-05 DOI:10.1080/10717544.2023.2299594
Ellen K G Mhango, Benjamin R Sveinbjornsson, Bergthora S Snorradottir, Sveinbjorn Gizurarson
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Abstract

Lipophilic drugs require more advance formulation, especially if the intention is to make solutions or semisolid formulations. This also accounts for most antimalarial drugs. Although some of these antimalarial drugs are soluble in lipid vehicles, few of them, such as lumefantrine (LF), are also poorly soluble in oily vehicles. Trying to dissolve and formulate LF as a liquid formulation together with other antimalarial drugs is, therefore, a major task. When mixed in solution together with artemether (AR), precipitation occurs, sometimes with LF precipitating out on its own, and sometimes with AR precipitating out alongside LF. In this study, it was hypothesized that the use of fatty acids could lead to enhanced solubility in lipid formulation. Addition of the fatty acid solved the dissolution challenges, making LF soluble for over a year at room temperature (21-23 °C); but further research is needed to test the mechanism of action of the fatty acid. In addition, design of experiments (MODDE® 13) revealed that the amount of fatty acid in the formulation was the only significant factor for LF precipitation.

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抗疟药物的不兼容性:配制治疗疟疾的复方产品所面临的挑战。
亲脂性药物需要更先进的配制方法,特别是如果要配制溶液或半固体制剂。大多数抗疟疾药物也是如此。虽然其中一些抗疟疾药物可溶于脂质载体,但也有少数药物,如氟苯胍(LF),在油性载体中的溶解度也很低。因此,如何将 LF 与其他抗疟药一起溶解并配制成液体制剂是一项艰巨的任务。当 LF 与蒿甲醚(AR)混合在溶液中时,会发生沉淀,有时 LF 会单独沉淀,有时 AR 会与 LF 一起沉淀。在这项研究中,假设使用脂肪酸可以提高脂质配方的溶解度。添加脂肪酸解决了溶解难题,使 LF 在室温(21-23 °C)下可溶解一年以上;但仍需进一步研究,以测试脂肪酸的作用机制。此外,实验设计(MODDE® 13)显示,配方中脂肪酸的含量是影响 LF 沉淀的唯一重要因素。
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来源期刊
Drug Delivery
Drug Delivery 医学-药学
CiteScore
11.80
自引率
5.00%
发文量
250
审稿时长
3.3 months
期刊介绍: Drug Delivery is an open access journal serving the academic and industrial communities with peer reviewed coverage of basic research, development, and application principles of drug delivery and targeting at molecular, cellular, and higher levels. Topics covered include all delivery systems including oral, pulmonary, nasal, parenteral and transdermal, and modes of entry such as controlled release systems; microcapsules, liposomes, vesicles, and macromolecular conjugates; antibody targeting; protein/peptide delivery; DNA, oligonucleotide and siRNA delivery. Papers on drug dosage forms and their optimization will not be considered unless they directly relate to the original drug delivery issues. Published articles present original research and critical reviews.
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