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Novel milk-based oral formulations: proof of concept.

机译:基于牛奶的新型口服制剂:概念验证。

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The aim of this study is to develop milk-based formulations for ionized and unionized lipophilic drugs. Solubility studies of the following non-steroidal anti-inflammatory drugs (NSAIDs): mefenamic acid, tolfenamic acid, ketoprofen, meloxicam, tenoxicam and nimesulide in phosphate- and glycine-NaOH buffers at nominal pH 8-12, were performed. The solubilities of cyclosporine and danazol in water-ethanol solutions were studied. NSAIDs-, cyclosporine-, danazol-, aspirin-milk oral liquid formulations were prepared by adding the appropriate volume of (i) NSAIDs-alkaline buffer solutions, (ii) water-ethanol solutions of cyclosporine and danazol and (iii) aspirin aqueous solution to 150-200ml of milk. All the non-steroidal anti-inflammatory drugs exhibited increased solubility in the alkaline buffers. The actual pH values (range 6.7-7.7) of the final NSAIDs-milk formulations were very close to milk pH. The higher ethanol content in ethanol-water mixtures increased the solubility of danazol and cyclosporine. A 15mg meloxicam-, a 100mg cyclosporine- and a 500mg aspirin-milk formulation was administered orally to healthy volunteers. All these formulations showed a satisfactory in vivo performance. The strong buffering capacity of milk that was observed and the high solubility of unionized drugs in ethanol allow the preparation of drug-milk formulations with enhanced pharmacokinetic properties.
机译:这项研究的目的是开发用于离子化和非离子化亲脂性药物的基于牛奶的配方。在标称pH 8-12的磷酸盐和甘氨酸-NaOH缓冲液中,对以下非甾体抗炎药(NSAID)进行了溶解度研究:甲芬那酸,甲苯磺那酸,酮洛芬,美洛昔康,替诺昔康和尼美舒利。研究了环孢霉素和达那唑在水-乙醇溶液中的溶解度。通过添加适量的(i)NSAIDs-碱性缓冲溶液,(ii)环孢素和达那唑的水-乙醇溶液以及(iii)阿司匹林水溶液来制备NSAIDs-,环孢素-,达那唑-阿司匹林奶口服液制剂到150-200ml牛奶。所有非甾体抗炎药在碱性缓冲液中均显示出增加的溶解度。最终NSAIDs-牛奶配方的实际pH值(范围6.7-7.7)非常接近牛奶pH。乙醇-水混合物中较高的乙醇含量增加了达那唑和环孢霉素的溶解度。将15毫克美洛昔康,100毫克环孢素和500毫克阿司匹林奶口服给健康志愿者。所有这些制剂显示令人满意的体内性能。观察到的强大的牛奶缓冲能力和联合药物在乙醇中的高溶解度使得制备具有增强的药代动力学特性的药物-牛奶配方成为可能。

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