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半氟化烷烃气溶胶作为赋形剂适合吸入性药物传递-初步研究。

Aerosolized semifluorinated alkanes as excipients are suitable for inhalative drug delivery--a pilot study.

机构信息

Department of Anaesthesiology and Intensive Care Medicine, University Medical Center Mannheim, Germany.

出版信息

Int J Pharm. 2012 Jan 17;422(1-2):194-201. doi: 10.1016/j.ijpharm.2011.10.051. Epub 2011 Nov 7.

Abstract

Semifluorinated alkanes (SFAs) have been described as potential excipients for pulmonary drug delivery, but proof of their efficacy is still lacking. We tested whether SFA formulations with the test drug ibuprofen can be nebulised and evaluated their pharmacokinetics. Physico-chemical properties of five different ibuprofen formulations were evaluated: an aqueous solution (H2O), two different SFAs (perfluorohexyloctane (F6H8), perfluorobutylpentane (F4H5)) with and without ethanol (SFA/EtOH). Nebulisation was performed with a jet catheter system. Inhalative characteristics were evaluated by laser diffraction. A confirmative animal study with an inhalative single-dose (6 mg/kg) of ibuprofen with each formulation was performed in anaesthetised healthy rabbits. Plasma samples at defined time points and lung tissue harvested after the 6-h study period were analyzed by HPLC-MS/MS. Pharmacokinetics were calculated using a non-compartment model. All formulations were nebulisable. No differences in aerodynamic diameters (MMAD) were detected between SFA and SFA/EtOH. The ibuprofen plasma concentration-time curve (AUC) was highest with F4H5/EtOH. In contrast, F6H8/EtOH had the highest deposition of ibuprofen into lung tissue but the lowest AUC. All tested SFA and SFA/EtOH formulations are suitable for inhalation. F4H5/EtOH formulations might be used for rapid systemic availability of drugs. F6H8/EtOH showed intrapulmonary deposition of the test drug.

摘要

半氟化烷烃 (SFAs) 已被描述为潜在的肺部药物传递赋形剂,但仍缺乏其疗效的证据。我们测试了含有试验药物布洛芬的 SFA 配方是否可以雾化,并评估了它们的药代动力学。评估了五种不同布洛芬配方的物理化学性质:水溶液(H2O)、两种不同的 SFA(全氟己基辛烷(F6H8)、全氟丁基戊烷(F4H5))和含乙醇的 SFA(SFA/EtOH)。使用射流导管系统进行雾化。通过激光衍射评估吸入特性。在麻醉健康兔中进行了一项具有吸入性单剂量(6 毫克/千克)布洛芬的确认性动物研究,使用了每种配方。使用 HPLC-MS/MS 分析在规定时间点采集的血浆样本和在 6 小时研究期后采集的肺组织。使用非房室模型计算药代动力学。所有配方都可雾化。SFA 和 SFA/EtOH 之间的空气动力学直径(MMAD)没有差异。F4H5/EtOH 的布洛芬血浆浓度-时间曲线(AUC)最高。相比之下,F6H8/EtOH 具有最高的肺部组织中布洛芬沉积,但 AUC 最低。所有测试的 SFA 和 SFA/EtOH 配方都适合吸入。F4H5/EtOH 配方可能用于药物的快速全身可用性。F6H8/EtOH 显示了试验药物在肺内的沉积。

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