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Towards crystal engineering via simulated pulmonary surfactant monolayers to optimise inhaled drug delivery.

机译:通过模拟的肺表面活性剂单层实现晶体工程,以优化吸入药物的输送。

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PURPOSE: To generate theophylline monohydrate crystals underneath Langmuir monolayers composed of material expressed at the alveolar air-liquid interface. Such monolayers can act as nucleation sites to direct crystallisation. The approach offers a novel route to rationally engineer therapeutic crystals and thereby optimise inhaled drug delivery. METHODS: Langmuir monolayers consisting of either dipalmitoylphosphatidylcholine (DPPC) or a surfactant mix reflecting pulmonary surfactant were supported on an aqueous theophylline (5.7 mg/ml) subphase. The monolayers were compressed to surface pressures reflecting inhalation and exhalation (i.e. 5 mNm(-1) or 55 mNm(-1)) with a period of 16 h to allow crystallisation. Analysis involved scanning electron microscopy (SEM), atomic force microscopy (AFM) and powder X-ray diffraction (PXRD). RESULTS: Condensed isotherms were acquired, which signified surfactant-theophylline interaction. Theophylline monohydrate crystals were obtained and exhibited needle-like morphology. SEM and AFM data highlighted regions of roughened growth along with smooth, stepwise growth on the same crystal face. The surfactant monolayers appeared to influence crystal morphology over time. CONCLUSIONS: The data indicate a favourable interaction between each species. The principal mechanism of interaction is thought to be an ion-dipole association. This approach may be applied to generate material with improved complementarity with pulmonary surfactant thus enhancing the interaction between inhaled drug particles and internal lung surfaces.
机译:目的:在Langmuir单层膜下生成茶碱一水合物晶体,该膜由在肺泡气液界面表达的物质组成。这样的单层可以充当成核位置以指导结晶。该方法提供了一种新颖的途径,可以合理地改造治疗性晶体,从而优化吸入药物的输送。方法:由二棕榈酰磷脂酰胆碱(DPPC)或反映肺表面活性剂的表面活性剂混合物组成的Langmuir单层被负载在茶碱水溶液(5.7 mg / ml)上。将单层压缩至反映吸入和呼出的表面压力(即5 mNm(-1)或55 mNm(-1)),持续16小时以使其结晶。分析涉及扫描电子显微镜(SEM),原子力显微镜(AFM)和粉末X射线衍射(PXRD)。结果:获得浓缩的等温线,表明表面活性剂与茶碱相互作用。获得茶碱一水合物晶体,并显示出针状形态。 SEM和AFM数据突出显示了同一晶面上粗糙的生长区域以及平滑,逐步的生长区域。表面活性剂单层似乎随时间影响晶体形态。结论:数据表明每个物种之间有利的相互作用。相互作用的主要机理被认为是离子-偶极缔合。该方法可用于产生与肺表面活性剂具有改善的互补性的材料,从而增强吸入药物颗粒与肺内部表面之间的相互作用。

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