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Investigations into the formulation of metered dose inhalers of salmeterol xinafoate and fluticasone propionate microcrystals.

机译:调查Salmeterol XinaFoate和氟替卡松丙酸盐微晶的计量剂量吸入器的制剂。

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摘要

PURPOSE: To investigate the aerosolization and behaviour of microparticles of salmeterol xinafoate (SX) and fluticasone propionate (FP) suspended in hydrofluoroalkane (HFA) propellant. METHODS: Microcrystals of SX and FP were produced from poly(ethylene glycol) by antisolvent crystallization. The suspension behaviour and aerosolization of the microcrystals when formulated as metered dose inhalers (MDIs) in HFA 134a propellant was compared with that of microparticles produced by micronization (mSX and mFP) using a glass twin stage impinger and by laser light diffraction using a pressurized cell. RESULTS: FP microparticles underwent non-reversible aggregation in suspension as seen by a doubling in the volume median diameter compared to the raw material. The degree of aggregation of SX particles in suspension was found to decrease as the particle size of the original particles increased. However, because the SX aggregate size was lowest for the particles with the smallest initial size (mSX), the highest fine particle fraction (FPF) of SX was obtained from a suspension of mSX. The FPFs following aerosolization of FP suspensions were similar although the FPF was lowest for particles with the largest original size. CONCLUSIONS: The size of the aggregates in the HFA suspensions was found to correlate directly with the FPFs determined by impaction.
机译:目的:探讨Salmeterol XinaFoate(SX)和氟替卡松丙酸盐(FP)悬浮在氢氟烷烃(HFA)推进剂中的雾化和行为的雾化和行为。方法:通过抗溶剂结晶从聚(乙二醇)产生Sx和Fp的微晶。将微晶作为在HFA 134A推进剂中配制时的微晶的悬浮行为和雾化与使用加压细胞的玻璃双级植物和激光衍射通过微粉化(MSX和MFP)产生的微粒进行比较。使用加压细胞。结果:FP微粒在悬浮液中经历了不可逆转的聚集,如同原料相比,在体积中间直径的加倍。由于原始颗粒的粒度增加,发现Sx颗粒在悬浮液中的聚集程度降低。然而,因为具有最小初始尺寸(MSX)的颗粒的Sx骨料尺寸最低,所以从MSX的悬浮液中获得Sx的最高细粒级分(FPF)。 FP悬浮液雾雾化后的FPF是相似的,尽管FPF对于具有最大尺寸最大的颗粒是最低的。结论:发现HFA悬浮液中的聚集体的大小直接与通过剥夺确定的FPFs相关。

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  • 来源
    《Pharmaceutical research》 |2008年第10期|共9页
  • 作者

    Murnane D; Martin GP; Marriott C;

  • 作者单位

    King's College London Drug Delivery Research Group Pharmaceutical Science Division 150 Stamford Street London SE1 9NH UK.;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 药学;
  • 关键词

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