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Development of an Optimised Application Protocol For Sonophoretic Transdermal Delivery of a Model Hydrophilic Drug

机译:亲水药物模型透声递送的优化应用方案的开发

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It has now been known for over a decade that low frequency ultrasound can be used to effectively enhance transdermal drug penetration - an approach termed sonophoresis. Mechanistically, acoustic cavitation results in the creation of defects in the stratum corneum that allow accelerated absorption of topically applied molecules. The aim of this study was to develop an optimised sonophoresis protocol for studying transdermal drug delivery in vitro. To this end, caffeine was selected as a model hydrophilic drug while porcine skin was used as a model barrier. Following acoustic validation, 20kHz ultrasound was applied for different durations (range: 5 s to 10 min) using three different modes (10%, 33% or 100% duty cycles) and two distinct sonication procedures (either before or concurrent with drug deposition). Each ultrasonic protocol was assessed in terms of its heating and caffeine flux-enhancing effects. It was found that the best regimen was a concurrent 5 min, pulsed (10% duty cycle) beam of SATA intensity 0.37 W/cm2. A key insight was that in the case of pulsed beams of 10% duty cycle, sonication concurrent with drug deposition was superior to sonication prior to drug deposition and potential mechanisms for this are discussed.
机译:十多年来,人们已经知道低频超声可用于有效地增强透皮药物的渗透性,这种方法被称为超声治疗。从机械上讲,声空化会导致角质层中产生缺陷,从而加速局部应用分子的吸收。这项研究的目的是开发一种优化的超声穿刺方案,以研究体外透皮药物的递送。为此,选择咖啡因作为模型亲水药物,而使用猪皮作为模型屏障。进行声学验证后,使用三种不同的模式(10%,33%或100%的占空比)和两种不同的超声处理程序(在药物沉积之前或同时进行),将20kHz超声波应用于不同的持续时间(范围:5 s至10分钟)。 。评估每种超声方案的加热和咖啡因通量增强效果。发现最佳方案是同时使用5分钟的SATA强度为0.37 W / cm2的脉冲(10%占空比)光束。一个关键的见解是,在占空比为10%的脉冲束的情况下,与药物沉积同时进行的超声处理优于在药物沉积之前进行的超声处理,并对此进行了探讨。

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