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Characterization of drug particle delivery to ex vivo human skin by needle-free powder injection systems

机译:通过无针粉末注射系统表征用无针粉末注射液中的药物颗粒递送给emvivo人皮肤

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The PowderJect~direct R needle-free injector delivers drugs in dry powder form into the skin by accelerating the particles to high velocity using pressurised helium gas (1). Relationship between particle size, pressure and bioavailability (2,3) as well as between dosage and plasma concentration were previously demonstrated (4). However, the barrier function of skin in this case has to be hypothetically regarded as different to the case of needle-free injection of liquids and even more different to application by transdermal diffusion. thus, for an better understanding of the relationship between drug application, skin structures and bioavailability, studies on excised human skin provide the most authentic conditions with respect to penetrability and mechanical resistance. For investigations of extent and depth of drug penetration a crystalline model compound was chosen, as it should easily be recovered from the biological material and previous pharmacokinetical studies on needle-free powder injection were mostly done with pure crystalline compounds (2,3). tape-stripping, as it is a common method to remove the stratum corneum, offers a first step towards characterisation of the barrier function of the particular skin layers. It is a simple way to demonstrate, whether or not an intact stratum corneum substantially affects the particle penetration.
机译:通过加压氦气(1)将颗粒加速至高速度,将粉末〜Direct r无无针注射器以干燥的粉末形式提供药物。先前证明了粒度,压力和生物利用度(2,3)以及剂量和等离子体浓度之间的关系(4)。然而,在这种情况下,皮肤的屏障功能必须被假设被认为与无针注射液体的情况不同,并且通过透皮扩散的施加更加不同。因此,为了更好地理解药物应用,皮肤结构和生物利用度之间的关系,对切除的人体皮肤的研究提供了相对于渗透性和机械性的最真实的条件。为了调查药物渗透的程度和深度,选择结晶模型化合物,因为它应该容易地从生物材料中回收,并且之前的针对无针粉末注射注射的药代动力学研究主要用纯晶体化合物(2,3)进行。胶带剥离,因为它是去除角质层的常见方法,提供了朝向特定皮肤层的阻挡功能表征的第一步。这是一种简单的方法,无论是否完整地层基本上影响粒子渗透率。

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