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A human skin high-throughput formulation screening method using a model hydrophilic drug

机译:一种使用模型亲水药物的人皮肤高通量配方筛选方法

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Franz cell (FC) experiments in topical and transdermal drug development represent the gold standard in vitro method but require a relatively high quantity of human skin, are low-throughput, and are time-consuming to perform. To address these issues, we studied a micro-well plate-based screening method for permeability and retention that could enable the direct screening of large numbers of formulations simultaneously across human skin. Using freshly excised dermatomed human skin modified to reflect poor barrier function and a model hydrophilic compound, Sulforhodamine B (SRB), FC permeation and retention quantification was compared to the 96-well high-throughput system (HTS). The skin was analyzed using 2-photon microscopy to determine the drug distribution within the skin. A screen of 15 different formulations in triplicate in a single piece of human skin, using full factorial design was then conducted. Permeability of SRB across the skin as well as the drug distribution profile of SRB retained in the skin were similar for the FC and HTS system. The influence of different excipients on drug retention was observed in the full factorial formulation screen. The HTS method is promising for the investigation of large numbers of formulations and the influence of formulations changes in skin retention of drug.
机译:术语和透皮药物开发中的Franz细胞(Fc)实验代表了金标准的方法,但需要相对大量的人体皮肤,是低通量,并且是耗时的表现。为了解决这些问题,我们研究了一种基于微孔板的筛选方法,用于渗透性和保留,可以使得能够在人体皮肤上同时直接筛选大量配方。使用新鲜切除的皮肤病的人体皮肤反射差反射功能和模型亲水化合物,与96孔高通量系统(HTS)进行比较苏尔磺胺胺B(SRB),Fc渗透和保留量化。使用2-光子显微镜分析皮肤以确定皮肤内的药物分布。然后,使用完整的因子设计,在一式一件式人体皮肤中的15种不同配方的筛网进行了​​三份。对于Fc和HTS系统,SRB对皮肤的渗透性以及皮肤中保留的SRB的药物分布曲线类似。在完整的因子制剂筛选中观察到不同赋形剂对药物保留的影响。 HTS方法是对大量配方的调查,以及配方对药物皮肤保留的影响的影响。

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