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Novel gel-niosomes formulations as multicomponent systems for transdermal drug delivery

机译:新型凝胶-脂质体制剂,可作为多组分系统用于透皮给药

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摘要

The percutaneous permeation profiles of sulfadiazine sodium salt, propranolol hydrochloride and tyrosol from novel liquid crystal-niosomes formulations as multicomponent systems, were investigated. The new carriers were prepared from mixture of water/surfactant, AOT or Pluronic L64 as anionic and nonionic surfactants, respectively, in order to obtain lamellar LLC phases. The same surfactants were used to prepare also the vesicular systems (niosomes) that were added to the corresponding gel. The obtained multicomponent drug carrier was characterized by deuterium nuclear magnetic resonance spectroscopy, in order to understand if the introduction of the drug or drug-loaded niosomal suspension, as third component in the formulations, could influence the microstructure of the system and then the drug delivery across the skin. Simple AOT and L64-based niosomal formulations and LLCs phases were then prepared and used as control. Different drugs percutaneous availability was achieved, and the results revealed that the obtained gel-niosomes carriers were affected by the chemical structure of the drugs and by their affinity for the components. As a consequence these systems could be proposed as novel transdermal drug delivery systems, since they were found able to control the percutaneous permeation of small drugs across the skin.
机译:研究了磺胺嘧啶钠盐,盐酸普萘洛尔和酪醇从新型液晶-脂质体制剂中作为多组分体系的透皮渗透特性。由水/表面活性剂,AOT或Pluronic L64分别作为阴离子和非离子表面活性剂的混合物制备新的载体,以获得层状LLC相。相同的表面活性剂也用于制备添加到相应凝胶中的囊泡系统(脂质体)。通过氘核磁共振波谱对获得的多组分药物载体进行表征,以了解引入药物或载有药物的微粒悬浮液作为制剂中的第三种成分是否会影响系统的微观结构,进而影响药物的递送穿过皮肤。然后制备简单的基于AOT和基于L64的染色体制剂和LLCs相,并将其用作对照。获得了不同的药物经皮可获得性,并且结果表明,所获得的凝胶-脂质体载体受药物的化学结构及其对组分的亲和力的影响。结果,这些系统可以被提议作为新型的透皮药物递送系统,因为发现它们能够控制小药物在皮肤上的经皮渗透。

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