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生育酚磷酸酯混合物(TPM)作为一种新型脂质体透皮给药载体:制剂与评价

Tocopheryl phosphate mixture (TPM) as a novel lipid-based transdermal drug delivery carrier: formulation and evaluation.

作者信息

Gavin Paul D, El-Tamimy Mahmoud, Keah Hooi Hong, Boyd Ben J

机构信息

Phosphagenics Limited, 11 Duerdin Street, Clayton, VIC, 3168, Australia.

Drug Delivery, Disposition and Dynamics, Monash Institute of Pharmaceutical Sciences, Monash University, 381 Royal parade, Parkville, VIC, Australia.

出版信息

Drug Deliv Transl Res. 2017 Feb;7(1):53-65. doi: 10.1007/s13346-016-0331-x.

DOI:10.1007/s13346-016-0331-x
PMID:27672079
Abstract

Transdermal drug delivery is a useful route of administration that avoids first-pass metabolism and more invasive delivery options. However, many drugs require enhancers to enable sufficient drug absorption to reach therapeutic effect. Alpha-tocopheryl phosphate (TP) and di-alpha-tocopheryl phosphate (T2P) are two phosphorylated forms of vitamin E which form tocopheryl phosphate mixture (TPM) when combined, and have been proposed to enhance the dermal and transdermal delivery of actives of interest. Here, we report the physicochemical characteristics and morphological properties of TPM formulations, including particle size, deformability and morphology, and its ability to facilitate the transport of carnosine, vitamin D3, CoEnzyme Q10 and caffeine into, and across, the skin. Results demonstrate that TPM self-assembles to form vesicular structures in hydroethanolic solutions ranging in mean size from 101 to 162 nM depending on the amount of TPM and ethanol present in the formulation. The ratio of TP to T2P in TPM formulations altered vesicle size and elasticity, with vesicles high in TP found to be more deformable than those rich in T2P. TPM produced a significant (p < 0.05) 2.4-3.4-fold increase in the absorption of carnosine, vitamin D3, CoEnzyme Q10 and caffeine into, or through, the skin. The TPM delivery platform was able to deliver a diverse range of actives with differing size and solubility profiles and therefore has significant potential to expand the number and types of drugs available for topical application and transdermal delivery.

摘要

经皮给药是一种有用的给药途径,可避免首过代谢和更具侵入性的给药方式。然而,许多药物需要渗透促进剂才能实现足够的药物吸收以达到治疗效果。α-生育酚磷酸酯(TP)和二-α-生育酚磷酸酯(T2P)是维生素E的两种磷酸化形式,它们组合时形成生育酚磷酸酯混合物(TPM),并且已被提议用于增强感兴趣的活性成分的真皮和经皮递送。在此,我们报告了TPM制剂的物理化学特性和形态学性质,包括粒径、可变形性和形态,以及其促进肌肽、维生素D3、辅酶Q10和咖啡因进入皮肤并透过皮肤转运的能力。结果表明,TPM在含乙醇的水溶液中自组装形成囊泡结构,其平均尺寸根据制剂中TPM和乙醇的含量在101至162 nM范围内变化。TPM制剂中TP与T2P的比例改变了囊泡大小和弹性,发现TP含量高的囊泡比富含T2P的囊泡更易变形。TPM使肌肽、维生素D3、辅酶Q10和咖啡因进入皮肤或透过皮肤的吸收显著增加(p < 0.05),增加了2.4至3.4倍。TPM递送平台能够递送具有不同大小和溶解度特征的多种活性成分,因此具有显著潜力来扩大可用于局部应用和经皮递送的药物数量和类型。

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