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己脒定的局部给药

Topical delivery of hexamidine.

作者信息

Parisi Nicola, Paz-Alvarez Miguel, Matts Paul J, Lever Rebecca, Hadgraft Jonathan, Lane Majella E

机构信息

UCL School of Pharmacy, 29-39 Brunswick Square, London, WC1N 1AX, United Kingdom.

Procter & Gamble Technical Centres Ltd., London Innovation Centre, Whitehall Lane, Egham, Surrey, TW20 9NW, United Kingdom.

出版信息

Int J Pharm. 2016 Jun 15;506(1-2):332-9. doi: 10.1016/j.ijpharm.2016.04.069. Epub 2016 Apr 26.

Abstract

Hexamidine diisethionate (HEX D) has been used for its biocidal actions in topical preparations since the 1950s. Recent data also suggest that it plays a beneficial role in skin homeostasis. To date, the extent to which this compound penetrates the epidermis has not been reported nor how its topical delivery may be modulated. In the present work we set out to characterise the interaction of HEX D with the skin and to develop a range of simple formulations for topical targeting of the active. A further objective was to compare the skin penetration of HEX D with its corresponding dihydrochloride salt (HEX H) as the latter has more favourable physicochemical properties for skin uptake. Candidate vehicles were evaluated by in vitro Franz cell permeation studies using porcine skin. Initially, neat solvents were investigated and subsequently binary systems were examined. The solvents and chemical penetration enhancers investigated included glycerol, dimethyl isosorbide (DMI), isopropyl alcohol (IPA), 1,2-pentanol (1,2-PENT), polyethylene glycol (PEG) 200, propylene glycol (PG), propylene glycol monolaurate (PGML) and Transcutol(®)P (TC). Of a total of 30 binary solvent systems evaluated only 10 delivered higher amounts of active into the skin compared with the neat solvents. In terms of topical efficacy, formulations containing PGML far surpassed all other solvents or binary combinations. More than 70% of HEX H was extracted from the skin following application in PG:PGML (50:50). Interestingly, the same vehicle effectively promoted skin penetration of HEX D but demonstrated significantly lower uptake into and through the skin (30%). The findings confirm the unpredictable nature of excipients on delivery of actives with reference to skin even where there are minor differences in molecular structures. We also believe that they underline the ongoing necessity for fundamental studies on the interaction of topical excipients with the skin.

摘要

自20世纪50年代以来,己脒二乙磺酸盐(HEX D)就因其杀菌作用而被用于局部制剂中。最近的数据还表明,它在皮肤稳态中发挥着有益作用。迄今为止,尚未报道该化合物穿透表皮的程度,也未报道其局部给药方式如何调节。在本研究中,我们着手表征HEX D与皮肤的相互作用,并开发一系列简单的制剂用于该活性成分的局部靶向给药。另一个目标是比较HEX D与其相应的二盐酸盐(HEX H)的皮肤渗透性,因为后者具有更有利于皮肤吸收的物理化学性质。通过使用猪皮的体外Franz细胞渗透研究来评估候选载体。最初,研究了纯溶剂,随后研究了二元体系。研究的溶剂和化学渗透促进剂包括甘油、二甲基异山梨醇(DMI)、异丙醇(IPA)、1,2 - 戊醇(1,2 - PENT)、聚乙二醇(PEG)200、丙二醇(PG)、丙二醇单月桂酸酯(PGML)和Transcutol(®)P(TC)。在总共评估的30种二元溶剂体系中,只有10种与纯溶剂相比能将更多的活性成分输送到皮肤中。就局部疗效而言,含有PGML的制剂远远超过所有其他溶剂或二元组合。在PG:PGML(50:50)中应用后,超过70%的HEX H从皮肤中被提取出来。有趣的是,相同的载体有效地促进了HEX D的皮肤渗透,但显示出进入皮肤和透过皮肤的摄取量显著更低(30%)。这些发现证实了辅料对活性成分经皮递送的影响具有不可预测性,即使分子结构存在微小差异。我们还认为,这些发现强调了对局部辅料与皮肤相互作用进行基础研究的持续必要性。

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