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基于胆碱和咪唑的离子液体作为局部给药系统中的功能成分:细胞毒性、溶解度和皮肤渗透研究

Choline- versus imidazole-based ionic liquids as functional ingredients in topical delivery systems: cytotoxicity, solubility, and skin permeation studies.

作者信息

Santos de Almeida Tânia, Júlio Ana, Saraiva Nuno, Fernandes Ana Sofia, Araújo Maria Eduarda M, Baby André Rolim, Rosado Catarina, Mota Joana Portugal

机构信息

a CBIOS - Universidade Lusófona's Research Center for Biosciences and Health Technologies , Lisboa , Portugal.

b Centro de Química e Bioquímica, Faculdade de Ciências , Universidade de Lisboa , Lisboa , Portugal.

出版信息

Drug Dev Ind Pharm. 2017 Nov;43(11):1858-1865. doi: 10.1080/03639045.2017.1349788. Epub 2017 Jul 12.

Abstract

BACKGROUND

Poor drug solubility represents a problem for the development of topical formulations. Since ionic liquids (ILs) can be placed in either lipophilic or hydrophilic solutions, they may be advantageous vehicles in such delivery systems. Nonetheless, it is vital to determine their usefulness when used at concentrations were cell viability is maintained, which was considered herein.

METHOD

Five different ILs were prepared-three imidazole-based ILs: [C2mim][Br], [C4mim][Br], and [C6mim][Br]; and two choline-based ILs: [Cho][Phe] and [Cho][Glu]. Their cytotoxicity in human keratinocytes (HaCat cells), their influence in drug solubility and in percutaneous permeation, using pig skin membranes, was evaluated.

RESULTS

Caffeine and salicylic acid were used as model actives. Choline-based ILs proved to be more suitable as functional ingredients, since they showed higher impact on drug solubility and a lower cytotoxicity. The major solubility enhancement was observed for caffeine and further solubility studies were carried out with this active in several concentrations of the choline-based ILs (0.1; 0.2; 0.5; 1.0; 3.0 and 5.0%, w/w) at 25 °C and 32 °C. Solubility was greatly influenced by concentrations up to 0.5%. The choline-based ILs showed no significant impact on the skin permeation, for both actives. The size of the imidazole-based ILs alkyl chain enhances the caffeine solubility and permeation, but also the ILs cytotoxicity. Stable O/W emulsions and gels were prepared containing the less toxic choline-based ILs and caffeine.

CONCLUSIONS

Our results indicate that the choline-based ILs were effective functional ingredients, since, when used at nontoxic concentrations, they allowed a higher drug loading, while maintaining the stability of the formulations.

摘要

背景

药物溶解度差是局部用制剂开发面临的一个问题。由于离子液体(ILs)可溶于亲脂性或亲水性溶液,它们可能是此类给药系统中的有利载体。尽管如此,确定其在维持细胞活力的浓度下使用时的有效性至关重要,本文对此进行了研究。

方法

制备了五种不同的离子液体——三种基于咪唑的离子液体:[C2mim][Br]、[C4mim][Br]和[C6mim][Br];以及两种基于胆碱的离子液体:[Cho][Phe]和[Cho][Glu]。评估了它们对人角质形成细胞(HaCat细胞)的细胞毒性,以及对猪皮肤膜药物溶解度和经皮渗透的影响。

结果

使用咖啡因和水杨酸作为模型活性成分。基于胆碱的离子液体被证明更适合作为功能成分,因为它们对药物溶解度的影响更大,细胞毒性更低。观察到咖啡因的溶解度有显著提高,并在25℃和32℃下,用该活性成分在几种浓度(0.1;0.2;0.5;1.0;3.0和5.0%,w/w)的基于胆碱的离子液体中进行了进一步的溶解度研究。浓度高达0.5%时,溶解度受到很大影响。对于两种活性成分,基于胆碱的离子液体对皮肤渗透均无显著影响。基于咪唑的离子液体烷基链的长度增加了咖啡因的溶解度和渗透率,但也增加了离子液体的细胞毒性。制备了含有毒性较小的基于胆碱的离子液体和咖啡因的稳定水包油乳液和凝胶。

结论

我们的结果表明,基于胆碱的离子液体是有效的功能成分,因为在无毒浓度下使用时,它们能实现更高的药物负载量,同时保持制剂的稳定性。

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