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阴离子表面活性剂渗透入人体皮肤的机制:探究单体、胶束和亚胶束聚集体渗透理论。

Mechanisms of anionic surfactant penetration into human skin: Investigating monomer, micelle and submicellar aggregate penetration theories.

作者信息

Morris Stephanie A V, Thompson Ryan T, Glenn Robert W, Ananthapadmanabhan K P, Kasting Gerald B

机构信息

James L. Winkle College of Pharmacy, University of Cincinnati, Cincinnati, Ohio, 45267-0004, USA.

Research & Development Department, The Procter & Gamble Company, Cincinnati, Ohio, USA.

出版信息

Int J Cosmet Sci. 2019 Feb;41(1):55-66. doi: 10.1111/ics.12511. Epub 2019 Feb 22.

Abstract

OBJECTIVE

Once penetrated into the stratum corneum, anionic surfactants bind to and denature stratum corneum proteins as well as intercalate into and extract intercellular lipids. With repeated exposures, this leads to skin dryness and irritation, compromising barrier function and skin health. The mechanisms of anionic surfactant penetration into the skin, however, are still widely debated. The objective of this study was to evaluate current theories of surfactant penetration into human skin.

METHODS

A test set comprising 15 anionic surfactant systems and one non-ionic surfactant, all having either dodecyl or lauryl alkyl chains, was tested for surfactant penetration into split-thickness human cadaver skin in vitro using radiolabelled sodium dodecyl sulphate ( C-SDS). Select physical properties of these formulations thought to be associated with skin penetration including critical micelle concentration, micelle diameter, filtrate concentration and zeta potential were also measured.

RESULTS

C-SDS penetration into human cadaver skin from surfactant systems in vitro was found to correlate well with CMC (R  = 0.34, P < 0.05), filtrate concentration (R  = 0.36, P < 0.05) and zeta potential (R  = 0.76, P < 0.001), but poorly with micelle diameter (R  = 0.12). Furthermore, the latter measure correlated inversely with penetration compared to what would be expected based on the micelle penetration theory.

CONCLUSION

Neither monomer nor micelle penetration theories are sufficient to explain anionic surfactant penetration into human skin. Submicellar (or premicellar) aggregate penetration theory is difficult to defend at relevant surfactant concentrations. We propose a new hypothesis for this mechanism in which short-term penetration is based on monomer concentration and longer term penetration is based on surfactant-induced damage to the skin barrier.

摘要

目的

一旦渗透进入角质层,阴离子表面活性剂会与角质层蛋白质结合并使其变性,同时嵌入并提取细胞间脂质。反复接触会导致皮肤干燥和刺激,损害屏障功能和皮肤健康。然而,阴离子表面活性剂渗透进入皮肤的机制仍存在广泛争议。本研究的目的是评估当前关于表面活性剂渗透进入人体皮肤的理论。

方法

使用放射性标记的十二烷基硫酸钠(C-SDS),对一组包含15种阴离子表面活性剂体系和1种非离子表面活性剂(均具有十二烷基或月桂基烷基链)的测试集进行体外测试,以检测表面活性剂渗透进入人尸体皮肤的情况。还测量了这些配方中被认为与皮肤渗透相关的一些物理性质,包括临界胶束浓度、胶束直径、滤液浓度和zeta电位。

结果

体外实验发现,C-SDS从表面活性剂体系渗透进入人尸体皮肤的情况与临界胶束浓度(R = 0.34,P < 0.05)、滤液浓度(R = 0.36,P < 0.05)和zeta电位(R = 0.76,P < 0.001)有良好的相关性,但与胶束直径的相关性较差(R = 0.12)。此外,与基于胶束渗透理论预期的情况相比,后者与渗透率呈负相关。

结论

单体渗透理论和胶束渗透理论都不足以解释阴离子表面活性剂渗透进入人体皮肤的现象。在相关表面活性剂浓度下,亚胶束(或前胶束)聚集体渗透理论难以成立。我们提出了一种关于该机制的新假设,即短期渗透基于单体浓度,长期渗透基于表面活性剂对皮肤屏障的损伤。

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