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皮肤溶解性决定了相似大小分子的最大经皮通量。

Skin solubility determines maximum transepidermal flux for similar size molecules.

作者信息

Zhang Qian, Grice Jeffrey E, Li Peng, Jepps Owen G, Wang Guang-Ji, Roberts Michael S

机构信息

Therapeutics Research Unit, School of Medicine, Princess Alexandra Hospital, The University of Queensland, Woolloongabba, QLD 4102, Australia.

出版信息

Pharm Res. 2009 Aug;26(8):1974-85. doi: 10.1007/s11095-009-9912-4. Epub 2009 Jun 5.

Abstract

PURPOSE

The maximum flux of solutes penetrating the epidermis has been known to depend predominantly on solute molecular weight. Here we sought to establish the mechanistic dependence of maximum flux on other solute physicochemical parameters.

METHODS

Maximum fluxes, stratum corneum solubilities and estimated diffusivities through human epidermis were therefore determined for 10 phenols with similar molecular weights and hydrogen bonding but varying in lipophilicity.

RESULTS

Maximum flux and stratum corneum solubilities of the phenolic compounds both showed a bilinear dependence on octanol-water partition coefficient (P), with solutes having a maximum solubility in the stratum corneum when 2.7<log P<3.1. In contrast, lag times and diffusivities were relatively independent of P. Stratum corneum-water partition coefficients and epidermal permeability coefficients were consistent with previously reported data.

CONCLUSION

A key finding is that the convex dependence of maximum flux on lipophilicity arises primarily from variations in stratum corneum solubility, and not from diffusional or partitioning barrier effects at the stratum corneum-viable epidermis interface for the more lipophilic phenols. Our data support a solute structure-skin transport model for aqueous solutions in which permeation rates depend on both partitioning and diffusivity: partitioning is related to P, and diffusivity to solute size and hydrogen bonding.

摘要

目的

已知溶质穿透表皮的最大通量主要取决于溶质分子量。在此,我们试图确定最大通量对其他溶质物理化学参数的机制依赖性。

方法

因此,我们测定了10种分子量相似、具有氢键但亲脂性不同的酚类化合物透过人体表皮的最大通量、角质层溶解度和估计扩散率。

结果

酚类化合物的最大通量和角质层溶解度均显示出对正辛醇-水分配系数(P)的双线性依赖性,当2.7<log P<3.1时,溶质在角质层中的溶解度最大。相比之下,滞后时间和扩散率相对独立于P。角质层-水分配系数和表皮渗透系数与先前报道的数据一致。

结论

一个关键发现是,最大通量对亲脂性的凸面依赖性主要源于角质层溶解度的变化,而不是来自角质层-活性表皮界面处亲脂性更强的酚类化合物的扩散或分配屏障效应。我们的数据支持了一种适用于水溶液的溶质结构-皮肤转运模型,其中渗透速率取决于分配和扩散率:分配与P相关,扩散率与溶质大小和氢键相关。

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