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槲皮素及其多甲氧基化合物和糖苷的抗炎活性和经皮吸收:与化学结构的关系。

Anti-inflammatory activity and percutaneous absorption of quercetin and its polymethoxylated compound and glycosides: the relationships to chemical structures.

机构信息

Department of Cosmetic Science, Chang Gung University of Science and Technology, Kweishan, Taoyuan, Taiwan.

出版信息

Eur J Pharm Sci. 2012 Dec 18;47(5):857-64. doi: 10.1016/j.ejps.2012.04.024. Epub 2012 May 17.

DOI:10.1016/j.ejps.2012.04.024
PMID:22609526
Abstract

The potential of quercetin-related compounds for topical application has not previously been systematically investigated. To better elucidate relationships of the structure and activity with skin permeation, some quercetin compounds were used as permeants, including aglycone, a polymethoxylated compound (quercetin 3,5,7,3',4'-pentamethylether, QM), and seven glycosides. Quercetin and the glycoside with glucopyranuronic acid (Q4) at a dose of 30 μM completely inhibited superoxide anion activated neutrophils. QM also potentially suppressed superoxide by 90%. Both quercetin and QM showed inhibitory activity on elastase release with respective IC(50) values of 6.25 and 15.76 μM. Glycosylation significantly diminished this activity. Both an infinite concentration and saturated solubility in pH 7 buffer were used as permeant doses for the in vitro permeation experiments. The flux or permeability coefficient, which is the indicator for total absorption of dermal delivery due to the use of nude mouse skin, was the greatest for QM, followed by the glycosides and quercetin. QM showed 26× greater flux compared to quercetin. No penetration of quercetin occurred at the dose of saturated solubility. Rutin generally exhibited the highest skin permeation among the glycosides. It was found that the glycoside enantiomers (Q2 and Q3) revealed completely different permeation profiles. The stratum corneum was the principal penetration barrier for quercetin and its glycosides but not QM. Rutin provoked some skin redness and inflammation after a 5-day administration in nude mouse. QM caused no irritation, suggesting that it is a superior candidate for topical delivery.

摘要

槲皮素相关化合物在局部应用方面的潜力以前尚未得到系统研究。为了更好地阐明结构与活性与皮肤渗透的关系,我们选择了一些槲皮素化合物作为渗透物,包括苷元、多甲氧基化合物(槲皮素 3,5,7,3',4'-五甲醚,QM)和七种糖苷。30 μM 剂量的槲皮素和带有葡萄糖醛酸的糖苷(Q4)可完全抑制超氧阴离子激活的中性粒细胞。QM 也有可能抑制 90%的超氧阴离子。槲皮素和 QM 对弹性蛋白酶释放均具有抑制活性,其 IC50 值分别为 6.25 和 15.76 μM。糖苷化显著降低了这种活性。在 pH7 缓冲液中,无限浓度和饱和溶解度均被用作体外渗透实验的渗透物剂量。通量或渗透系数是由于使用裸鼠皮肤导致的皮肤给药总吸收的指标,对于 QM 来说是最大的,其次是糖苷和槲皮素。QM 的通量比槲皮素大 26 倍。在饱和溶解度剂量下,槲皮素没有渗透。在糖苷中,芦丁的皮肤渗透性最高。发现糖苷的对映异构体(Q2 和 Q3)显示出完全不同的渗透特征。角质层是槲皮素及其糖苷的主要渗透屏障,但不是 QM。在 5 天的裸鼠给药后,芦丁引起一些皮肤发红和炎症。QM 没有引起刺激,这表明它是局部递送的较好候选物。

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