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外用糖皮质激素对细胞增殖、细胞周期进程及细胞凋亡的影响:对HaCaT细胞的体外比较

Effects of topical corticosteroids on cell proliferation, cell cycle progression and apoptosis: in vitro comparison on HaCaT.

作者信息

Guichard Alexandre, Humbert Philippe, Tissot Marion, Muret Patrice, Courderot-Masuyer Carole, Viennet Céline

机构信息

Research and Studies Center on the Integument (CERT), Department of Dermatology, Clinical Investigation Center (CIC INSERM 1431), Besançon University Hospital, France; Engineering and Cutaneous Biology Laboratory, INSERM UMR 1098, SFR FED 4234, University of Franche-Comte, Besançon, France.

Engineering and Cutaneous Biology Laboratory, INSERM UMR 1098, SFR FED 4234, University of Franche-Comte, Besançon, France.

出版信息

Int J Pharm. 2015 Feb 20;479(2):422-9. doi: 10.1016/j.ijpharm.2014.12.066. Epub 2014 Dec 30.

Abstract

Topical-corticosteroids are mainly used for the treatment of inflammatory or hyperproliferative skin diseases. The in vivo assay to rank topical-corticosteroids potency, based on the skin blanching, is not adapted to compare their anti-proliferative efficacy. We have compared the antiproliferative effect of six topical-corticosteroids on a model of hyperproliferant keratinocytes (HaCaT). Betamethasone-dipropionate; clobetasol-propionate; betamethasone-valerate; desonide; hydrocortisone-butyrate and hydrocortisone-base, at different concentrations (10(-8)-10(-4)M) have been compared. HaCaT proliferation has been evaluated by MTT-assay and the mechanism of the death was evaluated by annexin V/propidium iodide staining and cell cycle phases analysis. Topical corticosteroids reduced cell growth in a dose-dependent manner. At 10(-4)M, betamethasone dipropionate was the most antiproliferative compound while hydrocortisone-butyrate was the less. Hydrocortisone-base which is usually considered as the less potent topical-corticosteroids showed a clear cytotoxic effect. Betamethasone-dipropionate and betamethasone-valerate induced more apoptosis than necrosis whereas the reverse has been observed for other topical-corticosteroids. All topical-corticosteroids, except clobetasol-propionate, arrested cell cycle mainly in G2-phase. Clobetasol-propionate arrested cell cycle in S-phase population. At 10(-8)M, topical-corticosteroids induced HaCaT proliferation. In terms of antiproliferative effect at 10(-4)M, we propose to rank topical corticosteroids as follow: betamethasone-dipropionate>desonide≥betamethasone-valerate=hydrocortisone-base=clobetasol-propionate>hydrocortisone-butyrate. This classification differs from the current ranking, based on the vasoconstrictive effect, but is more adapted for hyperproliferative disease treatment.

摘要

外用皮质类固醇主要用于治疗炎症性或增殖性皮肤病。基于皮肤变白来对外用皮质类固醇效力进行排序的体内试验并不适用于比较它们的抗增殖功效。我们比较了六种外用皮质类固醇对增殖性角质形成细胞(HaCaT)模型的抗增殖作用。比较了不同浓度(10⁻⁸ - 10⁻⁴M)的倍他米松二丙酸酯、丙酸氯倍他索、倍他米松戊酸酯、地奈德、丁酸氢化可的松和氢化可的松。通过MTT试验评估HaCaT增殖情况,并通过膜联蛋白V/碘化丙啶染色和细胞周期阶段分析评估细胞死亡机制。外用皮质类固醇以剂量依赖方式降低细胞生长。在10⁻⁴M时,倍他米松二丙酸酯是最具抗增殖作用的化合物,而丁酸氢化可的松作用最小。通常被认为是效力最低的外用皮质类固醇氢化可的松显示出明显的细胞毒性作用。倍他米松二丙酸酯和倍他米松戊酸酯诱导的凋亡多于坏死,而其他外用皮质类固醇则观察到相反情况。除丙酸氯倍他索外,所有外用皮质类固醇主要将细胞周期阻滞在G2期。丙酸氯倍他索将细胞周期阻滞在S期群体。在10⁻⁸M时,外用皮质类固醇诱导HaCaT增殖。就10⁻⁴M时的抗增殖作用而言,我们建议对外用皮质类固醇进行如下排序:倍他米松二丙酸酯>地奈德≥倍他米松戊酸酯=氢化可的松=丙酸氯倍他索>丁酸氢化可的松。这种分类与基于血管收缩作用的当前排序不同,但更适用于增殖性疾病的治疗。

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