Effect of glycation focusing on the process of epidermal lipid synthesis in a reconstructed skin model and membrane fluidity of stratum corneum lipids.

Dermato-Endocrinology Pub Date : 2017-10-04 eCollection Date: 2017-01-01 DOI:10.1080/19381980.2017.1338992
Mami Yokota, Hitoshi Masaki, Yuri Okano, Yoshihiro Tokudome
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引用次数: 10

Abstract

We previously reported that epidermal glycation causes an increase in saturated fatty acid (FA) content in a differentiated reconstructed skin model and HaCaT cells. However, the relationship between ceramides (CERs) and glycation and their effects on stratum corneum (SC) barrier function was not elucidated. In this study, we investigated the effect of glycation on lipid content in 6-day-old cultured reconstructed skin. We used the EPISKIN RHE 6D model and induced glycation using glyoxal. In addition to transepidermal water loss, content of CERs, cholesterol and FA in the reconstructed epidermal model were analyzed by high performance thin layer chromatography. Expression of genes related to ceramide metabolism was determined by real time RT-PCR. Membrane fluidity of stratum corneum lipid liposomes (SCLL) that mimic glycated epidermis was analyzed using an electron spin resonance technique. It was found that FA was significantly increased by glycation. CER[NS], [AP], and cholesterol were decreased in glycated epidermis. Expression of ceramide synthase 3 (CERS3) was significantly decreased while fatty acid elongase 3 was increased by glyoxal in a dose dependent manner. Membrane fluidity of SCLL mimicking the lipid composition of glycated epidermis was increased compared with controls. Therefore, disruption of CER and FA content in glycated epidermis may be regulated via CERS3 expression and contribute to abnormal membrane fluidity.

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糖基化对重建皮肤模型中表皮脂质合成过程和角质层脂质膜流动性的影响。
我们之前报道过表皮糖基化导致分化重建皮肤模型和HaCaT细胞中饱和脂肪酸(FA)含量增加。然而,神经酰胺(CERs)与糖基化之间的关系及其对角质层(SC)屏障功能的影响尚不清楚。在本研究中,我们研究了糖基化对6日龄培养重建皮肤脂质含量的影响。采用EPISKIN RHE 6D模型,乙二醛诱导糖基化。除经皮失水外,采用高效薄层色谱法分析重建表皮模型中cer、胆固醇和FA的含量。实时RT-PCR检测神经酰胺代谢相关基因的表达。采用电子自旋共振技术分析了模拟糖基化表皮的角质层脂质脂质体(SCLL)的膜流动性。发现糖基化显著增加FA。糖基化表皮的CER[NS]、[AP]和胆固醇均降低。乙二醛显著降低了神经酰胺合成酶3 (CERS3)的表达,而脂肪酸延长酶3的表达呈剂量依赖性。与对照组相比,模拟糖基化表皮脂质组成的scl膜流动性增加。因此,糖基化表皮中CER和FA含量的破坏可能通过CERS3的表达来调节,并导致膜流动性异常。
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