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首页> 外文期刊>Experimental dermatology >Effects of a ceramide-containing water-in-oil ointment on skin barrier function and allergen penetration in an IL-31 treated 3D model of the disrupted skin barrier
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Effects of a ceramide-containing water-in-oil ointment on skin barrier function and allergen penetration in an IL-31 treated 3D model of the disrupted skin barrier

机译:含透明酰胺水油软膏对皮肤屏障的IL-31处理3D模型中皮肤屏障功能和过敏原渗透的影响

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Atopic dermatitis (AD) is a chronically relapsing, pruritic inflammation of the skin with dryness and disturbed skin barrier function. Recently, we established that IL-31 treatment of human 3D skin models resulted in a disrupted skin barrier phenotype resembling AD. In this model, we found that IL-31 interferes with the differentiation of keratinocytes and inhibits the expression of terminal differentiation markers. In the present study, we investigated the effects of a ceramide-containing water-in-oil skin care ointment on the physical skin barrier structure and function in disrupted skin barrier models, generated either by using primary normal human epidermal keratinocytes (NHEK) or HaCaT cells. We observed that the physical skin barrier of the models recovered after daily topical treatment with the ceramide-containing ointment. Topical application of the ointment prevented downregulation of filaggrin and disorganization of other differentiation markers, such as keratin 10 and 4-integrin, as demonstrated by immunohistological analysis. The expression of Ki67 was also upregulated in response to the ointment. Furthermore, functional studies revealed that local application of the ointment diminished the increased uptake of fluorescently labelled recombinant allergens of timothy grass (phl p1) in our model. In conclusion, our data revealed that topical application of a ceramide-containing skin care ointment reduced IL-31 induced impairments of the physical skin barrier and skin barrier function in an in vitro model of the disrupted skin barrier. This standardized model can be utilized in the future to monitor ex vivo effects of various topical therapies on skin morphology, physiology, and gene expression.
机译:特应性皮炎(AD)是一种慢性复发,具有干燥和干扰的皮肤屏障功能的皮肤瘙痒炎症。最近,我们建立了IL-31对人体31皮肤模型的治疗导致了类似广告的皮肤屏障表型。在该模型中,我们发现IL-31干扰了角质形成细胞的分化并抑制末端分化标志物的表达。在本研究中,我们研究了含神经酰胺的水包裹物质软膏对物理皮肤屏障结构的影响,并通过使用初级正常人体表皮角蛋白酶(NHEK)或HACAT产生的皮肤屏障模型中断的功能细胞。我们观察到,用含氨酰胺的软膏后,模型的物理皮肤屏障在日常局部处理后恢复。通过免疫组织学分析证明,软膏的局部施用防止了叶片氟化蛋白和其他分化标志物的紊乱,例如角蛋白10和4-整联蛋白。 KI67的表达也响应于软膏而上调。此外,功能研究表明,软膏的局部施用减少了我们模型中莫托草(PHL P1)的荧光标记的重组过敏原的增加。总之,我们的数据显示,在破坏皮肤屏障的体外模型中,含有含神经酰胺的皮肤护理软膏的局部应用降低了IL-31诱导的物理皮肤屏障和皮肤屏障功能的损伤。该标准化模型可以在未来使用,以监测各种局部疗法对皮肤形态,生理学和基因表达的exvivo效应。

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