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吡美莫司对特应性皮炎皮损中与皮肤屏障功能障碍相关基因表达的影响。

The effect of pimecrolimus on expression of genes associated with skin barrier dysfunction in atopic dermatitis skin lesions.

机构信息

Clinical Department of Internal Diseases, Dermatology and Allergology in Zabrze, Medical University of Silesia, Katowice, Poland.

出版信息

Exp Dermatol. 2012 Mar;21(3):184-8. doi: 10.1111/j.1600-0625.2011.01417.x. Epub 2011 Dec 6.

Abstract

The mechanism of action of pimecrolimus (PIM) on atopic lesions is still under consideration. Thus far, we have evidence of its anti-inflammatory and immunomodulatory activity, and recent papers focus on its effect on epidermal barrier function. This study analysed changes in the expression of genes associated with skin barrier dysfunction in atopic dermatitis (AD) skin lesions after 2 weeks of exposure to PIM 1% cream. A real-time quantitative PCR analysis of selected epidermal differentiation complex genes and three alternative pathway keratins was performed in skin biopsies from 11 individuals with AD before and after PIM exposure. The real-time quantitative PCR analysis was compared to non-lesional skin in the same patients. Involucrin, a small proline-rich region (SPRR) 2C gene, and alternative pathway keratin 16 showed significant over-expression in lesional skin followed by significant decrease after PIM therapy. The SPRR1A gene, S100A9, and keratin 6A were also increased; however, the decrease after PIM treatment was not significant. The changes in S100 A2, A7 and A8 followed a similar course with borderline significance. SPRR4 had a significant decrease in expression in lesional versus non-lesional skin, which persisted after PIM treatment. No significant changes were detected in mRNA expression levels of filaggrin and loricrin. Our results suggest that PIM can be effective in restoring the epidermal barrier in patients with AD at least in part by its impact on expression of genes, which are important for the normal barrier function of skin.

摘要

吡美莫司(PIM)在特应性皮炎病变中的作用机制仍在研究中。迄今为止,我们已经有证据表明其具有抗炎和免疫调节活性,并且最近的论文集中在其对表皮屏障功能的影响上。本研究分析了在特应性皮炎(AD)皮损中暴露于 PIM 1%乳膏 2 周后与皮肤屏障功能障碍相关的基因表达变化。对 11 例 AD 患者皮损和非皮损皮肤活检标本进行表皮分化复合物基因和三种替代途径角蛋白的实时定量 PCR 分析。将实时定量 PCR 分析与同一患者的非皮损皮肤进行比较。富含脯氨酸的小区域(SPRR)2C 基因 involucrin 和替代途径角蛋白 16 在病变皮肤中表达显著增加,然后在 PIM 治疗后显著减少。SPRR1A 基因、S100A9 和角蛋白 6A 也增加;然而,PIM 治疗后的减少并不显著。S100A2、A7 和 A8 的变化也具有类似的趋势,但具有边缘显著性。与非皮损皮肤相比,SPRR4 在皮损中的表达显著降低,PIM 治疗后仍持续存在。丝聚蛋白和兜甲蛋白的 mRNA 表达水平没有检测到显著变化。我们的结果表明,PIM 至少部分通过其对基因表达的影响,可以有效恢复 AD 患者的表皮屏障,这些基因对皮肤的正常屏障功能很重要。

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