RIS-1/牛皮癣蛋白在皮肤上皮细胞中的表达表明其在先天免疫和包括痤疮在内的炎症性皮肤病中的选择性作用。

Dermato-Endocrinology Pub Date : 2017-10-04 eCollection Date: 2017-01-01 DOI:10.1080/19381980.2017.1338993
Christos C Zouboulis, Claudia Beutler, Hans F Merk, Jens M Baron
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引用次数: 4

摘要

目的:RIS-1/psoriasin/S100A7是一种上皮抗菌肽,在炎症性皮肤病中表达上调,受类维生素a诱导。在皮肤细胞培养和皮肤标本中研究了其分子表达,以更好地了解其在毛囊皮脂腺单位炎症过程中的作用。方法:在细胞培养(角质形成细胞、皮脂细胞、成纤维细胞、内皮细胞、黑素细胞、淋巴细胞和前列腺细胞)中进行RIS-1/牛皮癣蛋白和类维甲酸代谢基因CYP26AI、CRABP-II的rt - pcr和northern blotting;在正常和发炎的皮肤(痤疮,牛皮癣)进行原位杂交。结果:a) RIS-1/牛皮癣蛋白在体外角质形成细胞和成纤维细胞中表达,在体内颗粒层角质形成细胞中表达。体外的类维甲酸和体内的炎症条件会增加角质形成细胞(两者)、皮脂细胞(仅炎症)和成纤维细胞(类维甲酸)中RIS-1/牛皮癣蛋白的水平。皮脂细胞和成纤维细胞是代谢最活跃的皮肤细胞,因为它们可以上调负责类视黄醇代谢的基因CRABP-II和CYP26AI的表达。炎症改变了皮脂腺和毛囊根鞘中RIS-1/银屑病蛋白的区隔。结论:目前的数据表明,针对皮肤上皮区室的抗炎治疗,包括抗菌肽,可能是治疗炎症性皮肤病的有希望的方法。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

RIS-1/psoriasin expression in epithelial skin cells indicates their selective role in innate immunity and in inflammatory skin diseases including acne.

RIS-1/psoriasin expression in epithelial skin cells indicates their selective role in innate immunity and in inflammatory skin diseases including acne.

RIS-1/psoriasin expression in epithelial skin cells indicates their selective role in innate immunity and in inflammatory skin diseases including acne.

RIS-1/psoriasin expression in epithelial skin cells indicates their selective role in innate immunity and in inflammatory skin diseases including acne.

Objective: RIS-1/psoriasin/S100A7 is an epithelial antimicrobial peptide, whose expression is upregulated in inflammatory skin diseases and is induced by retinoids. Its molecular expression was investigated in skin cell cultures and in skin specimens to better understand its role in inflammatory procedures of the pilosebaceous unit.

Methods: rtPCR and northern blotting of RIS-1/psoriasin and the retinoid-metabolizing genes CYP26AI and CRABP-II were performed in cells cultures (keratinocytes, sebocytes, fibroblasts, endothelial cells, melanocytes, lymphocytes and prostate cells; native and treated with retinoids) and in situ hybridization in normal and inflamed skin (acne, psoriasis).

Results: a) RIS-1/psoriasin is expressed in keratinocytes and fibroblasts in vitro and in keratinocytes of the stratum granulosum in vivo. Retinoids in vitro and inflammatory conditions in vivo increase the levels of RIS-1/psoriasin in keratinocytes (both), sebocytes (inflammation only) and fibroblasts (retinoids). Sebocytes and fibroblasts are the metabolically most active skin cells, since they can upregulate the expression of CRABP-II and CYP26AI, genes responsible for retinoid metabolism. Inflammation modifies the compartmentation of RIS-1/psoriasin in sebaceous glands and the follicular root sheaths.

Conclusion: The present data indicate that anti-inflammatory treatment targeting the epithelial compartments of the skin, including such with antibacterial peptides, may be promising for inflammatory skin diseases.

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