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环孢素A可抑制愈合期银屑病斑块乳头层内皮细胞的细胞间黏附分子-1表达。

Cyclosporin A suppresses ICAM-1 expression by papillary endothelium in healing psoriatic plaques.

作者信息

Petzelbauer P, Stingl G, Wolff K, Volc-Platzer B

机构信息

Department of Dermatology I, University of Vienna Medical School, Austria.

出版信息

J Invest Dermatol. 1991 Mar;96(3):362-9. doi: 10.1111/1523-1747.ep12465404.

Abstract

To analyze the mode of action of Cyclosporin A (CsA) in psoriasis, we examined the phenotypic profile of resident and passenger skin cells in seven psoriatic patients before and after 2 weeks of CsA treatment using a large panel of monoclonal antibodies in a three-step immunoperoxidase technique. For comparison, skin biopsies from psoriatic patients receiving psoralen + UVA (PUVA) therapy were examined. Although both treatment protocols were equally effective in inducing resolution of psoriatic lesions, the phenotypic changes induced by CsA differed greatly from those seen after PUVA. In CsA-treated patients there was a dramatic reduction in the ICAM-1 expression by papillary endothelial cells, but density, pattern, and phenotype of infiltrating inflammatory cells remained essentially unchanged. In contrast, PUVA therapy had no visible effect on ICAM-1 expression by papillary endothelial cells, but resulted in a significant reduction of the hemopoietic resident and infiltrating mononuclear cells within the epidermis. These results favor, but do not prove, the assumption that the CsA regimen chosen in this study exerts its anti-psoriatic effect primarily at the level of the keratinocyte, i.e., by inhibiting events leading to keratinocyte proliferation as well as by interfering with the secretion of mediators responsible for ICAM-1 expression by papillary endothelial cells.

摘要

为分析环孢素A(CsA)治疗银屑病的作用方式,我们运用一大组单克隆抗体,采用三步免疫过氧化物酶技术,检测了7例银屑病患者在CsA治疗2周前后常驻及过客皮肤细胞的表型特征。作为对照,我们检测了接受补骨脂素+紫外线A(PUVA)治疗的银屑病患者的皮肤活检样本。尽管两种治疗方案在诱导银屑病皮损消退方面同样有效,但CsA诱导的表型变化与PUVA治疗后的变化有很大差异。在接受CsA治疗的患者中,乳头内皮细胞ICAM - 1表达显著降低,但浸润性炎症细胞的密度、模式及表型基本保持不变。相比之下,PUVA治疗对乳头内皮细胞ICAM - 1表达无明显影响,但导致表皮内造血常驻细胞及浸润单核细胞显著减少。这些结果支持但未证实本研究中选用的CsA治疗方案主要在角质形成细胞水平发挥抗银屑病作用这一假设,即通过抑制导致角质形成细胞增殖的事件以及干扰负责乳头内皮细胞ICAM - 1表达的介质的分泌来发挥作用。

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