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银屑病中表皮白细胞介素-8受体表达增加。体外FK-506可使其下调。

Increased expression of epidermal IL-8 receptor in psoriasis. Down-regulation by FK-506 in vitro.

作者信息

Schulz B S, Michel G, Wagner S, Süss R, Beetz A, Peter R U, Kemény L, Ruzicka T

机构信息

Department of Dermatology, University of Munich, FRG.

出版信息

J Immunol. 1993 Oct 15;151(8):4399-406.

PMID:7691948
Abstract

IL-8 is a chemotactic cytokine with proinflammatory and growth-promoting activities. Recently it has been shown to influence several functions of keratinocytes, including HLA-DR expression, chemotaxis, and proliferation by binding to a specific receptor. Because psoriasis vulgaris is characterized by epidermal hyperproliferation and infiltration of inflammatory cells, we investigated the expression of IL-8 and its receptor in normal and psoriatic epidermis using semiquantitative reverse-transcriptase-polymerase chain reaction. In addition the mRNA levels of the proto-oncogenes c-ras, c-raf, c-myc, and HER-2 were also investigated as potential growth-promoting stimuli in psoriatic epidermis. IL-8 mRNA was only detected in lesional psoriatic epidermis, and IL-8R-specific mRNA was found to be 10 times increased in lesional psoriatic epidermis. There was no significant difference in the protooncogene mRNA levels. In order to test the relevance of the massively increased IL-8R levels in psoriatic epidermis, we investigated the effect of the antipsoriatic drug FK-506 on specific IL-8 and IL-8R mRNA expression. FK-506 dose dependently inhibited IL-8R expression and function. Our data suggest that in psoriatic skin, elevated IL-8 levels and markedly increased IL-8R expression may act in concert to induce the cardinal signs of psoriasis--epidermal hyperproliferation and leukocyte infiltration. IL-8R may prove a molecular target for antipsoriatic drugs such as FK-506.

摘要

白细胞介素-8是一种具有促炎和生长促进活性的趋化细胞因子。最近研究表明,它可通过与特定受体结合来影响角质形成细胞的多种功能,包括人类白细胞抗原-DR(HLA-DR)表达、趋化性和增殖。由于寻常型银屑病的特征是表皮过度增殖和炎性细胞浸润,我们采用半定量逆转录-聚合酶链反应研究了白细胞介素-8及其受体在正常和银屑病表皮中的表达。此外,还研究了原癌基因c-ras、c-raf、c-myc和HER-2的信使核糖核酸(mRNA)水平,将其作为银屑病表皮中潜在的生长促进刺激因素。白细胞介素-8 mRNA仅在银屑病皮损表皮中检测到,且白细胞介素-8受体特异性mRNA在银屑病皮损表皮中增加了10倍。原癌基因mRNA水平无显著差异。为了检验银屑病表皮中白细胞介素-8受体水平大量增加的相关性,我们研究了抗银屑病药物他克莫司(FK-506)对特异性白细胞介素-8和白细胞介素-8受体mRNA表达的影响。他克莫司剂量依赖性地抑制白细胞介素-8受体的表达和功能。我们的数据表明,在银屑病皮肤中,升高的白细胞介素-8水平和明显增加的白细胞介素-8受体表达可能共同作用,诱导银屑病的主要症状——表皮过度增殖和白细胞浸润。白细胞介素-8受体可能是他克莫司等抗银屑病药物的分子靶点。

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