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CC趋化因子配体18,一种与特应性皮炎相关且由树突状细胞产生的趋化因子,受葡萄球菌产物和过敏原暴露的调节。

CC chemokine ligand 18, an atopic dermatitis-associated and dendritic cell-derived chemokine, is regulated by staphylococcal products and allergen exposure.

作者信息

Pivarcsi Andor, Gombert Michael, Dieu-Nosjean Marie-Caroline, Lauerma Antti, Kubitza Robert, Meller Stephan, Rieker Juliane, Muller Anja, Da Cunha Ludivine, Haahtela Anna, Sonkoly Eniko, Fridman Wolf-Herman, Alenius Harri, Kemeny Lajos, Ruzicka Thomas, Zlotnik Albert, Homey Bernhard

机构信息

Department of Dermatology, Heinrich-Heine-University, Düsseldorf, Germany.

出版信息

J Immunol. 2004 Nov 1;173(9):5810-7. doi: 10.4049/jimmunol.173.9.5810.

Abstract

Atopic dermatitis is a chronic inflammatory skin disease with a steadily increasing prevalence. Exposure to allergens or bacterial superantigens triggers T and dendritic cell (DC) recruitment and induces atopic skin inflammation. In this study, we report that among all known chemokines CCL18/DC-CK1/PARC represents the most highly expressed ligand in atopic dermatitis. Moreover, CCL18 expression is associated with an atopic dermatitis phenotype when compared with other chronic inflammatory skin diseases. DCs either dispersed within the dermis or clustering at sites showing perivascular infiltrates are abundant sources of CCL18. In vitro, microbial products including LPS, peptidoglycan, and mannan, as well as the T cell-derived activation signal CD40L, induced CCL18 in monocytes. In contrast to monocytes, monocyte-derived, interstitial-type, and Langerhans-type DCs showed a constitutive and abundant expression of CCL18. In comparison to Langerhans cells, interstitial-type DCs produced higher constitutive levels of CCL18. In vivo, topical exposure to the relevant allergen or the superantigen staphylococcal enterotoxin B, resulted in a significant induction of CCL18 in atopic dermatitis patients. Furthermore, in nonatopic NiSO4-sensitized individuals, only relevant allergen but not irritant exposure resulted in the induction of CCL18. Taken together, findings of the present study demonstrate that CCL18 is associated with an atopy/allergy skin phenotype, and is expressed at the interface between the environment and the host by cells constantly screening foreign Ags. Its regulation by allergen exposure and microbial products suggests an important role for CCL18 in the initiation and amplification of atopic skin inflammation.

摘要

特应性皮炎是一种患病率持续上升的慢性炎症性皮肤病。接触过敏原或细菌超抗原会引发T细胞和树突状细胞(DC)募集,并诱发特应性皮肤炎症。在本研究中,我们报告在所有已知趋化因子中,CCL18/DC-CK1/PARC是特应性皮炎中表达最高的配体。此外,与其他慢性炎症性皮肤病相比,CCL18的表达与特应性皮炎表型相关。分散在真皮内或聚集在血管周围浸润部位的DC是CCL18的丰富来源。在体外,包括脂多糖、肽聚糖和甘露聚糖在内的微生物产物,以及T细胞衍生的激活信号CD40L,可诱导单核细胞产生CCL18。与单核细胞不同,单核细胞衍生的间质型和朗格汉斯型DC显示出CCL18的组成性高表达。与朗格汉斯细胞相比,间质型DC产生的CCL18组成性水平更高。在体内,特应性皮炎患者局部暴露于相关过敏原或超抗原金黄色葡萄球菌肠毒素B后,CCL18会显著诱导。此外,在非特应性硫酸镍致敏个体中,只有相关过敏原暴露而非刺激性暴露会诱导CCL18产生。综上所述,本研究结果表明CCL18与特应性/过敏性皮肤表型相关,并且在不断筛选外来抗原的细胞中,于环境与宿主的界面处表达。其受过敏原暴露和微生物产物的调节表明CCL18在特应性皮肤炎症的起始和放大中起重要作用。

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