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人淋巴结与慢性炎症皮肤中DC-Lamp+成熟树突状细胞CCL19的差异表达。

Differential expression of CCL19 by DC-Lamp+ mature dendritic cells in human lymph node versus chronically inflamed skin.

作者信息

Katou Fuminori, Ohtani Haruo, Nakayama Takashi, Nagura Hiroshi, Yoshie Osamu, Motegi Katsutoshi

机构信息

Department of Oral and Maxillofacial Surgery I, Tohoku University School of Dentistry, Sendai, Japan.

出版信息

J Pathol. 2003 Jan;199(1):98-106. doi: 10.1002/path.1255.

Abstract

De novo formation of lymphoid tissue is one of the characteristic features of chronic inflammation. The formation of T cell-mature dendritic cell (DC) clusters has been previously demonstrated in chronically inflamed skin infected with Candida albicans. A functional similarity was also found between chronic inflammation and the T-cell zone of lymph nodes (LNs), since a substantial fraction of phenotypically mature DCs in both tissues expressed CCL22 (macrophage-derived chemokine; MDC) and were closely surrounded by memory-type T cells expressing its receptor, CCR4. To analyse the nature of T cell-mature DC interactions further in chronically inflamed skin and LNs, the present study focuses on another chemokine system, namely CCL19 (EBI1 ligand chemokine; ELC), CCL21 (secondary lymphoid tissue chemokine; SLC) and their shared receptor, CCR7. RT-PCR analysis revealed expression of CCL19, CCL21, and CCR7 at high levels in LNs and at low levels in inflamed skin. Using immunohistochemistry, the majority of DC-Lamp(+) mature DCs in the T-cell area of LNs expressed CCL19 and were surrounded by CCR7(+) naïve-type lymphocytes, while CCL21 was expressed in reticular stromal cells and vascular endothelial cells. Very few mature DCs in LNs were found to express CCR7. In contrast, the majority of DC-Lamp(+) mature DCs in inflamed skin were totally negative for CCL19 and were surrounded by CCR7(-) memory-type T cells. Furthermore, CCL21 expression in the inflamed skin was detected in dermal lymphatic endothelial cells and rare CCR7(+) mature DCs were mostly seen within the lymphatic vessels. In normal skin, on the other hand, no cells immunoreactive for CCL19, CCL21, or CCR7 were found. The present study thus reveals a striking difference in the function of mature DCs between LNs and chronically inflamed skin.

摘要

淋巴组织的从头形成是慢性炎症的特征之一。先前已证实在感染白色念珠菌的慢性炎症皮肤中会形成T细胞-成熟树突状细胞(DC)簇。慢性炎症与淋巴结(LN)的T细胞区之间也发现了功能相似性,因为这两种组织中相当一部分表型成熟的DC表达CCL22(巨噬细胞衍生趋化因子;MDC),并被表达其受体CCR4的记忆型T细胞紧密包围。为了进一步分析慢性炎症皮肤和LN中T细胞与成熟DC相互作用的性质,本研究聚焦于另一个趋化因子系统,即CCL19(EBI1配体趋化因子;ELC)、CCL21(次级淋巴组织趋化因子;SLC)及其共同受体CCR7。逆转录聚合酶链反应(RT-PCR)分析显示,CCL19、CCL21和CCR7在LN中高表达,在炎症皮肤中低表达。利用免疫组织化学方法,LN的T细胞区中大多数DC-Lamp(+)成熟DC表达CCL19,并被CCR7(+)幼稚型淋巴细胞包围,而CCL21在网状基质细胞和血管内皮细胞中表达。在LN中发现很少有成熟DC表达CCR7。相反,炎症皮肤中大多数DC-Lamp(+)成熟DC对CCL19完全阴性,并被CCR7(-)记忆型T细胞包围。此外,在炎症皮肤的真皮淋巴管内皮细胞中检测到CCL21表达,并且很少有CCR7(+)成熟DC主要见于淋巴管内。另一方面,在正常皮肤中,未发现对CCL19、CCL21或CCR7呈免疫反应性的细胞。因此,本研究揭示了LN和慢性炎症皮肤中成熟DC功能的显著差异。

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