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人类次级淋巴器官基质的CCL21表达模式在伴有淋巴新生的炎症病变中是保守的。

CCL21 expression pattern of human secondary lymphoid organ stroma is conserved in inflammatory lesions with lymphoid neogenesis.

作者信息

Manzo Antonio, Bugatti Serena, Caporali Roberto, Prevo Remko, Jackson David G, Uguccioni Mariagrazia, Buckley Christopher D, Montecucco Carlomaurizio, Pitzalis Costantino

机构信息

Rheumatology Unit, Guy's, King's, and St. Thomas' School of Medicine, London, United Kingdom.

出版信息

Am J Pathol. 2007 Nov;171(5):1549-62. doi: 10.2353/ajpath.2007.061275.

DOI:10.2353/ajpath.2007.061275
PMID:17982129
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2043516/
Abstract

CCL21 is a homeostatic lymphoid chemokine instrumental in the recruitment and organization of T cells and dendritic cells into lymphoid T areas. In human secondary lymphoid organs (SLOs), CCL21 is produced by cells distributed throughout the T zone, whereas high endothelial venules (HEVs) lack CCL21 mRNA. A critical question remains whether the development of ectopic lymphoid tissue (ELT) in chronic inflammation recapitulates the features of SLOs. Thus, we systematically investigated in situ the cellular sources of CCL21 in SLOs and ELTs in several human diseases characterized by lymphoid neogenesis. By in situ hybridization and the use of combinatorial cell markers, we show that CCL21-producing vessels in inflamed tissues systematically display typical markers of lymphatic vessels, whereas, as in SLOs, ectopic HEVs do not synthesize detectable levels of CCL21. We also provide first-time evidence that a common pattern of CCL21 expression by CD45-negative myofibroblast-like cells localized in extra-HEV position and organized in a fibroblastic reticular network similarly characterizes human SLOs and organized ELTs. Altogether, our results demonstrate that in humans the pattern of CCL21 production in SLOs is maintained during inflammation and that the phenotypic and functional properties of stromal cells, found in SLO T-cell areas, are reproduced at ectopic sites.

摘要

CCL21是一种稳态淋巴细胞趋化因子,对T细胞和树突状细胞募集至淋巴T区并在其中组织排列起着重要作用。在人类二级淋巴器官(SLO)中,CCL21由分布于整个T区的细胞产生,而高内皮微静脉(HEV)缺乏CCL21 mRNA。一个关键问题仍然存在,即慢性炎症中异位淋巴组织(ELT)的发育是否重现了SLO的特征。因此,我们系统地原位研究了几种以淋巴新生为特征的人类疾病中SLO和ELT内CCL21的细胞来源。通过原位杂交和使用组合细胞标记物,我们发现炎症组织中产生CCL21的血管系统地显示出淋巴管的典型标记物,而与SLO一样,异位HEV不合成可检测水平的CCL21。我们还首次提供证据表明,位于HEV外位置并组织成成纤维细胞网状网络的CD45阴性肌成纤维细胞样细胞表达CCL21的常见模式同样是人类SLO和有组织的ELT的特征。总之,我们的结果表明,在人类中,SLO中CCL21的产生模式在炎症期间得以维持,并且在SLO T细胞区发现的基质细胞的表型和功能特性在异位部位得以重现。

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