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体外模拟的免疫监视:初始T细胞和记忆T细胞可自发穿过未受刺激的微血管内皮。

Immunosurveillance modelled in vitro: naive and memory T cells spontaneously migrate across unstimulated microvascular endothelium.

作者信息

Röhnelt R K, Hoch G, Reiss Y, Engelhardt B

机构信息

Max-Planck-Institut für physiologische, Abt. Molekulare Zellbiologie, Bad Nauheim, Germany.

出版信息

Int Immunol. 1997 Mar;9(3):435-50. doi: 10.1093/intimm/9.3.435.

DOI:10.1093/intimm/9.3.435
PMID:9088982
Abstract

As a model for T cell immigration into non-lymphoid tissue we set up an in vitro assay that would allow us to investigate the phenotype of T lymphocytes from peripheral lymph nodes (PLN), mesenteric lymph nodes (MLN) or peripheral blood (PBL) of mice, which were able to spontaneously migrate across unstimulated microvascular endothelium. The transendothelial migrating T cell population was enriched for T lymphocytes expressing a "recently activated/memory' phenotype: LFA-1/CD44/ICAM-1high, but also contained CD45RBhigh and LFA-1low T cells, which in the case of MLN T cells were phenotyped as CD4+ and thus characterized as naive T cells. Transmigrated T cells could be further distinguished from their original populations and from each other by their distinct but heterogeneous expression patterns for L-selectin, alpha 4 beta 7-integrin and PECAM-1. This observation suggests the presence of phenotypically different migratory T cells among MLN, PLN and PBL. Additional studies provided evidence that the capacity to migrate across unstimulated microvascular endothelium was a characteristic of a T cell population that could phenotypically be differentiated from activated T cells. The endothelial cells were found to play an active role in selecting the traversing T cell population, as they controlled the number and phenotype of spontaneously transmigrating T cells. Our studies suggest that the capacity to transmigrate across unstimulated microvascular endothelium and hence to immigrate into non-lymphoid tissue is owned by a phenotypically heterogeneous T cell population, which is enriched for memory T cells but not devoid of naive T cells.

摘要

作为T细胞迁移至非淋巴组织的模型,我们建立了一种体外试验,该试验使我们能够研究来自小鼠外周淋巴结(PLN)、肠系膜淋巴结(MLN)或外周血(PBL)的T淋巴细胞的表型,这些T淋巴细胞能够自发迁移穿过未受刺激的微血管内皮。经内皮迁移的T细胞群体富含表达“近期活化/记忆”表型的T淋巴细胞:LFA-1/CD44/ICAM-1高表达,但也包含CD45RB高表达和LFA-1低表达的T细胞,就MLN T细胞而言,其表型为CD4+,因此被表征为初始T细胞。迁移的T细胞可通过其L-选择素、α4β7整合素和PECAM-1的独特但异质性表达模式,与它们的原始群体以及彼此进一步区分开来。这一观察结果表明,在MLN、PLN和PBL中存在表型不同的迁移性T细胞。进一步的研究提供了证据,表明穿过未受刺激的微血管内皮的迁移能力是一个T细胞群体的特征,该群体在表型上可与活化T细胞区分开来。发现内皮细胞在选择穿越的T细胞群体中发挥积极作用,因为它们控制着自发迁移的T细胞的数量和表型。我们的研究表明,穿过未受刺激的微血管内皮并因此迁移至非淋巴组织的能力为一个表型异质性的T细胞群体所具有,该群体富含记忆T细胞,但也并非没有初始T细胞。

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