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克罗恩病中外周血单核细胞和初始T细胞的募集与激活

Peripheral monocyte and naive T-cell recruitment and activation in Crohn's disease.

作者信息

Burgio V L, Fais S, Boirivant M, Perrone A, Pallone F

机构信息

Istituti di Clinica Medica 1, Università La Sapienza, Rome, Italy.

出版信息

Gastroenterology. 1995 Oct;109(4):1029-38. doi: 10.1016/0016-5085(95)90560-x.

DOI:10.1016/0016-5085(95)90560-x
PMID:7557067
Abstract

BACKGROUND & AIMS: Transmural perivascular mononuclear cell infiltrates are a feature of Crohn's disease. The aim of this study was a molecular characterization of the mechanisms leading to the formation of these infiltrates.

METHODS

Endothelial cell and leukocyte expression of the adhesion molecules directing leukocyte transendothelial migration were studied in situ by immunohistochemical analysis of 10 samples from patients with Crohn's disease and 10 samples from normal controls. Double-staining methods were used to characterize the cells forming the infiltrates.

RESULTS

CD11a+ and L-selectin-positive mononuclear cells seemed to be the major component of perivascular infiltrates. The vast majority of these cells were CD68+, CD31+ monocytes/macrophages surrounded by CD3+, L-selectin-positive, CD31+, CD45RA+, and/or CD45RO+ T lymphocytes. T lymphocytes within the vessels expressed both CD45RA and CD45RO markers. Endothelial cells were intercellular adhesion molecule 1 positive and mostly CD34+. Strong adhesion between L-selectin-positive and CD11a+ intravascular mononuclear cells and CD34+ and intercellular adhesion molecule 1-positive endothelial cells were observed.

CONCLUSIONS

Data indicate that peripheral mononuclear cells are actively recruited in the submucosa of Crohn's disease tissue; endothelial cells express adhesion molecules highly permissive for transendothelial migration of monocytes and both naive and memory T cells contributing to infiltrates generation; and close membrane contact between migrated macrophages and naive T cells leads to the T-cell transition from naive to memory phenotype within Crohn's disease.

摘要

背景与目的

透壁性血管周围单核细胞浸润是克罗恩病的一个特征。本研究的目的是对导致这些浸润形成的机制进行分子特征分析。

方法

通过对10例克罗恩病患者的样本和10例正常对照的样本进行免疫组织化学分析,原位研究指导白细胞跨内皮迁移的黏附分子在内皮细胞和白细胞中的表达。采用双重染色方法对形成浸润的细胞进行特征分析。

结果

CD11a+和L-选择素阳性单核细胞似乎是血管周围浸润的主要成分。这些细胞绝大多数是CD68+、CD31+单核细胞/巨噬细胞,周围是CD3+、L-选择素阳性、CD31+、CD45RA+和/或CD45RO+ T淋巴细胞。血管内的T淋巴细胞同时表达CD45RA和CD45RO标记物。内皮细胞细胞间黏附分子1阳性,且大多为CD34+。观察到L-选择素阳性和CD11a+血管内单核细胞与CD34+和细胞间黏附分子1阳性内皮细胞之间有强烈黏附。

结论

数据表明,外周单核细胞被主动招募到克罗恩病组织的黏膜下层;内皮细胞表达对单核细胞以及有助于浸润形成的初始T细胞和记忆T细胞的跨内皮迁移高度允许的黏附分子;迁移的巨噬细胞与初始T细胞之间紧密的膜接触导致克罗恩病中T细胞从初始表型转变为记忆表型。

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