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人肺和骨髓源性肥大细胞中CCR3和CXCR3的差异表达:对组织肥大细胞迁移的影响

Differential expression of CCR3 and CXCR3 by human lung and bone marrow-derived mast cells: implications for tissue mast cell migration.

作者信息

Brightling Christopher E, Kaur Davinder, Berger Patrick, Morgan Angela J, Wardlaw Andrew J, Bradding Peter

机构信息

Institute for Lung Health, Department of Infection, Immunity and Inflammation, Leicester-Warwick Medical School and University Hospitals of Leicester, Groby Road, Leicester, LE3 9QP, UK.

出版信息

J Leukoc Biol. 2005 May;77(5):759-66. doi: 10.1189/jlb.0904511. Epub 2005 Jan 26.

DOI:10.1189/jlb.0904511
PMID:15673545
Abstract

The selective microlocalization of mast cells within specific airway structures, such as the airway smooth muscle and submucosal glands, in asthma is important in the pathophysiology of inflammatory lung disease. Chemokines are likely candidates mediating mast cell migration into these tissue compartments. In this study, we have defined the chemokine receptor profile of human lung mast cells (HLMC) compared with mast cells derived from human bone marrow (BM) and the human mast cell line HMC-1. CXC chemokine receptor 3 (CXCR3) was the most highly expressed chemokine receptor on ex vivo HLMC analyzed by flow cytometry, and CXCR3 expression by mast cells in the bronchial mucosa was confirmed by immuno-histochemistry. CXCR3 was functional, inducing a rise in cytosolic-free Ca2+, actin reorganization, and chemotaxis in response to the CXC ligands CXCL9, -10, and -11. CXCR3 activation did not induce degranulation or cytokine synthesis. In addition, more than 10% of ex vivo HLMC expressed CC chemokine receptor 3, CXCR1, and CXCR4. It is interesting that CXCR3 was not expressed by human BM-derived mast cells, suggesting its expression is induced during tissue maturation. As CXCR3 ligands are elevated in many pulmonary diseases, CXCR3 may be important for determining the anatomical microlocalization of mast cells within the human lung.

摘要

肥大细胞在特定气道结构(如气道平滑肌和黏膜下腺)中的选择性微定位在哮喘中对炎症性肺病的病理生理学很重要。趋化因子可能是介导肥大细胞迁移至这些组织区域的候选因子。在本研究中,我们已确定了人肺肥大细胞(HLMC)与源自人骨髓(BM)的肥大细胞及人肥大细胞系HMC-1相比的趋化因子受体谱。通过流式细胞术分析,CXC趋化因子受体3(CXCR3)是离体HLMC上表达最高的趋化因子受体,并且通过免疫组织化学证实了支气管黏膜中肥大细胞的CXCR3表达。CXCR3具有功能,可诱导胞质游离Ca²⁺升高、肌动蛋白重组以及对CXC配体CXCL9、-10和-11产生趋化作用。CXCR3激活不会诱导脱颗粒或细胞因子合成。此外,超过10%的离体HLMC表达CC趋化因子受体3、CXCR1和CXCR4。有趣的是,人BM来源的肥大细胞不表达CXCR3,这表明其表达是在组织成熟过程中诱导产生的。由于CXCR3配体在许多肺部疾病中升高,CXCR3可能对确定人肺内肥大细胞的解剖学微定位很重要。

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