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Chemokines and their receptors in allergic disease.过敏性疾病中的趋化因子及其受体
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CD127 expression inversely correlates with FoxP3 and suppressive function of human CD4+ T reg cells.CD127的表达与人类CD4+调节性T细胞的FoxP3及抑制功能呈负相关。
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Expression of interleukin (IL)-2 and IL-7 receptors discriminates between human regulatory and activated T cells.白细胞介素(IL)-2和IL-7受体的表达可区分人类调节性T细胞和活化T细胞。
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Recruitment of Foxp3+ T regulatory cells mediating allograft tolerance depends on the CCR4 chemokine receptor.介导同种异体移植耐受的Foxp3+调节性T细胞的募集依赖于CCR4趋化因子受体。
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来自特应性和非特应性供体的CD4+ CD25+调节性T细胞和CD4+ CD25-T细胞的趋化因子反应性。

Chemokine responsiveness of CD4+ CD25+ regulatory and CD4+ CD25- T cells from atopic and nonatopic donors.

作者信息

Ahern D, Lloyd C M, Robinson D S

机构信息

Leukocyte Biology Section, National Heart and Lung Institute, Imperial College London, London, UK.

出版信息

Allergy. 2009 Aug;64(8):1121-9. doi: 10.1111/j.1398-9995.2008.01962.x. Epub 2009 Feb 7.

DOI:10.1111/j.1398-9995.2008.01962.x
PMID:19208087
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3807784/
Abstract

BACKGROUND

Allergic inflammation is associated with Th2-type T cells, which can be suppressed by CD4+ CD25+ regulatory T cells (Tregs). Both express chemokine receptors (CCR) 4 and CCR8, but the dynamics of expression and effect of atopic status are unknown.

OBJECTIVE

To examine the expression of chemokine receptors by CD4+ CD25+ and CD4+ CD25- T cells from atopic and nonatopic donors, and document response to allergen stimulation in vitro.

METHODS

Chemokine receptor expression was examined by flow cytometry and quantitative PCR of CD4+ CD25hi and CD4+ CD25- T cells from atopics and nonatopics. Responsiveness to chemokines was by actin polymerization. Dynamics of chemokine receptor expression in 6-day allergen-stimulated cultures was analysed by carboxyfluoroscein succinimidyl ester labelling.

RESULTS

CD4+ CD25hi Tregs preferentially expressed CCR3, CCR4, CCR5, CCR6 and CCR8. CD4+ CD25hi Tregs responded to the chemokine ligands for CCR4, CCR6 and CCR8 (CCL17, 22, 20 and 1 respectively), with no differences between atopic and nonatopic donors. Over 6-day allergen stimulation, CD4+ CD25+ T-cells downregulated CCR4 and upregulated CCR7, in contrast to CD4+ CD25- effector cells, which downregulated CCR7 and upregulated CCR4.

CONCLUSIONS

CCR4, CCR6 and CCR8 have potential roles in localization of both CD4+ CD25+ regulatory and CD4+ CD25- effector T cells to sites of allergic inflammation. Upregulation of CCR7 and downregulation of CCR4 upon allergen stimulation of Tregs may allow their recirculation from sites of inflammation, in contrast to retention of effector T cells.

摘要

背景

过敏性炎症与Th2型T细胞相关,而CD4+CD25+调节性T细胞(Tregs)可抑制Th2型T细胞。二者均表达趋化因子受体(CCR)4和CCR8,但特应性状态下其表达动态及作用尚不清楚。

目的

检测来自特应性和非特应性供体的CD4+CD25+和CD4+CD25-T细胞趋化因子受体的表达,并记录体外对变应原刺激的反应。

方法

采用流式细胞术和定量PCR检测特应性和非特应性个体CD4+CD25hi和CD4+CD25-T细胞趋化因子受体的表达。通过肌动蛋白聚合反应检测对趋化因子的反应性。采用羧基荧光素琥珀酰亚胺酯标记分析变应原刺激6天的培养物中趋化因子受体表达的动态变化。

结果

CD4+CD25hi Tregs优先表达CCR3、CCR4、CCR5、CCR6和CCR8。CD4+CD25hi Tregs对CCR4、CCR6和CCR8的趋化因子配体(分别为CCL17、22、20和1)产生反应,特应性和非特应性供体之间无差异。在6天的变应原刺激过程中,与CD4+CD25-效应细胞下调CCR7并上调CCR4相反,CD4+CD25+T细胞下调CCR4并上调CCR7。

结论

CCR4、CCR6和CCR8在CD4+CD25+调节性T细胞和CD4+CD25-效应性T细胞向过敏性炎症部位的定位中具有潜在作用。与效应性T细胞的滞留相反,变应原刺激Tregs后CCR7上调和CCR4下调可能使其从炎症部位再循环。