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T细胞的过继转移可独立于气道嗜酸性粒细胞增多而诱导气道高反应性,但以信号转导及转录激活因子6依赖的方式进行。

Adoptive transfer of T cells induces airway hyperresponsiveness independently of airway eosinophilia but in a signal transducer and activator of transcription 6-dependent manner.

作者信息

Tomkinson Adrian, Duez Catherine, Lahn Michael, Gelfand Erwin W

机构信息

Division of Cell Biology, the Department of Pediatrics, National Jewish Medical and Research Center, Denver, Colo 80206, USA.

出版信息

J Allergy Clin Immunol. 2002 May;109(5):810-6. doi: 10.1067/mai.2002.123531.

DOI:10.1067/mai.2002.123531
PMID:11994705
Abstract

BACKGROUND

Activated T cells, through the release of specific cytokines (ie, IL-4, IL-5, and IL-13), regulate effector cell recruitment and function. In this way T cells orchestrate the inflammatory response, which leads to airway hyperresponsiveness (AHR), a cardinal feature of allergic asthma.

OBJECTIVE

In the present study the direct role of T cells and, in particular, the importance of signal transducer and activator of transcription 6 (STAT6) in T cells was investigated in the development of AHR.

METHODS

In a murine model of allergen-driven AHR, the effects of adoptive transfer of STAT6-containing (STAT6+/+) and STAT6-deficient (STAT6-/-) T cells from sensitized mice into allergen-challenged mice were tested.

RESULTS

Although greater in STAT6+/+ mice, both allergen-challenged STAT6+/+ and STAT6-/- mice had AHR after transfer of T cells from sensitized STAT6+/+ mice. In contrast, AHR did not develop in allergen-challenged STAT6-/- mice after transfer of T cells from sensitized STAT6-/- mice. Reconstitution of AHR after T-cell transfer was not associated with airway eosinophilia.

CONCLUSIONS

The data indicate that the STAT6 status of the donor mice is critical to the development of AHR. Although not critical for the development of AHR, the STAT6 status of the recipient mice might play a contributory-regulatory role in the AHR response. The results identify a STAT6-dependent T-cell pathway capable of modulating airway responsiveness, even in the absence of a significant airway eosinophilia.

摘要

背景

活化的T细胞通过释放特定细胞因子(即白细胞介素-4、白细胞介素-5和白细胞介素-13)来调节效应细胞的募集和功能。通过这种方式,T细胞协调炎症反应,进而导致气道高反应性(AHR),这是过敏性哮喘的一个主要特征。

目的

在本研究中,探讨了T细胞的直接作用,特别是信号转导和转录激活因子6(STAT6)在T细胞中的重要性对气道高反应性发展的影响。

方法

在变应原驱动的气道高反应性小鼠模型中,测试了将致敏小鼠中含STAT6(STAT6+/+)和缺乏STAT6(STAT6-/-)的T细胞过继转移到变应原激发小鼠中的效果。

结果

虽然在STAT6+/+小鼠中更为明显,但在从致敏的STAT6+/+小鼠转移T细胞后,变应原激发的STAT6+/+和STAT6-/-小鼠均出现气道高反应性。相比之下,在从致敏的STAT6-/-小鼠转移T细胞后,变应原激发的STAT6-/-小鼠未出现气道高反应性。T细胞转移后气道高反应性的重建与气道嗜酸性粒细胞增多无关。

结论

数据表明供体小鼠的STAT6状态对气道高反应性的发展至关重要。虽然对气道高反应性的发展并非至关重要,但受体小鼠的STAT6状态可能在气道高反应性反应中发挥辅助调节作用。结果确定了一条依赖STAT6的T细胞途径,即使在没有明显气道嗜酸性粒细胞增多的情况下,该途径也能够调节气道反应性。

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