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特应性哮喘:记忆性辅助性T细胞中的不同激活表型

Atopic asthma: differential activation phenotypes among memory T helper cells.

作者信息

Lara-Marquez M L, Moan M J, Cartwright S, Listman J, Israel E, Perkins D L, Christiani D C, Finn P W

机构信息

Respiratory Division, Brigham and Women's Hospital, Harvard Medical School, Boston, MA, USA.

出版信息

Clin Exp Allergy. 2001 Aug;31(8):1232-41. doi: 10.1046/j.1365-2222.2001.01146.x.

Abstract

BACKGROUND

T cells have been implicated in the pathogenesis of atopic asthma. We have previously shown that memory T helper cells (CD4+CD45RO+) are preferentially activated relative to naïve T helper cells (CD4+CD45RA+) after bronchial allergen challenge. However, specific T helper subpopulations that are activated in atopy and/or asthma remain undefined.

OBJECTIVE

To determine the T helper subpopulations and activation phenotypes relevant to acute and stable asthma that may be common with or distinct from atopy.

METHODS

Two groups of atopic asthmatics (ten acute and nine stable asthmatics) and two non-asthmatic groups (14 non-asthmatic atopics and eight normal non-atopic controls) were analysed. Ten acute asthmatics were assessed in the emergency room during an acute episode (FEV1 43.6% +/- 18.4). Nine stable asthmatics were assessed during a symptom-free period (FEV1 85% +/- 6). Using multiple colour flow cytometry we analysed T cell subpopulations and the expression of IL-2-receptor (IL-2R) and MHC-class II antigens (MHC II) on naïve and memory T helper cells in the peripheral blood of asthmatic and non-asthmatic groups.

RESULTS

Atopic asthmatics (acute and stable) had an increased percentage of memory T helper cells expressing IL-2R compared with normal non-atopics (mean SD 16.1 +/- 6%, 12.4 +/- 2% and 7.7 +/- 1.8%, P < 0.05) but not compared with non-asthmatic atopics (10 +/- 3.5%). Naïve T helper cells had low expression of IL-2R and MHC II in all four groups. MHC II antigen expression was increased in memory T helper cells of asthmatics (acute and stable) compared with normal non-atopics (13.9 +/- 7.5, 10.6 +/- 5 and 4.9 +/- 2.5, P < 0.05) but not compared with non-asthmatic atopics (7.92 4). A novel finding was that IL-2R and the MHC II molecules were mainly expressed in non-overlapping populations and coexpression was found predominantly on memory T helper cells. Asthmatics (acute and stable) had higher proportion of double positive memory T helper cells (IL-2R+MHC II+) compared with both non-asthmatic groups (P < 0.05).

CONCLUSIONS

We demonstrate a differential expression of IL-2R+ and MCH II+ on CD45RO+ T helper cells that would suggest that there are three subsets of activated memory T helper cells in asthmatics. Two non-overlapping IL-2R+ or MHC II+ CD45RO+ T helper cells and a third subpopulation of activated cells that coexpress IL-2R and MHC II (double positives). This latter subpopulation is significantly higher in asthmatics (acute or stable) compared with both non-asthmatic groups, suggesting a specific T helper activation phenotype distinct to atopic asthmatics as compared with atopic non-asthmatics.

摘要

背景

T细胞与特应性哮喘的发病机制有关。我们之前已经表明,在支气管过敏原激发后,记忆性辅助性T细胞(CD4+CD45RO+)相对于初始辅助性T细胞(CD4+CD45RA+)优先被激活。然而,在特应性和/或哮喘中被激活的特定辅助性T细胞亚群仍未明确。

目的

确定与急性和稳定期哮喘相关的辅助性T细胞亚群及激活表型,这些表型可能与特应性相同或不同。

方法

分析了两组特应性哮喘患者(10例急性哮喘患者和9例稳定期哮喘患者)以及两组非哮喘患者(14例非哮喘特应性个体和8例正常非特应性对照)。10例急性哮喘患者在急性发作期间于急诊室接受评估(第一秒用力呼气容积[FEV1]为43.6%±18.4)。9例稳定期哮喘患者在无症状期接受评估(FEV1为85%±6)。使用多色流式细胞术分析哮喘组和非哮喘组外周血中初始和记忆性辅助性T细胞上的T细胞亚群以及白细胞介素2受体(IL-2R)和主要组织相容性复合体II类抗原(MHC II)的表达。

结果

与正常非特应性个体相比,特应性哮喘患者(急性和稳定期)表达IL-2R的记忆性辅助性T细胞百分比增加(均值±标准差分别为16.1%±6%、12.4%±2%和7.7%±1.8%,P<0.05),但与非哮喘特应性个体相比无差异(10%±3.5%)。在所有四组中,初始辅助性T细胞的IL-2R和MHC II表达较低。与正常非特应性个体相比,哮喘患者(急性和稳定期)记忆性辅助性T细胞的MHC II抗原表达增加(分别为13.9±7.5、10.6±5和4.9±2.5,P<0.05),但与非哮喘特应性个体相比无差异(7.9±4)。一个新发现是,IL-2R和MHC II分子主要在不重叠的群体中表达,共表达主要见于记忆性辅助性T细胞。与两个非哮喘组相比,哮喘患者(急性和稳定期)双阳性记忆性辅助性T细胞(IL-2R+MHC II+)的比例更高(P<0.05)。

结论

我们证明了CD45RO+辅助性T细胞上IL-2R+和MCH II+的差异表达,这表明哮喘患者中有三个被激活的记忆性辅助性T细胞亚群。两个不重叠的IL-2R+或MHC II+ CD45RO+辅助性T细胞亚群以及第三个共表达IL-2R和MHC II的激活细胞亚群(双阳性)。与两个非哮喘组相比,后一个亚群在哮喘患者(急性或稳定期)中显著更高,这表明与非哮喘特应性个体相比,特应性哮喘患者存在特定的辅助性T细胞激活表型。

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