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免疫疗法对屋尘螨敏感型支气管哮喘患者单核细胞产生嗜酸性粒细胞黏附诱导活性的影响。

Effect of immunotherapy on the production of eosinophil adhesion-inducing activity from mononuclear cells in house-dust-mite-sensitive bronchial asthma.

作者信息

Nagata M, Tabe K, Hong Choo J, Sakamoto Y, Matsuo H

机构信息

Pulmonary Division, Second Department of Internal Medicine, Saitama Medical School, Saitama, Japan.

出版信息

Int Arch Allergy Immunol. 1998 Sep;117 Suppl 1:20-3. doi: 10.1159/000053565.

DOI:10.1159/000053565
PMID:9758891
Abstract

An initial step of eosinophil (EOS) accumulation in the sites of allergic inflammation is the adhesion to endothelial cells. There is increasing evidence that immunotherapy (IT) modulates the production of cytokines from mononuclear cells and hence attenuates allergic inflammation. To examine whether IT modifies the production of factor(s) which induce EOS adhesion, peripheral blood mononuclear cells (PBMC) from house-dust-mite-sensitive asthmatics treated with or without IT were cultured for 96 h in the presence or absence of 1/microg/ml Dermatophagoides farinae antigen. EOS were isolated from the peripheral blood of healthy subjects. EOS adhesion-inducing activity (EAIA) in the PBMC culture supernatants was examined by the ability to modify EOS adhesion to paraformaldehyde-fixed human umbilical vein endothelial cells (HUVEC) which were stimulated with IL-4 plus TNF-alpha. In asthmatics without IT, the addition of D. farinae antigen significantly promoted the production of EAIA from PBMC (EOS adhesion: 22.4+/-13.1% by medium control vs. 30.5+/-18.9% by D. farinae, n=10, p=0.023). This enhancing effect was blocked by an anti-beta2-integrin antibody. In contrast, the addition of D. farinae did not modulate EAIA production from PBMC in asthmatics treated with IT (23.1+/-10.3% vs. 21.5+/-12.3%, n=10, p=NS). These results suggest that IT induces the inhibition of antigen-dependent production of EAIA from PBMC. This may contribute to the inhibitory effect of IT on eosinophil recruitment in allergic inflammation.

摘要

嗜酸性粒细胞(EOS)在过敏性炎症部位积聚的初始步骤是黏附于内皮细胞。越来越多的证据表明,免疫疗法(IT)可调节单核细胞产生细胞因子,从而减轻过敏性炎症。为了研究IT是否改变诱导EOS黏附的因子的产生,将接受或未接受IT治疗的屋尘螨敏感哮喘患者的外周血单核细胞(PBMC)在存在或不存在1/μg/ml粉尘螨抗原的情况下培养96小时。从健康受试者的外周血中分离出EOS。通过检测PBMC培养上清液中改变EOS对用IL-4加TNF-α刺激的多聚甲醛固定的人脐静脉内皮细胞(HUVEC)黏附的能力,来检测PBMC培养上清液中的EOS黏附诱导活性(EAIA)。在未接受IT治疗的哮喘患者中,添加粉尘螨抗原可显著促进PBMC产生EAIA(EOS黏附:培养基对照为22.4±13.1%,粉尘螨为30.5±18.9%,n = 10,p = 0.023)。这种增强作用被抗β2整合素抗体阻断。相反,在接受IT治疗的哮喘患者中,添加粉尘螨并未调节PBMC产生EAIA(23.1±10.3%对21.5±12.3%,n = 10,p =无显著性差异)。这些结果表明,IT可抑制PBMC抗原依赖性产生EAIA。这可能有助于IT对过敏性炎症中嗜酸性粒细胞募集的抑制作用。

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Effect of immunotherapy on the production of eosinophil adhesion-inducing activity from mononuclear cells in house-dust-mite-sensitive bronchial asthma.免疫疗法对屋尘螨敏感型支气管哮喘患者单核细胞产生嗜酸性粒细胞黏附诱导活性的影响。
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Does allergen immunotherapy alter the natural course of allergic disorders?变应原免疫疗法会改变过敏性疾病的自然病程吗?
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