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Aeroallergen-induced eosinophilic inflammation lung damage and airways hyperreactivity in mice can occur independently of IL-4 and allergen-specific immunoglobulins.

机译：空气变应原诱导的嗜酸性粒细胞炎症肺损伤和小鼠气道高反应性可独立于IL-4和变应原特异性免疫球蛋白发生。

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In this investigation we have used a mouse model containing certain phenotypic characteristics consistent with asthma and IL-4- and CD40-deficient mice to establish the role of this cytokine and allergen-specific immunoglobulins in the initiation of airways hyperreactivity and morphological changes to the airways in responses to aeroallergen challenge. Sensitization and aerosol challenge of mice with ovalbumin resulted in a severe airways inflammatory response which directly correlated with the induction of extensive airways damage and airways hyperreactivity to beta-methacholine. Inflammatory infiltrates were primarily characterized by the presence of CD4+ T cells and eosinophils. In IL-4-deficient mice, the recruitment of airways eosinophils was impaired, but not abolished in response to aeroallergen. Moreover, the characteristic airways damage and hyperreactivity normally resulting from allergen inhalation were not attenuated. Induction of these structural and functional changes to the airways occurred in the absence of ovalbumin-specific IgE and IgG1, but IgG2a and IgG3 were detected in the sera of IL-4-deficient mice. CD4+ T cells isolated from both wild-type and IL-4-deficient mice given ovalbumin produced significant levels of IL-5 after in vitro stimulation. Treatment of IL-4-deficient mice with anti-IL-5 mAb before aeroallergen challenge abolished blood and airways eosinophilia, lung damage, and airways hyperreactivity. These results indicate that IL-4 is not essential for the development of IL-5-producing CD4+ T cells or for the induction of eosinophilic inflammation and airways damage and hyperreactivity. In response to sensitization and aerosol challenge, CD40-deficient mice did not produce ovalbumin-specific IgE, IgG isotypes, or IgA, and airways inflammation and hyperreactivity were not attenuated. Our results suggest that allergic airways disease can occur via pathways which operate independently of IL-4 and allergen-specific immunoglobulins. Activation of these pathways is intimately associated with IL-5 and eosinophilic inflammation. Such pathways may play a substantive role in the etiology of asthma.

机译：在这项研究中，我们使用了包含与哮喘以及IL-4-和CD40缺陷型小鼠一致的某些表型特征的小鼠模型，以建立这种细胞因子和过敏原特异性免疫球蛋白在气道高反应性和气道形态改变中的作用。应对空气过敏原的挑战。卵清蛋白对小鼠的致敏作用和气溶胶激发导致严重的气道炎症反应，这与引起广泛的气道损伤和气道对β-蛋氨酸高反应性直接相关。炎性浸润的主要特征是存在CD4 + T细胞和嗜酸性粒细胞。在IL-4缺陷型小鼠中，气道嗜酸性粒细胞的募集受到损害，但对气变应原的反应并未消失。此外，通常不会因吸入过敏原而导致的典型气道损害和反应过度。在不存在卵白蛋白特异性IgE和IgG1的情况下，这些气道的结构和功能发生改变，但是在IL-4缺陷小鼠的血清中检测到了IgG2a和IgG3。从野生型和IL-4缺陷型小鼠接受卵白蛋白分离的CD4 + T细胞在体外刺激后产生显着水平的IL-5。在气敏原刺激前，用抗IL-5 mAb治疗IL-4缺陷小鼠可消除血液和气道嗜酸性粒细胞增多，肺损伤和气道高反应性。这些结果表明，IL-4对于产生IL-5的CD4 + T细胞的发育或对嗜酸性粒细胞的炎症，气道损伤和反应过度的诱导不是必需的。响应敏化和气溶胶攻击，CD40缺陷型小鼠不产生卵清蛋白特异性IgE，IgG同种型或IgA，并且气道炎症和高反应性未减弱。我们的结果表明，过敏性气道疾病可通过独立于IL-4和过敏原特异性免疫球蛋白起作用的途径发生。这些途径的激活与IL-5和嗜酸性粒细胞炎症密切相关。这些途径可能在哮喘的病因中起实质作用。

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期刊名称 The Journal of Clinical Investigation
作者
S P Hogan; A Mould; H Kikutani; A J Ramsay; P S Foster;
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年(卷),期 1997(99),6
年度 1997
页码 1329–1339
总页数 11
原文格式 PDF
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中图分类医学史;
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专利

1. Phenotypic and physiologic characterization of transgenic mice expressing interleukin 4 in the lung: Lymphocytic and eosinophilic inflammation without airway hyperreactivity [J] . John A. Rankin, Dominic E. Picarella, Gregory P. Geba Proceedings of the National Academy of Sciences of the United States of America . 1996,第15期

机译：转基因小鼠在肺中表达白介素4的表型和生理学表征：淋巴细胞和嗜酸性粒细胞炎症，无气道高反应性
2. Interleukin-5-producing CD4+ T Cells Play a Pivotal Role in Aeroallergen-induced Eosinophilia, Bronchial Hyperreactivity, and Lung damage in Mice [J] . Simon P. Hogan, Aulikki Koskinen, Klaus I. Matthaei American journal of respiratory and critical care medicine . 1998,第1期

机译：产生白介素5的CD4 + T细胞在小鼠气变应原诱导的嗜酸性粒细胞增多，支气管高反应性和肺损伤中起关键作用
3. A novel T cell-regulated mechanism modulating allergen-induced airways hyperreactivity in BALB/c mice independently of IL-4 and IL-5. [J] . Hogan SP, Matthaei KI, Young JM, The Journal of Immunology: Official Journal of the American Association of Immunologists . 1998,第3期

机译：独立于IL-4和IL-5调节BALB / c小鼠中变应原诱导的气道高反应性的新型T细胞调节机制。
4. Enhancement of Antigen-Induced Eosinophilic Inflammation in the Airways of Mice by Urban Particles in Beijing [C] . Miao He, Takamichi Ichinose, Seiichi Yoshida, Conference on Environmental Pollution and Public Health . 2012

机译：北京城市颗粒增强抗原诱导的小鼠气道嗜酸性粒细胞炎症
5. Arhgef1 is required by T cells for the development of airway hyperreactivity and inflammation. [D] . Brown, Jeanette P. 2007

机译：T细胞需要Arhgef1来发展气道高反应性和炎症。
6. Phenotypic and physiologic characterization of transgenic mice expressing interleukin 4 in the lung: lymphocytic and eosinophilic inflammation without airway hyperreactivity. [O] . J A Rankin, D E Picarella, G P Geba, 1996

机译：在肺中表达白介素4的转基因小鼠的表型和生理学特征：淋巴细胞和嗜酸性粒细胞炎症无气道高反应性。
7. Aeroallergen-induced eosinophilic inflammation, lung damage, and airways hyperreactivity in mice can occur independently of IL-4 and allergen-specific immunoglobulins. [O] . Hogan, S P, Mould, A, Kikutani, H, 1997

机译：空气变应原诱导的嗜酸性粒细胞炎症，肺损伤和小鼠气道高反应性可独立于IL-4和变应原特异性免疫球蛋白发生。
8. Bronchial Hyperreactivity Protective in Grain Dust Induced Airway Inflammation [R] . Jagielo, P. J., Watt, J. L., Quinn, T. J., 1997

机译：支气管高反应性对谷物尘埃导致气道炎症的保护作用

Aeroallergen-induced eosinophilic inflammation lung damage and airways hyperreactivity in mice can occur independently of IL-4 and allergen-specific immunoglobulins.

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